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Metal-hydride reduction of isoxazoline-3-carboxylate esters
TeerruhedronVol. 42. No. 19, pp. 5267 to 5272. 1986 Pnnled in Grcal Bntain.
oo4a-w0/86 ss.oo+ .a0 Pcrgamon Journals Lld.
METAL-HYDRIDE
REDUCTION
OF
ISOXAZOLTNE-3-CARBOXYLATE
Patrizia
Csldirola,
Istituto
Marco
De
ESTERS
Amici,
Chimico-Farmaceutico Viale
Peter
A.
Abruszi,
Wade*,
Department
42
David of
and
-
T.
and
Micheli*
Milan0
-
Italy
James
Drexel PA
di
MILANO,
Trite,
Chemistry,
De
Universitd
20131,
Philadelphia,
Carlo
F.
Bereznak
University,
19104,
U.S.A.
(Received in USA 22 May 1986)
Abstract
The
sodium Reduction the
tro
by
with
Swern
cyclic
In
programs
acids3v4,
directed
two
following
Our approach
of the
isoxssoline-3-carboxylate
(in
Treatment
(Table
to
their
1).
There
apparently
because thus
protected
but
prepared
ethyl
by
particularly
suitable
base for
reduction
are
some
scattered
this
is
it
attached
is
high
the
reports
first
detailed
of
of
product
under
of
E-hydrory
can
in
be
the
the
genera
an excess
unusually
reaction. bond,
with
is
mild
of
ethoxyester
presence ted
recalcitrant
with
of
nitronic
or by thermal
preparations
double
have
acetals
reactions
the methyl
be used)
involving
similar
study
5267
from
can
to various
isoxazolines
of
from
isoxaeolines
conditions.
ethyl 9.
borohydride
in 34-989
The
acid
decomposition
of sodium
activated
of
dipolarophilesg.
3-(hydroxymethyl)isoxasolines
to a carbon-nitrogen
yields
cycloaddition
at room temperature
to the corresponding
3-(hy-
reodyavailabilityofethyl
methodology8)
cycloadditions
precursors
and nitroacetaldehyde
oxide
(Huisgen’s
of
antibiotics?,
advantageofthe
itself
derivatives
synthesis
3-a-oxygenated
can be generated
nitroacetate
the
isoxazoline-3-carboraldehydes.
to these
l,3-dipolar
oxide
active
for
aminosugars2,
nitroethanol
triol.
biologically
prepare
as
ethoxycarbonylformonitrile by using
permitting
of
are potential
such
takes
nitrile
either
smooth
’,
to
and the endo-
a monosilylated
methodology
approaches
of isoxazoline-3-carboxylates
isoxasoles’
esters,
compounds
procedure’.
for
prepared The
was silylated
synthesis
ways
suitably
This
Alternatively,
is
alsobe
produce
a general
Mukaiyama
some cases
chlorooximinoacetate, method
to
the
alternative
esters, oxide.
nitroacetate
The last
towards
to3-(hydrorymethyl)isoxazolines
carbonylformonitrile
catalysts7.
12
developed
Existing
with yield.
3-(hydroxymethyl)isoxezolines.
by ozonolysis
interesting
on the cycloaddition
74-98%
in 63 and 85% yields
and isoxszoline3-carboraldehydes
biologically
dipolarophiles
leads
corresponding
and +methylenelactones5.
centered
ethyl
the
, we have and
esters in
iaoxazoline-3-carboxaldehydes
was cleaved
3-(Hydroxymethyl)isoxazolines of
isoxazolinc-Fcarboxylate
3-(hydroxymethyl)isoxasoline
cycloaddition’
drorymethyl)isoxax.olines
of
3-(hydroxymethyl)isoxazolines
Isoxazoline-3-carboxaldehydescould
of
of bond
complementary
a series
studied.
oxidation group
double
1 ,%dipolar
classes
of gave
DIBAH gave
reactions
hydroryl
via
reduction
borohydride
ester
7*
yield ‘C
and
functionality,
compared
to simple
5268
P. C.uomot_4 et al. TABLE
i.
