Pyroglutamic acid: a unique chiral synthon

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Tetrahedron: Asymmetry 20 (2009) 1581–1632

Contents lists available at ScienceDirect

Tetrahedron: Asymmetry journal homepage: www.elsevier.com/locate/tetasy

Tetrahedron: Asymmetry Report Number 116

Pyroglutamic acid: a unique chiral synthon Sharad Kumar Panday a,*, Jagdish Prasad a, Dinesh Kumar Dikshit b a b

Department of Chemistry, Faculty of Engineering and Technology, M. J. P. Rohilkhand University, Bareilly, UP, India Medicinal Chemistry Division, Central Drug Research Institute, Lucknow, UP, India

a r t i c l e

i n f o

Article history: Received 26 March 2009 Accepted 8 June 2009 Available online 18 July 2009

a b s t r a c t jjj Ó 2009 Elsevier Ltd. All rights reserved.

Contents 1. 2.

3.

4.

Introduction . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Asymmetric use of pyroglutamates with prior modifications . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 2.1. Reduction of carboxylic groups . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 2.2. Activation of lactam carbonyl at C-5 by formation of thiolactam, imino, iminium ethers and as lactam acetals. . . . . . . . . . . . . . . . . . . Asymmetric use of pyroglutamates without prior modifications . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.1. Direct chain elongation reactions. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.2. Use of N-derivatized pyroglutamates for asymmetric synthesis . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.2.1. Diels–Alder reactions . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.2.2. Radical cyclization . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.2.3. N-Acylations/alkylations of native pyroglutamates . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.3. Functionalization at C-2, C-3, C-4, of pyroglutamates. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3.4. Conversion of pyroglutamic acid into prolines . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Conclusions. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . Acknowledgements . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . References . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .

1. Introduction Pyroglutamic acid or 5-oxo-proline has emerged as an important starting material for asymmetric synthesis of many natural products. From the ﬁrst reported application of pyroglutamic acid in an asymmetric synthesis of Domoic acid 161a in 1982, the last two decades have witnessed an exponential outgrowth of publications on chemistry and asymmetric/biological uses of pyroglutamic acid.1b Derived from glutamic acid, derivatives of pyroglutamic acids are a cheap source of chirality. The advantage of pyroglutamic acid in asymmetric synthesis lies in a rigid ﬁve-membered skeleton with strong stereo-electronic inﬂuence of two different carbonyl entities in the molecule which can be differentially functionalized. These features of pyroglutamates have been extensively exploited

* Corresponding author. Tel./fax: +91 581 2529138. E-mail address: [email protected] (S.K. Panday). 0957-4166/$ - see front matter Ó 2009 Elsevier Ltd. All rights reserved. doi:10.1016/j.tetasy.2009.06.011

1581 1581 1581 1593 1605 1605 1611 1611 1611 1611 1616 1625 1629 1630 1630

and the present review makes an attempt to list out all the major advances in this area. Pyroglutamic acid has two differentially activated carbonyls. The asymmetric use of pyroglutamic acid has exploited their reactivity differences as such or by accentuating these by further derivatizations. The review is aimed to describe these developments and to explore further possibilities on the uses of pyroglutamic acid as a chiral synthon. In the present communication the major uses of pyroglutamic acid as a chiral synthon have been classiﬁed on the following lines. 2. Asymmetric use of pyroglutamates with prior modiﬁcations 2.1. Reduction of carboxylic groups The ﬁrst use of pyroglutamates as chiral synthon in the synthesis of complex molecule was in the synthesis of ()-Domoic acid by Ofune et al.1a The N-protected pyroglutamic acid was reduced to

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the corresponding alcohol which was protected by TBS. This protected synthon has only one activated carbonyl which was a-alkylated in high enantiomeric excess. The reduction of carbonyl function and its subsequent protection by TBS not only excluded the deprotonation at C-2, that is, loss of chirality, but also inﬂuenced the a-approach of electrophile (Scheme 1). Similar reduction and protection sequence was also used2 in the synthesis of trans-4-cyclohexyl proline 24 (Scheme 2), an intermediate for the synthesis of fosinopril, a potent ACE inhibitor. In this case reaction of pyroglutaminol with benzaldehyde gave a bicyclic

system, where phenyl acquires an equatorial position. Alkylation of the lithio enolate proceeded with high facial selectivity to give 4-aproduct 24. Langlois et al. have carried out asymmetric synthesis of antihypertensive pyrrolidines3 34 by using 2-hydroxymethyl pyroglutamate 25 as a chiral synthon (Scheme 3). The protected 2hydroxymethylpyrrolidine-5-one was reduced to cyclic aminol 27 which was used in C–C-bond forming reaction at C-5. The carbonyl group in 29 was derivatized via thioketalization in the presence of TsOH followed by hydrogenation with Raney Ni to get

Boc

O

O

O 1. ClCO2Et/Et3N/THF, -10oC

N

terbutyldimethylsilyl chloride DMF/ imidazole

N

Boc

2. NaBH4/90%EtOH, -10oC HOOC 1

Boc

N

O

OH

3

2 O 1. LDA/THF/PhSeCl, -78oC to 0oC 2. O3/CH2Cl2, -78ºC, NaOAc, 0ºC

Boc

O OTMS

N

Boc

OTMS O 5

Bu

t

S

Bu

O

H O

N

BH3.DMS

Boc

HO

N

COOCH3 t

O S 6

OH O 7

Bu

S

t

Bu

O MeOH/p-TsOH, rt, 3h

O 1. Pyridinium dichromate, DMF, 40oC, 48h Boc N 2. CH2N2

HO

Boc N

OH

CHO H

Boc N

COOMe

Ph3P(Cl)CH2OCH3 / t-AmONa/ Benzene, rt

SePh CH-CHO H O3/CH2Cl2, -78oC

Boc N

COOMe

CHO 1. NBS/THF, rt 2. NaOAc COOMe

Boc N

12

COOMe MeOOC 12 CHO

Boc N COOMe MeOOC

CH=CHOMe H

Boc N MeOOC 11

MeOOC 10

PhSeCl/THF/Et3N/ H2O, rt

HO COOMe

MeOOC 9

OH 8

60%AcOH, 60oC, 24h

Bu

N

O

O

1. O3/CH2Cl2, -78oC, DMS, rt, 6h 2. CH2N2

t

S

t

H

135oC O 4

3. 2-methyl-2-ethyl-1,3dioxolane/p-TsOH, rt, 3h

Boc

S

Br- H Ph3+P

MeOOC

OH

H

Boc N

KOH

COOMe MeOOC

14

H

15

COOH

HN HOOC

16

COOH (-)-Domoic acid Scheme 1.

13 CH2OH 1. 2.5% KOH, rt 2. CF3COOH

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632 +

+

1. ROH/H O

COOH

N H 17

2. NaBH4

CH2OH

N H 18

O

N O 19

Ph

LAH,THF O

1. LDA 2. Br

PhCHO/H O

O

N O

Ph

Ph 20

CH2OH

N

Z-Cl/K2CO3

H2/Pd-C

CH2OH

N H 22

21

H2O-THF

1. Jones' oxidation 2. H2/Pd-C

CH2OH

N Z

COOH

N H

23

24 Scheme 2.

RO

Methylchloroformate RO DIBAH RO O O N N H COOCH3 R=H R=CH(CH3)OC2H5 R=CH(CH3)OC2H5 26 25 O

OH

N

Sodium enolate of 3',4'-methylenedioxy phenyl methyl ketone

COOCH3 27

O

O HO

RO TsOH

N

R=CH(CH3)OC2H5

N

N

O

COOCH3

O

O

COOCH3

O

O O

O

30

29

O

28 R'

H

R'' HO Reney Ni

HO 1. TsOH 29 2. Thioketalization

N COOCH3

OHC

O

32

Ph R''

1. PhMgBr

N COOCH3

O O

DMSO N COOCH3

O

R'=R''=S(CH2)2S 31

H

R'''

O O

N O

R'

2. KOH-MeOH heat

R'=R''=H R'''=OH R'=R'''=H R''=OH 34

33

SO3-Pyridine complex

O

Scheme 3.

compound 32. The resulting product on oxidation yielded an aldehyde 33 which was converted into the desired antihypertensive agent 34. Similarly the pyroglutamate-derived cyclic protected synthon has been used by Baldwin et al.4 for the generation of a Michael acceptor moiety which was used in one-pot Michael addition– alkylation sequence to yield stereodeﬁned 3,4-disubstituted pyroglutamate derivative 36 (Scheme 4). Investigations reported by Hamada et al. on the asymmetric use of pyroglutamates with prior reduction of carbonyl group describe

the synthesis of the 2,3-dihydroxy-4-dimethylamino-5-methoxypentanoic acid5 46 a fragment of calyculins, starting from (S)-5(hydroxymethyl)-2-pyrrolidinones 18 (Scheme 5). Making use of pyroglutamic acid as a cheap chiral source, Langlois et al. reported the synthesis of enamidoaldehyde 49 as new common synthons for the preparation of analogs of sibiromycin and other antitumour antibiotics6 (Scheme 6). Compound 47 was converted into N-acylated derivative 48, by reaction with NaH and p-nitrobenzoyl chloride. Resultant N-acyl derivative 48 was converted into aldehyde 49 in three steps as shown in Scheme 6.

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O

N

1. LDA 2. PhSeBr 3. O3

H O

H2C O

19

Ph

N

H

PhH2C

COOCH3

COOCH3

Sodium amide/ HMPA Alkylation with O benzyl bromide

O

35

Ph

COOCH3

COOCH3

N Ph

LDA Electrophile

H

O

36

E O

N

H

O

Ph 37 Scheme 4.

HO

MPMCl, NaH O DMSO, rt, 24 h

N H

1. DDQ, CH2Cl2-H2O (19:1), rt, 4 h

O

N

MPMO

2. CH3I, NaH, THF, rt, 1 h

H3CO

MPM 38

18

1. LDA, THF, −78 ºC, 30 min 2. PhSeCl, −78 ºC, 30 min 3. aq. H2O2, EtOAc, rt H3 CO

O

39

O

N

N MPM

1. OsO4, N-methylmorpholine N-oxide toluene-acetone-water, rt 2. 2,2-dimethoxypropane, p-TsOH, H2O, rt

MPM 40

O

O

O

O

O 20 min then rt

N

H3CO

N H

H3CO

MPM

O H3CO

42

41 O 1. LiOH, THF, H2O, 0 ºC, 30 min 2. PhCH2NH2, DPPA, Et3N DMF, 0 ºC, 1 h, rt

O H3CO N 45

O

O N Boc

O H N

H3CO BocHN

O

Ph

1. TMSOTf, CH2Cl2, 0 ºC, 1 h 2. aq. HCHO, AcOH, 5%Pd/C H2, MeOH, rt, 60 h 3. 2,2-dimethoxypropane, p-TsOH-H2O, rt

O

HO H N

O

43

44

H3C

O

(Boc)2O, DMAP Et3N, rt

CAN, CH3N-H2O, 0 ºC

Ph 6M aq HCl, MeOH 130 ºC, 1.5 h

COOH OH

H3CO H3C

CH3

N

CH3

46 Scheme 5.

A publication by Woo et al. has described the asymmetric synthesis of a-amino acids by reaction at C-3, C-4 and C-5, of pyroglutamate derivatives starting from (S)-pyroglutamic acid derivative 50.7 They also reported ring opening through 2-lithio-1,3-dithiane at low temperature furnishing compound 52, whereas reaction of 50 with vinyl magnesium bromide followed by reduction afforded compound 51 (Scheme 7). Total synthesis of (+)-monomorine 67, a natural attractant for Pharaoh ant workers was carried out from chiral cyclic b-enaminoester derived from (S) pyroglutamic acid in seven steps by Saliou et al.8 (Scheme 8). Pyroglutaminol 18 after tosylation was converted to o-tosyl derivative 62. Compound 62 on reaction with di-n-propyl lithium cuprate was converted to compound 63 having

n-Bu group at position 5. Compound 63 on reaction with dimethylsulfate followed by treatment with Meldrum’s acid and on subsequent reaction with sodium methoxide furnished b-enaminoester 64 which on hydrogenation in the presence of H2/Raney Ni afforded 65 with the desired stereochemistry. Compound 65 after the protection of NH with benzyloxy carbonyl chloride followed by reduction of alcohol group to aldehyde, was subjected to Witting reaction with CH3COCH@PPh3 ylid. The resultant compound on hydrogenation had undergone deprotection, reduction and cyclization to give (+)-monomorine 67. Stereoselective methylation of bicyclic lactams derived from Dpyroglutamic acid 68 has been reported by Armstrong et al.9 The bicyclic compound 70 was converted to 4-methyl pyroglutaminol,

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O

N H

HO

TBDMSO

NaH, KI

O

N H

O

N

TBDMSO

NO2C6H4COCl

O O2N

47

18

48 CHO

1. DIBAL-H 2. QCS 3. DMF-POCl3

N

R O

O2N 49 Scheme 6.

S 2-lithio-1,3-dithiane

1. Vinyl MgBr, THF

HO

LDA, THF, −78 ºC O to 44 ºC, MoOPh

O

N

OSiBu Ph2

Boc 53 HO

PhSe

OH

O

O

N Boc

OSiBut Ph2

57

N

N Boc

OSiBut Ph2

OSiBut Ph2

N Boc

55

OSiBut Ph2

OSiBut Ph2

59

N Boc

1. THF/CH2Cl2 2. BH3DMS. THF

H3C

N

OSiBut Ph2

Boc

56

58

H 54

H3C

CH3 Me2CuLi, Ether O −78 ºC

N

LDA, THF, −78 ºC then MeI

H2O2, Pyridine CH2Cl2, −78 ºC

O

H3 C

O

N

OSiBut Ph2

Boc 52

OSiBut Ph2

LDA, PhSeCl THF, −78 ºC

Boc OsO4.NMO

HN O

1. MeMgBr, ether 2. (i) TFA (ii) NaOH(2M) (iii) NaCNBH3

Boc 50

t

S

THF, −78 ºC

2. NaBH4, CeCl3, MeOH, 0 ºC OSiBut Ph2

HO HN Boc 51

OSiBut Ph2

60

Scheme 7.

HO

N H

tosylate O TsO

H nBu

63

HCl, MeOH, LAH, ether

nBu

N H

COOCH3

R

65 H2, Pd-C, 10%, atm N Cbz

1. MeSO4 O 2. Meldrum's acid Ni(acac)2, CHCl3 3. MeONa, MeOH 1. ClCOOCH2Ph 2. PCC, CH2Cl2

H

H2, RaneyNi, 100bar

H N H 64

N H

N H

62

18 H nBu

nPr2CuLi O Ether-CH2Cl2nBu −30 ºC

H

3. CH3=CO-CH=PPh3, THF 4. H2, PtO2, atm

H

nBu

N H

R

H3C

66

67 Scheme 8.

(+)-monomorine

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deprotection of hydroxyl groups with triﬂuoroacetic acid afforded (+)-hyacinthacine B1 80. Moeller et al. have modiﬁed carboxylic functional group of pyroglutamates with an objective to synthesize spirocyclic Lpyroglutamide building blocks12 86 (Scheme 12). Pyroglutamic acid was converted to its menthyl ester followed by deprotection at C-2 using Pt wire, n-Bu4PF6 and methanol as a solvent to afford C-2 methoxylated menthyl ester 82 which on reaction with allyltrimethylsilane and TiCl4 was converted to C-2 alkylated product 83. Compound 83 on reaction with methanolic ammonia and NaCN was converted to primary amide 84. Compound 84 on oxidation with aqueous OsO4/NaIO4 followed by reaction with triethylsilane and TFA using nitro methane as a solvent underwent hydrodehydroxylation to give 86 as building block. Magni et al. carried out the synthesis of (R)-3-[(S)-(5-oxo-2pyrrolidinyl)carbonyl]-thiazolidine-4-carboxylic acid (Pidotimod) 90 as an immunostimulating agent13a,b from pyroglutamic acid (Scheme 13). Here pyroglutamic acid was treated with ethyl L-thiaazolidine 4-carboxylate in the presence of DCC and CH2Cl2 to afford compound 88, which upon alkaline hydrolysis gave carboxylic acid

which on reduction afforded 2,4-dimethyl pyrrolidone 72 the chiral antipode, which was converted to N-protected cis-2,4-dimethylglutamide 73 in three steps (Scheme 9). Kohn et al.10 carried out the synthesis and characterization of chiral 1,2-diamines from pyroglutamic acid where pyroglutamic acid 17 on reaction with anhydrous chloral in the presence of toluene afforded bicyclic derivative 74 which on reaction with primary amine in toluene underwent ring opening of the oxazolidinone ring of bicyclic aminal 74 to furnish pyroglutamoyl amide derivative 75. Compound 75 on reduction of lactam carbonyl as well as amidic carbonyl group with lithium aluminium hydride furnished the desired 1,2-diamines 76 (Scheme 10). Sengoku et al.11 carried out asymmetric synthesis of pyrrolizidine alkaloids (+)-hyacinthacine B1 and (+)-B2. The representative synthesis of (+)-hyacinthacine B1 is described here (Scheme 11). Pyroglutamic acid derivative 77 on catalytic sharpless asymmetric dihydroxylation(AD) with AD-mix-a [(DHQ)2 PHAL ligand] afforded compound 78, which after protection, deprotection coupled with cyclization afforded compound 79. Deprotection of compound 79 with tetrabutyl ammonium ﬂuoride in THF followed by

O

ROH/H

O

COOH

N H 68

1. NaBH4 COOR 2. PhCHO/H+ O

N H

Ph 70

OH

N H

t

1. CBr4/PPh3, pyridine

H

2. Bu3SnH, AIBN reflux toluene

H O

71

3. pTSA, H2O/MeOH

O

H3 C

O

N

69

H3C

1. LDA, THF, −78 ºC 2. MeI

H

H

+

H

CH3

N H

1. Boc anhydride H3C Et3N Boc N 2. AlMe3/NH3 H CH2Cl2

CH3 NH2 O 73

72 Scheme 9.

O

anhydrous chloral O toluene, 40 h

COOH

N H

RNH2, toluene reflux, 2 h

O

N

O

O

17

Cl3C

O

N H RHN 75

74

LiAlH4 reflux, 2 h

N H 76 RHN

Scheme 10.

O

O

O

O AD-mix-alpha[(DHQ)2PHAL ligand] HO OTBS t-BuOH/ H O

N

N

2

OH

Cbz

Cbz 78

77 H

O

H O

N TBSO

OH OH

i. Bu4NF, HF OTBS ii. TFA, H2O

N

OH

HO hyacinthacine B1 80

79 Scheme 11.

i. TBSCl, Et3N ii. MsCl, Et3N OTBS

iii. H2, Pd/C, EtOH

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

[O] Pt wire

Menthol, DCC/DMAP O

CH2Cl2

COOH

N H

O

COOR n-Bu4PF6/MeOH

N H

17

COOR O

82

81 SiMe3

COOR O

TiCl4, CH2Cl2

O

NaCN

H2O

N H

83

84

O

O Et3SiH/TFA

NH

O

OsO4/NaIO4

CONH2

NH3/MeOH

N H

OMe

N H

NH O

MeNO2

N H

N H

OH

86

85 Scheme 12.

S O

COOH

N H

+

HN

S DCC CH2Cl2 O

N H

COOEt 87

17

S

−

OH N

O

O

N

N H

COOEt

O

COOH

89

88 S ImzCO HX

O

N

N H

COX

O

X= -OC2H5, -NH2, -NHC2H5

89

Scheme 13.

89. The carboxylic acid was converted to its derivatives 90 by reaction with various nucleophiles. Lin et al. synthesized14 (S)-3-methyl-5-(1-methyl-2-pyrrolidinyl)isoxasole 96 as a cholinergic channel activator with potent cognitive and anxiolytic activities from pyroglutamic acid 17 (Scheme 14). Pyroglutamic acid was converted to its methyl ester in situ and was subjected to Claisen condensation with acetone oxime dianion, thereby affording compound 93. The acetone oxime component in compound 93 in the presence of H2SO4 as a catalyst underwent cyclization to afford 94, which on reduction of lactam amide with borane, followed by N-methylation gave the desired ABT-418 derivative 96. Benoit Rigo et al. investigated15 various N- and C-protection and deprotection sequences in native pyroglutamate with an aim to develop different reaction methodologies for the synthesis of bioactive molecules (Scheme 15).

