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Heterodiene cycloadditions: Synthesis and oxidation of pyrano[3,2,b]indoles into spiro derivatives
Tetrahedron.Vol.
53, No. 3, pp. 987-1002,
Copyright
CY CLOADDITIONS:
PYRAN0[3,2d]INDOLES
1996 Elsevier
Pnnted in Great Britain.
PII: SOO40-4020(96)01040-X
HETERODIENE
0
1991
Scw~ce Ltd
All rights reserved
0040.4020/97
$17.00
+ 0.00
SYNTHESIS AND OXIDATION OF
INTO SPIRO DERIVATIVES
Jean-Yves M&our*, Ahmed Mamai, BCatrice Malapel, Philippe Gadonneix
Instttut
Organique et Analytique, assock? au
de Chimie
Orl&ins
C&x
Abstract:
l-Acetyl-2-benzyltdene-2,3-dihydroindol-3-ones
to afford
substituted
pyrano[3&b]indoles;
spirolactones
or to 0x0 acetals
Copyright
1996
0
Elsevier
with
Science
compounds
in the presence
reagents.3-6 dihydropyrans
High
of dihydropyrans;
pressure
also
vinyl
d’OrlCans,
ethers
oxidized,
of boron
and vmyl
using
45067
Jones
thioethers reagent,
to
trifluoride.
considerably
reactions (IEDDA)t,z a well-established
were catalyzed
accelerates
the
of electron rich and a powerful
by Lewis acids and lanthanides
Diels-Alder
or pyridines.
reactions;7,8
the
substituted
Tietze2 reported on asymmetric
using IEDDA in a key step of their synthesis.
has reported on the reactivity of chromones,
with electron-withdrawing
substituents,
in IEDDA reactions with vinyl ether. We wish to report here the synthesis of new pyrano[3,2-blindoles examine their reactivity towards oxidation in order to obtain lactonic derivatives. 2 position of 1-acetyl-lH-indol-3(2H)-onet1~12
aldol condensation
of 1-acetyl-lH-indol-3(2H)-one
with electron-rich
olefins
vinylsulfide
diastereomers
(1) (mixture of E/Z-isomers),
cisltmns,
days
with substituted
(except for 3f,g) (Scheme]).
obtained
and to of the C-
Cycloaddition
was performed
2d
Fax: 33 0238417281 E-mail: [email protected] Dedicated to Professor Wuldemar Adam on the occasion of his 60th birrhdq. 987
to an
reacted as heterodienes
3 as a mixture
of
at 110 “C in a sealed tube
2. The yields were high except for the phenyl vinylsulfide
of 24 h at 110 “C. The keteneacetal
according
(2a), 1-(4-methoxy)benzyloxyethene
(2d) to afford the cycloadducts
(2~) or 1, I-diethoxyethene
at 135 “C instead
benzaldehydes,l3
such as 1-ethoxyethene, 5 I-benzyloxyethene
with a large excess of dienophile
The easy oxidability
can interfere during the oxidation of cyclic ketals 3.
I-Acetyl-2-benzylidene-2,3-dihydroindol-3.ones
(2b), phenyl
1,6-
in the synthesis of carbohydrates.
We have recently described the synthesis of &carboline$ Also recently, Wallaceto
Universttk
has become
these reactions
formed give easy access to carbohydrates9
induction with chiral oxabutadienes
with
were
Diels-Alder
such as enol ethers, with I-oxa-1,3-butadienes
method for the synthesis
6759,
Ltd
The inverse electron demand (LUMOdiene- controlled) dienophiles,
BP
reacted
these
m-CPBA
CNRS,
2. France
2c which needed 6
(I,]-diethoxyethene)
was
highly
988
J.-Y. MBROUR et ~1
nucleophilic
and was the most reactive one. These IEDDA reactions worked only in the presence of a catalytic
amount (5%) of ytterbium salt, Yb(fod)3.3
CH,= Cm’)R3 2 Yb (fad), , 11 O’C t 50
98%
la R’ = 0CH3
3
lb R’ = CH, lc R’=H
Compound
R2
Rt
R’
Yield (%)
mp”C Oil
cis/trans (S)
3a
4-OCH, OBn
H
98
3b
4-CH,
OBn
H
98
113a
81/19
3c
4-CH,
OPMB
H
95
oil
85115
3d
4-OCH, SC,H,
H
53
oil
51143
3e
4-CH,
SC,H,
H
50
oil
62138
3f
4-CH,
OC*H,
OC,H,
92
oil
3g
4-H
OC>H,
OC,H,
75
oil
3h
4-OCH, OC,H,
H
98
oil
3i 4-CH, a major diastereomer cis.
WI5
84116
H 98 125a OC,H, Bn = Renzyl; PMB = 4-methoxybenzyi.
86114
Scheme I The use of methoxyallene diastereomers) Disubstituted
as dienophile
afforded
in only 40% yield due to polymerisation dienophiles
like 2$dihydropyran
(20%). No reaction occurred with vinylidene to its low energy HOMO. I ,4-Benzodioxin
afforded
the cycloadduct
4a
of the methoxyallene the cycloadduct
(ratio
66133 for the two
even at 50 “C (Figure
Sa (Figure
carbonate. The lack of the reactivity of this dienophile
was also unproductive
0' 5a
4a Figure 1
can be due
as dienophile in these cycloadditions.
of&
:&o,
I). 1,2-
I) but in a low yield
Synthesis
For all the cycloadducts endo/exo
configuration
of the anomeric (equatorial).
3a-e,
3h,i the major diastereomers
or respectively
proton
and oxidation of pyrano[3,2-hlindoles
cis/n~ns
Hz and its coupling
The major diastereomer
989
have the same relative configuration.
has been tentatively attributed by examining constants
with the inequivalent
has always a more deshielded
protons
The
the chemical shift
H,,
(axial) and H,,
Hz (6=5.36 ppm VERSUS5.27 ppm for 3a)
indicating an axial position for the ethoxy group but the coupling constant J2+ = 5. I Hz is only slightly inferior to J gsa = 5.9 Hz (minor diastereomer)
3a; the aspect of the signals
for compound
of the Hja and H3, also
depended on the value of the coupling constant, frans or cis, with the Ha (J3e4 = 7.2 Hz, J2a4 = 5.4 Hz) for the presumed
compound
ROESY experiments) pseudo
these two values were close and may be confusing.
indicated connectivities
planarity
of the pyrano
ring has an infhience
reported were not conclusive.
In order to have more information ethyl vinylether
and
on interactions
The major diastereomer
through
space since
the
the different
might be cis and the minor truns based on
[47c+ 2711since the Z-isomer should give the endo (c-is) cycloadduct.
the usual tenets of cycloaddition
we reacted the Z-4-methoxybenzylidene-2,3-dihydroindol-3.onet4
with
3j (80% yield) from an endo process
(Figure 2);
which afforded the expected cis cycloadduct
only a trace amount of the truns diastereomer
is observed
medium (K,CO,
/ethanol/HzO,
3j as a unique
cis diastereomer
= 9.4 Hz). The deacetylation
50°C. lh30, 67% yield) of the major diastereomer which confirms
of 3j is easily
(~5% yield). The cis configuration
assigned using tH NMR (Jzie = 1.8 Hz, J2Ja = 8.2 Hz, Jse4 = 6.8 Hz, J,,
cycloadduct
2Q NMR (NOESY
of the H, with Hga and to a some extend with H3e for the major
of 3a; for H, the presence of the 0CH2 signal with the same chemical shift was disturbing;
cis diastereomer
connectivities
cis-3a;
the cis configuration
in basic
of 3h15 afforded compound
of the major diastereomer
of the
3 obtained from la-c.
3.j
3h
/O
Figure 2
As reported previously
afforded respectively (compound
Id
isomerisation material
the ratio of diastereomers
in the cycloadduct
of the starting material 1 (which was predominantly
stereochemistry
the major cis diastereomer
of 3a, 3d in 85%, 57% yield; even starting from pure Z-isomer
R1 = NOz) gave also a mixture of cis and tram cycloadducts in the mixture, by Lewis acid Yb 3+, of the diastereomeric
1. It has been discussed
by Tietze 1 that isomerisation
reaction
configuration
and the exe or endo nature of the process; (the endo-E-syn-TS
products.
could occur with the possibility
of four transition
3). Some reports3 indicated in these cycloadditions
3. This can be due to an
cycloadducts
of the
cycloaddition
the cis-adduct
3 was not directly related to the
Z) t6,17; for example la (79% Z-isomer)
and/or of the starting
I-oxa-1,3-butadiene states according
and the exo-Z-syn-TS
the formation
during
the
to the E and Z would give
of a 1:l mixture of cisltrans
990
J.-Y. MBROURet al.
The population the coupling position
of the two conformers
constants
of the cis diastereomer
Jasa and Jsa4; for compound
for the 4-phenyl
and the 2-ethoxy
can be discussed by examining the values of
3j the values of these constants
group. A different
behavior
where a decrease of the coupling constants J 23aand Jas4 indicates
indicate
an equatorial
is shown by the other cycloadducts
a significant
contributionla
of the conformer
having the 2-ethoxy and the 4-phenyl group in axial position. (Scheme 2)
dc2J% Scheme 2 Compounds anomeric
3 were slightly different
carbon by TMSCN
(TMSOTf)
in the presence
corresponding
failed in presence
of a non-nucleophilic
the 2-position
hydroxylation in carbohydrate reactions
Treatment
of compound
base as N,N-diisopropylethylamine
in 2-position chemistry
for some years the oxidation
of indolic compounds
was sensitive
of I-substituted-lH-indol-3(2H)-ones. we submitted
the compounds
we have worked on pure diastereomer
diastereomers,
from usual acetals since nucleophilic
of TMSOTf.
attack on the
3 with Lewis acids
also failed to give the
enol ethers.19
We have been exploring process;*0
in reactivity
of indoles
which was an important
towards oxidation
1lvl* Using oxidation procedures
3h,i to a Jones oxidation*lg**
3i
E!%z!?a,
6h
RIzCH~~
R’=OCH3
6i Rl=CH3
\
F
R’
developed
(For the oxidation
cis or tram). We obtained only spirolactones
and not the expected lactones 7h,i (Scheme 3).
&a,
biological
and we have reported on the
6h,i, as single
Synthesis
The cis or truransdiastereomer or trans diastereomer mechanism23
and oxidation of pyrano[3,2-blindoles
of 3h afforded the same unique diasteromeric
of 3i gave the same diastereomeric
(Scheme 4) involving
initial epoxidation.
opening of the pyrano ring generates the intermediate to the Spiro compound
991
lactone 6h; similarly the cis
lactone 6i. These results were consistent
with a
The opening of the oxirane ring with a concomitant
oxonium ion (A). This oxonium ion may evoluate either
8 which is further oxidised to the lactone 6 or to an hydroxyaldehyde
which affords 6
after an oxidation via its hemiacetal. We have also shown that compound 8 gave product 6 under similar Jones oxidation.
3h,i
H30+
6h,i
Scheme 4
This type of Spiro structure was found in some oxindole alkaloids like Horsfiline24 which possess a 3,3Spiro structure; 2,2-Spiro pseudoindoxyl mitragynine
pseudoindoxyl
structure was encountered
Oxidation of 3h,i was also performed of BF3 etherate at room temperature The major diastereomer mixture of diastereomers of compound
pseudoindoxy125
or in
using meraperchlorobenzoic
acid in presence of a catalytic amount
as reported for the oxidation of cyclic acetals into lactones.27
(cis) of 3h afforded the rearranged
ketonic cyclic acetal 8h in 58% yield as a
in the ratio 1:3 and not the lactone 7h. (Scheme 3). Similarly the major diastereomer
3i gave 8i in 68% yield (mixture
afforded, in the same oxidation conditions, plausible mechanism
in tetrahydrocarbazole
alkaloid.26
for this transformation
of diastereomers
1:6). The minor diasteromer
a mixture of products 6h, Sh, 9h approximately of 3h,i into Sh,i was first the epoxidation
(trans)
of 3h
in the same ratio. A of the ethylenic
bond
J.-Y. MBROUR et al.
992
followed
by opening
intramolecular
of the oxirane after complexation
nucleophilic
displacement
(Scheme 5). This mechanism
of the Lewis acid BF3 (oxonium
the two diastereomers
cannot explain the mixture of epimers. Another possibility
pathways proceeding
A direct
which may occur via an attack of the anomeric carbon to afford Sh,i
may differentiate
discrete steps and that the rate-determining
species).
of the starting materials
is simply that the rearrangement
step differs from one diastereomer
3h or 3i but
proceeds via several
to the other one despite both
through an oxonium ion such as A (Scheme 4).
M = BF3-
Sh,i Scheme 5
It is noteworthy single diastereomeric
that the 0x0 acetal 8i (major diastereoisomer)
is oxidized by Jones reagent to the same
0x0 lactone 6i obtained previously.
TMSOTf m-CPBA
BF3
(W,),O * 40%
0
\
CF&OOH
CHO
.
63%
Scheme 6 The use of a stronger Lewis acid like TMSOTf in the oxidation procedure,
instead of BF3, afforded the
Synthesis
keto esters 9h,i in 51% and 60% yield respectively dihydropyran
as single diastereomers
6). The opening
presence of a protonic acid like trifluoroacetic Compounds
which cannot be directly alkylated.29
Another
route to obtain lactones 3a (diastereomer
3i afforded the acetal 1Oi; in
as the result of a formal alkylation in 2-position
lH-indol-3(2H)-one
3a,b. Compound
of compound
acid the unmasked aldehyde28 lli was obtained from 3i.