REDUCTION
ESTERS
R
R-COZEt
OF
ISOXAZOLINE-3-CARBOXYLATE
USING SODIUM BDROHYDRIDE
R-CH20H
YIELD
J,
Ph
9
IN
0.
“6-I
ml \
IN
a Preparation regioieomerg.
65-68’C (cyclohexane - EtOAc)
la
G!
81%
2a
-2b
18%
z!!
86%
eb
66%
Oil
‘“”
,b
78%
oil
6a
6b
83%
89-90°C (cyclohexane)
78
0
HP
oil
loo-102oc (Et20)
98%
129-31 oc (cyclohexane - EtOAc)
-8a
Ba
34%
oil
9”
s,b
52%
oil
66%
oil
89%
140.5-142’C (cc141
llb -
llab -
by 1,3-dipolar
cyoloaddition
b The methyl eater
gave a emall
xae employed.
amount of
the corresponding
Metal-hydride reduction of isoxaxoline-3-carboxylate esters The
methyl
ieorazoline-3-carboxylate
chlorooximinoacetate Ester I>
oxide.
89% yield. also
and triethylamine
out.
of the hydroxyl
Imidazole-catalyzed
reaction
ether 12 in 92% yield - dimethyl
sulfide
prepared12
(eq
by
generation
procedure
transformations
&butyldimethylsilyl aodium borohydride
was
the --in aitu
for
was reduced by the borohydrlde
Further
carried
12
5269
cycloeddition
with &-butyldimethylailyl
workup, gave the monosilylated
trio1
in
chloride
gave the
followed
by
13 in 62% yield. -
F O?iMe
12
double bond of IlJ were
Cleavage with one equivalentofozone,
1).
methyl
to the 3-(hydroxymethyl)iaoxaeoline
group and the endocyclic
of 12
using
of methorycarbonylformonitrile
Ye OSiMe
-
t-Bu
t- d u
OH
1)
(en
‘3
We have also
investigated
based on the direct
two alternative
reduction
of the corresponding
Direct
reduction
temperature. inmethylene
(Route
isoraeoline-3-carborylates
derived
Thiareactioniabestcarriedoutwithercesahydride
reagent
was observed.
In preliminary
Even at-78’C
due to the hi.gh reactivitn
3’
experimenta
asmallamount
lhs carbonpl
Route
R
(Scheme
(DIBAH) at low
(3-5 equivalents)
at-7S°C
in63%yieldandaldehyde
run at -20°C,
some overreduction
(<5% byNMRandTLC) ofalcoholuas
group attached
SCHEME
PhToh tt\v-
reduction
hydride
Undertheseconditions,thealdehyde14awaaobtained -
in 85% yield.
one
and the other
from sodium borohydride
di-iao-butglaluminum -
chloride.
A) was performed
isorazoline-3-carboraldehydes,
using
14b was obtained alcohol
ethyl
13 of the alcohols
indirectlythroughSwernoxidation 1).
ways to prepare
to the
produced,
to a carbon-nitrcweq
double
likely
bond.
1.
A
14a, -b,
DIBAH
CO,Et
R=H R =Ph
;CHO
\ Route
B
t
, Swern
NaBH, i=H20~
The second Swernoxidation the alcohol aldehyde
procedure
2_b to a DMSO-oxalyl chloride
12
in 82% yield.
In synthesizing
approach
for
is
preparation
of isoxazoline-3-carboxaldehydes
ofthecorresponding3-(hydroxymethyl)isorax.olines
DIBAH reduction reduction
investigated
or
Similar
at -6O’C
of alcohol
isorazoline-3-carboxaldehydes, the
two-step
somewhat quicker
requires
solution
reaction
less
stringent
borohydride
and givea control
(Scheme 1, Route B).
it reduction
a slightly
followed G
is necessary -
higher
of conditions.
by the addition
gave aldehyde
overall
yield.