O

N H 17

COOH

Reaction of pyroglutamic acid chloride with isopropylidine malonate (Meldrum’s acid) is reported to give C-acylated Meldrum’s derivative whose methanolysis gave b-keto ester 103 (Scheme 16), however the reaction of acyl chloride with sodium salt of Meldrum’s acid (isopropylidene malonate) in pyridine could not be repeated by Rigo et al.15,16 Nagasaka et al.17 established a new approach to get two enantiomers of 5,5-disubstituted 2-pyrrolidinones 108 with speciﬁed conﬁguration starting from pyroglutamic acid through its bicyclic lactam (2R,5S)-2-aryl-1-aza 3-oxabicyclo[3.3.0]oct-5-en-7-one 105 (Scheme 17). Bicyclic lactam 105 was deprotonated at C-5 by NaH and the resultant anion on Michael addition with methyl acrylate gave two diastereomeric Michael adducts 106 and 107, which were separated and pure compound 107 on acidic hydrolysis afforded the desired 5,5-disubstituted 2-pyrrolidinone 108.

1. MeOH, SOCl2 2. LiCH2CNOLi(Me)

O

Me N H 93

O

NOH

H2SO

O

Me N H 94

O

N

1. BH3, THF 2. (i) HCHO (ii) HCOOH

1. MeOH, SOCl2 2. NaH, MeI 3. LiCH2CNOLi(Me) 1. H2SO4 O

Me N Me 95

O

2. (i) BH3, THF (ii) CsF

NOH

Me N Me (ABT-418) 96

Scheme 14.

O

N

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

Pyroglutamic Acid HMDS

N

O

1. (CF3CO)2O

1. MeOCOCl 2. (COCl)2 O

COCl

COOMe 98

N 97

COOSiMe3

2. SOCl2

N

O

COCl

COCF3 99

SiMe3 (CF3CO)2O

COOSiMe3

N

O

(CF3CO)2O O CF3

COCF3 100

CF3

O

N

O

O

O 101

Scheme 15.

pyroglutamate derivative 110 through self-reproduction of chirality (Scheme 18). Ostendorf et al.19 established the synthesis of enantiopure hydroxyamidines 116, utilizing base-catalyzed enantioselective reactions such as Michael reaction (Scheme 19). Methyl pyroglutamate 111 was treated with PhMgBr at low temperature to afford tertiary alcohol, which was converted to silyl ether 112 with TBDMSOTf. Compound 112 on N-derivatization with acrylonitrile afforded compound 113 which on reductive amination of cyano group followed by N-Boc protection afforded compound 114. Compound 114 after a sequence of reactions furnished the desired bicyclic amidine 116. Acevedo et al.20 synthesized sterically constrained L-glutamine analogues (3S,4R)-3,4-dimethyl-L-glutamine 123 and (3S,4R)-3,4dimethyl-L-pyroglutamic acid from pyroglutamic acid (Scheme 20). Compound 117 already discussed1a on methylation with dimethyl lithium cuprate followed by reaction with MeI/Et2O afforded 118 which after a sequence of reactions was converted to the desired glutamine analogue 123. Marchalin et al. developed new methodology for the synthesis of (S)-thieno[f]indolizinedione 125 from N-alkylated (S)-pyroglutamic acid21 124 (Scheme 21). Olson et al.22a,b carried out reduction–iodination of methyl Nbenzyl pyroglutamate 126 to get iodide 127, which on reaction

O O OMe O

O

O

N

N H

HO O O

F3C 102

O

O

103 -

O O + DMF

O

O

Cl N O O

F3C

+

O

No reaction

O O

104

+ PY

O O Scheme 16.

In our studies on the asymmetric use of pyroglutamic acid we synthesized18 a-benzyl derivative through condensation of pyroglutamic acid with trimethylacetaldehyde to get a bicyclic derivative 109 as a chiral auxiliary which on deprotonation with LiHMDS followed by reaction with electrophiles gave chiral a-substituted

H O

O

N O Ar

COOMe

1. CH2=CHCOOMe N

2. NaH 3. DMSO.THF

+

COOMe O

N

O

O

Ar 105

Ar 107

106

107

AcOH.THF-H2O rt

COOMe O

N H

HO

108 Scheme 17.

H THF/Dioxane, TFA O

N H 17

COOH

trimethylacetaldehyde

O

N H O

109 Scheme 18.

O

1. LiHMDS, THF −78 ºC 2. Electrophile

R O

N

O H O R= -CH2Ph 110

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O

PhMgBr O COOMe TBDMSOTf

N H

CN

Ph Ph OR

N H

O

1. Lawesson's reagent Ph S Ph 2. TBAF

N

114

BocHN

OTBDMS

113

Ph 1. MeI Ph 2. TFA OH 3. NaOH

N

OTBDMS

BocHN

, CoCl2 Ph 1. NaBH4 2. (Boc)2O Ph

N

NC

112a, R=H 112b, R=TBDMS

111

O

N

Ph Ph

N

OH 116

115

Scheme 19.

O

1. (CH3)2CuLi, Et2O, −78 ºC

OTBS

N

O

2. CH3I, Et2O, −78 ºC

2. HOAc, −78 ºC

Boc

Boc

4

118

+ O

OTBS

N

O

OTBS

N

119

1. LiHMDS, THF, −78 ºC

OTBS

N

1. CrO3, H2SO4 O

acetone, 0 ºC

N

COOH

Boc

Boc

Boc

118

119

120

Ni-Pr a. i-PrHN

OtBu 121

O

NH3, KCN O

b. BF3.OEt2 c. C6H12, CH2Cl2

COOtBu

N

NHBoc

H2N

THF

COOtBu

Boc 122

123 Scheme 20.

HOOC

N

O

1. SOCl2

O

Altman et al. carried out the synthesis of (S)-5-(aminoxymethyl)pyrrolidone 130 from (S)-5-(hydroxymethyl)pyrrolidone 18 through Mitsunobu reaction with hydrazoic acid followed by the hydrogenation of the resulting azide23 (Scheme 23). Wei et al.24 synthesized (S)-5-alkenyl-2-pyrrolinones 132 from N-Boc protected methylpyroglutamate 131. Ester group of compound 131 was reduced to the corresponding aldehyde with diisobutylaluminium hydride at 78 °C. Witting reaction followed by oxidation with pyridinium chlorochromate (PCC) afforded (S)-5alkenyl-2-pyrrolidinones (Scheme 24). Langlois25 et al. carried out stereoselective synthesis of (2S)-2hydroxymethylglutamic acid 136 starting from (S)-pyroglutaminol

H N

2. AlCl3

O

S

S 124

125 Scheme 21.

with vinyl magnesium bromide and dilithium tetrachloro cuprate gave 128, a precursor for peptide mimetic of the thyrotropinreleasing hormone (Scheme 22).

O

N

COOMe

1. NaBH4 2. TsCl, DMAP

I O

3. NaI, Me2CO

Bn 126

MgBr

N

Li2CuCl4

Bn 127

N Bn 129 Scheme 22.

N Bn 128

O

O

O

O

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

OH O

N H 18

1. HN3, DEAD, Ph3P

salt to afford 141 which on treatment with CH3I was converted to quaternary ammonium salt 142. Compound 142 on passing through alkaline Dowex-550A afforded (±)-deoxydysibetaine (Scheme 27). Villeneuve et al.28 carried out the synthesis of pyroglutamic acid fatty esters 145 through lipase-catalyzed esteriﬁcation with medium chain alcohols (Scheme 28). Langlois et al.29 carried out diastereoselective synthesis of (±)deoxydysibetaine 152 which was prepared from methyl pyroglutamate through a regioselective Mannich reaction at C-2 (Scheme 29). Compound 146 on reaction with MsCl in pyridine followed by the introduction of azide group at position 2 using NaN3 was converted to 148, which on hydrogenation in the presence of H2/ Pd–C afforded 149. The resultant amine 149 on reaction with CH3I–iPr2NEt was converted to 151 and the desired product (±)deoxydysibetaine 152 was obtained from 151 according to the procedure already described in Scheme 27. Itoh et al.30 carried out asymmetric synthesis of 1-substituted 1,2,3,4-tetrahydro-b-carbolines employing pyroglutamic acid derivative as a chiral auxiliary (Scheme 30). Puschel et al. described the synthesis of pyrrolidinone PNA; novel conformationally restricted PNA analogues, for example, (3R,5R)(3S,5S)pyroglutamate-PNA monomers31 (Scheme 31). Compound 156, derived from pyroglutamic acid on reaction with MoOPh in the presence of LiHMDS and BuLi followed by the protection of OH group and deprotection of Boc group using Bomchloride and TFA was converted to 3-substituted product 158, which on reaction with NaH and BrCH2COOMe afforded N-acylated product 159. Compound 159 after deprotection gave an alcohol 160 which was converted to 162 by similar steps as described in Scheme 29. Compound 162 on hydrogenation with H2/Pd–C, followed by protection of amino group using Boc and subsequent reaction with H2 and Pd(OH)2 afforded 163 with deprotection of Bom. Further

NH2

O

N H 130

2. H2, Pd/C, EtOH Scheme 23.

O

N Boc 131

COOMe

1. DIBALH, PhMe

R

O

N

2. Ph3P=CHR 3. PCC

Boc 132

Scheme 24.

18 through a bicyclic silyloxypyrrole derived from versatile unsaturated lactam (Scheme 25). Compound 133 on reaction with SnCl4 and NaHCO3 was converted to 134 having hydroxyl group at position 5, which on reaction with Me3SiCN, SnCl4 followed by acidic hydrolysis afforded 136. Davies et al. achieved the synthesis and explored the utility of the 3,3-dimethyl-5-substituted-2-pyrrolidinone 140 using pyroglutamic acid as a chiral auxiliary26 (Scheme 26). Compound 18 on reaction with 2,2,dimethoxypropane in the presence of pTSA, followed by double alkylation at position 7 using LDA and MeI was converted to 138 which on acidic hydrolysis was changed to 4-substituted pyroglutaminol 139. Treatment of 139 with TBDMSCl in DMF afforded the desired product 140. Langlois et al. synthesized racemic and enantiopure (±)-deoxydysibetaine 143 from methyl pyroglutamate27 111. Compound 111 was deprotonated with LiHMDS and alkylated with Eschenmoser’s

Et3N/TBSOTf

OH O

O

N H 18

N

Bu

SnCl4

SiO

N

O Ph

35

Ph

OH O

t

CH2Cl2

NaHCO3 O 133 COOH

CN Me3SiCN

N

O

6M HCl

N

SnCl4

O

O

Ph

H3N Cl -

Ph 135

134

COOH OH

+

1. HCl 136

Scheme 25.

O OH O

N H

N

toluene, pTSA, heat

O

18

3. LDA, −78 ºC 4. MeI, −78 ºC

137

O

O MeOH

N

pTSA, heat O

138

1. LDA, −78 ºC 2. MeI, −78 ºC

2,2-dimethoxy propane

1. TBDMSCl, DMF.Im NH or Ph3CCl, DMAP OH NEt3, CH2Cl2 139

Scheme 26.

O NH R R= CH2OTBS R= CH2OCPh3 140

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O O

LiHMDS, THF Eschenmoser salt

COOMe

N H

O

CH3I

N

N H

111

O

OMe

THF

O

141

Dowex, 550A O

-

N+

N H

I-

142 O

OH

OMe

ON+

N H (±) 143

Scheme 27.

O

H2SO4 + C H OH 2 5 reflux, 24 h COOH

N H 17

Candida antarctica lipase

O

COOC2H5

N H 144

O

R=2-methyl-2-butanol

N H 145

COOR

Scheme 28.

R

R COOCH3 OH

O

R

MsCl-Py

COOCH3 OMs

O

N H 146

NaN3 DMF

N H 147

O

N H 148

COOCH3 H2-Pd/C N3

R

O

N H 149

MeI-iPr2NEt

HCHO H2, Pd/C

R

O

COOMe NH2

O

MeI

N H 150

R

R COOMe N+

N H 151

COOMe NMe2

Dowex, 550A OH-

I-

O

COOMe N+

N H R= H R= OH 152

Scheme 29.

N O

N

ClCOOCH2CCl3 N R

153

N

O

O

N

COOCH2CCl3

H

N H 155

Bu3Sn CH2Cl2, −40 ºC

N

NaOH, THF, -H2O

COOCH2CCl3

H

N R O 154 Scheme 30.

reaction of 163 under Mitsunobu conditions, followed by alkaline hydrolysis afforded 165. Oba et al.32 established novel stereocontrolled approach to conformationally constrained analogues of L-glutamic acid and L-proline via stereoselective cyclopropanation of 3,4-didehydro-Lpyroglutamic ABO ester. Compound 166 was subjected to 1,3-dipolar cycloaddition with CH2N2, followed by photolysis with benzophenone using Hg lamp and compound 168 thus obtained on hydrolysis with MeOH–HCl was converted to methyl ester 169 with deprotection of Boc group. N-Protected compound 170

on reduction with BH3–THF followed by acidic hydrolysis on Dowex 50-X8 afforded 172 (Scheme 32). Herdeis et al.33 carried out the synthesis of unsaturated orthopyroglutamic ABO ester 166 from pyroglutamic acid (Scheme 33). Pyroglutamic acid was converted to its alkenyl ester, which on reaction with mCPBA, followed by reaction with zirconocene catalyst and silver perchlorate afforded ABO ester 174, which was converted to N-protected compound 175. Compound 175 upon oxidation under usual conditions, followed by oxidative deselenenylation using H2O2 afforded 166.

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

OH TBDPSO

a. LiHMDS, BuLi, THF N

O

Bom-chloride, DIEA CH2Cl2

TBDPSO

Boc

156

O TFA: CH Cl , 0 ºC 2 2

N

b. MoOPh

Boc 157 OBom

OBom NaH, BrCH2COOMe

TBDPSO N H

O

Et3N.3HF

TBDPSO

THF

158 OBom

N

OBom

NaN3, DMF

MsCl MsO O Pyridine

HO

O

N

160

O

N

COOMe 162

161 AZ

OH

163

1. H2, Pd/C, (Boc)2O, AcOEt 2. H2, Pd(OH)2/C MeOH

N3

80 ºC

COOMe

COOMe

THF

COOMe

159 OBom

BocHN

O

N

1. adenine, PPh3 DEAD, dioxane BocHN O 2. N-benzyloxycarbonyl N -N'-methylimidazolium triflate CH2Cl2 COOMe

AZ LBiOH, THF BocHN

O then HCl

N 164

O

N

COOMe

165

COOH

Scheme 31.

N N CH2N2 O

ABO

N

ether

O

Boc 166 H O

N

H

H (Boc)2O, DMAP MeCN O COOMe

Boc 168 H

N

HCl-MeOH ABO 0 ºC

N

Boc 167 H

N H 169

H Hg-lamp(400W) ABO Benzophenone O MeCN, 0 ºC

H BH3-THF

COOMe

H

(*)

1M HCl H

H

Dowex 50-X8 COOMe

N

N H 172

Boc 171

Boc 170

*= ABO=5-methyl-2,7,8-trioxabicyclo[3,2,1]oct-lyl Scheme 32.

1. CH2=C(Me)CH2CH2OH O

N H

COOH

DCC, DMAP 2. mCPBA, CH2Cl2

N H 173

17 (Boc)2O, DMAP

CP2ZrCl2 AgClO4, CH2Cl2

O

O

O

N H

ABO

O

MeCN

N Boc 175

174

O NaN(SiMe3)2 ABO PhSeCl, DMPU THF, −78 ºC

PhSe 30% H2O2, THF O

N

O

ABO

Boc

N Boc 166

176 Scheme 33.

O

ABO

COOH

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

Stevens et al. reported a short and elegant synthetic pathway for the synthesis of 1,3-dioxo-hexahydropyrido[1,2-c][1,3]diazepine carboxylates, a new 1,3-diazepan-2,4-dione 181 containing bicyclic moiety, starting from pyroglutamate34 (Scheme 34). Compound 177 on reaction with LiHMDS was deprotected at C-2, resultant anion on reaction with electrophile afforded 178, where lactam carbonyl C–N bond was cleaved using NaH, RNCO to expend the ring and resulting product on reaction with electrophile in the presence of K2CO3 yielded 180. Compound 180 was subjected to cyclization with Grubb’s II generation catalyst thereby affording compound 181. Bourry et al. reported their studies on pyrrolidinones through reaction of methylene dichloride under Friedal–Crafts conditions, with an objective to synthesize a-hydroxymethyl ketone in the hexahydrobenzo[f]indolizine series35 (Scheme 35) using pyroglutamic acid as a chiral precursor. Mavromoustakos et al.36a,b reported the synthesis, binding studies and in vivo biological evaluation of antihypertensive analogues 188 using pyroglutamic acid as starting material (Scheme 36). Compound 111 on reaction with NaH, PhCH2Br, followed by reduction using LiBH4 was converted to N-benzyl methyl pyroglutaminol

186, which was converted to its o-tosyl derivative 187. Treatment of 187 with lithium imidazole afforded antihypertensive agent 188. Beal et al. described anodic oxidation/oleﬁn metathesis strategy thereby developing a uniﬁed approach to the synthesis of bicyclic lactam peptidomimetics using pyroglutamic acid37 (Scheme 37). Pyroglutamic acid derivative 189 on acidic hydrolysis was converted to intermediate product and subsequent reaction with pyroglutamic acid, followed by amination using NH3 and MeOH afforded 190. Langlois et al. reported the tandem electrophilic and nucleophilic addition to bicyclic tert-butyl-dimethylsilyloxypyrrole derived from (S) pyroglutaminol38 (Scheme 38). 2.2. Activation of lactam carbonyl at C-5 by formation of thiolactam, imino, iminium ethers and as lactam acetals Suitably activated lactams and amides possess great synthetic utility for the construction of many of the nitrogen-containing heterocycles. Activation of the lactam is generally being carried out by conversion to thiolactam, imino, iminium ethers or as lactam ace-

R'

O

N H 177

LiHMDS, THF, −40 ºC O COOEt Electrophile R'=H, CH2Cl

Electrophile, K2CO3 acetone, reflux

N H 178

Grubb's 2nd generation catalyst, CH2Cl2, reflux R''' R'=H, H R''=Pr, Ph R'''=H, H

N

N

R'= H, H R''= Pr, Ph R'''= H, H

R''

O 180

N

NH

R'' O 179 COOEt

COOEt R' O

COOEt R'

O

R''NCO, NaH COOEt THF R'=H, H R'=Pr, ' Ph

R'

O N

N R''

R''' O 181

Scheme 34.

O

1. (CF3CO)2O 2. BF3.Et2O, CH2Cl2

COOH

N

CH2OH O

O O

+

N

1. (CF3CO)2O 2. BF3.Et2O

O

N

ClCH2CH2Cl O

O

O

O

O

O

182

184

183 Scheme 35.

1. SOCl2 O

COOH

N H

2. MeOH

NaH, THF O

COOMe PhCH2Br

N H

17

LiBH4, THF O

N 185

111

COOMe

25 ºC

Ph

+

OH O

N 186

DMAP or Et3N CH2Cl2 Ph

Li-N

TsCl

OTs O

N 187

N DMSO

Ph Scheme 36.

N O

N 188 Ph

N

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

H O

Boc N

O

COOMe 1. 3M HCl/EtOAc

N

Ph

NH

N H

O

O Ph

2. 17, EDCl, HOBt, CH2Cl2 3. NH3, MeOH

CONH2 N

190

189 Scheme 37.

t Bu

OH

1. SnCl4 SiO

O

N

N

2. NaHCO3 O 133

Ph

N O Ph

191

SnCl4

SnCl4 MeOH

SnCl4

Me3SiCN

MeOH

OMe O

O

Me3SiCH2CH=CH2

O 134

Ph

SnCl4

CN O

N

N

O

O

Ph

Ph 135

192

Scheme 38.