9i, lOi, lli may be considered
alternative
7h,i was to prepare
cis) in methanol,
13b respectively
under a hydrogen
atmosphere,
in presence
of of
in 37% yield, rather than
(Scheme 7). Using a 100% weight of Pd/C 10% allowed us to obtain the indoline lactol 13a or in 42% and 40% yield as a mixture of diastereomers
be obtained from 12a by hydrogenolysis moiety was in this case particularly
sensitive to hydrogenation
substituent)
was readily transformed
presence
(10% weight),
of 10% PdK
substituent
of low stability. Compound
13a can also
of the benzyl group with a 100% weight of Pd/C (10%). The indole
instead of a benzyloxy
methoxybenzyl
of l-acetyl-
first a lactol by hydrogenolysis
10% (10% weightj was reduced into indoline derivative 12a (one diastereomer)
hydrogenolysed
of the
of the ethylenic
species to the carboxylic acid ester by the peracid (Scheme 6).
In the absence of oxidant, treatment with BF3 etheratelethanol
PdK
(Scheme
ring was, in this case, the first step of the oxidation instead of the epoxidation
bond, followed by oxidation of the carboxonium
compounds
993
and oxidation of pyrano[3,2-blindoles
since compound
3i (with an ethoxy substituent
into the corresponding
in the same conditions
indoline derivative
as for 12a. CA!! or DDQ oxidation
of the 4-
of compound 3c was unfruitful. OBn
OBn
HO
3”i? H
:I
oL
3a 3b
I_\
R’
12a
R’=OCHj
I
R’ = CH,
Hz/Pd
Scheme 7
In summary we have extended the [47t + 27~1cycloaddition one to different dienophiles
and prepared spiroindolic
compounds
of 1-acetyl-2-benzylidene-2,3-dihydroindol-3which were interesting intermediates.
12i in
J.-Y. MBROUR et al.
994
EXPERIMENTAL
PART
Melting points were determined recorded on a Perkin Elmer tetramethylsilane expressed
using a Kofler apparatus hot stage and were uncorrected.
1330. lH-NMR
as the internal standard
spectra were recorded
for solutions
in deuteriochloroform
on a Bruker AM 300 (300 MHz) and coupling
in Hertz. Mass spectra were obtained using chemical
ionisation
IR spectra were
(ammonia)
constants
on a Nermag
with were IO-1OC
apparatus.
IEDDA Reactions. General Procedure 1 (1.9 mmol) were dissolved
Compounds
in CH,Cl,
(2 ml) and vinylether
2 (1.5 ml) in presence
of
Yb(fod)3 (0.095 mmol); the mixture was heated in a sealed tube at 110 “C during 24 h (2a, 2b), at 135 “C during 6 d for 2c or at 90 “C for 20 h for 2d. Evaporation chromatographed
of the solvent under vacno gave an oil which was
on a silica gel column (230/400 mesh) using CH2C12/petroleum
of two diastereomers
ether 1: I as eluent; a mixture
was obtained; (see Scheme I, Table 1).
5-Acetyl-2-methoxy-4-(4-methoxyphenyl)-3-methylene-3,4-dihydro-2H-pyrano[3,2-b]indole Methoxyallene
(1.5 g, 21.4 mmol) was reacted on compound
50 “C during IO d in presence chromatographed diastereomers
of Yb(fod),
la (293 mg, 1 mmol) in CH,CI,
(32 mg, 0.030 mmol). After evaporation,
on a silica gel column (eluent: CH$l$petroleum
(1 ml) at
the residue was twice
ether 1:l) giving an oil as a mixture of
(ratio 66:33); yield: 145 mg (40%). IR (film): v=l68O(C=O) cm-t.
Major diastereomer:
lH-NMR (CDC13) : 6=2.41(s, 3H, CH,), 3.24(s, 3H, COCH,),
5.29, 5.33, 5.42(4s, 4xlH,
lH, J=l.4, 7.3, Hg), 7.98(d, IH, J=7.3, Hg).
Minor diastereomer:
(CD+)
tH-NMR
5.18, 5.31, 5.32(4s, 4xlH,
: 6=2.38(s, 3H, CH3), 3.55(s, 3H, COCHj), 3.72(s, 3H, OCH& 4.88,
HZ, H,, =CH,),
7.30(m, 2H, H7, HS), 755(dd, Anal. Calc. for C,,H21N0,:
6.76(d, 2H, J=8.8, H3’, HS’), 6.94(d, 2H, J=8.8, HZ’ , He), 7.20-
IH, J=2.0, 8.0, Hg), 7.93(d, lH, J=8.1, He). MS (U/NH,)
la (200 mg, 0.68 mmol) with dihydropyran
on a silica gel column (eluent: CH2C12/petroleum cm-t.
5,6]pyrano[3,2-blindole
(Sa).
(2 g, 24 mmol) were heated at 140 “C in presence
(40 mg, 0.038 mmol) during 8 d. After evaporation
IR (KBr): v=1695(C=O)
: m/z = 364(M+l)+.
C, 72.71; H, 5.82; N, 3.85. Found: C, 72.90; H, 5.67; N, 3.91.
6-Acetyl-5-(4-methoxyphenyl)-2,3,4,4a,S,lla-hexahydropyrano[3’,2’: Compound
3.69(s, 3H, OCHj), 5.18,
H,, H,, =CH,), 6.70(d, 2H, J = 8.8, H,’ ) HSn), 6.99(d, 2H, J=8.8, Hz* 3He’), 7.22-
7.33(m, 2H, H7, H8)~7.58(dd,
of Yb(fod),
(4a).
under vucuo the residue was chromatographed
ether 3: 1); yield:62 mg (24%). mp=149 “C (ethanol/water).
‘H-NMR (CDCI-,) : &1.60-1.82(m,
4H, CH,CH,),
2.09(m, lH, Haa), 2.41(s,
3H, COCH3), 3.70(s, 3H, OCH,), 3.70(m, lH, OCH,), 4.02(m, lH, OCH,), 4.31(s, lH, HS), 5.32(d, IH, J=2.2,
Synthesis
HI,,),
6.Wd,
2H, J=8.8,
8.0, Hlo), 7.99(d,
H,,, Hs~), 6.92(d,
lH, J=8.0,
995
of pyrano[3,2-blindoles
2H, J=8.8,
H7). MS (CVNH,)
6.14; N, 3.71. Found: C, 72.90;
Table 1. Compounds
and oxidation
Hz’, Hg), 7.23-7.33(m,
2H, Hg, Hg), 764(dd,
: m/z=378 (M + I)+. Anal. Calc. for Cz3Hz3N04:
lH, J=1.5, C, 73.19;
H, 5.99; N, 3.91.
3 Prepared
680a
Diastereomer
Z=O)
H3, J=2.4, J=6.8, J=13.5),
cis: 2.24(dt, lH, H3, J=5.1, J=13.5), 2.32(s, 3H, AC), 2,50(ddd,
J=11.9), 4.59(t,
3.69(s,
3H, OCH3),
lH, H4, J=6.0), 5.36(dd,
4.58 and 4.86(2s,
2xlH,
lH,
OCH2,
lH, H2, J=2.4, J=5.1), 6.67(d, 2H, Hg’,
H5’, J=8.7), 6.90(d, 2H, H2’, H6’, J=8.7), 7.06-7.32(m,
7H, Harom),
7.57(d, lH,
H9, J=6.5), 8.04(d, lH, H6, J=S.O). Diastereomer
2.00(ddd,
trms:
lH, H3, J=2.2,
J=7.1, J=13.8),
2.29(s,
3H, AC),
2.44(dt, lH, H3, J=5.6, J=13.8), 3.71(s, 3H, OCH3), 4.59(t, lH, H4, J=6.3), 4.67 et 4.92(2s,
2xlH,
0CH2,
J=11.9),
5.27(dd,
lH, H2, J=2.2, J=5.6), 6.76(d, 2H, Hg’,
H5’, J=8.7), 6.94(d, 2H, H2’, H6’, J=8.7), 7.06-7.32(m,
7H, Ha,,,),
7.57(d, lH,
H9, J=6.5), 8.04(d, lH, H6, J=B.O). 680b
Diastereomer
C=O)
AC), 2.51(ddd,
cis: 2.24(s, 3H, CH3), 2.25(dt,
lH, H3, J=2.2, J=7.35, J=14.0),
J=12.5),
lH, H4, J=6.2), 5.36(dd,
4.61(t,
H5’, J=8.1),
6.96(d,
Diastereomer
3H, AC), 2.46(dt,
4.64 and 4.87(2s,
2.32(s, 3H,
2xlH,
OCH2,
7.05-7.33(m,
7H, H7, H8, Harom),
8.05(d, IH, H6, J=8.1).
trans: 6=2.01(ddd,
CH3), 2.29(s,
4.59 and 4.88(2s,
lH, H2, J=2.2, J=5.1), 6.88(d, 2H, Hg’,
2H, H2’, H6’, J=S.l),
7.57(d, lH, H9, J=S.l),
lH, H3, J=5.1, J=13.5),
2xlH,
lH,
H3, J=2.2,
J=6.6,
lH, Hg, J=5.9, J=13.2),
OCH2, J=12.5), 5.27(dd,
2H, H2’, H6’, J=8.1), 7.15-7.33(m,
7H, Ha,,,),
J=13.2),
4.62(t,
2.26(s,
3H,
lH, H4, J=6.2),
lH, H2, J=2.2, J=5.9), 7.04(d, 7.57(d, lH, H9, J=7.3),
8.05(d,
lH, H6, ]=7.3). iC
690a
Diastereomer
C=O)
AC), 2.45(ddd, J=6.6),
cis: 2.17(dt,
lH, H3, J=5.9, J=13.9), 2.21(s, 3H, CH3), 2.28(s, 3H,
lH, H3, J=2.2, J=7.3, J=13.9), 3.69(s, 3H, OCH3), 4.55(t, lH, H4,
4.64, 4.87(2d,
2xlH,
0CH2,
J=11.7),
5.30(dd,
lH,
6.72(d, 2H, H3”, H5”, J=8.8), 6.83(d, 2H, H3’, H5’, J=S.l), J=8.1), 7.02(d, 2H, H2”, H6”, J=8.8), 7.15-7.30(m,
H2, J=2.2,
J=5.9).
6.93(d, 2H, H2’, H6’.
2H, H7, H8), 7.55(dd,
lH, H9.
J=6.6, J=2.2), 8.02(d, lH, H6, J=7.3). Diastereomer 2.29(s, 4.85(2d, J=5.9),
3H,
tram:
2xlH, 6.80(d,
lH,
OCH2, J=11.7), 2H, H3:
H2’, H6’, J=S.l), 7.57(dd,
1.99(ddd,
AC), 2.42(dt,
lH, H3, J=2.2, J=7.3, J=13.9), H3, J=5.9,
3.74(s,
2.26(s, 3H, CH3), 3H, OCH3),
4.61(t, lH, H4, J=6.6), 5.25(dd,
H5”, J=S.l),
7.20-7.33(m,
J=13.9),
lH, H2, J=2.2
6.91(d, 2H, Hg’, H5’, J=S.l),
2H, H7,
H8),
7.23(d,
lH, H9, J=7.3, J=1.5), 8.06(d, lH, H6, J=7.3).
2H,
4.57,
7.04(d, 2H
H2”, H6”, J=8.1)
12(M+l)+
H,
J.-Y.
996
Id
MBROUR et al.
1690”
Diastereomer
C=O)
J=2.9, J=7.3, J=14.4), 4.66(t, lH, H4, J=7.3), 5.62(dd,
cis: 2.19-2.29(m, lH, Hg), 2.32(s, 3H, AC), 2.76(ddd,
lH, H3,
lH, H2, J=2.9, J=S.l),
6.75(d, 2H, H3’, H5’, J=S.S), 6.95(d, 2H, H2’, Hg’, J=B.B), 7.99(d, lH, H6, J=S.S), 7.20.7.60(m, BH, H7, H8, H9, SPh). Diastereomer
truns: 2.19-2.29(m, lH, Hg), 2.36(s, 3H, AC), 2.4%2.60(m, lH,
H3), 3.71(s, 3H, OCH3), 4.65(t, lH, H4, J=5.1), 5.48(dd, lH, H2, J=2.9, J=8.86), 6.77(d, 2H, H3’, H5’, J-8.8), 6.95(d, 2H, H2’, Hg’, J=S.S), 7.20-7.60(m, BH, H7, H8, H9, SPh), 8.02(d, lH, H6, J=8.8) Le
69Ob
Diastereomer
C=O)
2.77(ddd, lH, H3, J=2.9, J=7.3, J=13.9), 4.66(t, lH, H4, J=7.3), 5.61(dd, lH, H2,
cis: 2.17.2.30(m, lH, Hg), 2.25(s, 3H, CH3), 2.31(s, 3H, AC),
J=2.9, J=8.8), 6.91(d, 2H, H3’, H5’, J=S.l), 7.01(d, 2H, H2’, Hg’, J=S.l), 7.197.60(m, BH, H7, H8, H9, SPh), 7.98(d, lH, H6, J=S.l). trarzs: 2.17-2.3(m,
Diastereomer 2.49-2.59(m,
lH,
H3), 4.66(t,
6.92(d, 2H, H3’, H5’, J=S.l),
lH, lH,
H3), 2.25(s,
H4, J=7.3),
3H, CH3),
5.48(dd,
lH,
7.04(d, 2H, H2’, Hg’, J=S.l),
2.35(s,
3H, AC),
H2, J=2.9,
7.19-7.60(m,
J=B.B), BH, H7,
H8, H9, SPh), B.Ol(d, lH, H6, J=S.O).