Addition
of
of base gave the
14a in SO% yield. -
to choose
Swern oxidation
involved
either
the one-step
sequence.
The direct
However,
the two-step
P. CALDIROLAel al.
5270
Experimsntal
‘H-NER spectra
GeneralHethode.
otherwise
noted)
Infrared
spectrawere
were obtained
were recorded
on Hitachi-Perkin
out on Merck and Analtech
0.25
was carried
in toluene
(10
AfterlShatreflux,
mL).
approximately
2 h to a stirred
portions
of ether.
pressure.
Prooedlue solution
residue
in this
solution
stripped
(‘Baker
solution
(final
ex@osives!).
Analyzed’
Hetbyl
acid
g. 0.017
kugelrohr
silica
distillation
gel,
60-200
[Lit’7
Anal. Calcd forC3H4ClNO3:
The procedure
acetate)
C, 26.20;
followed
~orr],
nithonic
U&U
(16.5
was reflured
g, 0.16 for 2 h,
Na2S04). concentration
and column chromatography
gave 2.32
g (66% yield)
was analagous
of pure &.
to the preparation
from CC14 giving
N,l0.18;
of ethyl
a 34% yield
Found:
C1.25.78.
ProcsdureB8usedinpreparingthe
C, 26.23:
attack
4.50 (dt,
of the ester until
gave an 85:15
on the fulvene
1 H, J - 7.92,
mixture,
Of white
H, 2.97:
N,
(15 mL) and extracted concentrated
chromatography
at
of the starting
1J: 6 7.4 (m, 5H. aryl),
- 18 Hz, H-4),
2a: 6 7.43 (a, lOH, aryl)
(dd,
H, 2 H-7 and OH), 1.9
(m, 2 H. 2 H-6). aryl),
alcohols
2.3
J4’,5 (8.
4.25 (s,
6.06 (dd,
1 H, J-5.64,
2.17Hs,
excess ofNaBH4wasadded h).
R-6),
and 3.88 (s, 3 H); ES m/e 331 (E+). The reaction
portionwise
was stirred
at room
The mixture was then poured into
(Table
were dried
1)
were
(snhyd.
purified
Na2SC4)
by column
-8Hs,
H-5), 4.5 (8, 2H, C&OH), 3.5 (dd,
1 H,
1 H, OH). H-5).
4.45 (a, 2H, Cl&OH),3.25
(m, 3 H, 2 H-7 and OH), 1.7-2.2
52: 6 7.25 (m, 4H. sryl).
(3-4
J1,5=9.0Hz,H-1),4.5
42: 6 7.0-7.8(m,4H,
of NER
NMRspectra.
1 H. H-4’).
(d,lH,
bond. Recrystallization
The combined extracts
5.52 (d, 1 H, J4,5 =6.8Hs,
32: 6 7.3(m,4H,aryl),5.5
3 H. Me).
material
5.7 (dd, 1 H, J4,5=1OHs,
3.1
H-7).
or CH2C12 (10 mL).
The crude
pressure.
and gave characteristic
double
(95:5
(NMR) of 1111and the
mp 160-161 OC; IR (CHC13 1720 cm-l (C-0);
2.17 Hz, H-5),
with CHCl3 (3 X 20 mL).
reduced
ethyl esters
Column chromatography
respectively,
endocyclic
Aten-fold
(1 .O mmol) in ethanol
disappearance
analogous
and w,w-diphenylfulvens.
EeductionofEthyl Ieo-lime-3-carboxylatea.
(a.
solution
added
The resulting
by styrene
Drying(anhyd.
recrystallized
H, 2.93;
on the crude product
formed from reverse
to a solution
2.5-2.9
and I&
25.83.