Fang et al. have carried out41 the annulation of diazomethylvinyl ketone with a variety of thiolactams prepared from (S)-pyroglutamic acid. Thiolactam derivative of pyroglutamic acid 209 was converted to 210 by Michael addition which was cyclized to get 211 in the presence of [Rh(OAc)2]2, W-2 and Ra-Ni. Resultant material on oxidation with OsO4 and H2S in methanol, followed by protection of OH group with TBSCl was converted to 212. Lithium enolate-derived reaction of 212 with t-butyl propionate afforded 213 which upon selective reduction of the double bond of side chain followed by deprotection afforded 214. Thus this synthetic strategy provided a novel route for dihydropyridones like ISO A58365A 214, the c-pyridone analog of the potent ACE inhibitor A58365A (Scheme 41). Rosset et al. have described42 the enantioselective synthesis of (5R)-2-(5-hexenyl)-5-nonyl-3,4-dihydro-2H-pyrrole and (2R,5R), 2-(5-hexenyl)-5-nonyl pyrrolidine, Monomorium minutum ant venum alkaloids, from (S)-pyroglutamic acid through lactam ether (Scheme 42). Both D- and L-pyroglutamic acids have been used43a,b with prior activation at C-5 for the synthesis of semicorrin metal complexes as enantioselective catalysts (Scheme 43). These semicorrins43b

tals. Among the activated lactams, lactam acetals are particularly useful as these react with both nucleophiles and electrophiles at C1 and C2, respectively, and with bifunctional reagents to form annulated products. Because of these reasons many workers have made use of pyroglutamates via the activation of the lactam carbonyl at C-5 of pyroglutamate. L-Pyroglutamic acid has been used as chiral starting material for the synthesis of anatoxin-a, a potent nerve depolarizing agent, via intermediacy of thiolactam.12 C–C bond formation at C-5 was effected by a sulﬁde contraction reaction39 (Scheme 39). Bachi et al. have described40 the synthesis of carbapenam-3carboxylates 207(a) and 207(b) starting from ethyl (S)-pyroglutamate which was converted to the corresponding 5-thioxo derivative for C–C bond formation at C-5 (Scheme 40). Compound 200 on reaction with ethyl-2-bromo-3-oxobutyrate, followed by hydrogenolysis with CH3COOH and TFA (20%) was converted to diastereomeric compounds 202, 203a and 203b, in which 203a on reaction with KOH and (Boc)2O afforded N-protected acid 204. Compound 204 was converted to its PNB ester 205 which after N-Boc deprotection followed by cyclization was converted to 207a and 207b using substituted carbodiimide.

Methyl bromo acetate in CH3CN tBuOOC

S

N

t BuOOC

CH2Cl2, PPh3, Et3N

COOCH3

2. LiBH4 in Et2O

N

Bu

Bu

193

194

O Ph3P+

1. Me2SO, CH2Cl2 OH

t

BuOOC

N

Oxalyl Chloride

CHO

t

BuOOC

Bu 195

N Bu 196

O t BuOOC

N

1. degassed N2, Pt/C, H2

Anatoxin A O

199

Bu 198 Scheme 39.

197

O

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

ethyl-2-bromo3-oxobutyrate O

COOH

N H 17

S

Et COOEt +

N H

N H

EtOOC

OH 202

203a

H 1M HCl Et in EtOAc HOOC

O

H Et COOEt + EtOOC

Et COOH

N

HOOC

Boc 204

201

COOEt

N H 203b

203a

H 1. KOH 2. DMAP, (Boc)2O, Et3N

COOEt

N H H3C

H

hydrogenation EtOOC Pt/C in H3C CH3COOH

EtOOC

COOEt NaHCO , CH Cl 3 2 2

N H 200

H dicyclohexylamine Et p-nitrobenzeldehyde KI, DMF HOOC

COOPNB

N Boc 205

H

H

CH2Cl2, Pyridine N H 206

COOPNB 1-(3'-dimethylaminopropyl)-3-ethylcarbodiimide hydrochloride

+

N

N

O

O COOPNB

COOPNB 207b

207a Scheme 40.

N2

S O

O

X +

CH2 X=CHN2 X=OCH3 208

S

NaOH, THF

HN

1. [Rh(OAc)2]2 Benzene, reflux

N

O N

2. W-2, Ra-Ni, acetone

t

t BuOOC

COO Bu tBuOOC

211

210

209 OR

1. OsO4, Pyridine

OTBS

O

2. H2S, MeOH

N COOt Bu

R= H R= TBS 212

O

1. LiCA, THF, −78 ºC 2. t-Butylpropiolate, −78 ºC 3. AcOH, −78 ºC

t

BuOOC

N 213

COOtBu

TBSCl, NEt3, CH2Cl2

OH 1. W-2, Ra-Ni, acetone

O

2. HCOOH

N

HOOC

COOH ISO A 58365 A 214 Scheme 41.

225–228 possess several features that make them attractive ligands for enantioselective control of metal-catalyzed reactions. Singh et al. described44 a simple and efﬁcient synthesis of 8methyl-3,8-diazabicyclo[3.2.1]octane (azatropane) and 3-substituted azatropanes using pyroglutamic acid as starting material and exploiting amide activation methodology (Scheme 44). Pyroglutamic acid was converted to N-methyl pyroglutamate which on reaction with Lawesson’s reagent was converted to the corresponding thio lactam. Treatment of thio lactam with methyl iodide in benzene, followed by reaction with nitro methane in the presence of triethylamine yielded nitroenamine 230. Nitroenamine

230 after catalytic hydrogenation over Pd–C in the presence of ammonium formate in absolute methanol afforded compound 231. Compound 231 on reduction of lactam carbonyl with LiAlH4 followed by N-alkylation under usual conditions furnished the desired compound 233. Liyanage et al. established45 the synthetic route for carbapyochelins via diastereoselective azidation of 5-(ethoxycarbonyl) methyl proline derivative (Scheme 45). Pyroglutamic acid derivative 234 on reduction of azide group, followed by EDC-mediated coupling of crude amine with O-benzyl salicylic acid afforded compound 235, which was subjected to the reduction

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

HOOC

1. MeOH, SOCl2 O 2. NaBH4, EtOH

N H

N

OAc HO

N 216

215

17 1. Lawesson's reagent 2. CH3I then MeONa-MeOH

OH 1. n-C9H19MgBr

MeS

ether-CH2Cl2

N

OH n-C9H19

N 218

217 n-C9H19

+

N X 219(a)

toluene

N X 219(b)

CBzCl NaHCO3 H2O

X= H

CBzCl NaHCO3 H2O

1. NaBH(OAc)3

OH

OH n-C9H19

Ac2O, Pyridine

OH HO

X= CBz

TsCl, Pyridine 2. [CH2=CH-(CH2)3]2CuLi

n-C9H19

X= H X= CBz

Me3Sil, CHCl3

R N CBZ

n-C9H19

R N H R= (CH2)4CH=CH2

R= (CH2)4CH=CH2 220

221

Scheme 42.

CN HOOC

H3COOC

O

N H 61

OEt

N 222

H3COOC

N H 223

CN

CN MeMgBr

222 CN

COOCH3

N H

N

N

Et2O

H H3 COOC

224

N

N H

COOCH3

H3 C CH3 H3 C OH 226 HO CH3

225

CN 225

COOtBu

CN (t-Bu)Me2SiCl, DMF

LiBH4 N

THF, 32 ºC

H HOH2C

N

imidazole, 40 ºC

H

CH2OH

227

N

N t Bu

OSi

OSi

t

Bu

228 Scheme 43.

Lawesson's reagent O

N Me

S

COOMe

COOMe

i. CH3I, PhH

O2N

ii. CH3NO2, Et3N, DMF

H

229b

229a

HCO2NH4

N Me

Pd-C, MeOH N H 231

LAH pellets O

THF

COOMe

230 Me N

Me N

N Me

RCl K2CO3 DMF

N H 232

Me N

N R 233

Scheme 44.

of ethyl ester group in the presence of lithium borohydride to give 236. Compound 236 on further hydrogenolysis followed by cyclization with Burgess reagent afforded 237. Compound 237 on deprotection of t-butyl group afforded the desired carbapyochelins 238. In a view to develop methodologies for the chirospeciﬁc synthesis of 5-butyl-2-heptyl pyrrolidines, Shiosaki et al. reported a pro-

cedure46 for the asymmetric synthesis of 5-substituted prolines from pyroglutamates, in which the key steps adopted were the thiolactam formation from lactam of pyroglutamates followed by induction of side chain at C-5 through sulﬁde contraction and reduction sequences (Scheme 46). Corey et al.47 have utilized C-5 centre of the pyroglutamate by reduction for the synthesis of poly functional, structurally deﬁned

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

OBn N3 N Me 234

EtOOC

COOtBu

O

i. Pd/C, H2, EtOH

LiBH4. Et2O

ii. O-Bn-salicylic acid EDC, Et3N, DMAP

HN COOtBu

N Me

EtOOC 235

OBn

HN HO 236

O

i. Pd/C,H2, EtOH ii. Burgess reagent THF t COO Bu

O

N Me

OH

O TFA/DCM anisole

COOtBu

N Me

N

237

COOH N Me. TFA

N OH 238

Scheme 45.

R1 t

Bu O O

S

N

But O

R2 R2 =SOOCF3

O

Bu

Ph3P

ButO

( )5

CH2Cl2

ButO

O

Bu

PtO2,

( )5 N O

CH3

50Psi, H2

CH3 COOBu

N Bu

240

239 Pd/charcoal cyclohexane

COOBu CH ( )5 3 S

+ N

241

But O

( )5 N O

242

CH3

But O +

N O

Bu 243

( )5 CH3

Bu 244

Scheme 46.

catalyst 252, which ﬁnds use in the enantioselective addition of dialkylzinc reagents to aldehydes (Scheme 47). Wistard et al. have reported the synthesis of 5-substituted pyrrolidines from N-acylated pyroglutamic acid48a,b (Scheme 48). Agarwal et al. established a concise asymmetric approach to the bridged bicyclic tropane alkaloid (+)-Ferreiginine using enyne ringclosing metathesis49 (Scheme 49). Pyroglutamic acid was converted to its benzyl ester, followed by reduction using LiEt3BH 1. DIBAL-H THF, -78oC 2. pTSA

H O

COOEt

N

H H3CO

H

Methanol-Formalin

H trimethylsilylcyanide, CH2Cl2

COOEt

N

Stannic chloride, -40oC

COOEt 246

COOEt 245 Red, H2, W-II Reney-Ni

and MeOH/pTSA to afford C-5 methoxylated ester 257, which was subsequently subjected to C-5 allylation to afford 258 with stereoselectivity. Compound 258 on reduction followed by acetylenic carbon insertion under modiﬁed Witting conditions and subsequent hydrolysis of the resultant product afforded 260. Treatment of 260 with Grubb’s catalyst yielded 261 which after a sequence of reactions afforded the desired product (+)-ferreiginine 263.

H

NMe2

N

H N NMe2 H 250

H

H

PhMgBr, THF, 0oC

Ph Ph 249 LiAlH4 OH

NMe2

H

H

NMe2

N Me

251

Scheme 47.

H N

COOEt

COOEt 247

COOEt

COOEt 248

H NC

Ph Ph OH

H N

Ph Ph OH

KOH, CH3OH, H2O

COOEt 249

H Et2Zn

H

Ph Me Ph Zn O Me2N Et 252 N

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

HO

HO

COOR''

N

COOR''

N

Nu Nu

COOR'

COOR' 253

COOR''

N

COOR'

254

255

Scheme 48.

1. iPr2EtN, BnBr O

COOH

N H

CH2Cl2 O 2. (Boc)2O, DMAP MeCN

COOBn

N

1. LiEt3BH, −78 ºC, THF

Boc 257 CH3COCN2PO(OEt)2

reduction COOBn

N

Boc N

Boc 260

259 Boc N

Me N 1. TFA, CH2Cl2, then K2CO3

H2O, DMF

PCy3 Ru Cl PCy Ph

N

Boc

PdCl2, CuCl2

Cl

2. CH2O, NaCNBH3 CH3CN

3

O

261

Grubb's 10 mol%

CHO K2CO3, MeOH

N

Boc 258

CH2Cl2

COOBn

N

Boc 256

17

BF3.OEt2 Allyltrimethylsilane −78 ºC, Et2O

MeO

2. MeOH, pTSA, 25 ºC

O

262

263

Scheme 49.

of this reaction is in the addition of trimethylsilane to various Nacyliminium ions bearing ester side chains. As a result the precursor 264 could be converted to its allylated derivative 265. Mandal et al. described an efﬁcient synthesis of the constrained peptidomimetic 2-oxo-3-(N-9-ﬂuorenyloxy carbonylamino)-1-azabicyclo[4.3.0]nonane-9-carboxylic acid from pyroglutamic acid51 (Scheme 51). N-Boc methyl pyroglutamate 131 on reaction with vinyl magnesium bromide afforded Micheal acceptor 266, which on reaction with Schiff’s base in the presence of Cs2CO3 followed by hydrogenation using Pd/C in EtOH/AcOH (9:1) coupled with cyclization, was converted to diastereomeric compounds 268a and 268b. Compound 268b was epimerized to 268C in the

Another approach for the preparation of pyrrolidine allylation products involving diastereoselective enzymatic ester hydrolysis (Scheme 50) has also been reported.50 An important application

XR3 '' R'O

N

COOR

COOR

N

Lewis acid

PG

PG

264

265 Scheme 50.

O

131

MeOOC

COOMe

vinylmagnesium bromide

COOtBu

(Ph)2=NCH2COOtBu NHBoc

o

THF, -40 C

CS2CO3, THF

NHBoc

O 266

267

H N

BocHN

O 268a

H NaHMDS

N

BocHN COOtBu

O

N O 269a

Ph

N O 268c

268b 1. TFA, Et3SiH, CH2Cl2 2. Fmoc-OSu, 10% Na2CO3 1,4-dioxane H H

FmocHN

10% Pd/C

EtOH/AcOH(9:1)

H

+ BocHN COOtBu

Ph

N

COOtBu

1. TFA, Et3SiH, CH2Cl2 2. Fmoc-OSu, 10% Na2CO3 1,4-dioxane H

+ FmocHN COOH

N

FmocHN

COOH O 269b Scheme 51.

N COOH O 269c

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

presence of NaHMDS. Treatment of each diastereoisomer of 268 under usual conditions afforded the desired stereospeciﬁc isomers of 269. Hanessian et al.52 synthesized N-acyloxyiminium ions generated from 4-substituted L-pyroglutamic esters with 4-(3-butenyl),4-(3-butynyl),4-(3-cinnamylmethyl) and 4-allenic ethers which subsequently underwent rapid Lewis acid-mediated carboxycyclization to afford stereodeﬁned azacyclic compounds (Scheme 52). Conchon et al. described53 asymmetric synthesis of 3,5-disubstituted indolizidines by intramolecular addition of an allylsilane on an N-acyliminium ion derived from pyroglutamic acid. Compound 273 on reaction with benzylchloroformate in the presence of n-BuLi, followed by reduction was converted to 274, which on reaction with a-hydroxy b-trimethylsilyl-c-allyl derivative in the presence of SnCl4 was converted to 276 and subsequent reaction with PDC led to cyclization, thereby affording 278. Compound 278 after hydrogenation afforded isomers 279 and 280 (Scheme 53). Peng et al. reported the designing and synthesis of a 1,5-diazabicyclo[6,3,0]dodecane amino acid derivatives as novel dipeptide reverse-turn mimetics54 (Scheme 54). Pyroglutamic acid derivative 281 on reaction with TBSCl, followed by hydrogenation using Pd/C catalyst was converted to 282, which after N-acylation coupled with the deprotection of OH group afforded 283. Oxidation of side chain OH group of 283 followed by N-deprotection coupled with cyclization gave the desired compound 285. Angiolini et al. carried out55 synthesis of azabicyclo alkane amino acid scaffolds as reverse-turn inducer dipeptide mimics (Scheme 55). Compound 286 upon oxidation, followed by reaction with (±)-(Z)-a-phosphonoglycine trimethyl ester and subsequent protection of NH group afforded 287. Compound 287 on alkaline hydrolysis afforded 288, which on hydrogenolysis followed by

cyclization was converted to the desired molecules 289 and 290 as diastereomers. Ghammarti et al. described the synthesis of 1,5,6-10b-tetrahydro2H-pyrrolo[1,2-c]quinazoline-3-ones from pyroglutamic acid56 (Scheme 56). Danishefsky et al.57 described total synthesis of salinosporamide A, (Scheme 57) using pyroglutamic acid as a chiral starting material. Manzoni et al. reported the synthesis of spiroazabicycloalkane amino acid scaffolds as reverse-turn inducer dipeptide mimics58 starting from pyroglutamate (Scheme 58). Compound 303 on swern oxidation afforded aldehydic ester 304, which on witting reaction as described in Scheme 55 gave 305. Compound 305 after protection, deprotection and cyclization sequences afforded diastereomers 307a and 307b. Mulzer et al. synthesized rigid dipeptide mimetics. They have carried out stereocontrolled synthesis of all eight stereoisomers of 2-oxo-3-(N-Cbz-amino)-1-azabicyclo[4,3,0]nonane-9-carboxylic acid esters59 (Scheme 59). Compound 308 upon oxidation followed by witting reaction as described in Scheme 55 was converted to 310 and alkene component was subsequently reduced to get 311. Compound 311 after t-butyl ester hydrolysis, cyclization and conversion of carboxylic to its methyl ester afforded 312. Hussaini et al.60 reported a concise approach for the synthesis of cis-2,5-disubstituted pyrrolidines starting from pyroglutamic acid (Scheme 60). 5-Thioxo ethyl prolinate 200 was converted to 5alkylidine derivative 313 on reaction with diethyl bromomalonate in the presence of sodium bicarbonate. Compound 313 after Nbenzolylation afforded N-protected derivative 314. Compound 314 on hydrogenation in the presence of H2 (Pd–C), EtOH and CH2Cl2 gave N-benzoyl 2,5 disubstituted pyrrolidine 315. In another publication the same researchers have described a new methodology for the diastereoselective synthesis of 2,5-disubstituted pyrrolidine by the reduction of enamines derived from

H

H COOMe N

R'

H

Lewis acid

COOMe Lewis acid

R'=Me TMS

H O

X

N+ Boc

R'

H

O 271

N

COOMe

Boc 272 X= Cl, Br, aryl

270 Scheme 52.

1. SOCl2, NaBH4 HOOC

N H 61

O

2. TsCl, Et3N 3. Pr2CuLi, ether −20 ºC

Bu

O

N H 273

1. n-BuLi Benzylchloroformate 2. NaBH4, H2SO4 EtOH

H Bu Bu

OEt

N CBz 274

PDC, CH2Cl2

Bu

CBz

SiMe3 H

N

H2, Pd/C

CBz

MeOH

CBz

Bu

N+ R

275

R

OH

R

276

H

H Bu

N R 279

Bu

N

+ R Scheme 53.

280

O 277

OH R

H

N

N+

SnCl4 Bu

278

1600

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

1. TBSCl, N,N-diisoprpyl ethyl amine, CH2Cl2 TBSO

O O

COOH

N H

HO

N

2. H2, 10%, Pd/C, EtOAc

O

Bn 281

17

O

1. Boc-Dap(Z)-OH,EDC HOBT

HO

N,N-diisopropyl ethyl amine 2. TBAF, THF

CbzHN

O N H 282

O

Dess-Martin Periodinane

N O

CH2Cl2

O

O

O

N O

CbzHN

O

NHBoc 283

NHBoc 284

O

10%Pd/C,H2, MeOH

N O O

HN

NHBoc 285 Scheme 54.

Cbz 1. (COCl)2, DMSO, Et3N, CH2Cl2, −60 ºC

HO

(±)-(Z)-α−Phosphonoglycine trimethy lester

COOtBu

N

NBoc MeOOC

BuOK, CH2Cl2, −78 ºC, (Boc)2O, DMAP, THF

Ph 286

COOtBu

N

t

287

Ph

NHBoc HOOC

NaOH MeOH

287

COOtBu

N

1. H2, Pd/C, MeOH

Ph H2, Pd/C MeOH

N

N

2. Xylene, reflux BocHN

288

COOtBu +

O

COOtBu

N

BocHN

O 290

289

COOtBu COOMe NHBoc 291 Scheme 55.

O

N

O

COOH

SOCl2 O or ClCOCOCl

N

O

N N

COCl AlCl3 or SnCl4, CHCl3

O

N N

R

O R

R 292

294

293 Scheme 56.

pyroglutamic acid61 (Scheme 61). Compound 316 was converted to its N-Boc derivative which upon reduction in the presence of NaBH4 gave the desired product 318. Moloney et al. described62,144 a direct and versatile synthetic route for the reliable synthesis of trans-2,5-disubstituted pyrrolidines from pyroglutamic acid. N-Boc ethyl pyroglutamate 319 was reduced to 5-substituted product 320, which on reaction with PhSO2H gave 321 (Scheme 62).