690a
1.10 and l.l1(2t,
2x3H, 2xCH3, J=7.3), 2.04(dd, lH, H3, J=7.0, J=13.6), 2.24 and
C=O)
2.26(2s, 2x3H, AC, CH3), 2.54(dd, 6.90(d, 2H, H3’, H5’, J=S.l),
lH, H3, J=8.4, J=13.6), 4.57(t, lH, H4, J=7.7),
7.01(d, 2H, H2’, Hg’, J=B.l),
7.19-7.31(m,
2H, H7,
H8), 7.59(d, lH, H9, J=B.l), 8.02(d, lH, H6, J=S.l).
k
.690a
1.09 and l.l3(2t,
C=O)
3H, AC), 2.57(dd,
2x3H, 2xCH3, J=7.3), 2.09(dd, lH, H3, J=8.4, J=13.6), lH, H3, J=7.0, J=13.6),
3.46-3.82(m,
lH, H4, J=7.3), 7.00-7.35(m, 7H, H7, Hg
Harom),
2x2H, 2xOCH2),
380(M+l)+
2.23(s, 4.64(t,
7.61(d, lH, H9, J=7.0),
B.OO(d,lH, H6, J=B.l). ‘j
i400a
Diastereomer
NH)
J3a3e=13.6), 2.47(ddd,
cis: 1.29(t, 3H, CH, J=7.3), 2.27((m, lH, Hg,, J2sa=8.2, J~~4’9.4, lH, Hze, JzJe= 18, J3e4=6.8, J~~3~=13.6), 3.82 (m, IH,
OCH2), 4.11(s, 3H, OCH3), 4.17 (m, lH, OCH2), 4.33(dd, lH, H4, J~~4’6.8, J3a4=9.4), 5.31(dd, lH, H2, J~3~=l.8, J2sa=8.2), 7.15(d, 2H, H2’, Hg’, J=S.l), ]7.05-7.20(m, Ic = CH$O,
6H, Harom, NH); 7.63(d, lH, Harom, J=S).
a film, b KBr.
l-Acetyl-3’-(4-methoxyphenyl)-2’,3’,4’,S’-tetrahydrospiro[indole-2(3~)-2’-furan]-3,S’-dione Compound
3hs as a single trans or cis diastereomer
(6h).
(1 IO mg, 0.3 mmol) was dissolved
in acetone (3 ml)
at 0 “C; Jones reagent21 was dropwise added till all 3h has reacted (circcc 30 min). Excess of the oxidant was destroyed
with isopropanol;
the solution was filtered on celite and evaporated;
water and CH,C12 and the organic layer was dried over MgSO,; chromatographed
on
a silica
gel
column
(eluent:
evaporation
CH2C12/petroleum
the residue was treated with in vucuo left an oil which was
ether
5:l);
yield:44mg
(4270),
Synthesis
mp=70 “C. IR (KBr): v= ISlO(C=O), 3.OO(dd, lH, J=l2.5,
and oxidation of pyrano[3,2-blindoles
997
173O(C=O), 168O(C=O) cm-l. IH-NMR (CDCI,) : 6=2.5.5(s, 3H, CH,),
16.9, H4.). 3.65(s, 3H, OCH,), 3.68(dd,
IH, 5=8X, 16.9, H4’), 4.49(dd,
IH, J=8.8, 12.5,
H3’), 6.63(d, 2H, J=8.8. H3”, HS,,), 6.97(d. 2H, J=8.8, HZ”, Hs.e), 7.04(t, IH. J=7.3, HS), 7.39(d, lH, J=7.3, H7), 7.56(t,
lH, J=7.3, Hg), 8.14(d,
IH, J=8.1, H,).
I%-NMR
(CDCI,)
: 6=25.8(CH,),
32,O(C4’), 45.3(C3’),
96.O(C2), 1 13&C3”, C5”), 117.1(C7), 120.O(C3a), 124.1 (C4), 124.2(C 1‘I), 124,9(C5), 129,2(C2”,
55.O(OCH$,
C6”), 138.9(C6),
152.6(C7a),
158.8(C4”), 168.9(C=O C5’). 172.9(C=O AC), 194.4(C=O C3). MS (Cl/NH,)
:
m/z=352 (M +I)+. Anal. Calc. for CZ0H,7NOs: C, 68.37; H, 4.88; N, 3.99. Found: C, 68.62; H. 4.68; N, 3.92.
l-Acetyl-3’-(4-methyIphenyl)-2’,3’,4’,5’-tetrahydrospiro[indole-2(3~),2’-furan]-3,S’-dione Same procedure v=l SlO(C=O),
as described
(6i).
for 6h starting from 3i5; yield:61%. mp=62 “C (ethanol/water).
IR (KBr):
173O(C=O). 1685(C=O) cm-l. IH-NMR (CDCI?) : 6= 2.1 l(s, 3H, CH,), 2.53(s, 3H. COCH,),
2.97(dd. IH, J=l2.9,
17.6, H4’), 3.65(dd, III, J=8.8, 17.6, H4.)>4.49(dd, IH, J=8.8, 12.9, H3,), 6.87(d. 2H. J=8.1,
H,,,, HS*,), 6.9l(d, 2H, J=8.1. H,,‘, H,,,), 7.00(t, IH, J=7.3, HS), 7.35(d, IH, J=7.3, H7), 7.53(dt, IH, J=2.5, 8.1, Hb), 8.1 l(d, IH, 5=8X, H4). Anal. Calc. for C2~~H1,N04: C. 71.63; H. 5.1 1; N, 4.18. Found: C, 71.72; H, 5.28; N, 4.03.
l-Acetyl-5’-ethoxy-3’-(4-methoxyphenyl)-2’,3’,4’,S’-tetrahydrospiro[indole-2(3~),2’-furan]-3-one Compound and m-CPBA temperature.
3h (250 mg, 0.685 mmol) was dissolved in CH,C12 (3.5 ml); BF,, Et,0
(142 mg, 0.822 mmol) were successively
Ether (25 ml) was added, then the mixture was sequentially
ml), saturated NaHC03
(0.04 ml, 0.33 mmol)
was stirred 2 h at room
treated with aqueous 5% Na2S0,
(10 ml) and brine ( 10 ml). The organic layer was dried over MgSO,
The obtained residue was chromatographed diastereomers
added and the solution
(Sh).
were obtained
and evaporated.
on a silica gel column (eluent: petroleum ether /CH,Cl,
in the ratio 1:3; yield:149 mg (58’%,) mp=l40
(15
“C (ethanol),(major
3:7). Two isomer). IR
(KBr): v=172O(C=O), 1675(C=O) cm-l. Major diastereomer: 3H, CH,), 3.37(dt,
IH-NMR (CDCI,)
: 6=1.2l(t, 3H, J=7.0, CH,), 2.24(dd, IH, J=l3.3, J=7.3, H,‘), 2.69(s,
IH, J=6.6, 13.3, Hq’), 3.58(dq,
J=7.0, 9.7, OCH,), 4.19(dd,
IH, J=7.0, 9.7, OCH$,
3.59(s. 3H, OCH,),
3.86(dq,
IH, J=7.3, 13.3, H3e), 5.63(d, IH, J=6.6, HSt), 6.55(d, 2H, J=9.0, H3”, H,,,), 6.91(t,
IH, J=7.3, HS), 6.93(d, 2H, J=9.0, H,,,, He’.), 7.27(d, IH, J=7.3, H7), 7.44(t, IH, .l=7.3, Hg). 8.4l(d, H4). ‘3C-NMR (CDCI,): 6=14.9(CH,). 113.8(C3”, C5” PhOMe),
IH,
1 l8.4(C7),
34.6(C4’), 46.5(C3’), 55,0(OCH3). 64.l(OCH,), 12l.O(C3a), 123.4(C4), 124.l(C5).
IH, J=9.0.
lOO.O(C2), 104.6(C5’),
124.4(Cl” PhOMe),
128.8(C2”, C6”),
137.5(C6), 153.4(C7a). 158.9(C4”), 17O.l(C=O ), 198.O(C=O C3). Minor diastereomer:
IH-NMR
(CDC13) : 6=1.24(t, 3H, J=7.0, CH3), 2.53(m,
3.04(dt, IH, J=7.3, 13.2, H,,), 3.59(s, 3H, OCH,), OCH$, 4.14(dd,
3.63(dq,
IH, H4’), 2.54(s, 3H, CH3),
IH, J=7.0, 9.5, OCH;?), 3.86(dq,
IH, J=7.0, 9.5,
IH, J=7.3, 13.2, H3’), 5.69(dd, IH. J=5.1, 7.3, HS,), 6.54(d, 2H, J=8.8, H,,‘, H,,,), 6.92(t, IH,
J.-Y. MI~ROUR et al.
998
J=7.3, H5), 6.94(d, 2H, J=8.8, Hz*,, He”), 7.30(d, IH, J=8.1, H7), 7.45(t, IH, J=8.1, He), 8.13(d large, IH, Hd). MS (CI/NH$
: m/z=382 (M + I)+. Anal. Calc. for C,,H,,NO,:
C, 69.28; H, 6.08; N, 3.67. Found: C, 69.47; H,
5.95; N, 3.83.
l-Acetyl-5’-ethoxy-3’-(4-methylphenyl)-2’,3’,4’,5’-tetrahydrospiro[indole-2(3H),2’-furan]-3-one Same procedure
as described
for 8h starting from the major diastereomer
obtained in the ratio 1:6; yield=68%,
mp=l16
(8i).
of 3i. Two diastereomers
“C (ethanol), (major diastereomer
were
). JR (KBr): v=172O(C=O),
167O(C=O ) cm-t. tH-NMR (CDCl,) : 6=1.20(t, 3H, J=7.3, CH,), 2.07(s, 3H, CH,), 2.24(dd, lH, J=13.2, 7.3,
Major diastereomer:
Ha,), 2.69(s, 3H, CH,), 3.40(dt, lH, J=5.9, 13.2, H4’), 357(dq, OCH,), 4.21(dd,
lH, J=7.3, 9.5, OCH,), 3.85(dq, lH, J=7.3, 9.5,
lH, J=7.3, 13.2, Hjs), 5.62(d, IH, J=5.9, Hg’), 6.80(d, 2H, J=8.0, H,jj , HStt), 6.89(t, IH, J=7.3,
HS), 6.90(d, 2H, J=8.0, H,‘!, H,,‘), 7.26(d, lH, J=7.3, H7), 7.42(t, IH, J=8.1, H6), 8.41(d, lH, J=8.8, H4). Minor diastereomer: 3H, CH,),
tH-NMR (CDCI,) : 6=1.24(t, 3H, J=7.3, CH& 2.09(s, 3H, CH,), 2.55(m, lH, H4e), 2.55(s,
3.07(dt,
lH, J=7.3, 13.2, HA’), 3.63(dq,
lH, J=7.3, 9.5, OCH*), 3.86(dq,
lH, J=7.3, 9.5, OCH$,
4.18(m, IH, H31), 5.70(dd, lH, J=4.4, 7.3, HS*). 6.80(d, 2H, J=8.1. H,‘*, Hg”), 6.92(t, lH, J=7.3, HS), 6.90(d, 2H, J=8.1, Hz”, Hg”), 7.30(d, IH, J=7.3, H7), 7.42(dt, lH, J=1.5, 7.3, H6), 8.41(d large, lH, H4). Anal. Calc. for C22H23N04: C, 72.31; H, 6.34; N, 3.83. Found: C, 72.54; H, 6.42; N, 3.89.
3-[(1-Acetyl-3-oxo-2,3-dihydroindol-2-yi)(4-methoxypheny~)]propanoic Compound
3h (310 mg, 0.85 mmol) was dissolved
was added dropwise
in CH,Cl,
(4 ml). TMSOTf (0.08 ml, 0.042 mmol)
at -25 “C; mCPBA (176 mg, 1 mmol) was then added. After 1 h, the mixture was treated
with ether (20 ml) and washed with 5% aqueous sodium thiosulfate drying over MgSO, silica gel column
acid Ethyl Ester (9h).
and evaporation
under wzcuo of the organic layer, the residue was chromatographed
(eluent: CH2Clz/petroleum
yield:51% (oil). JR (film): v=1715(C=O), 2.61(s, 3H, COCH,),
(15 ml) and saturated NaHCO,.
ether 3: 1). Only one diastereomer
167O(C=O) cm-t. tH-NMR (DMSO-d6)
was obtained;
After on a
m=165 mg,
: 6=1.26(t, 3H, J=7, CH,),
3.08(m, lH, CH,), 3.54(m, lH, CH2), 3.67(s, 3H, OCH,), 4.03(m, lH, CH), 4.18(dq, 2H,
J=2.6, 7.0, OCH,), 4.91(d, IH, J=4.3, Hz), 6.69(d, 2H, J=8.6, H3’, HS’), 6.99(d, 2H, J=8.6, HT, H6), 7.15(t, lH, J=7.3, HS), 7.53(d, lH, J=7.7, H,), 7.61(t, IH, J=7.7, H6), 8.17(d large, lH, H4). Anal. Calc. for C~~H,,NOS: C, 69.28; H, 6.08; N, 3.67. Found: C, 69.54; H, 6.22; N, 3.69.