5.42 (d, 1 H, J = 7.92 He, H-l),
54.4’
several
at reduced
62, 72, 2,
conceded
The resulting
this mixture from methanol gave lla (51% yield) as a solid: d 7.3-8.0 (m, lOH, aryl), 6.41 (dd, 1 H, J-5.64, 2.17Hs,
and
(2
with
oc].
lIethylIsoxasoli.n~J-Carborylatel&.
rater
over
chlorooximinoacetate
12, 214,
tide
(bp 140-16OoC [0.025
was repeated with methyl chlorooximinoacetate
temperature
fashion.
dropwise
(60 mL, 0.024 x101) was cautiously
mesh; CH2C12 elution)
mp 57-60
regioisomer
in this
and extracted
(30 mL) was sdded followed mol).
solid:
cc14 - ethyl
esters
ethyl
(5 mmol)
Na2SO4) and concentrated
(5OmL) and water.
The product was twice
Cl,
of
pressure and the resulting
(2.11 g, 0.016 mol) in CH2C12 (10 mL).
chlorooximinoacetate16.
10.23;
(anhyd.
noted. (5aL)
mL) was added
water,
volume was 10 mL; caution!
(3.0
Chlorooximinoacetate.
mp 61-620C
into
of diasomethanel5
Methylene chloride
andwashed successivelyxith5%NaOH
at reduced pressure,
poured
Column
of the dipolarophile
(10 mmol) and ethyl
were dried
of ethyl nitroacetate
and ptoluenesulfonic
cooled,
3 h,
otherwise solution
at reduced (10
was carried
plates.
GF254
and 82 were prepared
ether
Massspectra
fashion.
was partially
Me potem
for
solution
52,
diethyl
gel
toluene
A
was column chromatographed:
A 0.4 I etheral
c.
to a cold (0-50~)
was stirred
silica
stripped 42,
of dipolarophile
The combined extracts
The resulting
were prepared
mmol) in
(3
in CDC13, unless
HFT-80 instruments.
chromatography
mesh, unless
A.
to a refluxing
volatileswere
solution
slurry
60-200
Proeedw
Compounds 2,
Triethylamine
Bs.
The resulting
mmol).
mol)
1clOa.
was column chromatographed.
Procedure
gel,
_(5 mmol) was added dropwise
chlorooximinoacetate
Thin-layer
1 mm precoated
out on Merck silica
standard
and Varian
and137 spectrophotometers.
spectrometers.
mm and Analtech
IXthFl Isoxasolime-3-carboxylatee
residue
Me4Si as internal
JEOL FX-300,
obtainedusingPerkinElmerl3l0,457,
on Finnegan 4023 CC-ES orA.E.1.
chromatography
(vith
Elmer R-600FT.
(s,2H, (dd.
(m, 2 H, 2 H-6),
2H, C&OH), 4.15 (a.
4.38 (d,
1
H, H-4),4.0-4.5
C&OH), 3.7 (m.
1 H, J5,6’6.OHs. 1.6
(s,
(m,3H,
Cl&O&.
1 if, H-5), 2.7 (m, 3
55,6”9*OHs,R-5)s
3 H, Ee).
1 H, H-l), 2.0-3.0
(m, 4H, 2H-6 and2R-7).
1.5
Metal-hydride reduction of isoxazoline-3-carboxylate
(;_a: 6 4.55
1 H, +,6 -8.OHs.
(d,
5271
4.4 ( s, 2H, C&OH), 3.2 (d, 1 H, H-6).
2.5 (ba,3H,
H-l, H-7and
.8 (m, 6 H, 2 H-8, 2 H-9 and 2 H-10).
OH), 0.9-l
7b: 6 7.1-7.8 3.2
H-2).
esters
(ba,
(m, 6 H, aryl).
(d, 1 H. J1.5 - 9.0Hs, H-l ), 5.2 (d, 1 H, H-5).