Chan et al.63a–c described the conjugated addition of activated nitrogen nucleophiles, to a,b-unsaturated bicyclic lactams with an objective to synthesize enantiopure b-aminopyrrolidinones (Scheme 63) and a,b-diaminopyrrolidinones64 (Scheme 64), respectively, from (S)-pyroglutamic acid. Lithium enolate-derived Michael addition of 324 with di.tert-butyl azodicarboxylate afforded diamino lactam 325. This compound was transformed to the corresponding lactam 326 by deprotection with TFA which on

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O

Ph N

R' β-face R

O

COOBn

296

N

O

O

Me

O

297

O

H

ZnCl2

PMB

CHO

COOBn

PhS-H

OEt

PMB t

H

COOtBu

N

O

O BnO

COO Bu

PMB

O

R add β to C2

H α-face 295

N

-

R add α to C3

O

PMB BnOH

COOtBu

N

EtO

C

N

O

COOtBu Me

OH COOtBu

THF, −78 ºC O

OBn

Me

OBn OBn

299

298

300

H 1. CAN, CH3CN-H2O

H N

O

2. Na, liq.NH3, −78 ºC 3. NaBH4, THF-H2O (2:1) HO

Me 301

H

OH 1. BCl3, CH2Cl2, 0 ºC O CH2 OOBn OH 2. BOPCl, TEA, CH2Cl2 3. Ph3PCl2, Pyridine, Cl CH CN, rt 3

H N

OH O

Me

O

302 Salinosporamide A

Scheme 57.

Ot Bu N HO

Ot Bu

(COCl2)2, DMSO

N

Et3N, CH2Cl2

O COCF3 303

304

Ot Bu

Ot Bu (Boc)2O, DMAP N MeOOC

THF

O COCF3 NHCbz

t-BuOK, CH2Cl2, −78 ºC

O H COCF3

O

(±)-Z-α-Phosphonoglycine trimethy lester

N

MeOOC

O COCF3 NBoc Cbz

305

2. NaBH4,MeOH 3. MeOH, reflux

306

OtBu

Ot Bu

+

N

1. H2, Pd-C, MeOH

N

O

O

O

O

BocHN

BocHN 307a

307b Scheme 58.

hydrogenolysis using Pd/C in glacial acetic acid afforded 3,4 diamino pyroglutaminols 327a and 327b. Hara et al.65 described remarkable endo selectivity on hydroxylation of bicyclic lactam enolates 328 with MoOPD and MoOPH to afford hydroxylated products 329a and 329b (Scheme 65) derived from pyroglutamic acid. In another approach Bailey et al. described the diastereoselectivity during alkylation of bicyclic lactams66 (Scheme 66). Compound 330 on reaction with acetophenone dimethyl acetal using

pTSA (catalytic amount) was converted to the corresponding product 331a, which after Li enolate-derived benzylation reaction at C7 was converted to 331b. Colombo et al. reported67 synthesis of new bicyclic lactam peptidomimetics through ring-closing metathesis reactions (Scheme 67). N-Boc-5-allyl-L-proline methyl ester 332 was converted to 333 by acidic hydrolysis with deprotection of Boc group, compound 333 on reaction with 2 benzyl 2 benzyloxycarbonylamine but-3-enoic acid and PyBropR in the presence of DIEA and DMAP

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

MeOOC COOtBu

N

HO

Dess-Martin-Periodinane CH2Cl2

Boc 308

P(O)(OMe)2

COOtBu

N

O

NHCbz

KOtBu, CH2Cl2, −78 ºC

Boc 309

CbzHN

Pt/C, ethylacetate

COOtBu

N

CbzHN

Boc

MeOOC

COOtBu

N

H COOMe

310

Boc

HCl-gas, CH2Cl2 then SOCl2, MeOH. DMF then MeOH, Hunig's base

311 H N

CbzHN

COOMe

O 312

Scheme 59.

O

N H

BrCH(COOEt)2

Lawesson's reagent COOEt CH2Cl2

S

N H

144

COOEt

(EtOOC)2C

NaHCO3

200 EtOOC

PhCOCl, Et3N

N

DMAP, CH2Cl2

EtOOC

COOEt

COPh

COOEt

N H 313

EtOOC

H2(5atm)

COOEt

N

Pd/C, EtOH CH2Cl2

EtOOC

314

COPh 315

Scheme 60.

(Boc)2O, Et3N EtOOC

EtOOC PhOC

COOMe

N H

N

DMAP

PhOC

316

COOMe

NaBH4

EtOOC

OH N

PhOC

Boc 317

Boc 318

Scheme 61.

O

N

COOEt

LiBEt3H, THF

X

−78 ºC

N

COOEt

Boc X=OH or MeO

Boc 319

320

PhSO2H CaCl2, DCM

PhO2S

N

COOEt

Boc 321

Scheme 62.

EtOOC

EtOOC

R

Nitrogen nucleophile (RH) O

N Ph

MeOH, rt O 322

O

N Ph

O 323

Scheme 63.

afforded dipeptide 334. Compound 334 on cyclization in the presence of Grubb’s reagent, followed by catalytic hydrogenation gave the desired peptidomimetic 336.

Hanessian et al.68 reported design and synthesis of diversiﬁed azacyclic inhibitors of endothelin converting enzyme. A series of azacyclic phosphonic acids were synthesized from L-pyroglutamic acid (Scheme 68) N-Boc methyl pyroglutamate 131 on reaction with allyl bromide in the presence of LiHMDS was converted to 4-substituted diastereomeric products 337a and 337b, where compound 337a was converted to its dimethylphosphonates 338a and 338b. Further reaction of allyl intermediate 338a with BH3THF and NaOH, followed by tosylation and induction of the naphthalamide moiety gave 339. Compound 339 after a sequence of reaction was converted to 340. Brana et al.69 developed a route for the synthesis of spiro-bis-clactam utilizing a chemoselective Michael reaction as a key step for

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

EtOOC

N(Bn)OBn

RHNRN

N(Bn)OBn

LDA, then O

O

N

N

O

O

Ph 322

Ph

324

N(Bn)OBn

H2N

NH2

H2, Pd/C O

N

O

Ph

(RHN)RN

TFA, DCM, rt

O

BocN=NBoc

H2 N OH

CH2OH HOAc

N H

O

NH2

+

OH O

N H

326

325

N H

327a

327b

Scheme 64.

R'' H O

R''

HO

N O R'

1. base, THF, −78 ºC

HO R'' H

H +

O

N

2. MoOPD or MoOPH −78 ºC

O

N

O R'

R''= allyl 328

O R'

(endo)

(exo) 329b

329a Scheme 65.

the synthesis (Scheme 69). Methyl N-(-p-methoxybenzyl) pyroglutamate on deprotonation with LiHMDS followed by reaction with electrophiles gave 2-substituted product 342, which on hydrogenation with Raney Ni afforded spirobis cyclic lactam 343. Harris et al.70 developed a route for the synthesis of seven macrocyclic analogues of the neuroprotective tripeptide glycyl-L-prolyl-L-glutanic acid (GPE) using pyroglutamic acid (Scheme 70) as

a chiral precursor. N-Protected pyroglutamate 311 on selective reduction of lactam carbonyl group with LiEt3BH followed by BF3Et2O mediated allylation with allyltributylstannane was converted to 344 which after deprotection of Boc, followed by N-acylation gave 347. Compound 347 after cyclization under normal conditions afforded 348 which on hydrolysis of ethyl ester afforded acid 349. Subsequent reaction of 349 with 350 in the presence of BOP-Cl gave oleﬁn 351. Treatment of oleﬁn over PtO2 followed by immediate deprotection of Boc and esters group afforded 352. Langlois et al. described71 the synthesis of new polyhydroxylated indolizidines from bicyclic silyloxy pyrrole (Scheme 71). Compound 134 upon oxidation was converted to regioselective isomers 353 and 354, where bicyclic derivative 353 after deprotection followed by protection with TBDMSCl, and subsequent sodium enolate-derived reaction with allyl bromide gave N-allylated products 356 and 357 which on treatment with Grubb’s catalyst underwent cyclization to give 358. Compound 358 on oxidation with OsO4 gave diols 359 and 360.

CH2Ph

H

H

H O

OR''

N R' R'= R''= H 330

Toluene, toluene p-sulphonic acid

O

LDA, TsCl

N

acetophenone dimethyl acetal ZnCl2

N

PhCH2Br

O R'

O

O R'

R'' 331a

R'' 331b

Scheme 66.

Ph PyBrop(R) CbzHN

HCl/MeOH N

COOMe

N H 333

Boc 332

N

Toluene, reflux

COOMe

COOH

DIEA, DMAP, CH 2Cl2

O NHCbz Ph cis 334

N

COOMe

COOMe

10%Pd/C

Grubb's reagent

O

N

O

H2, EtOH NH2 Ph

NHCbz Ph 335

336 Scheme 67.

COOMe

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

R''

R''

LiHMDS, THF O

−78 oC

COOMe allylbromide,

N

O

+ COOMe O

N

Boc

Boc

131

Boc

337a R''

337b

R''

O MeO

N

R''= allyl

+

P

N

OMe

COOMe

1.(i) BH3.THF, THF, 0 oC (ii) NaOH, H2O2

O MeO

Boc

o 337a 1. Super hydride,THF, −78 C COOMe 2. Ac2O, Et3N, DMAP, DCM 3. P(OMe)3, BF3.OEt2, DCM −78 oC

338a

P

N

OMe

Boc

338a

2. TsCl, Et3N, DMAP, DCM N-(1,8-dicarboxynaphthalimido) Na+ salt, DMF

COOMe

338b R'''

R''' 1.LiOH.H2O, THF/H2O/MeOH(5:4:1) 2. i-Pr2NEt, EDCl, HOBt, H-Phe-OtBu.HCl, DCM

O MeO

P

N

COOMe

O NaO P

3. HCl(gas) dioxane, reflux 4. TMSBr, DCM then 1 equiv of NaOH 0.05M

OH

OMe Boc 339 R'''= N-(1,8-dicarboxynaphthalimido)ethyl

H N

N H

R''''

O HOOC R''''=CH2(3-indolyl) 340

Scheme 68.

O

N

O

1. LiHMDS/THF NO2 Ph COOMe 2. CAN, H O

COOMe O

N H

2

PMB 341

H2,Ni/Ra

NO2

NH

O

MeOH

N H Ph 343

Ph 342 Scheme 69.

O

N H 17

COOH

1. EtOH, SOCl2

1. LiEt 3BH,THF, −78 oC, H2O2, 0 oC

O

N

2. DMAP, (Boc) 2O CH3CN

CF3COOH, CH2Cl2

tBuO COOEt +

N H

H

COOEt

H N

COOH

DCC, Et3N

O

345

N

2. BF3.OEt2, allyltributyl stannane H CH2Cl2, −78 oC

COOtBu 311

N

H

CH2Cl2

H

N

COOEt

CH2Cl2 then DMSO

HN

CH2Cl2, 0 oC

H

N

H N

COOtBu

1. PtO2, H2, THF COOtBu

H

N

2. CF3COOH, CH2Cl2

COOtBu .HCl COOtBu 350

H N

COOH

H O

O COOH

NH2.TFA 352 Scheme 70.

H2N

+

NHCOOtBu

COOtBu

O

NHCOOtBu 351

COOH O

349

H O

H

N

Dioxane

NHCOOtBu

348

BOP-Cl, Et3N,

1M eq NaOH, H2O

O

COOEt O

346

347

Cl2(PCy3)2Ru=CHPh

COOEt

COOtBu 344

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

TBDMSO

SnCl4, −78 ºC O NaHCO3

N

OH N

O

CF3COOH

O

+

N

O

Ph 133

353

SnCl4, −78 ºC Me3SiCH2CH=CH2

N H

353

O

O

+

N

N

O

O

OTBDMS R= H R= TBDMS

357

356

OTBDMS 356

354

Allyl bromide

RO TBDMSCl Im., DMF 355

Second Grubb's cat.

O Ph

Ph

NaH-KI

O

N

O

Ph 134

THF, -H 2O

O

OsO4.NMO

N

O

OTBDMS O +

N

CH3COCH3-H2O

OTBDMS N

OH

358

OH

OH 359

OH 360

Scheme 71.

Deyine et al. reported stereoselective synthetic route for the synthesis of enantiopure 3,4,5-trisubstituted piperidines, using (S)-pyroglutaminol as a chiral precursor72 (Scheme 72). Davies et al. reported73 the synthesis of an external b-turn, based on the GLDV motif of cell adhesion proteins. Pyroglutamates 364 was converted to thio ester 366 then to 5-substituted product 367 which upon hydrogenation followed by treatment with MeOH–TFA gave 368 as starting material for cyclization to get 370 (Scheme 73). Gedu et al. established the synthesis of new isoquinolines 372 starting with pyroglutamic acid via substituted ketones74 (Scheme 74). Olivo et al. achieved75 the synthesis of ()-stemoamide 377 in 11 steps from 5 acetoxy-N-crotyl-pyrrolidinone. A chiral N-acyl thiazolidinethione synthesized as an intermediate was employed for stereoselective addition to a cyclic N-acyl iminium ion (Scheme 75). Manzoni et al. reported76 stereoselective alkylation approaches for the synthesis of eight enantiopure, sterically constrained Catetrasubstituted azabicyclo alkane amino acids (Scheme 76). Pyroglutamate derivative when reacted with benzyl bromide in the presence of base gave alkylated derivatives 379 and 380 as diastereoisomers. Bracci et al. described stereoselective synthesis of functionalized 2-oxo-1-azabicyclo alkane through a ring-closing metathesis reaction thereby able to construct a seven-membered lactam 388, starting with pyroglutamate derivatives77 (Scheme 77). Compound 381 on reduction, followed by reaction with MeOH and PPTS was converted to 383 with methoxy group at C-5 O-silyl derivative 383 was converted to O-acetyl derivative 384 so as to

avoid O-deprotection. Compound 384 was transformed to 5-propenyl proline 385 on reaction with propenyl bromide in the presence of Li, CuBrMe2S and BF3Et2O. Compound 385 after N-Boc deprotection followed by N-acylation was converted to 387. Compound 387 was subjected to cyclization in the presence of Grubb’s catalyst and followed by reduction in the presence of nickel boride thereby affording cyclized products 388. 3. Asymmetric use of pyroglutamates without prior modiﬁcations Even though the earlier studies on the asymmetric use of pyroglutamates required prior modiﬁcations such as reduction at C-2 or activation at C-5 so as to prevent racemization, however few of the reports are available describing asymmetric use of pyroglutamates without prior modiﬁcations. 3.1. Direct chain elongation reactions Katritzky et al.78 discovered an expedient route for the synthesis of N-Z-pyroglutamoyl-amino acid derivative by direct coupling of the C-terminus activated N-protected pyroglutamate (Scheme 78). Toyooka et al. discovered enantioselective synthesis of a hydroxyindolizidine alkaloid using pyroglutamic acid as a starting material79 (Scheme 79). Methyl pyroglutamate was ﬁrst subjected to N-protection using benzyloxy carbonyl chloride and subsequent reaction with n-butyl magnesium bromide in the presence of TMEDA resulted in ring opening coupled with the introduction of nbutyl group thereby furnishing 392. Compound 392 on Martin’s

Ph

Ph N

Ph +

N O heat

OH O

N H 18

HN

O

O

N

OH

LAH, THF O

heat

N

O

O

Ph

Ph

361

362 Scheme 72.

OH N Ph 363

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

H O

H

NaHMDS COOtBu PhCH2Br

N H 364

t

O

COO Bu THF

N

THF, −78 oC

t

S

COO Bu

N Ph

365

H

366

O

F3COCHN

H

MeOOC

COOtBu

N

H2/Pd/C/60-200 PSi

H H

MeOOC

MeOH-TFA

N H

H

H

H

BuMgCl/Et 2O/0 oC

H

COOtBu

N

t

H

K2CO3/MeOH heat

COOtBu

N

O H

COOtBu

368

Ph

367

COCH2Br

MeOOC

Ph3P/Et3N, CH3CN

Ph

F3COCHN

F3COCHN H

H

P4S10

O H

NHCOCF3 369

NH2 370

Scheme 73.

O

O

O

PPA

N

N

o

140 C

371

R

R

372 Scheme 74.

transformation produced 2,5-cis-disubstituted pyrrolidine 393. Treatment of 393 with DIBAL followed by the addition of vinyl Grignard reagent to resultant aldehyde provided alcohol 394 as a mixture of diastereomers. The cross-metathesis reaction of 394 with 1-hexen-3-one in the presence of Grubbs II generation catalyst afforded the homologated product 395. Exposure of 395 to hydrogenation in the presence of Pearlman’s catalyst furnished the two indolizidines 396a and 396b, which were separated to get ()-396a as a major diastereomer and 396b as a minor isomer. Li et al. reported80 ﬁrst enantioselective synthesis of (D)-2-tertbutoxycarbonylamino-5,5-diﬂuoro-5-phenyl-pentanoic acid 400 with an objective to incorporate in growth hormone secretagogues (Scheme 80). N-Boc ethyl pyroglutamate 319 on treatment with phenyl magnesium bromide, followed by reaction with 1,2-thioe-

S S

thane in the presence of BF3Et2O afforded two compounds 397a and 397b. Subsequent N-acylation with acetic anhydride in the presence of triethylamine afforded the desired acetamide 398. Treatment of acetamide 398 with NOBF4, HF/pyridine, followed by deacetylation yielded amino carboxylic ester 399b which after protection of primary amine with Boc group followed by ester hydrolysis afforded the desired compound 400. Gu et al. reported81 a concise synthesis of (2S,4S)-4-methylglutamic acid 406 (Scheme 81) starting from pyroglutamic acid. Compound 402 on reaction with LiN(SiMe3)2 in THF and MeI was converted to isomers 403 and 405, which after alkaline hydrolysis followed by N-Boc deprotection afforded 404 and 406. Dieterich et al.82 reported the synthesis of (2S,3S)-[3-2H1]-4methylglutamic acid and (2S,3R)-[2,3-2H2]-4-methyleneglutamic acid. Compound 131 was converted to 4-[N,N-dimethyl amino]methylene derivative 407. Compound 407 on hydrido deamination with DIBAL-H afforded 4-methylene pyroglutamate 408. Compound 408 on reaction with LiOMe in the presence of MeOH, followed by acidic hydrolysis using HBr furnished substituted glutamic acid 410 (Scheme 82). Dinsmore et al.83 described the use of a modiﬁed ring-switching strategy for the synthesis of glutamate antagonist (2S)-2-amino-3(2,4-dioxo-1,2,3,4-tetrahydropyrimidin-5-yl)propionate 417 and related compounds having two asymmetric centres, from pyroglu-

S

O N

+

AcO

O

N

Iminium ion addition

S

N

Me

Ph 373

O

Ph

374

Me H

O S

N Ph Ph 376

N

Me

375

OH

O

S

anti-aldol addition

O

N

9 steps

H

O

N

H

Me

(-)-Stemoamide 377

O Scheme 75.

O

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

( )n

COOtBu 1. base, THF, −78 oC

N

COOtBu ( )n

N

COOtBu

N

+

2. PhCH2Br 3. NaBH4, MeOH

O N 378

( )n Ph

O

Ph

O

R HN

HN

Ph

Ph 380

379 Scheme 76.

TDSO

TDSO

TDSO

LiEt3BH, THF O

N

−78 oC

COOtBu

MeOH, HO

N

1.TBAF, THF MeO

PPTS

COOt

Bu

AcO

AcO

N

COO Bu

COO Bu

AcO tBuOAc,

1-propenyl bromide LiCuBr.Me 2S BF3.Et2O

t

2.AcCl, Et3N CH2Cl2

t

Boc 383

Boc 382

Boc 381

MeO

N

N

Boc

HClO4

0 oC

t

COO Bu

N H 386

Boc

384

385 AcO

COOtBu

AcO

1. Grubb's cat.

Allyl glycine N

NMM, isopropyl chloroformate THF, −30 oC

COOtBu NHCbz

O

N

2. NaBH4-NiCl2, MeOH

COOtBu O

NHCbz 387

388 Scheme 77.

R O

BtH, SOCl2

COOH

N Z 389

O

N Z 390a

COBt + H2N

H N

CH3CN/H2O

COOH

O

Et3N

390b

N Z

O

391 Scheme 78.

i. LiHMDS, CbzCl

H MeOOC

N H 111

O

ii. nBuMgBr, TMEDA

i. Ph3SiH, BF3.OEt2

H MeOOC

NH

O

Cbz 392

H

H MeOOC

then vinylMgBr

H

H

i. DIBAL, CH 2Cl2

N

HO

Cbz 393

Cbz 394 H

H HO

N

1-hexen-3-one Grubb's II generation Catalyst

N

Pd(OH)2, EtOH

HO

H

H N

Cbz

H 396a

O 395 Scheme 79.

HO +

H

H N

H 396b

COOH R

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O

i. PhMgBr ii. 1,2-di-thioethane BF3Et2O

COOEt

N Boc 319

S

S

397a

Ac2O, Et3N

S

S

F

F

F

NH2

R= Et, Me COOR 399b

COOEt

HCl/MeOH

NHAc COOEt

399a

COOEt

Ph

N 397b

Ph

HF/pyridine 398

Ph

COOEt

F

NOBF4

NHAc

Ph

+

NH2

Ph

(Boc)2O

F

LiOH

Ph

F

NHBoc

400

COOH

Scheme 80.