3-[(l-Acetyl-3-oxo-2,3-dihydroindol-2-yl)(4-methylphenyl)]propanoic Compound v=1725(C=O),
9i was similarly obtained
from the major diastereomer
171O(C=O), 167O(C=O) cm-t. tH-NMR
CH,), 2.48(s, 3H, CH&
2.96(m,
acid Ethyl Ester (9i).
(DMSO-d6)
of 3i; yield: 60% (oil). JR (film):
: 6=1.13(t, 3H, J=7, CH,), 2.04(s, 3H,
IH, CH,), 3.40(m, lH, CH,), 3.93(m,
lH, CH), 4.05(dq,
2H, J=2.0, 7.0,
Synthesis
OCH,), 4.SO(d, lH, J=4.3, H2), 6.75-6.85(m, H7), 7.47(t,
999
and oxidation of pyrano[3,2-blindoles
4H, H2,, H,,, H,!, H6’), 7.0l(t,
lH, J=7.3, Hg), S.OO(d large, IH, H4). MS (U/NH,)
IH, J=7.3, HS), 7.39(d, lH, J=7.7,
: m/z=366
(M + I)+. Anal. Calc. for
C22H23N04: C, 72.31; H, 6.34; N, 3.83. Found: C, 72.46; H, 6.22; N, 3.91.
l-Acetyl-2-[3,3-diethoxy-l-(4-methylphenyl))propyl]-2,3-dihydroindol-3-one The cis diastereomer
of 3i (100 mg, 0.287 mmol) was dissolved
(lOi).
in ethanol (20 ml) and BF3.Et20
ml, 0.285 mmol) was added and the mixture stirred at reflux for I h. Evaporation which was treated with aqueous NaHC03 dried over MgS04 and evaporated CHzCl$petroleum
(DMSO-d6) : 6=1.12(t, 3H, J=7.0, CH$ 3H, COCH,),
of the solvent leaves a residue
(25 ml) and extracted with CH2C12 (25 ml). The organic layer was
in vacua. the residue was chromatographed
ether 5: I); yield:42mg
(0.035
on a silica gel column (eluent:
(40% ); oil. JR (film): v=l705(C=O), l.l4(t,
167O(C=O) cm-t.
t H-NMR
3H, J=7.0, CH& 2.03(s, 3H, CH& 2.20(m, IH, CH,). 2.39(s,
2.5S(m, lH, CH,), 3.30-3.70(m, 5H, 2xCH2, CH), 4.57(d, IH, J=4.4, Hz), 6.7l(d, 2H, J=S.l, H3’,
HS’), 6.79(d, 2H, J=S.l, H,,, He,), 6.89(t, IH, J=7.3, HS), 7.3l(t,
IH, H6, J=7.9), 7.37(d, lH, J=7.3, H7), 8.20(d
large, IH, Hb). MS (CJ/NH3) : m/z=396 (M + l)+. Anal. Calc. for C24H,,N04:
C, 72.89 H, 7.39; N, 3.54.
Found: C, 72.70; H, 7.55; N, 3.37.
3-[(1-Acetyl-3-oxo-2,3-dihydroindol-2-yl)(4-methy~phenyl)]propanal
(lli).
The cis isomer of 3i (120 mg. 0.344 mmol) was dissolved in a mixture TFA-H@THF
(4 mU2.5 mU2.5
ml) and the mixture was stirred 1 h at 25°C. Ether (20 ml) was then added followed by a solution of saturated NaHCO,;
the two layers were separated
and the organic layer was dried over MgS04.
vacua, the residue was chromatographed
on a silica gel column (eluent: CH,Cl,);
(film): v=1715(C=O),
tH-NMR
3.17(m, IH, CH$,
167O(C=O) cm-l.
(DMSO-d6)
After evaporation
yield:7lmg
in
(63%); oil. JR
: 6=2.05(s, 3H, CH,), 2.5 I(s, 3H, COCH&
3.54(m, IH, CH,), 4.05(m, lH, CH), 4.77(d, lH, J=4.7, Hz), 6SO(d, 2H, J=S.S, H,‘, Hs’),
6.83(d, 2H, J=S.S, H2’, H6’), 7.02(t, IH, J=7. I, H5), 7.40(d, lH, J=7.9, H7), 7.4S(t, lH, J=7.9, H6), S.O2(d broad, IH, HJ), 9.70(s, IH, CHO). Anal. Calc. for C,oHtgNO,:
C, 74.75; H, 5.96; N, 4.36. Found: C, 74.56; H, 5.81;
N, 4.49.
5-Acetyl-2-henzyloxy-4-(4-methoxyphenyl)-3,4,4a,9b-dihydro-2~-pyrano[3,2-~]indole Compound
3a (major diastereomer)
(10 mg) was introduced.
cm-t.
tH-NMR
in MeOH (6 ml) and Pd/C 10%
The mixture was stirred 8 h under a hydrogen atmosphere
filtration on celite and evaporation, Only one diastereomer
(90 mg, 0.21 mmol) was dissolved
(12a).
the residue was chromatographed
at room temperature.
on a silica gel column (eluent: CH,CI,).
was obtained; yield:38 mg (37%) mp=14S”C (ethanol/HzO).
(DMSO-d6)
: 6=1.63-l.Sl(m,
3.72(s, 3H, OCH,), 4.54(d, lH, J=l2.0,
2H, CH,),
After
1.74(s large, 3H, COCH,),
OCH,), 4.85(dd, lH, J=5.1, J=S.6, H&,
JR (KBr): v=l66O(C=O) 3.22-3.3l(m,
4.95(d, IH, J=l2.0,
IH, H4), OCH&
J.-Y. MBROUR et al.
I 000
5.10(t, IH, J=5.1, H,), 5.92(d, IH, J=8.6, Hgn), 6.86(d, 2H. J=8.6, H3’, Hgs), 6.98(t, IH, J=7.7, H7) , 7.06(d, 2H, J=8.6, H,,,H,O, 7.20(t, lH, J=7.0, Hx), 7.257.38(m,
SH, Harom), 7.42(d, lH, J=7.7, H9), 7.88(d large, IH, H6).
: m/z=430 (M + I)+. Anal. Calc. for C27H27N04: C, 75.50 H, 6.34; N, 3.26. Found: C, 75.37; H,
MS (CVNH$ 6.16; N, 3.40.
S-Acetyl-2-hydroxy-4-(4-methoxyphenyl)-3,4,4a,9b-tetrahydro-2~-pyrano[3,2-~]indole Compound
(13a).
3a (710 mg, 1.66 mmol) was dissolved in presence of Pd/C( 10%) (700mg) in MeOH (23 ml)
under a hydrogen atmosphere
of at room temperature.
After 8 h the mixture was filtered and evaporated;
obtained solid was washed twice with ethyl acetate (2 ml). Two diastereomers yield:240 mg (42%). mp=214 “C (mixture of diastereomers). Major diastereomer:
)H-NMR (DMSO-d6)
: 6=1.60-1.75(m,
were obtained in the ratio 1:2;
IR (KBr): v=3280(0-H),
163O(C=O) cm-t.
IH, H3), 1.77(s large, 3H, COCH,),
J=6.6, 14.0, H3), 3.66(s, 3H, OCH,), 3.68(m, IH, H4), 4.83(t, IH, J=8.1, H,,), 4.93(m, J=8.l, H&,
the
2.04(dt, IH,
IH, Hz), 5.63(d, IH,
6.73(d, 2H, J=8.8, H,,, HSa), 7.03(m, IH, H7), 7.05(d, 2H, J=8.8, Hz’, H6#), 7.24(t, IH, J=8.1, Hs),
7.32(d, IH, J=7.35, H9), 7.80(d large, IH, Hg). Minor diastereomer:
i H-NMR (DMSO-d(1) : 6=1.60-l .75(m, 2H, CH,). I .77(s large, 3H, COCH,), 3.27(m, I H,
H4), 3.69(s, 3H, OCH,), 4.78(dd, IH, J=5.1, 8.8, H&,
5.19(m, IH, Hz), 5.78(d, lH, J=8.8, Hgh), 6.79(d, 2H,
J=8.8, H,,, HS’), 7.03(m, IH, H7), 7.08(d, 2H, J=8.8, Hz*, He’), 7.19(t, IH, J=S.l, Hx), 7.37(d, IH, J=7.3, Hg), 7.85(d large, IH. H6). Anal. Calc. for C2uH2,N04:
C, 70.78; H, 6.24; N, 4.13. Found: C, 70.65; H, 6.15; N,
4.27.
5-Acetyl-2-hydroxy-4-(4-methylphenyl)-3,4,4a,9b-tetrahydro-2~-pyrano[3,2-~]indoie Compound
3b was treated as described
for compound
l:2); yield:40%, mp=210 “C (mixture of two diastereomers). Major diastereomer:
IH-NMR (DMSO-d6)
(13b).
13a and two diastereomers IR (KBr): v=3280(0-H),
were obtained
1630(C=O)cm-t.
: 6=1.60- I .75(m, IH, H3), I .69(s large, 3H, COCH,),
J=6.6, 14.7, H3), 2.20(s, 3H, CH,), 3.68( m, IH, H4), 4.84(t, lH, J=8.7, H&, J=8.7, Hgn), 6.46(d, IH, J=4.4. OH), 6.94-7.lO(m,
(ratio
4.91(m,
2.04(dt, I H,
IH, Hz), 5.64(d, IH,
5H, Hz,, H,,, H,,, He,, H7), 7.33(d, lH, J=7.3, Hy), 7.34(t,
lH, J=7.7, Hg), 7.82(d broad, lH, H,). Minor diasteromer:
rH-NMR (DMSO-d6)
CH,), 3.25(m, IH, H4), 4.78(dd, J=3.7, OH), 6.94-7.10(m,
:6=1.60-1.75(m,
IH, J=5.1, 8.7, H&,
2H, CH,),
1.69(s large, 3H, COCH3), 2.24(s, 3H,
5.23(m, IH, H2), 5.79(d, IH, J=8.7, H,h), 6.47(d, IH,
5H, Hz’, H,,, H,‘, H6,, H,), 7.34(t, IH, J=7.7, Hs), 7.37(d, IH, J=7.4, Hg), 7.83(d
large, IH, He). MS (WNH,)
: m/z=324 (M + I)+. Anal. Calc. for C,oH,,N07:
Found: C, 74.40; H. 6.38; N, 4.24.
C, 74.28 H, 6.55; N, 4.33.
Synthesis
and oxidation of pyrano[3,2-hlindoles
1001
REFERENCES
1.
Boger, D.L. In: Comprehensive
Organic Synthesis, Vol. 5; Trost, B.M.; Pergamon:
New York, 1991,
~451-512. Tietze, L.F.; Bachmann, J.; Wichmann, J.; Burkhard, 0. Synthesis, 1994, I 185- 1193. Tietze, L.F. Chem. Rev. 1996, 96, 115-136. Tietze, L.F.; Biefuss, U. Angew. Chem. Int., Ed. Eng. 1993,32, Tietze, L.F..Geissler, 2.
131-163.
H.; Fennen, J.; Brumby, T.; Brand, S.; Schulz, G. J. Org. Chem. 1994,59,
Schneider, C.; Montenbruck,
182-191
A. Angew. Chem. Int., Ed. Eng. 1994,33,980-982.
Tie&e, L.F.; Schneider, C.; Grote, A. Chem. Eur. J. 1996,2,
139-148.
3.
Ciufolini , M.A.; Byrne, N.E. J. Am. Chem. Sot. 1991, 113, 8016-8024.
4.
Marko, I.E.; Evans, G.R. Synlett. 1994,43 l-433.
5.
M&our, J.Y.; M&our, A. Synthesis 1994,767.769.
6.
Danishefsky,
I.
Tietze, L.F.; Hubsch, T.; Ott, C.; Kutcha, G.; Buback, M. Liehig Ann. 1995, l-7.
8.
Buback, M.; Abeln, J.; Hubsch,T.; Ott, C.; Tietze, L.F. Liebig Ann. 1995,9-l
S.; Bednarski, M. Tetrahedron Let?. 1984,25,721-724.
1.
Buback, M.; Kutcha, G.; Niklaus, A.; Henrich, M.; Tietze, L.F. Liebig Arm. 1996, 1151-l 158. 9.
Ager, D.J.: East, M.B. Tetrahedron 1993,49, 5683-5765.
10.
Coutts, S.J.; Wallace, T.W. Tetruhedron 1994,50,
11755-l 1784.
Wallace,
P.; Redhouse,
T.W.; Wardwell,
I.; Li, K.D.; Leening,
A.D.; Challand,
S.R. J. Chem. Sot.,
Perkin Trans. 1 1995, 2293-2308. 11.
Bourlot, AS.; Desarbre, E.; M&our, J.Y. Synthesis 1994,411-416.
12.
Desarbre, E.; Savelon, L.; Cornet, 0.; M&our, J.Y. Tetrahedron 1996,52,2983-2994.
13.
Buzas, A.; Mtrour, J.Y. Synthesis 1989,459-461
and references therein.
Stetinova, J.; Kovac, J. Collect. Czech. Chem. Comm. 1975,40. Patonay, T.; LCvai; A. Arch. &arm. 14.
The configuration
1994,327,
Z has been attributed
showing connectivities
18 I - 186.
according
to 2D NMR NOESY
experiments
The structure cis of the major diastereomer
16.