6.35
4.4 (bs,
2 H, C&OH),
1 H, OH).
a_b: (pyridlna-D5)
6 5.22
92: 6 6.3(d,lH,
J~,5-6.0Hz,H-l),4.4(s,2H,C~OH),3.3-4.3(mr4H,H-5,2H-7andOH),2.2(m,2
(d,
2.7-4.8
1 H, H-l),
(m, 7 H, C&OH, H-5,
2 H-6 and 2 H-8).
H, 2 H-6).
lob: 6 4.90 (m, 1 H, H-51, 4.5 (s, 2 H, C&OH) 3.60 (d, 2 H, CH_$l,J = 5.0Hs), 3.20 (m, 2 H, 2 H-4). ?l_b:6 7.3-8(m,lOH, aryl),6.29 (dd.1 H, J-5.20, 2.28Hz,H-7), 5.95 (dd, 1 H, H-6). 5.20 (d, 1 H, J = 7.49Hz, 5.82
H-l),
4.41 (d, 2H, J-5.82Hz,
C&OH), 4.27 (dt,
1 H, J-7.49,
2.28Hz,
H-5),
DILUIImhction (1.4 mL of an 0.79
solution
of
Btbl t~.5-D~~.5-dipbenjllsoraMl~Fcarbo~late
I cyclohexane
1 .l mmol) was added dropxiae
solution;
of & (103 mg, 0.3 mmol) in CH2C12 (5 mL) under N2.
min and then water (10 mL) was added, the mixture was allowed The organic
products
were extracted
1 H. J-
Preparative
to an oil.
mg, 85% yield)
Kugelrohrdistillationofthe
as an oil.
(0.025 Torr);
IR (neat)
J = 6.1 Hz, H-5). A satisfactory
(d,
elemental
sample was converted Anal.
1690 cm-l (C-O);
and 4.5
Calcd
analysis
C22H17N505:
were washed (water),
outanalogouslyto
1 H, CHO). 7.1-7.5
(63% yield)
Torr);
as an oil.
IR (neat)
Kugelrohr
1690 cm-1 (C-O);
(m, lOH, aryl),
in several
Found:
11.4Hz,H-5),3.55
(dd, 1 H, J-11.4,
attempts
C, 61.12;
for aldehyde 12.
A
H. 4.03.
TLC (CH2C12) gave pure (NMR, TLC) aldehyde
gave the analytical
1 H, CHO), 7.2-7.5
17.6Hz,H-41,
1 H,
The reductionof
Preparative
distillation
5.68 (d,
mp 194-95OC.
H, 3.97.
NHR 6 9.97 (s,
(74
MS m/e 251 CM+).
could not be obtained
reductionof&.
(anhyd.
bp140-145°C
DI~BeductionofBt~l4,5-Dihyd~5_pha~lis~~I~~~rbo~late(l~~. was carried
for 50
dried
oilgavetheanalyticalsample:
Hz, H-4);
C, 61.21;
(-780C)
was stirred
to warm and 1% aqueous HCl (3 mL) was added.
to the 2,4-dinitrophenylhydrazone:
for
solution
TLC (CH2C12) gave pure (NHE, TLC) aldehyde 1s
NKR d 9.91 (8,
1 H, J = 6.1
(22). DIBAH
over 1 qin to a cold
The resulting
with CH2C12 and the extracts
Na2SO4). and concentrated
l&
1.86 (t,
Hz, OH).
and3.11
sample:
(m, 5 H, aryl),
(dd.1
H, J-9,
bp 90-loO°C 5.81 (dd,
(3.025
1 H, J = 9,
17.6Hz.H_4’);MSm/el75
CM+). Anal.
Calcd
for
C8HgN02:
8ve~rn Oxidation13 sol.ution
of DWSO(0.1
solution
of oxalyl
of
C, 68.57;
g, 1.3 zmol)
chloride
H, 5.14.
Found:
C, 68.76;
H, 5.36.
trans_4,5-D~~J-(hJd~~e~l)-4.5-dipbenjlisoxasole (0.07
in CH2C12 (1 mL) was added dropwise
g, 0.6 mmol) in CH2C12 (2 mL) under N2.
After
The resulting
solution
mixture was then allowed
was stirred
to warm to OoC and water was added.
phase was washed (water),
dried
(anhyd.
procedure
Oxidation13 was repeated
(CH2C12) to give Silylation dimethylsilyl
of
12.
using 51mg of alcohol
of aldehyde
of Alcoholl&2.