SOCl2 O

COOH

N H

(Boc)2O, DMAP

MeOH

O

COOMe

N H

Et3N, CH2Cl2

O

N Boc

1. LiN(SiMe3)2/THF COOMe 2. MeI

402

17 Me

Me 401

Me +

O

COOR

N H 403

O

N H 405

1. LiOH/ H2O/THF

1. LiOH/ H2O/THF

2. TFA/CH 2Cl2

2. TFA/CH 2Cl2

Me

Me

NH2

Me

NH2

COOH

HOOC

COOH

HOOC

COOR

406

404 Scheme 81.

NMe2

H

H O

N

COOMe

DIBAL-H Hexane

(ButO)CH(NMe2)2 MeOCH2CH2OMe

O

Boc 131

COOMe

N

H

O

THF, −70 oC

Boc 407

COOMe

Boc 408 H

H H

H LiOMe, MeOH THF

N

9M aq. HBr MeOOC HN

reflux

COOMe

Boc 409

HOOC H2N

COOH

410 Scheme 82.

tamic acid (Scheme 83). Aldehydic group was introduced at C-4 of N-protected pyroglutamate 411. The resultant compound 412 on amination with NH4OAc–AcOH, followed by reaction with ClSO2NCO gave diastereomers 414 and 415, subsequent reaction with K2CO3–EtOH, followed by hydrolysis afforded 417. Langlois84a,b et al. described the diastereospeciﬁc formal synthesis of (2R,3S)-2-amino-tetradeca-5,7-dien-3-ol 423, a natural product isolated from xestopongia species using epoxidation and epoxide ring-opening sequences in native pyroglutamate moiety

(Scheme 84). Compound 418 was converted to 419, which after O-deprotection at C-4 and O-protection at C-5 gave 420. Compound 420 on iodonation using NaI in DMF gave 421, which on hydrogenolysis using H2–Pd/C was converted to 422. Compound 422 on reaction with KCN in the presence of EtOH–THF underwent ring opening to give 423. Ring opening of N-alkoxycarbonyl c-lactam 424 with lithium methylphenylsulfone, resulted in the synthesis of enantiopure cis 2,5-disubstituted pyrrolidines85 (Scheme 85). Pyroglutamic acid

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

NH2 H

OHC O

ClSO2NCO

NH4OAc-AcOH

LiHMDS HCOOMe

COOtBu

N

H

O

COO Bu

N

COOtBu

O

t

NH2

H N

H 2N

HN

H HN

O H O

CH2Cl2

COOtBu 413

COOtBu 412

411

COOtBu

N

+ COOtBu

N

O

K2CO3-EtOH O

COOt

HN

heat

COOtBu

N

O COOtBu O HN COOtBu 416

COOt

Bu

Bu

415

414

HN O HCl

HN COOH

O H 2N 417 Scheme 83.

O

O

OH

OR

O

N

N

O

0.1N. HCl MsCl-Py

OR

O

Boc R= OMs 420

Boc R= CH(Me)OEt 419

Ph 418 OH

R

N

OH NHBoc

NaI DMF

O

N

I

H2/Pd/C O

N

Boc

CH3

EtOH-THF KCN

Boc 422

421

COOEt OH 423

Scheme 84.

O OR O

PhSO2CH2Li

O

PhO2S

OR

THF, −72 ºC

N

O

OR

NHCOOBn

COOBn O

NHCOOBn 426

425

R= tBu 424 H2, 1 atm Pearlman's Catalyst H3C

O

Na-Hg Amalgam

OR LiAlH4 N H 427

OH H3C

O

N H 428

Scheme 85.

derivative 424 on reaction with methylphenylsulfone in nBuLi using THF as a solvent, followed by desulfonylation using Na–Hg and Pearman’s catalyst afforded compound 425, which after hydrogenation followed by reaction with LiAlH4 afforded 428. New diastereoselective synthetic route for 2-substituted cis(2S,5S)-and trans-(2S,5R)-5-alkylprrolidinones as indolizidine and pyrrolizidine scaffolds has been reported by Mota et al.86 (Scheme 86).

Oba et al.87 reported the synthesis and reactions of novel 3,4didehydropyroglutamate derivatives through hydrogenation and ring-opening sequences with H2 and Pd/C in the presence of CH3OH. The ABO ester 432 on hydrogenation followed by ring opening afforded L-glutamic acid (Scheme 87). Another ring-opening strategy via copper (1) mediated crosscoupling of pyroglutamic acid-derived organo zinc reagent with acid chloride was reported by Hjelmgaard et al.88 (Scheme 88).

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O

O

PhO2S

O

OR NHCbz

O

H

Na-Hg Na2HPO4/MeOH

430

429

H

H2 OR Pd(OH) 2 NHCbz

OR N H 431

O

Scheme 86.

O

N

ABO

1. H2, Pd/C, CH3OH

Makino et al. described89 stereoselective synthesis of (S)-(+)lycoperdic acid through an endo selective hydroxylation of the chiral bicyclic lactam enolate with MoOPH (Scheme 89). Lienolate-derived reaction of 19 with allyl bromide afforded 4-allyl derivative 439a, which on further reaction with LDA and MoOPH gave 4-allyl-4-hydroxy derivative 439b. Allyl group of 439b was subjected to hydroboration–oxidation sequences to get diol 440. Compound 440 after a sequence of reactions was converted to (+)-lycoperdic acid 442. Cohen et al. described the synthesis of (S)-(+)-lycoperdic acid90 442 starting with pyroglutamic acid derivative 443 (Scheme 90). Bromo lactam compound 443, when subjected to tandem oxidation–annulation reaction with Jones reagent at 0 °C followed by workup with potassium carbonate delivered spirolactam 444a. Sequential Boc protection and TBAF desilyation afforded pyroglu-

L-Glutamic acid 433

2. 1M HCl Reflux then Dowex 50W-X8

Boc 432 ABO= 2,7,8-trioxabicyclo[3.2.1]octane Scheme 87.

Compound 18 after tosylation, followed by reaction with NaI and MeCN was converted to iodo products 434 and subsequently to organo zinc compound 435. Compound 435 on reaction with CuCN2LiCl and RCOCl gave 438a and 438b on the one hand and through acidiﬁcation afforded 436 or 437 on the other hand.

1. TsCl, Et3N, DMAP

O CH2Cl2 2. NaI, MeCN, heat

N H 18

OH

N H 434

I

0.1M HCl

Zn O DMA, 0 ºC

N H

ZnI

O 435 CuCN.2LiCl RCOCl

NHR

H

N H 436

O

and/or

+

O

O

N H 438a

R= H 437

N Ph O 438b

Scheme 88.

H O

N O

HO

H

LDA Allyl bromide -78oC

O

N

O

MoOPH

N

-78oC

O

Ph

O Ph 439b

Ph

439a

19

H

LDA

O OH O HO

BH3·THF, THF, 0oC

H

O

then CH2Cl2, NaOH

H

i. Jones' reagent

O

acetone

N

N

O

O

Ph

Ph 441a

440

O

H

O i. RuCl3, NaIO4 CCl4/CH3CN/H2O

H O

N H 441b

O O

Ph

i. 6M HCl reflux

O Scheme 89.

O

COOH NH2 COOH

O

(+)-lycoperdic acid 442

O

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

OTBS O

O

O

i. Jones reagent acetone

Br O

O

(Boc)2O, DMAP O

ii. K2CO3, acetone

N H 443

OTBDPS

O

ii. TBAF, AcOH

N H

N H

OTBDPS

444a

444b

OH

O HOOC

O

O

O

i. RuCl3, NaIO4 CCl4/CH3CN ii. TMSCHN2

O

EtOAc/ MeOH

i. 6M HCl reflux ii. ion exchange chromatography

COOH

N H 444c

-

COO H3N (+)-Lycoperdic acid 442

+

Scheme 90.

O

OMOM

N

R

O

O

Et2AlCl, Cyclopentadiene Toluene, −78 ºC

OMOM

N

R O

445

446 Scheme 91.

taminol 444b. Oxidation of 444b with RuCl3 followed by exposure of crude mixture to TMSCHN2 afforded methyl ester 444c which after acidic hydrolysis followed by puriﬁcation yielded the desired (S)-(+)-lycoperdic acid 442. 3.2. Use of N-derivatized pyroglutamates for asymmetric synthesis 3.2.1. Diels–Alder reactions Highly asymmetric Diels–Alder reactions have been carried out using (S)-pyroglutamic acid derivatives as chiral dienophiles. Asymmetric Diels–Alder reaction of cyclopentadiene with chiral dienophile 445 derived from (S)-pyroglutamic acid derivatives in

O R

R N

O

O

N

OO

O R1 447

a. R= COOEt, R1= H b. R= COOEt, R1= Me

R1 448

O

the presence of a Lewis acid catalyst such as diethylaluminium chloride in toluene afforded cyclo adducts 446 with high stereoselectivity91 (Scheme 91). Strong chiral inﬂuence of pyroglutamate has also been utilized in diene component of Diels–Alder reaction. Menezes et al. have explored the use of ethyl-N-dienyl pyroglutamates as novel asymmetric diene where chiral cyclohexenyl amine derivatives 448 were obtained in good yields92 (Scheme 92). Defoin et al.93 have carried out asymmetric hetero Diels–Alder cycloadditions using chiral N-dienyl lactam and acyl nitrosodienophiles (Scheme 93). 3.2.2. Radical cyclization Asymmetric synthesis of pyrrolidinones by radical cyclization of N-allylic pyroglutamates which were synthesized from ethyl-(S)pyroglutamate has been carried out94 (Scheme 94). 3.2.3. N-Acylations/alkylations of native pyroglutamates Boisse et al. discovered95 synthetic strategies for new comptothecin analogs starting with pyroglutamic acid derivative. In one of the approaches methyl pyroglutamate after N-benzoylation with 2-nitrobenzoyl chloride in the presence of NaH, followed by reductive cyclization with SnCl2 in ethanol afforded modiﬁed precursor of camptothecins 457 (Scheme 95).

Scheme 92.

MeOOC

MeOOC N

O

N

O

RCON=O

449

450 Scheme 93.

MeOOC +

N

O

O

O

NCOR

NCOR 451

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

1. R2CH=C(R)3CHR1Br/THF/ I Sonification, Bu4NBr, KOH EtOOC

N H

O 2. LiAlH4/ SiO4 3. CH3SO2Cl/NEt3 4. NaI/ acetone

452

N

O

R3 R1

AIBN Bu3SnH, PhH reflux

N

O

R2

R2

R3

R1

R3

453

O

N +

R1 455

R2

454 Scheme 94.

O

COOMe

N H

O

NaH, THF then

COOMe

N

2-nitrobenzoyl chloride

N

COOMe

N

NO2

O

111

SnCl2, EtOH

O R1

456

R2

457

Scheme 95.

458

1. NaH, CH3COSCH2CH(CH3)COCl O

N H 177

COOEt

O

o

2. TFA, 0 C 3. HSCH2CH2NH2

N

N

CF3COOH

COOR H N

O

N

COOEt

CH3

COOH H N

H2/Pd

COOEt

O

O 460

SH

O 459

O

COOR

CH3 CH2CH2Ph

461

CH3 CH2CH2Ph

Scheme 96.

H

AcO

COOMe

N

1. SnX4, CH2Cl2 −78 ºC

X H

Boc

462

H

COOMe

N

Boc X= Cl

Bu4NOAc toluene or NaN3.DMF

R H

N

COOMe

Boc R= OAc, N3

463

464

Scheme 97.

In an attempt to develop potent ACE inhibitors such as 459 and 461 derived from pyroglutamates, N-acylations of pyroglutamates have been reported96a,b (Scheme 96). These N-acylations have been accomplished by the reaction of pyroglutamate derivative 177 with NaH and acid chloride for the synthesis of modiﬁed captopril analog 459, and with NaH and p-nitrophenylester of Z-Ala-OH for the synthesis of enalapril analog 461. Hanessian et al.97 reported the synthesis of 6-substituted hydroindole 2-carboxylic acids from pyroglutamic acid derivatives, where compound 462 on reaction with SnX4 was converted to bicyclic ester 463, and the resulting product was subsequently converted to 464 using Bu4NOAc in toluene (Scheme 97). Straight forward ring expansion of pyroglutamates to Perhydro1,3-diazepine-2,4-diones was reported by Stevens et al.98 (Scheme 98).

Bourry et al. described99 their studies on pyrrolidinones oxidation and rearrangements in the hexahydrobenz[f]indolizine-3,10dione series (Scheme 99). N-Benzyl pyroglutamic acid 466 on reaction with thionyl chloride and ClCH2CH2Cl afforded compounds 467a–467c, where compound 467a was converted to pyrrolinone 468 with HCl and O2 at room temperature. Enders et al. delivered a synthetic strategy for enantiopure triazolium salts from pyroglutamic acid and their evaluation in the benzoin condensation (Scheme 100). Pyroglutamic acid after esteriﬁcation followed by reaction with phenyl magnesium bromide yielded substituted c-bytyrolactam 112a. Reduction of tertiary alcohol group of compound 112a led to lactam 469, which was then converted to triazolium salt 470100 under usual conditions. Dudot et al. described the synthesis of chiral pyroglutamate amines through hydrogenation followed by alkaline hydrolytic

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

COOR1

O O

NaH

COOR1

N H

O

COOR1

N

R2NCX N-

177

NR2

NH

O

O

R1=Bn R2=Ph

R2 465b

465a Scheme 98.

O

COOH

N Ph 466

OH

O

1. SOCl2 O ClCH2CH2Cl2 2. AlCl 3

O +

N

O

N

467b

467a

O +

O

N

HOOC 467c

conc. HCl, O2

OH

O

N

468 Scheme 99.

Ph

i. SOCl2, MeOH O

COOH

N H 17

ii. PhMgBr, THF

O

N H 112a

Ph

t-BuLi, Et3SiH

Ph

DCM

O

N H 469

OH

Ph

Ph i. Me3O+BF4-, DCM

N

ii. PhNHNH2, DCM iii. HC(OMe)3, 80 oC Ph

N

Ph

N+ BF4470

Scheme 100.

O

H CH3

N

NHPh

PhOOC

1. H2, Pd/C, MeOH 2. NaOH, MeOH 3. Separation

O HO

Ph 471a

H CH3

N

H NHPh Ph 471b

1. LiAlH4 2. H2, Pd(OH)2/C

O

H CH3

N HH

NHPh

472

Scheme 101.

cleavage of benzoyl ester101 (Scheme 101). Compound 471a was subjected to hydrogenation, followed by alkaline hydrolytic cleavage to get 471b which on reduction afforded diamine 472. Zampella et al.102 discovered amphiasterins; a new family of cytotoxic metabolites from the marine sponge plakortis quasiamphiaster, which is N-alkylated pyroglutamic acid unit (Scheme 102). Bourry et al.103 carried out studies on pyrrolidones. They described an improved synthesis of N-arylmethyl pyroglutamic acids (Scheme 103). They have also carried out studies on pyrrolidinones with an objective to improve the anticancer properties of methyl N-(3,4,40 ,5-tetramethoxybenzhydryl)pyroglutamate (HEI 81)104 (Scheme 104). In our recent publication we described the synthesis of N-[30 (acetylthio) alkanoyl] and N-[30 -mercaptoalkanoyl]-4-a-(S)-(phe-

O

COOCH3

N

OH

OH (CH)m O

O

(CH)n

(CH)m O

473a

O

(CH)n

473b Scheme 102.

nyl methyl) pyroglutamic acids and proline as potent ACE inhibitors. Lithium enolate-derived N-acylation of 4-a(S)-phenylmethyl pyroglutamate 478 with 3-acetylthioalkanoyl chloride and 3-acet-

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O

N H 111

COOCH3

O

ArCH2Cl

NaH

N- + COOCH3 Na 474a

O

O

COOCH3

N

N

COOH O

O

O

O 474b

O

O

475

Scheme 103.

OSiMe3 O

O O

+ COOMe

N

H -O(SiMe3)2

O O

SiMe3

COOMe

N

+

O O O

O

476a

O

476b

477 Scheme 104.

Ph

Ph O

N H 478

COOtBu

LiHMDS, −78 oC

O

CH3COSCH2CH(R)COCl

TFA/anisole

COOtBu O

N O

S R R=H, Me 479

Ph

Ph

O

N O R R=H, Me 480a

DCHA/Et2O COOH O EtOAc/1M HCl S

Ph

O

N O

COO- DCHA O S R R=H, Me 480b

2 M H2SO4

O

N

COOH

O R R=H, Me 481

SH

Scheme 105.

ylthio-2(S)-methyl alkanoyl chloride afforded compound 479. Subsequent deprotection and puriﬁcation yielded the desired ACE inhibitors 481105 (Scheme 105). Hanessian et al.106 reported the N-acyloxyiminium ion azaPrins route to octahydroindoles leading to total synthesis and structural conﬁrmation of the antithrombolic marine natural product oscillarin (Scheme 106). Pyroglutamic acid derivative 482 after Boc deprotection was subjected to N-acylation using 483 as an acylating agent to get 484. The resultant material was converted to precursor 486 by coupling with proline derivative 485, compound 486 on deprotection under acidic condition afforded oscillarin 487. They have also described the total synthesis and structural assignment of the marine natural product Dysinosin A: a novel inhibitor of thrombin and Factor vlla107a (Scheme 107), utilizing a carbon construct strategy that generates subunits originating from L-glutamic acid, whereas Carroll et al. reported the isolation and structure determination of this new marine natural product Dysinosin A.107b Daiya et al.108 described diastereoselective heterogeneous catalysis of 2-methyl nicotinic acid 496 using pyroglutamic as chiral auxiliary (Scheme 108). Methyl pyroglutamate 111 on reaction with 2-methyl-nicotinoyl chloride (generated in situ by reaction of 2-methyl nicotinic acid 494 with thionyl chloride) under Schautann Baumann conditions afforded N-acylated pyroglutamate 495

having side chain corresponding to 2-methyl nicotinic acid, which on catalytic hydrogenation afforded N-(Z-methyl piperidine-3-oyl) methyl pyroglutamate 496 with reduction of N-acyl side chain. Lee et al.109 carried out asymmetric synthesis of trans-1-aminoindolo[2,3-a]quinolizidine 502. N-Benzyloxy carbonyl 2(S)-methyl pyroglutamate 497 on reaction with arylethylamine in the presence of Me3Al underwent ring opening. The resultant product on subsequent reduction afforded 499, which upon dehydration coupled with cyclization gave a tricyclic compound 500. Compound 500 on hydrogenation using H2/Pd–C followed by reduction afforded the desired molecule 502 (Scheme 109). Belvisi et al. reported110 stereoselective synthesis of conformationally constrained unnatural proline-based amino acids and peptidomimetics, N-Boc 4-allyl pyroglutamate derivative 503 was subjected to reduction, allylation sequence on lactam carbonyl thereby furnishing stereoisomers 505 and 506 which on treatment with Grubb’s catalyst, followed by hydrogenolysis gave 508 and 510 as stereoisomers (Scheme 110). Stereoselective alkylation of a bicyclic lactam derived from pyroglutamic acid has been reported by Zhang et al.111 (Scheme 111). Zhang et al.112 described a convenient and versatile synthesis of 6,5- and 7,5-fused lactams as peptidomimetics starting with pyroglutamate derivatives (Scheme 112). N-Boc-2(S)-ethyl pyroglutamate 131 was converted to its corresponding 4-cinnamyl

1615

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

H 1. TFA, CH 2Cl2 then EDC HOBt, CH2Cl2

H

MOMO AcO H

PhH N

COOMe

N

MOMO

Boc

H Ph

Ph O 2. NaOMe/ MeOH 3. MOMCl,iPr2NEt, CH2Cl2

482

O

COOH 483

NH O

O H N aq.HCl/THF. 6M HO

N Boc

N

N

H

N

O

Ph

NHBoc 485

H O H N

H

Boc N

Ph MOMO 484

H

MOMO

1. LiOH, H2O/THF 2. EDC, HOBt, Et3N NH2 HCl COOMe N

COOMe

N

N

O

NHBoc

NH2

HN

Ph

NH

NH

O

O Ph

Ph

MOMO

HO

486

Oscillarin

487 Scheme 106.

MOMO OMe

MOMO H + H

H N

RO

H BopCl

COOH

(i-Pr2) NEt MeCN

O HN COOMe

488

NH2

MOMO

MOMO

H

N COOMe

MeO

TBDPSO

N

O

NH

489

+ N

Boc

490

O

NHBoc

491 HO

MOMO HO

MOMO

H

H

1. LiOH, H2O/THF H

2. EDC, HOBt, Et3N MeO NH RO

N O

1. TBAF, THF

2. Py-SO3, Bu2SnO, CH2Cl2 CO 3. TFA, CH 2Cl2

H

CO MeO NH

HN HO3SO

O

N O

HN

O dysinosin A

N

N

492 BocHN

493

NBoc

H2N

NH

Scheme 107.