The configuration
of 3h has been precedently
wrongly attributed as truns.5
213~1~ of l-acetyl-2-benzylidene-2,3-dihydroindol-3-ones
the IH-NMR spectra and more particularly
has been attributed
the chemical shift of the CH,CO
versus 2.62 ppm for the E-isomers 17.
in acetone-d6
between the 1-H and the ortho protons of the phenyl substituent.
15.
examining
1750-1756.
An, Z.W.; Catellani, M.; Chiusoli, G.P. J. Organomet. Chem. 1990,397, C31-C32.
by
at 1.94 ppm
J.-Y. MBROUR et al.
1002
18.
Arduini, A.; Bosi, A.; Pochini, A.. Ungaro, R. Tetrahedron 1985,41, 3095-3103.
19.
Gassman, P.G.; Burns, S.J.; Pfister, K.B. J. Org. Chem. 1993,58,
20.
Hirata, F.; Hayaishi, 0. J. Biol. Chem. 1975,250,
21.
Hudlicky,
1449-1457.
5960-5966.
M. Oxidation in Organic Chemistry, American
Chemical
Society, Washington
D.C., 1990,
p 273. 22.
Hackmann, C.; Schafer, H.J. Tetrahedron 1993,49,4559-4579.
23.
We thank one of the referees for suggesting this mechanism
24.
Bascop, S.I.; Sapi, J.; Laronze, J.Y.; Levy, J. Heterocycles 1994,38,725-732.
25.
Mateo, C.A.; Urrutia, A.; Rodriguez, J.G.; Fonseca, I.; Cano, F.H. J. Org. Chem. 1996,61,810-812.
26.
of oxidation.
Rodriguez, J.G.; And&s, A.S. J. Heterocyclic Chem. 1991,28,
1293-1299.
Takayama,
M.; Aimi, N.; Sakai; S-I. Heterocycles
H.; Kurihara, M.; Subhadhirasakul,
S.; Kitajima,
1996,42, 87-92. 27.
Grieco, P.A.; Oguri, T.; Yokoyama, Y. Tetrahedron Lett. 1978, 19,419-420.
28.
Sevodin, V.P.; Veleszheva,
V.S.; Suvorov, N.N. Khim. Geterotsikl. Soedin 1981, 368-371. Chem. Abstr.
1981,95, 24878e. 29.
Kawasaki,
T.; Nonaka,
Y.; Kobayashi
, M.; Sakamoto,
2445-2448.
(Received in Belgium 25 July 1996; accepted 6 November 1996)
M. J. Chem. Sot.,
Perkin
Trans. 1 1991,
53, No. 3, pp. 987-1002,
Copyright
CY CLOADDITIONS:
PYRAN0[3,2d]INDOLES
1996 Elsevier
Pnnted in Great Britain.
PII: SOO40-4020(96)01040-X
HETERODIENE
0
1991
Scw~ce Ltd
All rights reserved
0040.4020/97
$17.00
+ 0.00
SYNTHESIS AND OXIDATION OF
INTO SPIRO DERIVATIVES
Jean-Yves M&our*, Ahmed Mamai, BCatrice Malapel, Philippe Gadonneix
Instttut
Organique et Analytique, assock? au
de Chimie
Orl&ins
C&x
Abstract:
l-Acetyl-2-benzyltdene-2,3-dihydroindol-3-ones
to afford
substituted
pyrano[3&b]indoles;
spirolactones
or to 0x0 acetals
Copyright
1996
0
Elsevier
with
Science
compounds
in the presence
reagents.3-6 dihydropyrans
High
of dihydropyrans;
pressure
also
vinyl
d’OrlCans,
ethers
oxidized,
of boron
and vmyl
using
45067
Jones
thioethers reagent,
to
trifluoride.
considerably
reactions (IEDDA)t,z a well-established
were catalyzed
accelerates
the
of electron rich and a powerful
by Lewis acids and lanthanides
Diels-Alder
or pyridines.
reactions;7,8
the
substituted
Tietze2 reported on asymmetric
using IEDDA in a key step of their synthesis.
has reported on the reactivity of chromones,
with electron-withdrawing
substituents,
in IEDDA reactions with vinyl ether. We wish to report here the synthesis of new pyrano[3,2-blindoles examine their reactivity towards oxidation in order to obtain lactonic derivatives. 2 position of 1-acetyl-lH-indol-3(2H)-onet1~12
aldol condensation
of 1-acetyl-lH-indol-3(2H)-one
with electron-rich
olefins
vinylsulfide
diastereomers
(1) (mixture of E/Z-isomers),
cisltmns,
days
with substituted
(except for 3f,g) (Scheme]).
obtained
and to of the C-
Cycloaddition
was performed
2d
Fax: 33 0238417281 E-mail: [email protected] Dedicated to Professor Wuldemar Adam on the occasion of his 60th birrhdq. 987
to an
reacted as heterodienes
3 as a mixture
of
at 110 “C in a sealed tube
2. The yields were high except for the phenyl vinylsulfide
of 24 h at 110 “C. The keteneacetal
according
(2a), 1-(4-methoxy)benzyloxyethene
(2d) to afford the cycloadducts
(2~) or 1, I-diethoxyethene
at 135 “C instead
benzaldehydes,l3
such as 1-ethoxyethene, 5 I-benzyloxyethene
with a large excess of dienophile
The easy oxidability
can interfere during the oxidation of cyclic ketals 3.
I-Acetyl-2-benzylidene-2,3-dihydroindol-3.ones
(2b), phenyl
1,6-
in the synthesis of carbohydrates.
We have recently described the synthesis of &carboline$ Also recently, Wallaceto
Universttk
has become
these reactions
formed give easy access to carbohydrates9
induction with chiral oxabutadienes
with
were
Diels-Alder
such as enol ethers, with I-oxa-1,3-butadienes
method for the synthesis
6759,
Ltd
The inverse electron demand (LUMOdiene- controlled) dienophiles,
BP
reacted
these
m-CPBA
CNRS,
2. France
2c which needed 6
(I,]-diethoxyethene)
was
highly
988
J.-Y. MBROUR et ~1
nucleophilic
and was the most reactive one. These IEDDA reactions worked only in the presence of a catalytic
amount (5%) of ytterbium salt, Yb(fod)3.3
CH,= Cm’)R3 2 Yb (fad), , 11 O’C t 50
98%
la R’ = 0CH3
3
lb R’ = CH, lc R’=H
Compound
R2
Rt
R’
Yield (%)
mp”C Oil
cis/trans (S)
3a
4-OCH, OBn
H
98
3b
4-CH,
OBn
H
98
113a
81/19
3c
4-CH,
OPMB
H
95
oil
85115
3d
4-OCH, SC,H,
H
53
oil
51143
3e
4-CH,
SC,H,
H
50
oil
62138
3f
4-CH,
OC*H,
OC,H,
92
oil
3g
4-H
OC>H,
OC,H,
75
oil
3h
4-OCH, OC,H,
H
98
oil
3i 4-CH, a major diastereomer cis.
WI5
84116
H 98 125a OC,H, Bn = Renzyl; PMB = 4-methoxybenzyi.
86114
Scheme I The use of methoxyallene diastereomers) Disubstituted
as dienophile
afforded
in only 40% yield due to polymerisation dienophiles
like 2$dihydropyran
(20%). No reaction occurred with vinylidene to its low energy HOMO. I ,4-Benzodioxin
afforded
the cycloadduct
4a
of the methoxyallene the cycloadduct
(ratio
66133 for the two
even at 50 “C (Figure
Sa (Figure
carbonate. The lack of the reactivity of this dienophile
was also unproductive
0' 5a
4a Figure 1
can be due
as dienophile in these cycloadditions.
of&
:&o,
I). 1,2-
I) but in a low yield
Synthesis
For all the cycloadducts endo/exo
configuration
of the anomeric (equatorial).
3a-e,
3h,i the major diastereomers
or respectively
proton
and oxidation of pyrano[3,2-hlindoles
cis/n~ns
Hz and its coupling
The major diastereomer
989
have the same relative configuration.
has been tentatively attributed by examining constants
with the inequivalent
has always a more deshielded
protons
The
the chemical shift
H,,
(axial) and H,,
Hz (6=5.36 ppm VERSUS5.27 ppm for 3a)
indicating an axial position for the ethoxy group but the coupling constant J2+ = 5. I Hz is only slightly inferior to J gsa = 5.9 Hz (minor diastereomer)
3a; the aspect of the signals
for compound
of the Hja and H3, also
depended on the value of the coupling constant, frans or cis, with the Ha (J3e4 = 7.2 Hz, J2a4 = 5.4 Hz) for the presumed
compound
ROESY experiments) pseudo
these two values were close and may be confusing.
indicated connectivities
planarity
of the pyrano
ring has an infhience
reported were not conclusive.
In order to have more information ethyl vinylether
and
on interactions
The major diastereomer
through
space since
the
the different
might be cis and the minor truns based on
[47c+ 2711since the Z-isomer should give the endo (c-is) cycloadduct.
the usual tenets of cycloaddition
we reacted the Z-4-methoxybenzylidene-2,3-dihydroindol-3.onet4
with
3j (80% yield) from an endo process
(Figure 2);
which afforded the expected cis cycloadduct
only a trace amount of the truns diastereomer
is observed
medium (K,CO,
/ethanol/HzO,
3j as a unique
cis diastereomer
= 9.4 Hz). The deacetylation
50°C. lh30, 67% yield) of the major diastereomer which confirms
of 3j is easily
(~5% yield). The cis configuration
assigned using tH NMR (Jzie = 1.8 Hz, J2Ja = 8.2 Hz, Jse4 = 6.8 Hz, J,,
cycloadduct
2Q NMR (NOESY
of the H, with Hga and to a some extend with H3e for the major
of 3a; for H, the presence of the 0CH2 signal with the same chemical shift was disturbing;
cis diastereomer
connectivities
cis-3a;
the cis configuration
in basic
of 3h15 afforded compound
of the major diastereomer
of the
3 obtained from la-c.
3.j
3h
/O
Figure 2
As reported previously
afforded respectively (compound
Id
isomerisation material
the ratio of diastereomers
in the cycloadduct
of the starting material 1 (which was predominantly
stereochemistry
the major cis diastereomer
of 3a, 3d in 85%, 57% yield; even starting from pure Z-isomer
R1 = NOz) gave also a mixture of cis and tram cycloadducts in the mixture, by Lewis acid Yb 3+, of the diastereomeric
1. It has been discussed
by Tietze 1 that isomerisation
reaction
configuration
and the exe or endo nature of the process; (the endo-E-syn-TS
products.
could occur with the possibility
of four transition
3). Some reports3 indicated in these cycloadditions
3. This can be due to an
cycloadducts
of the
cycloaddition
the cis-adduct
3 was not directly related to the
Z) t6,17; for example la (79% Z-isomer)
and/or of the starting
I-oxa-1,3-butadiene states according
and the exo-Z-syn-TS
the formation
during
the
to the E and Z would give
of a 1:l mixture of cisltrans
990
J.-Y. MBROURet al.
The population the coupling position
of the two conformers
constants
of the cis diastereomer
Jasa and Jsa4; for compound
for the 4-phenyl
and the 2-ethoxy
can be discussed by examining the values of
3j the values of these constants
group. A different
behavior
where a decrease of the coupling constants J 23aand Jas4 indicates
indicate
an equatorial
is shown by the other cycloadducts
a significant
contributionla
of the conformer
having the 2-ethoxy and the 4-phenyl group in axial position. (Scheme 2)
dc2J% Scheme 2 Compounds anomeric
3 were slightly different
carbon by TMSCN
(TMSOTf)
in the presence
corresponding
failed in presence
of a non-nucleophilic
the 2-position
hydroxylation in carbohydrate reactions
Treatment
of compound
base as N,N-diisopropylethylamine
in 2-position chemistry
for some years the oxidation
of indolic compounds
was sensitive
of I-substituted-lH-indol-3(2H)-ones. we submitted
the compounds
we have worked on pure diastereomer
diastereomers,
from usual acetals since nucleophilic
of TMSOTf.
attack on the
3 with Lewis acids
also failed to give the
enol ethers.19
We have been exploring process;*0
in reactivity
of indoles
which was an important
towards oxidation
1lvl* Using oxidation procedures
3h,i to a Jones oxidation*lg**
3i
E!%z!?a,
6h
RIzCH~~
R’=OCH3
6i Rl=CH3
\
F
R’
developed
(For the oxidation
cis or tram). We obtained only spirolactones
and not the expected lactones 7h,i (Scheme 3).
&a,
biological
and we have reported on the
6h,i, as single
Synthesis
The cis or truransdiastereomer or trans diastereomer mechanism23
and oxidation of pyrano[3,2-blindoles
of 3h afforded the same unique diasteromeric
of 3i gave the same diastereomeric
(Scheme 4) involving
initial epoxidation.
opening of the pyrano ring generates the intermediate to the Spiro compound
991
lactone 6h; similarly the cis
lactone 6i. These results were consistent
with a
The opening of the oxirane ring with a concomitant
oxonium ion (A). This oxonium ion may evoluate either
8 which is further oxidised to the lactone 6 or to an hydroxyaldehyde
which affords 6
after an oxidation via its hemiacetal. We have also shown that compound 8 gave product 6 under similar Jones oxidation.