A solution
(111 mg; 0.74 mol), The resulting
solution
- sodium acetate
mL acetic
acid
(CH2C12), washing (water), silyl
ether 12.
(128 mg; 92% yield) (dd,l
H, J-5.51,
4.45 (s. 2H),
drying
(anhyd.
This was purified
and the organic
at reduced pressure.
which crystallized 1 H, J-7.42,
(I?).
The crude product
containing
solution
Preparative
was purified
The preceding by preparative
alcohol
TLC
12 (101 mg: 0.33 mmol), t-butyl-
(118 mg; 1 .70 mmol) in DMF(0.3
was poured into
buffer
concentrate,
TLC (60:40
on standing:
water containing diluted
Na$30,+), and concentration
by preparative
2.12Hz,H-7),6.02(dd.
4.32 (dt,
were separated
at
The reaction
l&.
and imidazole
for 8 h at 40-450C under Ar. (5.0
mL) was added.
4.5-Di~-3-(~~~eth~l)-5-phenjli~~sole
41 mg (80% yield)
chloride
The layers
Na2SO4), and concentrated
of
the temperature
of pure (NME, TLC) 14b.
TLC (CH2C12) gave 56 mg (82% yield) Slrern
for 15 min and Et3N (0.35
(-65OC)
10 min, a solution
2b14 (66 mg, 0.26 mmol) In CH2C12 (1 mL) was added dropwise over 1 min maintaining <-600~.
(22). A
over 1 min to a cold
(s,9H,
acetate)
NHE 6 7.3-8.0
1 H, J=5.51,2.12Hz.H-6),5.20(d. 2.12Hz,H-5),0.90
pH 7.0 buffer
to 25 mL).
Extraction
at reduced pressure
hexanes - ethyl
mp 108-lll°C;
mL) was heated
CHgC).andO.lO
gave crude
to give
an oil
(m. 10 H, aryl),
6.31
1 H. J-7.42Hz.H-1). (8.6H.Ke2Si);
MSm/e
of 12 (128 mg; 0.31 mmol) in absolute
methanol
417 (n+).
Osonolymsis ofally1ether1212.
A cloudy
solution
P. CALDIROLA
5272
(25 mL) and CH2C12 (2OmL) was cooled in aDry
et
al.
ice bath for15 min.
wes carefully stenderdieed iodometricelly to deliver0.0262
An02 streamconteiningce.
mm01 ! min of 03.
of delivered 03).
passed through the solution for12 min (0.31 mm01
for20 min et -780C end ves then elloved to verm to -250C.
The reactionmixture was stirred
After 5 min NaBH4 (0.21 g; 5.52 mmol) was
added end stirring et -20 to -250C was continued for en additional25 min. wes added end the reactionwas allowed to vew
to 1OoC over 5 h.
pressure and the residue was taken up in CH2C12.
3% oeone
This stream was then
Dimethyl sulfide (0.3 mL)
Voletiles were removed under reduced
The resulting solution was washed (water), dried
(enhyd. Na2SO4). and concentrated to en oil containing one major end five minor products (TLC). Preparative
TLC (80:20 hexanes- ethyl
enoff-whiteeolid:mp113.5-114.5°C;
acetate)
gevethemonosilylated
triol1_2(86.6mg; 62%yield) es
IR(CHC13) 2.95 (b, OH) cm-l; NNB 6 7.3-8.0 (m, IOH, eryl), 5.75
(d, 1 H, J - 11.2 Hz, 5-H),4.80 (dd, 2H),4.62
(dd, 2H).4.22
(dd, 2 H, J-3.75
11.2, 3.75 Hz, 4-H), 1.6 ( 8, 2 H, 2 OH), 0.86 (a, 9 H), and 0.11 (d, 6 H, J -
Achowld&ment.
Hz), 3.45 (dt, 1 H, J 1 He); MS m/s 453 (a').
FlnencielsupportfromtheMiniaterodellePubbliceIatruzione(Italy)
end IBN
Corporation Is gratefully acknowledged.