COOH O

+ O

N H 111

COOMe

N

1. SOCl2 CH3 494

N

COOMe O

2. NEt3,CHCl3 reflux N 495

CH3

O

COOMe

N

H2(cat.)

O N H

CH3 496

Scheme 108.

derivative 515, which after deprotection of Boc group followed by Lienolate-derived N-acylation with Boc (D)-ser-Bzl-Osu afforded

compound 517. Compound 517 on hydrogenolysis using H2/Pd–C was converted to N-acylated products 518 with deprotection of

1616

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O O

arylethylamine N

COOMe

Ar

Cbz

O H MeO

497

498

Me3Al, CH2Cl2

DIBALH

N H

N

THF

H2, Pd/C N

O

500

499

N

O

H

N

N HH H2N

THF, −78 oC

H H2N

H

CH2Cl2, −78 oC

CbzHN

LiAlH4-AlCl3

Ar

MeOH

H CbzHN

O

HO

NHCbz

Ar

BF3.Et2O

Ar

H 502

H 501 Scheme 109.

H

H

H LiEt3BH, THF O

o COOMe −78 C

N

HO

N

COOMe

Boc

Boc

Boc 503

505

504

H

H H2/Pd/C

Grubb's cat.

505

CH2Cl2

EtOH

N

H

COOMe

N

H

508

507

H

H

H H2/Pd/C

Grubb's cat. N

COOMe

COOMe

Boc

Boc

H

+ 506 COOMe

N

H

CH2Cl2 H

Boc

N

COOMe

EtOH H

Boc

506

N

COOMe

Boc 510

509 Scheme 110.

O

Ph N

H 511

O

O 1. Base 2. RX

R

Ph N

O

O +

N

R

H

H

512

R

Ph

513

O

HOOC

N Boc

R= CH2CH=CH2 514

Scheme 111.

o-benzyl group of side chain. Compound 518 on the reduction of lactam carbonyl with LiBEt3H followed by acid-catalyzed dehydration cyclization sequences gave 520. Compound 520 upon alkaline hydrolysis afforded the desired peptidomimetics 521. An expedient synthesis of (+)-trans-5-allyl hexahydroindolizidin-3-one was carried out by Potts et al.113 (Scheme 113). Thanh et al. reported114 enantioselective synthesis of indolizidine ()-237A [(3R,5S,8aR)-3-butyl-5-(1-oxopropyl)octahydroindolizine], starting from pyroglutamate derivative. Compound 524 on nucleophilic addition with (CH3O)2PO–CH2CO–C(OEt2)Et produced 525 which after hydrogenation with H2 (1 bar), PtO2 in methanol followed by cyclization gave 527 and the resultant material was reduced with NaBH3CN to afford a stereoisomer of ()Myrmicarine 237A (Scheme 114).

Legrand et al. reported115 studies on condensation of pyrrolidinones with silyl derivatives. Trimethoxyphenyl naphthylcarbinol trimethyl silyl ether was condensed with the methyl N-trimethylsilyl pyroglutamate affording two separable esters (Scheme 115). 3.3. Functionalization at C-2, C-3, C-4, of pyroglutamates Yamada et al. established116 an efﬁcient asymmetric synthesis of the functionalized pyroglutamate core unit common to oxazolomycin and neooxazolomycin (Scheme 116). Pyroglutamic acid derivative 533 on protection of carboxylic group as t-butyl ester and subsequent N-methylation afforded 534. Compound 534 on debenzylation at C-3 followed by carboxymethylation of resultant alcoholic functionality delivered a carbonate 535. The quarterniza-

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

Ph

O

LiHMDS, THF Cinnamyl Bromide −78 oC

COOEt

N Boc

Ph

O

COOEt

N

O

N H

Boc

516

515

319 Ph

Ph

H2/Pd/C O

COOEt

N

O

MeOH

Ph

LiBEt3H COOEt THF, −78 oC

N

O BnO

LIHMDS, THF −30 oC Boc(D)-Ser COOEt (Bzl)-OSu

TFA, CH 2Cl2

TFA(Cat), CH 2Cl2 HO

COOEt

N

O HO

NHBoc

O HO

NHBoc

517

519

518

O

H

Ph

O LiOH, H2O/THF

N

BocHN

H

Ph

N

BocHN

COOEt

O

NHBoc

COOH

O 521

520 Scheme 112.

O

COOEt

thesized core unit 540 could be a useful scaffold for stereoselective functionalization corresponding to the oxazolomycin’s polyene segments. Panday et al. have reported117 the simple pathway for the synthesis of ()-bulgecinine (Scheme 117) starting with pyroglutamate derivative. Bicyclic lactam derivative 541 was converted to 6-a-hydroxy substituted product 543 via epoxidation and ringopening sequences. OH group at C-6 was protected prior to hydrolysis of bicyclic ring to get 4-benzyloxy pyroglutaminol, in which OH group at C-5 was also protected with ethyl vinyl ether in the presence of acid catalyst to get 546 followed by protection of free

H t

BuOK

N H 522

O

N

EtOOC 523 Scheme 113.

tion of C-2 followed by the introduction of exomethylene group at C-3 was carried out by internal nucleophilic trap of the carbonate 535 and lactone opening with the phenylselenide anion. The syn-

O

nBu

(CH3O)2PO-CH2-CO-C(OEt)2-Et

N Cbz

OEt OEt

KHMDS THF, 0 oC

CHO

nBu

N Cbz

524

525

1. H2(1bar), PtO2, MeOH, RT

nBu

1. TFA-H 2O nBu

N H

2.H2(1bar),Pt/C, MeOH, RT

526

O (OEt)2

nBu

N

+

O (+)-myrmicarine 237B 529

528 Scheme 114.

HCl (1eq.) O

nBu

N

O (−)-myrmicarine 237A

NaBH3CN

N

K2CHO3 527

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

OSiMe3 O

COOMe

N

O

H+, 130 oC

+ Ph

SiMe3 530

COOMe

N

O

COOMe

N

-Me3SiOSiMe3

531

R'

R''

R''

R' 532b

532a Scheme 115.

OBn O

COOH

N H

OBn

i. t-BuOAc 70% HClO4

1. H2, Pd/C, MeOH O

ii. MeI, NaH, THF

N Me

533

OH

O

NaHMDS N Me

2. ClCOOMe, Py

534

OCOOMe O

COOtBu

O

COOtBu

O + COOtBu

N Me 536

535

O

N Me

COOH

i. Ph2Se2 NaBH4, EtOH

COOtBu

ii. CH2N2

537

CH2N2

SePh O

N Me

COOMe

H2O2

COOtBu

THF

COOMe O

538

Zn(BH4)2 Et2O

COOtBu

N Me

OH O

COOtBu

N Me 540

539 Scheme 116.

OH

O

O

SmI2

t-BuOOH K2CO3-n-Bu4NF DMF

N O

O

N

THF-MeOH

542

544 OCOPh

OCOPh OEt

CH2=CHOEt

OH

O

H+

OCHMe

N H

OEt

(Boc)2O DMAP

O

N Boc

OCOPh

OCOPh OEt OCHMe N

MeOH,

H+ MeO

Boc 548

OCHMe

547

546

545

DIBAL-H Hexane-THF HO

Ph 543

OCOPh

N H

O

Ph

541

O

N

O

Ph

CF3COOH

PhCOCl CH2Cl2-Et3N O

N

O

Ph

THF-H2O

O

OCOPh

OH

N H 549

OCOPh Me3SiCN SnCl4 NC CH2Cl2

N H 550

OH

OH HCl HOOC

OH N H (−)-bulgecinine 551

Scheme 117.

NH to N-Boc. Compound 547 was subjected to reduction of lactam carbonyl with DIBAL-H to get 548. Treatment of 548 with MeOH/ HCl led to the protection of OH group at C-2 as OMe and deprotection at C-5. The resultant product 549 on the introduction of cyano group at C-2 followed by acidic hydrolysis afforded ()-bulgecinine.

Lenda et al. reported118 synthetic strategies for new tetrazole and triazole substituted pyroglutamic acid and proline derivatives (Scheme 118). Dimethyl-2,4-dibromoglutarate 552a was allowed to react with sodium azide, where mono-substituted derivative 552b was obtained as a major product. 1,3-dipolar addition of azide 552b with acetylene afforded 1,2,3-triazole derivative 553a. The

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

Br

Br

MeOOC

Br

NaN3 acetone

COOMe

N3

MeOOC 552b

552a

N Br N

N

MeOOC

COOMe

COOMe

NaN3 acetone

N3 N

N

COOMe

N

COOMe

COOMe

COOMe

553b COOMe

N N

COOMe

O

N

COOH

N

COOH

N

i. BH3·THF

N

N H

Pd/C, MeOH

MeOOC

553a

HOOC

acetylene COOMe

ii. 6M HCl propylene oxide, CH2Cl2 N H

HOOC

554

555 Scheme 118.

triazole derivative was subsequently reacted with 3 equiv of sodium azide to give 553b. Compound 553b on hydrogenation furnished the corresponding substituted pyroglutamic acid 554 via an intramolecular aminolysis. Lactam 554 on selective reduction with BH3 in THF followed by acid hydrolysis and subsequent neutralization with propylene oxide yielded fully deprotected (±)-4(4,5-substituted-1H-1,2,3-triazol-1-yl) proline derivative 555. In an attempt to carry out total synthesis of novel amino acid antibiotic TAN-950, Tsubotani et al. have made asymmetric use119 of (S)-pyroglutamate without prior modiﬁcation through functionalization at C-4 (Scheme 119). Later on in their studies on the reactivity of pyroglutamates towards the asymmetric synthesis of 4-substituted pyroglutamates, Baldwin et al. reported120 that reactions of lithium enolate-derived from 2(S)-pyroglutamates with various electrophiles, give exclusively 4-a-substituted products (Scheme 120). Subsequently in our continuing studies121 on the behaviour of protected pyroglutamate towards electrophiles we reported detailed studies on chiral alkylation and aldol reaction at C-4 of pyroglutamates through their lithium enolates (Scheme 121) where alkylation at C-4 gave exclusively 4-a-products, whereas aldol reactions afforded 4-a- and 4-b-substituted aldol adducts 566 and 567 in the ratio of 4:1. We have also explored122 the direct synthetic pathway for 4(S)-substituted pyroglutamate through 1,3-dipolar addition of

R

O

N

2. Electrophile

N Boc

COOMe

560

N

N

COOMe

Dioxane/H2O

556

O

N

557 COOH

1. NaOH 2. CF3COOH

HO

Boc

Boc

131

COOtBu

menthylacrylate with amino acid Schiff’s bases followed by hydrogenolytic sequences (Scheme 122). These 4-substituted pyroglutamate and prolinates are part of many of the bioactive molecules. As a part of their work on the synthesis of nonproteinogenic amino acids, Bowler et al. reported123 reactions of lactam enolates of L-pyroglutamic acid derivatives with various electrophilic imines and found that the reaction proceeds in good yield with complete stereospeciﬁcity at C-4 and impressive stereo selectivity at the third asymmetric centre (Scheme 123). Young et al.124 reported double stereo differentiation in aldol reaction of pyroglutamic urethane esters 576 (Scheme 124) and the same authors reported the use of acid and aldehyde of pyroglutamate in ring switching reaction leading to lactone 580 as kinetic products125 (Scheme 125). The 4-substituted pyroglutamate 577 by ozonolysis was converted to aldehyde, in which aldehydic

H2NOH·HCl O

N

Scheme 120.

1. LDA or LiN(TMS)2/THF 2. i-PrOCHO

O

Boc

Boc 559

OHC O

1. LDA or LiHMDS

COOtBu

NH2 HN O TAN-950 558 Scheme 119.

O

COOMe

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

OH

OH

R'

O

O

E

N Z 561

R'

R'

562

1. LiHMDS, THF, −78 oC

E O abs MeOH, 50psi

N H 564

+

2. R'CHO, THF, −78 oC

H2, 10%Pd,C

H2, 10%Pd,C E abs EtOAc O

N Z

N H

E

566

H2, 10%Pd,C abs MeOH, 50psi

OH

OH

R'

R'

R'

O

H2, 10%Pd,C E abs EtOAc O

N Z

H2, 10%Pd,C E

N H

abs MeOH, 50psi

O

N H

565

563

E

567

Scheme 121.

O

O

O

R'

O

568 +

LiBr/ TMEDA

R''

THF

R'

R'-CH=N-CH-COOMe

O

COOMe N H 571

Ph H

H Tos NH

COOMe

N H

570

R''

R''

H2/Pd-C

569

TMEDA= N,N,N',N'-tetra methyl ethylene diamine Scheme 122.

Tos

H N

H Ph

H

+

1. Lactam enolate O

N

2. LiHMDS

COOBzl

O

572

N

COOBzl

N

H

Ph

Boc

Ts

O

N

Boc

Boc

573

574

COOBzl

Scheme 123.

H

Ph N O

N

Ph

Tos

H

NH

H Ts

COOCH2Ph O

Boc 575

COOCH2Ph

N Boc 576

Scheme 124.

group on reduction was converted to alcohol 579 to get ring switched lactone 580. Diastereoselective formation of a quaternary centre in pyroglutamate derivative was reported by Oliveira et al.126 (Scheme 126). Lithium enolate-derived alkylation of pyroglutamic acid derivative 581 with N-Boc-bromomethylindole 582 in the presence of DMPU, furnished intermediate 583, where lactam part of 583 on alkaline hydrolysis with LiOH gave 584 which after deprotection afforded ()-monatin 586.

O

OH H

H 1. O3-CH2Cl2, -78oC

O

N

COOtBu

2. Ph3P

O

N

H

H NaBH3CN COOtBu MeOH

O

N

Boc

Boc

Boc

577

578

579 Scheme 125.

H COOtBu

O 580

COOtBu NHBoc O

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

1. LiHMDS, THF, −78 oC 2. DMPU, −78 oC

CBzO

OCBz

OTBS O

OTBS

N

Br , −78 oC

3.

Boc

N Boc

581

O

N

N

LiOH, THF H2O

Boc

Boc 583

582

COOH

OTBS Jones' reagent, 0 oC NHBoc OH HOOC acetone

NHBoc HOOC OH

N

N

Boc

Boc 585

584 COOH NH2 HOOC OH N H (−)-Monatin 586 Scheme 126.

N(CH3)2 H

H

O

H

COOR

N

HN

OHC

H O

N

COOR

H

COOR

O

HN O 2 (Willardiine) 590

COOR

588

587

HN

COOR

N

COOR

H

O

589

COOH

Scheme 127.

novel dehydroﬂuorination (Scheme 128). Substrate 591 on reaction with triethylamine in CH2Cl2 was converted to compound 592b, along with compound 592a, in which compound 592b after catalytic hydrogenation using Pd–BaSO4 in ethanol afforded 593a

Dinsmore et al. reported the extension of ring switching strategy to the glutamate antagonist 2-(pyrimidin-2,4-dione-5-ylmethyl)-(2S)-glycine 590127 (Scheme 127). Qiu et al.128 carried out the synthesis of 4-monoﬂuoromethylenyl 594 and cis-monoﬂuoromethyl-L-pyroglutamic acid 595 via a

H F2HC

F2HC

F

Et3N, CH2Cl2 O

COOtBu

N

O

Boc 591

N

Boc

Boc

592a

592b

COOtBu

TFA CH2Cl2

H F

Pd-BaSO4 EtOH

O

FH2C

H3C 592b

+ COOtBu

N

+ O

COOtBu

N

O

COO

N

Boc

Boc

593a

593b

tBu

O

594

FH2C 593b

TFA CH2Cl2

O

N H

N H 595

Scheme 128.

COOH

COOH

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

Cl

Cl

O

HO

O

COOMe

N

PPh3, DEAD, THF, −0 oC

O

COOMe

N

2. Ac 2O Pyridine

RO

COOMe

N

Boc

Boc R= Ac

597

598

Boc 596

O

1.LiBEt3H THF, −78 oC

4-chloro-1-naphthol

Cl

O TMSCN,BF3.Et2O NC

CH2Cl2, −60 oC

COOMe

N Boc 599

Scheme 129.

Stevens et al.130 reported the regioselectivity in the alkylation of pyroglutamates (Scheme 130). N-Boc benzyl pyroglutamate was converted to its 4-carboxylate 601 using Li enolate chemistry, which on further generating lithium enolate at position C-2 and subsequent reaction with electrophiles afforded 604. In the same way [1,2] Boc migration during pyroglutamate alkylations has also been reported by the same group131 (Scheme 131). Kotoh et al.132 carried out stereoselective synthesis of Nuphor quinolizidine alkaloid ()-deoxynupharidines 618–619 (Scheme

and 593b and subsequently 593b on hydrolysis using TFA gave the desired compound 595. Zhang et al.129 carried out the synthesis of N-Boc-4-O-substituted-5-cynomethyl pyroglutamate 599 (Scheme 129). 4-Hydroxypyroglutamate derivative 596 on Mitsunobu reaction with 4choro-1-nepthol afforded 597, which after reduction at C-5 using LiBEt3H, followed by induction of cyano group at C-5 on reaction with TMSCN and BF3Et2O gave the desired target molecule 599.

OR' R'OOC

O

2 eq. LiHMDS/ −78 oC O

COOBn

N Boc

ClCOOR1

3 eq. −78 oC, THF

3eq. LiHMDS, THF O

COOBn

N

Li+ O-

−78 C o

Boc R= Me 601

600

N

COOBn

Boc 602

OR' R'OOC

O Li

+

O-

(-)Li+ COOBn

N Boc

1. 3 eq. RX/ −78 oC

R O

2. H2O/NH4OH NH4Cl(sat)

N

COOBn

Boc R= CH2Cl, Et, Allyl 604

603 Scheme 130.

E EX O

N

COOR

E

OLi+

N

COOR OtBu

O

LiHMDS EX

O

R' 608

607 Scheme 131.

N

COOR

LiHMDS EX

O

N

R' R'= Boc

R'

605

606

COOR

1623

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

132). Compound 609 on reaction with LiBEt3H, followed by witting reaction gave amide 611, where amidic part was transformed into aldehydic ester 612 by using DIBAL and subsequently resultant aldehyde 612 on acidic hydrolysis was converted to 613, which on deamination with SmI2 in THF–HMPA and methanol gave sixmembered ring product 614. N-Alkylation of 614 with 3-bromo2-methyl propane in the presence of NaH provided 615, which on reaction with Grubb’s catalyst was converted to 616. Compound 616 was treated with 3-lithiofuran, subsequently reduced with NaBH4, ﬁnally subjected to hydrogenolysis using Pd(OH)2 thereby affording diastereomers 618 and 619. Merino et al. described133 the diastereoselective approach with an objective to synthesize 4-hydroxy derivatives 623 (Scheme 133). 3-Hydroxy-pyrrolidinone 620 after protection of all the functional groups was converted to 622 which on reaction with H5IO6 and NaH2PO4 gave target molecule 623.

Me

Langlois et al. achieved the total synthesis of salinosporamideA, a potent proteasome inhibitor, starting from pyroglutamate derivative134 (Scheme 134). Compound 624 was converted to 625 on reaction with N-methylnitrone in toluene through 1,3-dipolar addition and resulting adduct 625 was subjected to hydrogenolysis leading to ring opening, methylation of amino group and subsequently cope elimination to afford salinosporamide-A 628. Hill et al. synthesized135 stereocontrolled spirocyclic bislactams derived from pyroglutamic acid, compound 629 on reaction with NaH and BrCH2CN afforded 630 which on treatment with NaBH4 and COCl2 underwent reduction coupled with cyclization to give spirobicyclic lactams 631 and 632 (Scheme 135). Herdeis et al.136 carried out a stereoselective synthesis of 3substituted (S)-pyroglutamic acid and glutamic acids through ABO ester derivatives (Scheme 136). Pyroglutamic acid was converted to its ester through condensation, which after protection

Me NaH, THF

LiBEt3H, THF O

−78 oC

COOMe

N

HO

(EtO)2P(O)CH2CON(Me)OMe

COOMe

N

Boc

Boc

609

610

Me

Me

O DIBAL, THF

Me COOMe

N

N

OMe

Boc

Me 1. NaHMDS, Ph3PCH3+Br-

OHC

−78 oC

N

COOMe

Boc 612

611

Me HMPA, MeOH 0 oC

N H 614

O

COOMe

N H 613

Me

3-bromo-2methylpropene

SmI2, THF

THF, −78 oC 2. TFA, CH 2Cl2

2 mol% Grubb's cat N

o

NaH, DMF, 20 C

O

Benzene, 60 oC

615 Me

Me H N

O

(a) 3-lithiofuran, THF, −78 oC

Me

H

(b) NaBH4, MeOH

H

H2, Pd(OH)2

N O

N

O

617

616

+ H

N

MeOH, rt

Me (S)-furan

Me

Me

O

Me

Me

618

619

Scheme 132.