3h,i
H30+
6h,i
Scheme 4
This type of Spiro structure was found in some oxindole alkaloids like Horsfiline24 which possess a 3,3Spiro structure; 2,2-Spiro pseudoindoxyl mitragynine
pseudoindoxyl
structure was encountered
Oxidation of 3h,i was also performed of BF3 etherate at room temperature The major diastereomer mixture of diastereomers of compound
pseudoindoxy125
or in
using meraperchlorobenzoic
acid in presence of a catalytic amount
as reported for the oxidation of cyclic acetals into lactones.27
(cis) of 3h afforded the rearranged
ketonic cyclic acetal 8h in 58% yield as a
in the ratio 1:3 and not the lactone 7h. (Scheme 3). Similarly the major diastereomer
3i gave 8i in 68% yield (mixture
afforded, in the same oxidation conditions, plausible mechanism
in tetrahydrocarbazole
alkaloid.26
for this transformation
of diastereomers
1:6). The minor diasteromer
a mixture of products 6h, Sh, 9h approximately of 3h,i into Sh,i was first the epoxidation
(trans)
of 3h
in the same ratio. A of the ethylenic
bond
J.-Y. MBROUR et al.
992
followed
by opening
intramolecular
of the oxirane after complexation
nucleophilic
displacement
(Scheme 5). This mechanism
of the Lewis acid BF3 (oxonium
the two diastereomers
cannot explain the mixture of epimers. Another possibility
pathways proceeding
A direct
which may occur via an attack of the anomeric carbon to afford Sh,i
may differentiate
discrete steps and that the rate-determining
species).
of the starting materials
is simply that the rearrangement
step differs from one diastereomer
3h or 3i but
proceeds via several
to the other one despite both
through an oxonium ion such as A (Scheme 4).
M = BF3-
Sh,i Scheme 5
It is noteworthy single diastereomeric
that the 0x0 acetal 8i (major diastereoisomer)
is oxidized by Jones reagent to the same
0x0 lactone 6i obtained previously.
TMSOTf m-CPBA
BF3
(W,),O * 40%
0
\
CF&OOH
CHO
.
63%
Scheme 6 The use of a stronger Lewis acid like TMSOTf in the oxidation procedure,
instead of BF3, afforded the
Synthesis
keto esters 9h,i in 51% and 60% yield respectively dihydropyran
as single diastereomers
6). The opening
presence of a protonic acid like trifluoroacetic Compounds
which cannot be directly alkylated.29
Another
route to obtain lactones 3a (diastereomer
3i afforded the acetal 1Oi; in
as the result of a formal alkylation in 2-position
lH-indol-3(2H)-one
3a,b. Compound
of compound
acid the unmasked aldehyde28 lli was obtained from 3i.
9i, lOi, lli may be considered
alternative
7h,i was to prepare
cis) in methanol,
13b respectively
under a hydrogen
atmosphere,
in presence
of of
in 37% yield, rather than
(Scheme 7). Using a 100% weight of Pd/C 10% allowed us to obtain the indoline lactol 13a or in 42% and 40% yield as a mixture of diastereomers
be obtained from 12a by hydrogenolysis moiety was in this case particularly
sensitive to hydrogenation
substituent)
was readily transformed
presence
(10% weight),
of 10% PdK
substituent
of low stability. Compound
13a can also
of the benzyl group with a 100% weight of Pd/C (10%). The indole
instead of a benzyloxy
methoxybenzyl
of l-acetyl-
first a lactol by hydrogenolysis
10% (10% weightj was reduced into indoline derivative 12a (one diastereomer)
hydrogenolysed
of the
of the ethylenic
species to the carboxylic acid ester by the peracid (Scheme 6).
In the absence of oxidant, treatment with BF3 etheratelethanol
PdK
(Scheme
ring was, in this case, the first step of the oxidation instead of the epoxidation
bond, followed by oxidation of the carboxonium
compounds
993
and oxidation of pyrano[3,2-blindoles
since compound
3i (with an ethoxy substituent
into the corresponding
in the same conditions
indoline derivative
as for 12a. CA!! or DDQ oxidation
of the 4-
of compound 3c was unfruitful. OBn
OBn
HO
3”i? H
:I
oL
3a 3b
I_\
R’
12a
R’=OCHj
I
R’ = CH,
Hz/Pd
Scheme 7
In summary we have extended the [47t + 27~1cycloaddition one to different dienophiles
and prepared spiroindolic
compounds
of 1-acetyl-2-benzylidene-2,3-dihydroindol-3which were interesting intermediates.
12i in
J.-Y. MBROUR et al.
994
EXPERIMENTAL
PART
Melting points were determined recorded on a Perkin Elmer tetramethylsilane expressed
using a Kofler apparatus hot stage and were uncorrected.
1330. lH-NMR
as the internal standard
spectra were recorded
for solutions
in deuteriochloroform
on a Bruker AM 300 (300 MHz) and coupling
in Hertz. Mass spectra were obtained using chemical
ionisation
IR spectra were
(ammonia)
constants
on a Nermag
with were IO-1OC
apparatus.
IEDDA Reactions. General Procedure 1 (1.9 mmol) were dissolved
Compounds
in CH,Cl,
(2 ml) and vinylether
2 (1.5 ml) in presence
of
Yb(fod)3 (0.095 mmol); the mixture was heated in a sealed tube at 110 “C during 24 h (2a, 2b), at 135 “C during 6 d for 2c or at 90 “C for 20 h for 2d. Evaporation chromatographed
of the solvent under vacno gave an oil which was
on a silica gel column (230/400 mesh) using CH2C12/petroleum
of two diastereomers
ether 1: I as eluent; a mixture
was obtained; (see Scheme I, Table 1).
5-Acetyl-2-methoxy-4-(4-methoxyphenyl)-3-methylene-3,4-dihydro-2H-pyrano[3,2-b]indole Methoxyallene
(1.5 g, 21.4 mmol) was reacted on compound
50 “C during IO d in presence chromatographed diastereomers
of Yb(fod),
la (293 mg, 1 mmol) in CH,CI,
(32 mg, 0.030 mmol). After evaporation,
on a silica gel column (eluent: CH$l$petroleum
(1 ml) at
the residue was twice
ether 1:l) giving an oil as a mixture of
(ratio 66:33); yield: 145 mg (40%). IR (film): v=l68O(C=O) cm-t.
Major diastereomer:
lH-NMR (CDC13) : 6=2.41(s, 3H, CH,), 3.24(s, 3H, COCH,),
5.29, 5.33, 5.42(4s, 4xlH,
lH, J=l.4, 7.3, Hg), 7.98(d, IH, J=7.3, Hg).
Minor diastereomer:
(CD+)
tH-NMR
5.18, 5.31, 5.32(4s, 4xlH,
: 6=2.38(s, 3H, CH3), 3.55(s, 3H, COCHj), 3.72(s, 3H, OCH& 4.88,
HZ, H,, =CH,),
7.30(m, 2H, H7, HS), 755(dd, Anal. Calc. for C,,H21N0,:
6.76(d, 2H, J=8.8, H3’, HS’), 6.94(d, 2H, J=8.8, HZ’ , He), 7.20-
IH, J=2.0, 8.0, Hg), 7.93(d, lH, J=8.1, He). MS (U/NH,)
la (200 mg, 0.68 mmol) with dihydropyran
on a silica gel column (eluent: CH2C12/petroleum cm-t.
5,6]pyrano[3,2-blindole
(Sa).
(2 g, 24 mmol) were heated at 140 “C in presence
(40 mg, 0.038 mmol) during 8 d. After evaporation
IR (KBr): v=1695(C=O)
: m/z = 364(M+l)+.
C, 72.71; H, 5.82; N, 3.85. Found: C, 72.90; H, 5.67; N, 3.91.
6-Acetyl-5-(4-methoxyphenyl)-2,3,4,4a,S,lla-hexahydropyrano[3’,2’: Compound
3.69(s, 3H, OCHj), 5.18,
H,, H,, =CH,), 6.70(d, 2H, J = 8.8, H,’ ) HSn), 6.99(d, 2H, J=8.8, Hz* 3He’), 7.22-
7.33(m, 2H, H7, H8)~7.58(dd,
of Yb(fod),
(4a).
under vucuo the residue was chromatographed
ether 3: 1); yield:62 mg (24%). mp=149 “C (ethanol/water).
‘H-NMR (CDCI-,) : &1.60-1.82(m,
4H, CH,CH,),
2.09(m, lH, Haa), 2.41(s,
3H, COCH3), 3.70(s, 3H, OCH,), 3.70(m, lH, OCH,), 4.02(m, lH, OCH,), 4.31(s, lH, HS), 5.32(d, IH, J=2.2,
Synthesis
HI,,),
6.Wd,
2H, J=8.8,
8.0, Hlo), 7.99(d,
H,,, Hs~), 6.92(d,
lH, J=8.0,
995
of pyrano[3,2-blindoles
2H, J=8.8,
H7). MS (CVNH,)
6.14; N, 3.71. Found: C, 72.90;
Table 1. Compounds
and oxidation
Hz’, Hg), 7.23-7.33(m,
2H, Hg, Hg), 764(dd,
: m/z=378 (M + I)+. Anal. Calc. for Cz3Hz3N04:
lH, J=1.5, C, 73.19;
H, 5.99; N, 3.91.
3 Prepared
680a
Diastereomer
Z=O)
H3, J=2.4, J=6.8, J=13.5),
cis: 2.24(dt, lH, H3, J=5.1, J=13.5), 2.32(s, 3H, AC), 2,50(ddd,
J=11.9), 4.59(t,
3.69(s,
3H, OCH3),
lH, H4, J=6.0), 5.36(dd,
4.58 and 4.86(2s,
2xlH,
lH,
OCH2,
lH, H2, J=2.4, J=5.1), 6.67(d, 2H, Hg’,
H5’, J=8.7), 6.90(d, 2H, H2’, H6’, J=8.7), 7.06-7.32(m,
7H, Harom),
7.57(d, lH,
H9, J=6.5), 8.04(d, lH, H6, J=S.O). Diastereomer
2.00(ddd,
trms:
lH, H3, J=2.2,
J=7.1, J=13.8),
2.29(s,
3H, AC),
2.44(dt, lH, H3, J=5.6, J=13.8), 3.71(s, 3H, OCH3), 4.59(t, lH, H4, J=6.3), 4.67 et 4.92(2s,
2xlH,
0CH2,
J=11.9),
5.27(dd,
lH, H2, J=2.2, J=5.6), 6.76(d, 2H, Hg’,
H5’, J=8.7), 6.94(d, 2H, H2’, H6’, J=8.7), 7.06-7.32(m,
7H, Ha,,,),
7.57(d, lH,
H9, J=6.5), 8.04(d, lH, H6, J=B.O). 680b
Diastereomer
C=O)
AC), 2.51(ddd,
cis: 2.24(s, 3H, CH3), 2.25(dt,
lH, H3, J=2.2, J=7.35, J=14.0),
J=12.5),
lH, H4, J=6.2), 5.36(dd,
4.61(t,
H5’, J=8.1),
6.96(d,
Diastereomer
3H, AC), 2.46(dt,
4.64 and 4.87(2s,
2.32(s, 3H,
2xlH,
OCH2,
7.05-7.33(m,
7H, H7, H8, Harom),
8.05(d, IH, H6, J=8.1).
trans: 6=2.01(ddd,
CH3), 2.29(s,
4.59 and 4.88(2s,
lH, H2, J=2.2, J=5.1), 6.88(d, 2H, Hg’,
2H, H2’, H6’, J=S.l),
7.57(d, lH, H9, J=S.l),
lH, H3, J=5.1, J=13.5),
2xlH,
lH,
H3, J=2.2,
J=6.6,
lH, Hg, J=5.9, J=13.2),
OCH2, J=12.5), 5.27(dd,
2H, H2’, H6’, J=8.1), 7.15-7.33(m,
7H, Ha,,,),
J=13.2),
4.62(t,
2.26(s,
3H,
lH, H4, J=6.2),
lH, H2, J=2.2, J=5.9), 7.04(d, 7.57(d, lH, H9, J=7.3),
8.05(d,
lH, H6, ]=7.3). iC
690a
Diastereomer
C=O)
AC), 2.45(ddd, J=6.6),
cis: 2.17(dt,
lH, H3, J=5.9, J=13.9), 2.21(s, 3H, CH3), 2.28(s, 3H,
lH, H3, J=2.2, J=7.3, J=13.9), 3.69(s, 3H, OCH3), 4.55(t, lH, H4,
4.64, 4.87(2d,
2xlH,
0CH2,
J=11.7),
5.30(dd,
lH,
6.72(d, 2H, H3”, H5”, J=8.8), 6.83(d, 2H, H3’, H5’, J=S.l), J=8.1), 7.02(d, 2H, H2”, H6”, J=8.8), 7.15-7.30(m,
H2, J=2.2,
J=5.9).
6.93(d, 2H, H2’, H6’.
2H, H7, H8), 7.55(dd,
lH, H9.
J=6.6, J=2.2), 8.02(d, lH, H6, J=7.3). Diastereomer 2.29(s, 4.85(2d, J=5.9),
3H,
tram:
2xlH, 6.80(d,
lH,
OCH2, J=11.7), 2H, H3:
H2’, H6’, J=S.l), 7.57(dd,
1.99(ddd,
AC), 2.42(dt,
lH, H3, J=2.2, J=7.3, J=13.9), H3, J=5.9,
3.74(s,
2.26(s, 3H, CH3), 3H, OCH3),
4.61(t, lH, H4, J=6.6), 5.25(dd,
H5”, J=S.l),
7.20-7.33(m,
J=13.9),
lH, H2, J=2.2
6.91(d, 2H, Hg’, H5’, J=S.l),
2H, H7,
H8),
7.23(d,
lH, H9, J=7.3, J=1.5), 8.06(d, lH, H6, J=7.3).