OH O O

N H 620

O

OR

OR 1. TBSCl, THF or 2. PhCOCl

(Boc)2O

O O

N H R= tBuMe2Si R= PhCO 621

O

DMAP

H5IO6, then NaClO2

MeOOC

622

N Boc 623

Scheme 133.

N Boc

OBz

NaH2PO4, then CH2N2

O O

O

O

1624

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

N

O

COOMe OBn

COOMe OBn

N-methylnitrone O

toluene, heat

N

R

624

625

EtOAc-MeOH

O

TFA

626

N+

COOMe OBn

O

N H

R= Boc R= H

OH

H2, Pd(OH)2

625

COOMe OBn

SmI2, THF

N

Boc

HN

OH

HN

O

N

I-

OH

MeI, THF

Et3N

COOMe OBn

O

N Boc

Boc 627

OH COOMe OBn

O

N Boc 628

Scheme 134.

17

O

NaH BrCH2CN

N

O

+

O

N

O

O Ph

O

O NaBH4 CoCl2

N

HN

HN

EtOOC CH2CN

EtOOC

Ph

629

O

N O

O Ph

630

Ph 631

632

Scheme 135.

17

3-hydroxymethyl-3 methyl-oxetane DCC, DMAP, CH2Cl2

O

N H 633

BF3.OEt2, CH2Cl2 Et3N,

O

O

0 oC

O

N

1. BuLi/DABCO, CbzCl, −78 o C, THF

N

2. BuLi/HMDS, (Boc)2O, −78 oC

O

CH3

1. Acc: Cbz 2. Acc: Boc 3. Acc: Moc 634

1. BuLi/HMDS, PhSeCl −78 oC, THF 2. mCPBA, DABCO

O

O O O

N Cbz

Acc 635

R

R O

CH3

636

RMgBr, CuBr, S(CH 3)2 −78 oC to −20 oC

O

Acc

3. BuLi/DABCO, CNCOOCH 3 −78 oC, THF

O O O

O

O O

N

O O O

1. H2/Pd/C, EtOAc/MeOH CH3

Cbz 637

2. TFA/H2O/CH2Cl2 3. Cs2CO3/H2O

O

N H

COOH

638 Scheme 136.

of –NH followed by oxidation was converted to ABO ester 635. Formation of epoxide at C-3, 4 of 635 following usual chemistry and subsequent ring opening with Grignard reagent afforded 637. Compound 637 after protection and deprotection sequences afforded the desired 3-substituted pyroglutamate 638.

Cienfuegos et al. reported stereoselective synthesis of conformationally constrained (2S,3S)-3-hydroxyornithine137 (Scheme 137). Cai et al.138 described the application of (S)-and (R)-methyl pyroglutamates as inexpensive, yet highly efﬁcient chiral auxilia-

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

Bn N

BnHN

O

OH

O

LiAlH4 O

O Ph 639

Bn 640

Bn

TFA, THF-H 2O

OH

CH2Cl2

N

N

639

CDI

OH

THF, Heat

N

Bn N

O

N H

O OR LiAlH4

CCl3COOH, CH2Cl2

O

N H

BnAcN

OH OEVE

BnAcN

OAc

Ac2O

OEVE

Py

N H

THF, heat

643

642 BnHN

N H 641

OH ethylvinylether O

O

Bn N

OAc

CH3COOH-H2O

OH

N

N

Ac

Ac

645

644 BnAcN

646 BnHN

OAc

Jones' Reagent

OH

3M HCl

acetone

COOH

N

COOH

N H

Ac 648

647 Scheme 137.

N

O

O

Ni O

N

O

N

R O

N

N

COOMe O

650

N

DBU, DMF R= Me

O Ni

R H O

N

Me

O

649

Me N

COOMe

651

N

R 1. MeOH/HCl 2. NH4OH 3. Dowex

O H

O

N H

+ COOH

652

O

NH

O Me

653 Scheme 138.

ries in the asymmetric Michael addition reactions (Scheme 138). Michael acceptor 650 reacts with Ni(II) complex to give exclusively 651. Compound 651 on treatment with methanoic HCl and subsequently treatment with NH4OH and Dowex yielded 3-substituted pyroglutamic acid 652. Langlois et al.139 reported the stereoselective formal synthesis of the proteasome inhibitor salinosporamide A, from (S)-methyl 2-hydroxymethylpyroglutamate through chemoselective O-protection (Scheme 139). Fujita et al. reported reactions of optically active 5-substituted2-pyrrolidinone derivatives having atropisomeric behaviours. They

carried out 3,5-cis-selective reactions of their enolates with electrophiles140 (Scheme 140). 3.4. Conversion of pyroglutamic acid into prolines Pyroglutamates can readily be converted into prolines. Rapoport et al. converted 4-phenylpyroglutamate 664 to 4-phenyl prolinate 665 by reducing with BH3THF in the presence of a catalytic amount of NaBH4141 (Scheme 141). Pyroglutamates could directly be converted into L-proline in 2step one-pot reaction. The conversion involves the treatment of

1626

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

N COOMe OBn

O

COOMe OBn

Cs2CO3, PMBBr

N H

O

DMF

COOMe OBn +

N-methylnitrone O toluene, heat

N

N

PMB

654 N

OH

HN

EtOAc-MeOH

N

OH

COOMe OBn

H2, Pd(OH)2

COOMe OBn

O

PMB

656

655 O

O

N

1. MeI, MeOH 2. Na2CO3, CH2Cl2

COOMe OBn

O

N

PMB

PMB 657

O

PMB

658

659

Scheme 139.

E E O

N OR2

O

N OR2

R1

660

-

N

E+

OR2

R1

O R1

OR2

662

661

N H

O

663

Scheme 140.

pyroglutamic acid with triethyl oxonium ﬂuoro borate and reduction of the resulting crude imino ether with NaBH4142 (Scheme 142). We have also reported a simple procedure121 for the conversion of 4-substituted pyroglutamates to 4-substituted prolinates 669 via the conversion of pyroglutamate to thio lactam followed by reduction to the corresponding prolinate in the presence of nickel boride generated in situ (Scheme 143). Drauj et al. have converted143 L-pyroglutamate 111 to 5,5-dichloro-N-chloro carbonyl 2(S)-methyl pyroglutamate 670 on reaction with COCl2 in dichloromethane at 0 °C with the elimination of HCl and CO2. Compound 670 on reaction with Bu3N gave 671 with the elimination of HCl at positions 4 and 5 leading to induction of double bond. Compound 671 on hydrogenation using Pd/C with Bu3N gave unsaturated product 672, which on further hydrogenation gave saturated products 673. Compound 673 after several protection and deprotection sequences afforded L-proline (Scheme 144). Harris et al.144 reported the synthesis of cyclic proline containing peptides via ring-closing metathesis (Scheme 145). N-Acyl-5allyl diene 677, which was obtained from pyroglutamic acid was

Ph

Ph BH3·THF O

N

COOtBu

NaBH4

COOtBu

N PhF1

PhF1

665

664 Scheme 141.

O

N H 17

COOH

triethyloxonium fluoroborate NaBH4

N H 666

COOH

Scheme 142.

Ph

Ph

Ph Nickel boride

Lawessons reagent O

N H 667

E

CH2Cl2, rt

S

N H 668

Scheme 143.

E

N H 669

E

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O

COCl2, CH2Cl2

COOMe

N H

0 oC, -HCl, -CO2

H

Bu3N, 70 oC

Cl Cl

COOMe

N O

111

Cl

-Bu3NHCl

O

Cl

H

H

-Bu3NHCl

H2, Pd/C

COOMe

N

Cl 671

670

H2, Pd/C, Bu3N

COOMe

N

COOMe

N

H

H+, H2O -CO2

+ N

COOMe

H O

O

Cl

673

672

H

Cl 674

H H+, H2O -CH3OH

+ N H

COOH

H

Basic ion exchange

COOH

N H

H

675

676 Scheme 144.

COOtBu

N

COOtBu

Grubbs' cat. (20%) CH2Cl2/reflux

O

O N

N

COOBn

COOBn 678

677 Scheme 145.

1. LiHMDS O

O

COOH

N

N

2.

Ph 177

COOH

N

O

COOCH2Ph

N Ph

680

toluene

Raney Ni S

COOCH2Ph

N Ph

681

682

H2, Pd/C (10%)

+ COOH

N

COOCH2Ph

CH3OH, 2h

N H

Ph

Ph 683

Et3N

Ph

Lawesson's reagent

PhCH2Br

N

PhCH2Br O

Ph 679

Br

Et3N

Pd/C (10%) COOH H2

685

684 Scheme 146.

COOH

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

subjected to cyclization in the presence of Grubb’s catalyst to afford the expected cyclononenes 678. Chen et al. reported a convenient method for the synthesis of trans-4-cyclohexyl-L-proline145 (Scheme 146). N-Benzyl pyroglutamic acid was reacted with bromocyclohexene in the presence of LiHMDS, followed by hydrogenolysis with Pd/C to get 4-substituted N-benzyl pyroglutamic acid 680 which was condensed with PhCH2Br to get ester 681. Treatment of 681 with Lawesson’s reagents, followed by reduction with Raney Ni afforded 683 and 684. Both these products were subjected further to hydrogenolysis using H2/Pd–C to get 4-cyclohexyl proline 685. Langlois et al.146 reported diastereoselective syntheses of (2S,3S,4S)-3-hydroxy-4-methylproline 691, a common constituent of several antifungal cyclopeptides (Scheme 147). Compound 686 on reduction using BH3–DMS was converted to 687, resultant material on hydrogenolysis, followed by NH protection was converted to 688. Treatment of 688 with TBDMSCl gave 689 and sub-

OH

sequent reaction with NaIO4–RuCl3 followed by acidic hydrolysis afforded the desired molecule 691. Two separate and distinct syntheses of stereospeciﬁcally deuterated samples of (2S)-proline were reported by Barraclough et al.147 (Scheme 148). Compound 131 on reduction using H3BSMe2, followed by acidic hydrolysis afforded proline 666. Oba et al.148 carried out the synthesis of non-proteinogenic amino acids using Michael addition to unsaturated orthopyroglutamate derivative (Scheme 149). Unsaturated pyroglutamate derivative 166 on reaction with Gilman reagent delivered a compound 693 having methyl group at C-3. The ABO ester functionality of 693 was converted to methyl ester through ester exchange reaction with MeOH/HCl. The N-Boc group of 693 which was deprotected during acidic conditions was protected again with Boc group to afford 694. Reduction of lactam carbonyl of 694 with BH3THF followed by deprotection of methyl ester of 695 in reﬂuxing 1 M. HCl and subsequently ion exchange treatment with DOWEX 50WX8

OH OH 1. H2/Pd/C

BH3-DMS

O

N

N

86%

OH

2. (Boc)2O

Ph

R 686

Boc

R

688

687 OSit-BuMe2

OR2 OR1

NaIO4-RuCl3

Boc

OH 6M HCl + N Cl- H2

COOH

N

CCl4-CH3CN-H2O R1=R2=OSit-BuMe2 R1=H, R2=OSit-BuMe2

N

TBDMSCl

N

O

Ph

O

OH

Boc

689

COOH

691

690 Scheme 147.

H3B·SMe2

(Boc)2O, DMAP O

COOMe

N H 111

CH3CN

131

THF, 0 oC

6M HCl N

COOMe

reflux

N H 666

Boc 692

COOH

Scheme 148.

Me

Me

O

N

ABO

Me2CuLi

O

Boc

N

ABO

HCl, MeOH then

O

(Boc)2O, DMAP

Boc

Boc 693

166

694 Me

Me BH3-THF N

COOMe

1M HCl then Dowex 50WX8

Boc 695

N H 696

Scheme 149.

N

COOH

COOMe

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

1629

OBn

i. LiBEt3H, THF

LiHMDS, BnOCH2Cl O

COOEt

N

O

HMPA, THF

COOEt

N

Boc 319

Boc 697 OR

OR i. MeMgBr, CuBr-Me 2S BF3-OEt2, Et2O MeO

ii. p-TsOH, MeOH

N

COOEt

ii. (Boc)2O, NaHCO3

Jones' reagent Me

N

COOEt

acetone

Boc

Boc

699a, R= Bn H2, Pd/C, MeOH 699b, R= H

698

Me N Me HOOC

O Me2NH, EDC

Me

N

COOEt

L-ProCN, EDC

Me

HOBt, Et3N

COOEt

N

Boc

Boc

700

701a, R= Et NaOH, MeOH 701b, R= OH

Me

Me N Me

N Me

O

O N

Me

HOBt, Et3N

p-TsOH, EtOH

N Me

N Boc

O

CN

702

N H

O CN

703 Scheme 150.

resin furnished (2S,3S)-3-methylene proline 696 in quantitative yield. Kondo et al.149 discovered long acting N-(cyanomethyl)-N-alkyl-L-prolinamide inhibitors of dipeptidyl peptidase IV (Scheme 150) starting with pyroglutamic acid derivative. Lithium enolatederived alkylation of N-protected ethyl-L-pyroglutamate 319 with benzyloxymethyl chloride afforded 4-substituted pyroglutamate 697. Partial reduction of cyclic imide carbonyl of 697, followed by acetalization gave the methyl acetal 698. Stereoselective 5 amethylation of 698 with methyl Grignard reagent and copper(I) bromide-dimethylsulﬁde complex in the presence of boron triﬂuoride-etherate, followed by protection of deprotected nitrogen, led to 699a. Catalytic hydrogenation of 699a provided the alcohol 699b. Jone’s oxidation of 699b resulted in carboxylic acid 700, which on condensation with N,N-dimethyl amine produced 701a. Alkaline hydrolysis of compound 701a provided carboxylic acid 701b, which on peptide formation with (2S)-2-cyanopyrrolidine afforded 702. Acidic deprotection of 702 led to the desired compound 703. Einsiedel et al. developed a molecular building kit of fused-proline derived peptide mimetics allowing speciﬁc adjustment of the dihedral w-angle (Scheme 151). Unsaturated pyroglutamic acid derivative 704 on reaction with allyl bromide in the presence of TMSCl and HMPA, followed by reduction of lactam carbonyl deliv-

ered 706, which after deprotection of alcoholic group furnished prolinol derivative 707. Jones oxidation led to the formation of the C-3 functionalized proline 708. Amide formation between the asymmetric building block 708 and N-substituted glycine derivatives using coupling mixture HATU/HOAt allowed an efﬁcient synthesis of RCM precursor 709. Oleﬁn metathesis using Grubb’s II generation catalyst afforded seven-membered and eight-membered unsaturated bicyclic lactams 710. Aminolysis of 710 with methylamine delivered the model peptides 711.150 4. Conclusions Thus this review gives explicit information about the versatility and importance of pyroglutamate with special attention to asymmetric synthesis of bioactive molecules, natural products as well as chiral intermediates. On the one hand this important moiety has allowed the researchers to synthesize bioactive natural products such as anatoxin A, ()-bulgecinine and salinosporamide A, whereas on the other hand the use of pyroglutamic acid as a chiral precursor has enabled the researchers to explore the synthetic analysis for designed bioactive molecules such as ACE inhibitors like fosinipril, conformationally constrained peptides as well as peptidomimetics. Various derivatives of pyroglutamic acid have also been used to develop catalyst such as semicorrin metal com-

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S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632

O O

Ph tBu Ph

Si

N

O

AllMgBr

O

N

TMSCl, HMPA

Boc

Boc

704

705

O N

Si

Ph tBu Ph

i. LiAlH4, Et2O ii. Et3SiH, BF3.Et2O

H2O, Me2O

N Boc

706

707

COOH

N Boc 708

COOMe

COOMe N H

Ph tBu Ph

OH CrO3, H2SO4

Bu4NF, HOAc

Boc

( )n

Si

( )n

( )n N

COOMe

N

n=1

Grubb's catalyst

HATU, HOBt, NEM, NMP

O

CH2Cl2

N Boc 709

O N Boc 710

NHCH3 ( )n H2NMe, EtOH

N

O

O N Boc 711 Scheme 151.

plexes or 2,5-disubstituted pyrrolidines. Therefore it may be concluded that pyroglutamate has undoubtedly emerged as an important chiral synthon and has provided researchers a useful chiral tool to exploit the reactivity differences within the molecule and to use it for the asymmetric synthesis of wide variety of bioactive compounds. The present review is an attempt to describe the useful and important applications on the use of this unique chiral synthon by the researchers all over the world in the recent past, and shall certainly be valuable, to make further progress and to develop new strategies for the asymmetric synthesis based on these literature reports. Acknowledgements The corresponding author is thankful to the University Grants Commission, New Delhi, India for ﬁnancial assistance and to Central Drug Research Institute, Lucknow, UP, India for extending library facilities to us. References 1. (a) Ohfune, Y.; Tomita, M. J. Am. Chem. Soc. 1982, 104, 3511; (b) Najera, C.; Yus, M. Tetrahedron: Asymmetry 1999, 10, 2245. 2. Thottahil, J. K.; Moniot, J. L.; Mueller, R. H.; Wong, M. K. Y.; Kissick, T. P. J. Org. Chem. 1986, 51, 3140. 3. Langlois, N.; Andriamialisoa, R. Z. Tetrahedron Lett. 1988, 29, 3259. 4. Baldwin, J. E.; Moloney, M. G.; Shim, S. B. Tetrahedron Lett. 1991, 32, 1379. 5. Hamada, Y.; Tanada, Y.; Yokokawa, F.; Shioiri, T. Tetrahedron Lett. 1991, 32, 5983.

6. Langlois, N.; Favre, F. Tetrahedron Lett. 1991, 32, 2233. 7. Woo, K. C.; Jones, K. Tetrahedron Lett. 1991, 32, 6949. 8. Saliou, C.; Fleurant, A.; Celerier, J. P.; Lhommet, G. Tetrahedron Lett. 1991, 32, 3365. 9. Armstrong, R. W.; Demattei, J. A. Tetrahedron Lett. 1991, 32, 5749. 10. Kohn, U.; Schramm, A.; Klob, F.; Gorls, H.; Arnold, E.; Anders, E. Tetrahedron: Asymmetry 2007, 18, 1735. 11. Sengoku, T.; Satoh, Y.; Oshima, M.; Takahashi, M.; Yoda, H. Tetrahedron 2008, 64, 8052. 12. Moeller, K. D.; Rutledge, L. D. J. Org. Chem. 1992, 57, 6360. 13. (a) Magni, A.; Signorelli, G.; Bocchiola, G. Arzneim-Forsch/Drug. Res. 1994, 44, 1402; (b) Crimella, T.; Olandi, R.; Bocchiola, G.; Anders, U.; Stradi, R. ArzneimForsch/Drug. Res. 1994, 44, 1405. 14. Lin, N. H.; He, Y.; Kopecka, R. Tetrahedron Lett. 1995, 36, 2563. 15. Rigo, B.; Erb, B.; Ghammarti, S. E.; Gautret, P. J. Heterocycl. Chem. 1995, 32, 1599. 16. Rigo, B.; Cauliez, P.; Fasseur, D.; Sauvage, F. X. Trends Heterocycl. Chem. 1991, 2, 155. and references cited therein. 17. Nagasaka, T.; Imai, T. Heterocycles 1995, 41, 1927. 18. Dikshit, D. K.; Maheshwari, A.; Panday, S. K. Tetrahedron Lett. 1995, 36, 6131. 19. Ostendorf, M.; Dijkink, J.; Rutjes, F. P. J. T.; Hiemstra, H. Eur. J. Org. Chem. 2000, 1, 115. 20. Acevedo, C. M.; Kogut, E. F.; Lipton, M. A. Tetrahedron 2001, 57, 6353. 21. Marchalin, S.; Szemes, F.; Bar, N.; Decroix, B. Heterocycles 1999, 50, 445. 22. (a) Olson, G.; Cheung, H. C.; Chiang, E.; Madison, V. S.; Sepinwall, J.; Vincent, G. P.; Winokur, A.; Gary, K. A. J. Med. Chem. 1995, 38, 2866; (b) Li, W.; Moeller, K. D. J. Am. Chem. Soc. 1996, 118, 10106. 23. Altman, J.; Ben-Ishai, D. Tetrahedron: Asymmetry 1993, 4, 91. 24. Wei, Z. Y.; Knous, E. E. Synlett 1994, 345. 25. Chaudhury, P. K.; Nguyen, B. K. L.; Langlois, N. Tetrahedron Lett. 2002, 43, 463. 26. Davies, S. G.; Dixon, D. J.; Doisneau, G. J. M.; Prodger, J. C.; Sanganee, H. J. Tetrahedron: Asymmetry 2002, 13, 647. 27. Nguyen, B. K. L.; Langlois, N. Tetrahedron Lett. 2003, 44, 5961. 28. Villeneuve, P.; Barea, B.; Sarrazin, P.; Davrieux, F.; Baulanger, R.; Caro, Y.; Figueroa-Espinoza, M. C.; Pina, M.; Graille, J. Enzyme Microb. Technol. 2003, 33, 79.

S. K. Panday et al. / Tetrahedron: Asymmetry 20 (2009) 1581–1632 29. Langlois, N.; Nguyen, B. K. L. J. Org. Chem. 2004, 69, 7558. 30. Itoh, T.; Nagata, K.; Yokoya, M.; Miyazaki, M.; Ikeda, S.; Matsuya, Y.; Enomoto, Y.; Ohsawa, A. Synlett 2002, 6, 1005. 31. Puschel, A.; Boesen, T.; Zuccarello, G.; Dahl, O.; Pitsch, S.; Nielsen, P. E. J. Org. Chem. 2001, 66, 707. 32. Oba, M.; Nishiyama, N.; Nishiyama, K. Tetrahedron 2005, 61, 8456. 33. Herdies, C.; Kelm, B. Tetrahedron 2003, 59, 217. 34. Dieltiens, N.; Claeys, D. D.; Allaert, B.; Verpoort, F.; Stevens, C. V. Chem. Commun. 2005, 4477. 35. Bourry, A.; Gedu, R. A.; Henichart, J. P.; Sanz, G.; Rigo, B. Tetrahedron Lett. 2004, 45, 2097. 36. (a) Mavromoustakos, T.; Minakakis, P. M.; Kokotos, C. G.; Kontogianni, P.; Politi, A.; Zoumpoulakis, P.; Findlay, J.; Cox, A.; Balmforth, A.; Zoga, A.; Iliodromitis, E. Bioorg. Med. Chem. 2006, 14, 4353; (b) Minakakis, P. M.; Gianni, M.; Stougiannou, H.; Zoumpoulakis, P.; Zoga, A.; Vlahakos, A. D.; Iliodromitis, E.; Mavromoustakos, T. Bioorg. Med. Chem. Lett. 2003, 13, 1737. 37. Beal, L. M.; Liu, B.; Chu, W.; Moeller, K. D. Tetrahedron 2000, 56, 10113. 38. Langlois, N.; Chaudhury, P. K. Tetrahedron Lett. 1999, 40, 2525. 39. Peterson, J. S.; Fels, G.; Rapoport, H. J. Am. Chem. Soc. 1984, 106, 4539. 40. Bachi, M. D.; Breiman, R.; Meshulam, H. J. Org. Chem. 1983, 48, 1439. 41. Fang, F. G.; Prato, M.; Kim, G.; Danishefsky, S. J. Tetrahedron Lett. 1989, 30, 3625. 42. Rosset, S.; Celerier, J. P.; Lhommet, G. Tetrahedron Lett. 1991, 32, 7521. 43. (a) Pfaltz, A. Bull. Soc. Chim. Belg. 1990, 99, 729; (b) Fritschi, H.; Leutenegger, U.; Siegmann, K.; Pfaltz, A.; Keller, W.; Kratky, C. Helv. Chim. Acta 1988, 71, 1541. 44. Singh, R. K.; Jain, S.; Sinha, N.; Mehta, A.; Naqvi, F.; Agarwal, A. K.; Anand, N. Tetrahedron Lett. 2007, 48, 545. 45. Liyanage, W.; Weerasinghe, L.; Srong, R. K.; Valle, J. R. D. J. Org. Chem. 2008, 73, 7420. 46. Shiosaki, K.; Rapoport, H. J. Org. Chem. 1985, 50, 1229. 47. Corey, E. J.; Yuen, P. W.; Hannon, F. J.; Wierda, D. A. J. Org. Chem. 1990, 55, 784. 48. (a) Wistard, L. G.; Skringir, M. Tetrahedron Lett. 1990, 31, 1775; (b) Wistard, L. G.; Skringir, M. Tetrahedron 1991, 47, 573; (c) Thaning, M.; Wistard, L. G. Acta Chem. Scand. 1992, 46, 14. 49. Agarwal, V. K.; Astle, C. J.; Evans, M. R. Org. Lett. 2004, 6, 1469. 50. Agarwal, V. K.; Astle, C. J.; Iding, H.; Werz, B.; Evans, M. R. Tetrahedron Lett. 2005, 46, 945. 51. Mandal, P. K.; Kaluarachchi, K. K.; Ogrin, D.; Bott, S. G.; McMurray, J. S. J. Org. Chem. 2005, 70, 10128. 52. Hanessian, S.; Tremblay, M.; Marzi, M.; Del Valle, J. R. J. Org. Chem. 2005, 70, 5070. 53. Conchon, E.; Mialhe, Y. G.; Ramuson, R. Tetrahedron: Asymmetry 2006, 17, 1253. 54. Peng, Y.; Sun, H.; Wang, S. Tetrahedron Lett. 2006, 47, 4769. 55. Angiolini, M.; Araneo, S.; Belvisi, L.; Cesarotti, E.; Checchia, A.; Crippa, L.; Manzoni, L.; Scolastico, C. Eur. J. Org. Chem. 2000, 14, 2571. 56. Ghammarti, S. E.; Rigo, B.; Mejdi, H.; Henichart, J.-P.; Couturier, D. J. Heterocycl. Chem. 2000, 37, 143. 57. (a) Endo, A.; Danishefsky, S. J. J. Am. Chem. Soc. 2005, 127, 8298; (b) Reddy, L. R.; Saravanan, P.; Corey, E. J. J. Am. Chem. Soc. 2004, 126, 6230. 58. Manzoni, L.; Colombo, M.; May, E.; Scolastico, C. Tetrahedron 2001, 57, 249. 59. Mulzer, J.; Schulzchen, F.; Bats, J.-W. Tetrahedron 2000, 56, 4289. 60. Hussaini, S. R.; Moloney, M. G. Tetrahedron Lett. 2004, 45, 1125. 61. Hussaini, S. R.; Moloney, M. G. Org. Biomol. Chem. 2006, 4, 2600. 62. Moloney, M. G.; Panchal, T.; Pike, R. Org. Biomol. Chem. 2006, 4, 3894. 63. (a) Chan, P. W. H.; Cottrell, I. F.; Moloney, M. G. J. Chem. Soc., Perkin Trans. 1 2001, 2997; (b) Bailey, J. H.; Cherry, D. T.; Dyer, J.; Moloney, M. G.; Bamford, M. J.; Keeling, S.; Lamont, R. B. J. Chem. Soc., Perkin Trans. 1 2000, 2783; (c) Dyer, J.; Keeling, S.; King, A.; Moloney, M. G. J. Chem. Soc., Perkin Trans. 1 2000, 2793. 64. Chan, P. W. H.; Cottrell, I. F.; Moloney, M. G. J. Chem. Soc., Perkin Trans. 1 2001, 3007. 65. Hara, O.; Takizawa, J.-I.; Yamatake, T.; Makino, K.; Hamada, Y. Tetrahedron Lett. 1999, 40, 7787. 66. Bailey, J. H.; Byﬁeld, A. T. J.; Davis, P. J.; Foster, A. C.; Leach, M.; Moloney, M. G.; Muller, M.; Prout, C. K. J. Chem. Soc., Perkin Trans. 1 2000, 1977. 67. Colombo, L.; Di Giacomo, M.; Vinci, V.; Colombo, M.; Manzoni, L.; Scolastico, C. Tetrahedron 2003, 59, 4501. 68. Hanessian, S.; Gauchet, C.; Charron, G.; Marin, I.; Nakache, P. J. Org. Chem. 2006, 71, 2760. 69. Brana, M. F.; Garranzo, M.; Terera, B. D. P.; Castells, J.-P.; Torres, M. R. Tetrahedron 2002, 58, 4825. 70. Harris, P. W. R.; Brimble, M. A. Org. Biomol. Chem. 2006, 4, 2696. 71. Langlois, N.; Nguyen, B. K. L.; Retailleau, P.; Tarnus, C.; Salomon, E. Tetrahedron: Asymmetry 2006, 17, 53. 72. Deyine, A.; Delcroix, J. M.; Langlois, N. Heterocycles 2004, 64, 207. 73. Davies, D. E.; Doyle, P. M.; Farrant, R. D.; Hill, R. D.; Hitchcock, P. B.; Sanderson, P. N.; Young, D. W. Tetrahedron Lett. 2003, 44, 8887. 74. Gedu, R. A.; Bourry, A.; Camus, F.; Norberg, B.; Durant, F.; Coulurier, D.; Baker, M. D.; Rigo, B. Heterocycles 2004, 8, 1855. 75. Olivo, H. F.; Miranda, R. T.; Barragan, E. J. Org. Chem. 2006, 71, 3287. 76. Manzoni, L.; Belvisi, L.; Colombo, M.; Carlo, E. D.; Forni, A.; Scolastico, C. Tetrahedron Lett. 2004, 45, 6311. 77. Bracci, A.; Manzoni, L.; Scolastico, C. Synthesis 2003, 15, 2363.

1631

78. Katritzky, A. R.; Angrish, P.; Todadze, E.; Ghiviriga, I. Bioorg. Med. Chem. Lett. 2007, 17, 6000. 79. Toyooka, N.; Zhou, D.; Nemoto, H.; Tezuka, Y.; Kadota, S.; Jones, T. H.; Garraffo, H. M.; Spande, T. F.; Daly, J. W. Synlett 2008, 12, 1894. 80. Li, J.; Chen, S. Y.; Murphy, B. J.; Flynn, N.; Seethala, R.; Slusarchyk, D.; Yan, M.; Sleph, P.; Zhang, H.; Humphreys, W. G.; Ewing, W. R.; Robl, J. A.; Gordon, D.; Tino, J. A. Bioorg. Med. Chem. Lett. 2008, 18, 4072. 81. Gu, Z. Q.; Li, M. Tetrahedron Lett. 2003, 44, 3203. 82. Dieterich, P.; Young, D. W. Org. Biomol. Chem. 2006, 4, 1492. 83. Dinsmore, A.; Doyle, P. M.; Young, D. W. J. Chem. Soc., Perkin Trans. 1 2002, 155. 84. (a) Langlois, N. Tetrahedron Lett. 2001, 42, 5709; (b) Langlois, N.; Calvez, O. Tetrahedron Lett. 2000, 41, 8285. 85. Mota, A. J.; Langlois, N. Tetrahedron Lett. 2003, 44, 1141. 86. Mota, A. J.; Chiaroni, A.; Langlois, N. Eur. J. Org. Chem. 2003, 21, 4187. 87. Oba, M.; Nishiyama, N.; Nishiyama, K. Chem. Commun. 2003, 776. 88. Hjelmgaard, T.; Tanner, D. Org. Biomol. Chem. 2006, 4, 1796. 89. Makino, K.; Shintani, K.; Yamatake, T.; Hara, O.; Hatano, K.; Hamada, Y. Tetrahedron 2002, 58, 9737. 90. Cohen, J. L.; Chamberlin, A. R. J. Org. Chem. 2007, 72, 9240. 91. Ikota, N. Chem. Pharm. Bull. 1989, 37, 2219. and references cited therein. 92. Menezes, R. F.; Zezza, C. A.; Shiu, J.; Smith, M. B. Tetrahedron Lett. 1989, 30, 3295. 93. Defoin, A.; Pires, J.; Streith, J. Synlett 1991, 417. 94. Kothen, P. F. K.; Smith, M. B. Tetrahedron Lett. 1989, 30, 3369. 95. Boisse, T.; Gavara, L.; Henichart, J.-P.; Rigo, B.; Gautret, P. Tetrahedron 2009, 65, 2455. 96. (a) Imaki, K.; Sakuyama, S.; Okada, T.; Tada, M.; Hayasi, M.; Miyamoto, T.; Kawasaki, A.; Okegawa, T. Chem. Pharm. Bull. 1981, 29, 2210; (b) Jonnson, A. L.; Price, W. A.; Wong, P. C.; Vavala, R. F.; Stump, J. M. J. Med. Chem. 1985, 28, 1596. 97. Hanessian, S.; Tremblay, M. Org. Lett. 2004, 6, 4683. 98. Stevens, C. V.; Dieltiens, N.; Claeys, D. D. Org. Lett. 2005, 7, 1117. 99. Bourry, A.; Couturier, D.; Sanz, G.; Hijfte, L. V.; Henichart, J.-P.; Rigo, B. Tetrahedron 2006, 62, 4400. 100. Enders, D.; Han, J. Tetrahedron: Asymmetry 2008, 19, 1367. 101. Dudot, B.; Chiaroni, A.; Royer, J. Tetrahedron Lett. 2000, 41, 6355. 102. Zampella, A.; Giannini, C.; Debitus, C.; Valeria, M.; Auria, D. Tetrahedron 2001, 57, 257. 103. Bourry, A.; Akue-Gedu, R.; Rigo, B.; Henichart, J.-P.; Sanz, G.; Couturier, D. J. Heterocycl. Chem. 2003, 40, 989. 104. Bourry, A.; Rigo, B.; Sanz, G.; Couturier, D. J. Heterocycl. Chem. 2002, 39, 119. 105. Panday, S. K.; Dikshit, M.; Dikshit, D. K. Med. Chem. Res., doi:10.1007/s00044008-9150z. 106. Hanessian, S.; Tremblay, M.; Peterson, J. F. W. J. Am. Chem. Soc. 2004, 126, 6064. 107. (a) Hanession, S.; Margarito, R.; Hall, A.; Johnstone, S.; Tremblay, M.; Parlanti, L. J. Am. Chem. Soc. 2002, 124, 13342; (b) Carroll, A. R.; Pierens, G. K.; Fechner, G.; Almeida, P. D.; Ngo, A.; Simpson, M.; John, E. H.; Hooper, N. A.; Bostrom, S.L.; Musil, D.; Quinn, R. J. J. Am. Chem. Soc. 2002, 124, 13340. 108. Daiya, N.; Malacea, R.; Banceu, M.; Besson, M.; Pinel, C. Tetrahedron Lett. 2003, 44, 6991. 109. Lee, Y. S.; Cho, D. J.; Kim, S. N.; Choi, J. H.; Park, H. J. Org. Chem. 1999, 64, 9727. 110. Belvisi, L.; Colombo, L.; Colombo, M.; Giacomo, M. D.; Manzoli, L.; Vodopivec, B.; Scolastico, C. Tetrahedron 2001, 57, 6463. 111. Zhang, R.; Brownewell, F.; Madelengotia, J. Tetrahedron Lett. 1999, 40, 2707. 112. Zhang, X.; Jiang, W.; Schmitt, A. C. Tetrahedron Lett. 2001, 42, 4943. 113. Potts, D.; Stevenson, P. J.; Thomson, N. Tetrahedron Lett. 2000, 41, 275. 114. Thanh, G. V.; Celerier, J.-P.; Lhommet, G. Tetrahedron Lett. 1999, 40, 3713. 115. Legrand, A.; Rigo, B.; Henichart, J.-P.; Narberg, B.; Camus, F.; Durrant, F.; Cauturier, D. J. Heterocycl. Chem. 2000, 37, 215. 116. Yamada, T.; Sakaguchi, K.; Shinada, T.; Ohfune, Y.; Soloshonok, V. A. Tetrahedron: Asymmetry 2008, 19, 2789. 117. Panday, S. K.; Langlois, N. Synth. Commun. 1997, 27, 1373. 118. Lenda, F.; Guenoun, F.; Martinez, J.; Lamaty, F. Tetrahedron Lett. 2007, 48, 805. 119. Tsubotani, S.; Funabashi, Y.; Takamoto, M.; Hakada, S.; Harada, S. Tetrahedron 1991, 47, 8079. 120. Baldwin, J. E.; Miranda, T.; Moloney, M.; Hokelek, T. Tetrahedron 1989, 45, 7459. 121. Dikshit, D. K.; Panday, S. K. J. Org. Chem. 1992, 57, 1921. and references cited therein. 122. Goswami, L. W.; Srivastava, S.; Panday, S. K.; Dikshit, D. K. Tetrahedron Lett. 2001, 42, 7891. 123. Bowler, A. N.; Doyle, P. M.; Hitchcock, P. B.; Young, D. W. Tetrahedron Lett. 1991, 32, 2679. 124. Starkmann, B. A.; Young, D. W. J. Chem. Soc., Perkin Trans. 1 2002, 725. 125. Dinsmore, A.; Doyle, P. M.; Steger, M.; Young, D. W. J. Chem. Soc., Perkin Trans. 1 2002, 613. 126. Oliveira, D. de J.; Coelho, F. Tetrahedron Lett. 2001, 42, 6793. 127. Dinsmore, A.; Doyle, P. M.; Hitchcock, P. B.; Young, D. W. Tetrahedron Lett. 2000, 41, 10153. 128. Qiu, X.-L.; Meng, W.-D.; Qing, F.-L. Tetrahedron 2004, 60, 5201. 129. Zhang, X.; Schmitt, A. C.; Jiang, W. Tetrahedron Lett. 2001, 42, 5335. 130. Stevens, C. V.; Rammeloo, T.; Kimpe, N. D. Synlett 2001, 10, 1519. 131. Dieltiens, N.; Stevens, C. V.; Masschelein, K. G. R.; Rommeloo, T. Tetrahedron 2005, 61, 6749. 132. Katoh, M.; Mizutani, H.; Hondo, T. Tetrahedron Lett. 2005, 46, 5161.

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133. Merino, P.; Mates, J. A.; Revuelta, J.; Tejero, T.; Chiacchio, U.; Romeo, G.; Iannazzo, D.; Romeo, R. Tetrahedron: Asymmetry 2002, 13, 173. 134. Caubert, V.; Langlois, N. Tetrahedron Lett. 2006, 47, 4473. 135. Hill, T. J.; Kocis, P.; Moloney, M. G. Tetrahedron Lett. 2006, 47, 1461. 136. Herdeis, C.; Kelm, B. Tetrahedron 2003, 59, 217. 137. Cienfuegos, L. A. D.; Langlois, N. Tetrahedron: Asymmetry 2006, 17, 1863. 138. Cai, C.; Yamada, T.; Tiwari, R.; Hruby, V. J.; Soloshonok, V. A. Tetrahedron Lett. 2004, 45, 6855. 139. Caubert, V.; Masse, J.; Retailleau, P.; Langlois, N. Tetrahedron Lett. 2007, 48, 381. 140. Fujita, M.; Kitagawa, O.; Yamada, Y.; Izawa, H.; Hasegawa, H.; Taguchi, T. J. Org. Chem. 2000, 65, 1108. 141. Koshinen, A. M. P.; Rapoport, H. J. Org. Chem. 1989, 54, 1859.

142. Monteiro, H. J. Synthesis 1974, 137. 143. Drauj, K.; Kleemann, A.; Marteus, J.; Scherberich, P. J. Org. Chem. 1986, 51, 3494. 144. Harris, P. W. R.; Brimble, M. A.; Gluckman, P. D. Org. Lett. 2003, 5, 1847. 145. Chen, X.; Du, D.-M.; Hua, W.-T. Tetrahedron: Asymmetry 2002, 13, 43. 146. Langlois, N.; Rakotondradany, F. Tetrahedron 2000, 56, 2437. 147. Barraclough, P.; Dieterich, P.; Spray, C. A.; Young, D. W. Org. Biomol. Chem. 2006, 4, 1483. 148. Oba, M.; Saegusa, T.; Nishiyama, N.; Nishiyama, K. Tetrahedron 2009, 65, 128. 149. Kondo, T.; Nekado, T.; Sugimoto, I.; Ochi, K.; Takai, S.; Kinoshita, A.; Hatayama, A.; Yamamoto, S.; Kawabata, K.; Nakai, H.; Toda, M. Bioorg. Med. Chem. 2008, 16, 190. 150. Einsiedel, J.; Lanig, H.; Waibel, R.; Gmeiner, P. J. Org. Chem. 2007, 72, 9102.

Pyroglutamic acid: a unique chiral synthon

Pyroglutamic acid: a unique chiral synthon

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