2H,
4.57,
7.04(d, 2H
H2”, H6”, J=8.1)
12(M+l)+
H,
J.-Y.
996
Id
MBROUR et al.
1690”
Diastereomer
C=O)
J=2.9, J=7.3, J=14.4), 4.66(t, lH, H4, J=7.3), 5.62(dd,
cis: 2.19-2.29(m, lH, Hg), 2.32(s, 3H, AC), 2.76(ddd,
lH, H3,
lH, H2, J=2.9, J=S.l),
6.75(d, 2H, H3’, H5’, J=S.S), 6.95(d, 2H, H2’, Hg’, J=B.B), 7.99(d, lH, H6, J=S.S), 7.20.7.60(m, BH, H7, H8, H9, SPh). Diastereomer
truns: 2.19-2.29(m, lH, Hg), 2.36(s, 3H, AC), 2.4%2.60(m, lH,
H3), 3.71(s, 3H, OCH3), 4.65(t, lH, H4, J=5.1), 5.48(dd, lH, H2, J=2.9, J=8.86), 6.77(d, 2H, H3’, H5’, J-8.8), 6.95(d, 2H, H2’, Hg’, J=S.S), 7.20-7.60(m, BH, H7, H8, H9, SPh), 8.02(d, lH, H6, J=8.8) Le
69Ob
Diastereomer
C=O)
2.77(ddd, lH, H3, J=2.9, J=7.3, J=13.9), 4.66(t, lH, H4, J=7.3), 5.61(dd, lH, H2,
cis: 2.17.2.30(m, lH, Hg), 2.25(s, 3H, CH3), 2.31(s, 3H, AC),
J=2.9, J=8.8), 6.91(d, 2H, H3’, H5’, J=S.l), 7.01(d, 2H, H2’, Hg’, J=S.l), 7.197.60(m, BH, H7, H8, H9, SPh), 7.98(d, lH, H6, J=S.l). trarzs: 2.17-2.3(m,
Diastereomer 2.49-2.59(m,
lH,
H3), 4.66(t,
6.92(d, 2H, H3’, H5’, J=S.l),
lH, lH,
H3), 2.25(s,
H4, J=7.3),
3H, CH3),
5.48(dd,
lH,
7.04(d, 2H, H2’, Hg’, J=S.l),
2.35(s,
3H, AC),
H2, J=2.9,
7.19-7.60(m,
J=B.B), BH, H7,
H8, H9, SPh), B.Ol(d, lH, H6, J=S.O).
690a
1.10 and l.l1(2t,
2x3H, 2xCH3, J=7.3), 2.04(dd, lH, H3, J=7.0, J=13.6), 2.24 and
C=O)
2.26(2s, 2x3H, AC, CH3), 2.54(dd, 6.90(d, 2H, H3’, H5’, J=S.l),
lH, H3, J=8.4, J=13.6), 4.57(t, lH, H4, J=7.7),
7.01(d, 2H, H2’, Hg’, J=B.l),
7.19-7.31(m,
2H, H7,
H8), 7.59(d, lH, H9, J=B.l), 8.02(d, lH, H6, J=S.l).
k
.690a
1.09 and l.l3(2t,
C=O)
3H, AC), 2.57(dd,
2x3H, 2xCH3, J=7.3), 2.09(dd, lH, H3, J=8.4, J=13.6), lH, H3, J=7.0, J=13.6),
3.46-3.82(m,
lH, H4, J=7.3), 7.00-7.35(m, 7H, H7, Hg
Harom),
2x2H, 2xOCH2),
380(M+l)+
2.23(s, 4.64(t,
7.61(d, lH, H9, J=7.0),
B.OO(d,lH, H6, J=B.l). ‘j
i400a
Diastereomer
NH)
J3a3e=13.6), 2.47(ddd,
cis: 1.29(t, 3H, CH, J=7.3), 2.27((m, lH, Hg,, J2sa=8.2, J~~4’9.4, lH, Hze, JzJe= 18, J3e4=6.8, J~~3~=13.6), 3.82 (m, IH,
OCH2), 4.11(s, 3H, OCH3), 4.17 (m, lH, OCH2), 4.33(dd, lH, H4, J~~4’6.8, J3a4=9.4), 5.31(dd, lH, H2, J~3~=l.8, J2sa=8.2), 7.15(d, 2H, H2’, Hg’, J=S.l), ]7.05-7.20(m, Ic = CH$O,
6H, Harom, NH); 7.63(d, lH, Harom, J=S).
a film, b KBr.
l-Acetyl-3’-(4-methoxyphenyl)-2’,3’,4’,S’-tetrahydrospiro[indole-2(3~)-2’-furan]-3,S’-dione Compound
3hs as a single trans or cis diastereomer
(6h).
(1 IO mg, 0.3 mmol) was dissolved
in acetone (3 ml)
at 0 “C; Jones reagent21 was dropwise added till all 3h has reacted (circcc 30 min). Excess of the oxidant was destroyed
with isopropanol;
the solution was filtered on celite and evaporated;
water and CH,C12 and the organic layer was dried over MgSO,; chromatographed
on
a silica
gel
column
(eluent:
evaporation
CH2C12/petroleum
the residue was treated with in vucuo left an oil which was
ether
5:l);
yield:44mg
(4270),
Synthesis
mp=70 “C. IR (KBr): v= ISlO(C=O), 3.OO(dd, lH, J=l2.5,
and oxidation of pyrano[3,2-blindoles
997
173O(C=O), 168O(C=O) cm-l. IH-NMR (CDCI,) : 6=2.5.5(s, 3H, CH,),
16.9, H4.). 3.65(s, 3H, OCH,), 3.68(dd,
IH, 5=8X, 16.9, H4’), 4.49(dd,
IH, J=8.8, 12.5,
H3’), 6.63(d, 2H, J=8.8. H3”, HS,,), 6.97(d. 2H, J=8.8, HZ”, Hs.e), 7.04(t, IH. J=7.3, HS), 7.39(d, lH, J=7.3, H7), 7.56(t,
lH, J=7.3, Hg), 8.14(d,
IH, J=8.1, H,).
I%-NMR
(CDCI,)
: 6=25.8(CH,),
32,O(C4’), 45.3(C3’),
96.O(C2), 1 13&C3”, C5”), 117.1(C7), 120.O(C3a), 124.1 (C4), 124.2(C 1‘I), 124,9(C5), 129,2(C2”,
55.O(OCH$,
C6”), 138.9(C6),
152.6(C7a),
158.8(C4”), 168.9(C=O C5’). 172.9(C=O AC), 194.4(C=O C3). MS (Cl/NH,)
:
m/z=352 (M +I)+. Anal. Calc. for CZ0H,7NOs: C, 68.37; H, 4.88; N, 3.99. Found: C, 68.62; H. 4.68; N, 3.92.
l-Acetyl-3’-(4-methyIphenyl)-2’,3’,4’,5’-tetrahydrospiro[indole-2(3~),2’-furan]-3,S’-dione Same procedure v=l SlO(C=O),
as described
(6i).
for 6h starting from 3i5; yield:61%. mp=62 “C (ethanol/water).
IR (KBr):
173O(C=O). 1685(C=O) cm-l. IH-NMR (CDCI?) : 6= 2.1 l(s, 3H, CH,), 2.53(s, 3H. COCH,),
2.97(dd. IH, J=l2.9,
17.6, H4’), 3.65(dd, III, J=8.8, 17.6, H4.)>4.49(dd, IH, J=8.8, 12.9, H3,), 6.87(d. 2H. J=8.1,
H,,,, HS*,), 6.9l(d, 2H, J=8.1. H,,‘, H,,,), 7.00(t, IH, J=7.3, HS), 7.35(d, IH, J=7.3, H7), 7.53(dt, IH, J=2.5, 8.1, Hb), 8.1 l(d, IH, 5=8X, H4). Anal. Calc. for C2~~H1,N04: C. 71.63; H. 5.1 1; N, 4.18. Found: C, 71.72; H, 5.28; N, 4.03.
l-Acetyl-5’-ethoxy-3’-(4-methoxyphenyl)-2’,3’,4’,S’-tetrahydrospiro[indole-2(3~),2’-furan]-3-one Compound and m-CPBA temperature.
3h (250 mg, 0.685 mmol) was dissolved in CH,C12 (3.5 ml); BF,, Et,0
(142 mg, 0.822 mmol) were successively
Ether (25 ml) was added, then the mixture was sequentially
ml), saturated NaHC03
(0.04 ml, 0.33 mmol)
was stirred 2 h at room
treated with aqueous 5% Na2S0,
(10 ml) and brine ( 10 ml). The organic layer was dried over MgSO,
The obtained residue was chromatographed diastereomers
added and the solution
(Sh).
were obtained
and evaporated.
on a silica gel column (eluent: petroleum ether /CH,Cl,
in the ratio 1:3; yield:149 mg (58’%,) mp=l40
(15
“C (ethanol),(major
3:7). Two isomer). IR
(KBr): v=172O(C=O), 1675(C=O) cm-l. Major diastereomer: 3H, CH,), 3.37(dt,
IH-NMR (CDCI,)
: 6=1.2l(t, 3H, J=7.0, CH,), 2.24(dd, IH, J=l3.3, J=7.3, H,‘), 2.69(s,
IH, J=6.6, 13.3, Hq’), 3.58(dq,
J=7.0, 9.7, OCH,), 4.19(dd,
IH, J=7.0, 9.7, OCH$,
3.59(s. 3H, OCH,),
3.86(dq,
IH, J=7.3, 13.3, H3e), 5.63(d, IH, J=6.6, HSt), 6.55(d, 2H, J=9.0, H3”, H,,,), 6.91(t,
IH, J=7.3, HS), 6.93(d, 2H, J=9.0, H,,,, He’.), 7.27(d, IH, J=7.3, H7), 7.44(t, IH, .l=7.3, Hg). 8.4l(d, H4). ‘3C-NMR (CDCI,): 6=14.9(CH,). 113.8(C3”, C5” PhOMe),
IH,
1 l8.4(C7),
34.6(C4’), 46.5(C3’), 55,0(OCH3). 64.l(OCH,), 12l.O(C3a), 123.4(C4), 124.l(C5).
IH, J=9.0.
lOO.O(C2), 104.6(C5’),
124.4(Cl” PhOMe),
128.8(C2”, C6”),
137.5(C6), 153.4(C7a). 158.9(C4”), 17O.l(C=O ), 198.O(C=O C3). Minor diastereomer:
IH-NMR
(CDC13) : 6=1.24(t, 3H, J=7.0, CH3), 2.53(m,
3.04(dt, IH, J=7.3, 13.2, H,,), 3.59(s, 3H, OCH,), OCH$, 4.14(dd,
3.63(dq,
IH, H4’), 2.54(s, 3H, CH3),
IH, J=7.0, 9.5, OCH;?), 3.86(dq,
IH, J=7.0, 9.5,
IH, J=7.3, 13.2, H3’), 5.69(dd, IH. J=5.1, 7.3, HS,), 6.54(d, 2H, J=8.8, H,,‘, H,,,), 6.92(t, IH,
J.-Y. MI~ROUR et al.
998
J=7.3, H5), 6.94(d, 2H, J=8.8, Hz*,, He”), 7.30(d, IH, J=8.1, H7), 7.45(t, IH, J=8.1, He), 8.13(d large, IH, Hd). MS (CI/NH$
: m/z=382 (M + I)+. Anal. Calc. for C,,H,,NO,:
C, 69.28; H, 6.08; N, 3.67. Found: C, 69.47; H,
5.95; N, 3.83.
l-Acetyl-5’-ethoxy-3’-(4-methylphenyl)-2’,3’,4’,5’-tetrahydrospiro[indole-2(3H),2’-furan]-3-one Same procedure
as described
for 8h starting from the major diastereomer
obtained in the ratio 1:6; yield=68%,
mp=l16
(8i).
of 3i. Two diastereomers
“C (ethanol), (major diastereomer
were
). JR (KBr): v=172O(C=O),
167O(C=O ) cm-t. tH-NMR (CDCl,) : 6=1.20(t, 3H, J=7.3, CH,), 2.07(s, 3H, CH,), 2.24(dd, lH, J=13.2, 7.3,
Major diastereomer:
Ha,), 2.69(s, 3H, CH,), 3.40(dt, lH, J=5.9, 13.2, H4’), 357(dq, OCH,), 4.21(dd,
lH, J=7.3, 9.5, OCH,), 3.85(dq, lH, J=7.3, 9.5,
lH, J=7.3, 13.2, Hjs), 5.62(d, IH, J=5.9, Hg’), 6.80(d, 2H, J=8.0, H,jj , HStt), 6.89(t, IH, J=7.3,
HS), 6.90(d, 2H, J=8.0, H,‘!, H,,‘), 7.26(d, lH, J=7.3, H7), 7.42(t, IH, J=8.1, H6), 8.41(d, lH, J=8.8, H4). Minor diastereomer: 3H, CH,),
tH-NMR (CDCI,) : 6=1.24(t, 3H, J=7.3, CH& 2.09(s, 3H, CH,), 2.55(m, lH, H4e), 2.55(s,
3.07(dt,
lH, J=7.3, 13.2, HA’), 3.63(dq,
lH, J=7.3, 9.5, OCH*), 3.86(dq,
lH, J=7.3, 9.5, OCH$,
4.18(m, IH, H31), 5.70(dd, lH, J=4.4, 7.3, HS*). 6.80(d, 2H, J=8.1. H,‘*, Hg”), 6.92(t, lH, J=7.3, HS), 6.90(d, 2H, J=8.1, Hz”, Hg”), 7.30(d, IH, J=7.3, H7), 7.42(dt, lH, J=1.5, 7.3, H6), 8.41(d large, lH, H4). Anal. Calc. for C22H23N04: C, 72.31; H, 6.34; N, 3.83. Found: C, 72.54; H, 6.42; N, 3.89.
3-[(1-Acetyl-3-oxo-2,3-dihydroindol-2-yi)(4-methoxypheny~)]propanoic Compound
3h (310 mg, 0.85 mmol) was dissolved
was added dropwise
in CH,Cl,
(4 ml). TMSOTf (0.08 ml, 0.042 mmol)
at -25 “C; mCPBA (176 mg, 1 mmol) was then added. After 1 h, the mixture was treated
with ether (20 ml) and washed with 5% aqueous sodium thiosulfate drying over MgSO, silica gel column
acid Ethyl Ester (9h).
and evaporation
under wzcuo of the organic layer, the residue was chromatographed
(eluent: CH2Clz/petroleum
yield:51% (oil). JR (film): v=1715(C=O), 2.61(s, 3H, COCH,),
(15 ml) and saturated NaHCO,.
ether 3: 1). Only one diastereomer
167O(C=O) cm-t. tH-NMR (DMSO-d6)
was obtained;
After on a
m=165 mg,
: 6=1.26(t, 3H, J=7, CH,),
3.08(m, lH, CH,), 3.54(m, lH, CH2), 3.67(s, 3H, OCH,), 4.03(m, lH, CH), 4.18(dq, 2H,
J=2.6, 7.0, OCH,), 4.91(d, IH, J=4.3, Hz), 6.69(d, 2H, J=8.6, H3’, HS’), 6.99(d, 2H, J=8.6, HT, H6), 7.15(t, lH, J=7.3, HS), 7.53(d, lH, J=7.7, H,), 7.61(t, IH, J=7.7, H6), 8.17(d large, lH, H4). Anal. Calc. for C~~H,,NOS: C, 69.28; H, 6.08; N, 3.67. Found: C, 69.54; H, 6.22; N, 3.69.
3-[(l-Acetyl-3-oxo-2,3-dihydroindol-2-yl)(4-methylphenyl)]propanoic Compound v=1725(C=O),
9i was similarly obtained
from the major diastereomer
171O(C=O), 167O(C=O) cm-t. tH-NMR
CH,), 2.48(s, 3H, CH&
2.96(m,
acid Ethyl Ester (9i).
(DMSO-d6)
of 3i; yield: 60% (oil). JR (film):
: 6=1.13(t, 3H, J=7, CH,), 2.04(s, 3H,
IH, CH,), 3.40(m, lH, CH,), 3.93(m,
lH, CH), 4.05(dq,
2H, J=2.0, 7.0,
Synthesis
OCH,), 4.SO(d, lH, J=4.3, H2), 6.75-6.85(m, H7), 7.47(t,
999
and oxidation of pyrano[3,2-blindoles
4H, H2,, H,,, H,!, H6’), 7.0l(t,
lH, J=7.3, Hg), S.OO(d large, IH, H4). MS (U/NH,)
IH, J=7.3, HS), 7.39(d, lH, J=7.7,
: m/z=366
(M + I)+. Anal. Calc. for
C22H23N04: C, 72.31; H, 6.34; N, 3.83. Found: C, 72.46; H, 6.22; N, 3.91.
l-Acetyl-2-[3,3-diethoxy-l-(4-methylphenyl))propyl]-2,3-dihydroindol-3-one The cis diastereomer
of 3i (100 mg, 0.287 mmol) was dissolved
(lOi).
in ethanol (20 ml) and BF3.Et20
ml, 0.285 mmol) was added and the mixture stirred at reflux for I h. Evaporation which was treated with aqueous NaHC03 dried over MgS04 and evaporated CHzCl$petroleum
(DMSO-d6) : 6=1.12(t, 3H, J=7.0, CH$ 3H, COCH,),
of the solvent leaves a residue
(25 ml) and extracted with CH2C12 (25 ml). The organic layer was
in vacua. the residue was chromatographed
ether 5: I); yield:42mg
(0.035
on a silica gel column (eluent:
(40% ); oil. JR (film): v=l705(C=O), l.l4(t,
167O(C=O) cm-t.
t H-NMR
3H, J=7.0, CH& 2.03(s, 3H, CH& 2.20(m, IH, CH,). 2.39(s,
2.5S(m, lH, CH,), 3.30-3.70(m, 5H, 2xCH2, CH), 4.57(d, IH, J=4.4, Hz), 6.7l(d, 2H, J=S.l, H3’,
HS’), 6.79(d, 2H, J=S.l, H,,, He,), 6.89(t, IH, J=7.3, HS), 7.3l(t,
IH, H6, J=7.9), 7.37(d, lH, J=7.3, H7), 8.20(d
large, IH, Hb). MS (CJ/NH3) : m/z=396 (M + l)+. Anal. Calc. for C24H,,N04:
C, 72.89 H, 7.39; N, 3.54.
Found: C, 72.70; H, 7.55; N, 3.37.
3-[(1-Acetyl-3-oxo-2,3-dihydroindol-2-yl)(4-methy~phenyl)]propanal
(lli).
The cis isomer of 3i (120 mg. 0.344 mmol) was dissolved in a mixture TFA-H@THF
(4 mU2.5 mU2.5
ml) and the mixture was stirred 1 h at 25°C. Ether (20 ml) was then added followed by a solution of saturated NaHCO,;
the two layers were separated
and the organic layer was dried over MgS04.
vacua, the residue was chromatographed
on a silica gel column (eluent: CH,Cl,);
(film): v=1715(C=O),
tH-NMR
3.17(m, IH, CH$,
167O(C=O) cm-l.
(DMSO-d6)
After evaporation
yield:7lmg
in
(63%); oil. JR
: 6=2.05(s, 3H, CH,), 2.5 I(s, 3H, COCH&
3.54(m, IH, CH,), 4.05(m, lH, CH), 4.77(d, lH, J=4.7, Hz), 6SO(d, 2H, J=S.S, H,‘, Hs’),
6.83(d, 2H, J=S.S, H2’, H6’), 7.02(t, IH, J=7. I, H5), 7.40(d, lH, J=7.9, H7), 7.4S(t, lH, J=7.9, H6), S.O2(d broad, IH, HJ), 9.70(s, IH, CHO). Anal. Calc. for C,oHtgNO,:
C, 74.75; H, 5.96; N, 4.36. Found: C, 74.56; H, 5.81;
N, 4.49.
5-Acetyl-2-henzyloxy-4-(4-methoxyphenyl)-3,4,4a,9b-dihydro-2~-pyrano[3,2-~]indole Compound
3a (major diastereomer)
(10 mg) was introduced.
cm-t.
tH-NMR
in MeOH (6 ml) and Pd/C 10%
The mixture was stirred 8 h under a hydrogen atmosphere
filtration on celite and evaporation, Only one diastereomer
(90 mg, 0.21 mmol) was dissolved
(12a).
the residue was chromatographed
at room temperature.
on a silica gel column (eluent: CH,CI,).
was obtained; yield:38 mg (37%) mp=14S”C (ethanol/HzO).
(DMSO-d6)
: 6=1.63-l.Sl(m,
3.72(s, 3H, OCH,), 4.54(d, lH, J=l2.0,
2H, CH,),
After
1.74(s large, 3H, COCH,),
OCH,), 4.85(dd, lH, J=5.1, J=S.6, H&,
JR (KBr): v=l66O(C=O) 3.22-3.3l(m,
4.95(d, IH, J=l2.0,
IH, H4), OCH&
J.-Y. MBROUR et al.
I 000
5.10(t, IH, J=5.1, H,), 5.92(d, IH, J=8.6, Hgn), 6.86(d, 2H. J=8.6, H3’, Hgs), 6.98(t, IH, J=7.7, H7) , 7.06(d, 2H, J=8.6, H,,,H,O, 7.20(t, lH, J=7.0, Hx), 7.257.38(m,
SH, Harom), 7.42(d, lH, J=7.7, H9), 7.88(d large, IH, H6).
: m/z=430 (M + I)+. Anal. Calc. for C27H27N04: C, 75.50 H, 6.34; N, 3.26. Found: C, 75.37; H,
MS (CVNH$ 6.16; N, 3.40.
S-Acetyl-2-hydroxy-4-(4-methoxyphenyl)-3,4,4a,9b-tetrahydro-2~-pyrano[3,2-~]indole Compound
(13a).
3a (710 mg, 1.66 mmol) was dissolved in presence of Pd/C( 10%) (700mg) in MeOH (23 ml)
under a hydrogen atmosphere
of at room temperature.
After 8 h the mixture was filtered and evaporated;
obtained solid was washed twice with ethyl acetate (2 ml). Two diastereomers yield:240 mg (42%). mp=214 “C (mixture of diastereomers). Major diastereomer:
)H-NMR (DMSO-d6)
: 6=1.60-1.75(m,
were obtained in the ratio 1:2;
IR (KBr): v=3280(0-H),
163O(C=O) cm-t.
IH, H3), 1.77(s large, 3H, COCH,),
J=6.6, 14.0, H3), 3.66(s, 3H, OCH,), 3.68(m, IH, H4), 4.83(t, IH, J=8.1, H,,), 4.93(m, J=8.l, H&,
the
2.04(dt, IH,
IH, Hz), 5.63(d, IH,
6.73(d, 2H, J=8.8, H,,, HSa), 7.03(m, IH, H7), 7.05(d, 2H, J=8.8, Hz’, H6#), 7.24(t, IH, J=8.1, Hs),
7.32(d, IH, J=7.35, H9), 7.80(d large, IH, Hg). Minor diastereomer:
i H-NMR (DMSO-d(1) : 6=1.60-l .75(m, 2H, CH,). I .77(s large, 3H, COCH,), 3.27(m, I H,
H4), 3.69(s, 3H, OCH,), 4.78(dd, IH, J=5.1, 8.8, H&,
5.19(m, IH, Hz), 5.78(d, lH, J=8.8, Hgh), 6.79(d, 2H,
J=8.8, H,,, HS’), 7.03(m, IH, H7), 7.08(d, 2H, J=8.8, Hz*, He’), 7.19(t, IH, J=S.l, Hx), 7.37(d, IH, J=7.3, Hg), 7.85(d large, IH. H6). Anal. Calc. for C2uH2,N04:
C, 70.78; H, 6.24; N, 4.13. Found: C, 70.65; H, 6.15; N,
4.27.
5-Acetyl-2-hydroxy-4-(4-methylphenyl)-3,4,4a,9b-tetrahydro-2~-pyrano[3,2-~]indoie Compound
3b was treated as described
for compound
l:2); yield:40%, mp=210 “C (mixture of two diastereomers). Major diastereomer:
IH-NMR (DMSO-d6)
(13b).
13a and two diastereomers IR (KBr): v=3280(0-H),
were obtained
1630(C=O)cm-t.
: 6=1.60- I .75(m, IH, H3), I .69(s large, 3H, COCH,),
J=6.6, 14.7, H3), 2.20(s, 3H, CH,), 3.68( m, IH, H4), 4.84(t, lH, J=8.7, H&, J=8.7, Hgn), 6.46(d, IH, J=4.4. OH), 6.94-7.lO(m,
(ratio
4.91(m,
2.04(dt, I H,
IH, Hz), 5.64(d, IH,
5H, Hz,, H,,, H,,, He,, H7), 7.33(d, lH, J=7.3, Hy), 7.34(t,
lH, J=7.7, Hg), 7.82(d broad, lH, H,). Minor diasteromer:
rH-NMR (DMSO-d6)
CH,), 3.25(m, IH, H4), 4.78(dd, J=3.7, OH), 6.94-7.10(m,
:6=1.60-1.75(m,
IH, J=5.1, 8.7, H&,
2H, CH,),
1.69(s large, 3H, COCH3), 2.24(s, 3H,
5.23(m, IH, H2), 5.79(d, IH, J=8.7, H,h), 6.47(d, IH,
5H, Hz’, H,,, H,‘, H6,, H,), 7.34(t, IH, J=7.7, Hs), 7.37(d, IH, J=7.4, Hg), 7.83(d
large, IH, He). MS (WNH,)
: m/z=324 (M + I)+. Anal. Calc. for C,oH,,N07:
Found: C, 74.40; H. 6.38; N, 4.24.
C, 74.28 H, 6.55; N, 4.33.
Synthesis
and oxidation of pyrano[3,2-hlindoles
1001
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The configuration
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Z has been attributed
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18 I - 186.
according
to 2D NMR NOESY
experiments
The structure cis of the major diastereomer
16.
The configuration
of 3h has been precedently
wrongly attributed as truns.5
213~1~ of l-acetyl-2-benzylidene-2,3-dihydroindol-3-ones
the IH-NMR spectra and more particularly
has been attributed
the chemical shift of the CH,CO
versus 2.62 ppm for the E-isomers 17.
in acetone-d6
between the 1-H and the ortho protons of the phenyl substituent.
15.
examining
1750-1756.
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by
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1002
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(Received in Belgium 25 July 1996; accepted 6 November 1996)
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