Eeferemces
1.
DeNicheli, C.; DeAmici,N.;
1983,2,
817.
and
?ootmotes
SantagoatinoBerbone, M.G.; Zonta, F.;Grene,
E. I1 Fermeco Ed. Sci.
(b) Wade, P. A.; Pilley, H. K.; Singh, S. W. Tetrahedron Lett. 19e2.3,
Micheli, C.; De Amici, !I.;Scelfi, M. 11 Fermeco Ed. Sci.1984,2,487.
4563.
(c) De
(d)Hede,P. A.;Singh, S.M.;
Pilley, M. K. Tetrahedron 1964, 40, 601. 2.
(a) Jliger,V.; Grund, H.; Buss, V. Schwab, Y.; Mllller, I. Schohe, R.; Franz, R.; Ehler, R. Bull.
Sot. Chim. Belg. 1983,92, 1039.
(b)Jiiger, V.; Schohe, R. Tetrahedron lW,g,
cited therein. (c) JAiger,V.; Hillier,I. Tetrahedron Lett. 1985.26, 2997.
2199 end references
(d) Wade, P. A.: Price, D.
T.; Bereenek, J. F.; unpublished studies. 3.
Kosikowski, A. P.; Ghoah, A. K. J. Org. Chem. 14,
4.
Curren, D. P.; Scange, S. A.: Fenk, C. J. J. Org. Chem. 1984, 49, 3474.
2,
2762.
5.
Kozikowski, A. P.; Ghosh, A. K. Tetrahedron Lett. 1983, 3,
6.
Mukeiyeme, T.; Hoshino, T. J. Am. Chem. Sot. 1960, g,
2623.
5339.
7.
Wade, P. A.: Amin, N. V.; Yen, H.-K.; Price, D. T.; Huhn, G. F. J. Org. Chem. 1984. 49, 4595.
8.
Chriatl, N.; Huiagen, R. Chem. Ber. 1973, 106, 3345.
9.
Celdirole, P.; De Amici, M.; De Micheli, C. Heterocyclea 1985, 2J, 2479.
IO. The isorasoline-3-cerborylete ester obtained from reaction of ethoxycerbonylformonitrile oxide
withexcesacycloherenehesbeenreducedwithsodiumborohydride:
Lee,V.; Yoodwerd, R. B.; unpublished
studies performed et Harvard University, 1975-1976 [Personal communication from V. Lee (Lederle Laboratories)].
This is apparently the first example of the transformation of an isoxezoline-3-
cerboxylete ester to a 3-(hydroxymethyl)ieoxesoline. 11. (a) Barco, A.; Benetti, S.; Bereldi,P.G.; Chem. Commun. 1981, 599.
Guemeri,M.;Pollini,G.P.;
Simoni, D.; J. Chem. SoC.,
(b) Bereldi, P. G.; Simonl, D.; Moroder, F.; Menfredlni, S.; Mucchi. L.;
DelleVecchie, F.; Orsolini, P. J. Heterocyclic Chem. 1982,fi, 557.
(c) Beraldi, P.G.;Moroder,
Pollini, G. P.; Simoni, D. Berco, A.: Benetti, S. J. Chem. Sot., Chem. Commun. 1982. 2983.
F.; (d)
Bereldi, P. G.; Berco, A.; Benetti, D.; Menfredini. S.; Polllni, G. P.; Simoni, D. Tetrahedron Lett. 1984,2,4313.
(e) Forthereleted
reductionofethylthieeolidine-4-cerboxylete,
aee:Hebermehl,G.
G.; Ecsy, W. Heterocyclea 1977, 1, 1027. 12. This work was Performed in the Converse Research Laboratories, Harvard University, 1975-1976. 13. Omure, K.; Swern, D. Tetrahedron 1978, 74, 1651.
14.
Ester 2~ used in the eldehyde studies was prepared directly from ethyl nitroecetete by TSA-
catalyzed reaction with stilbene7. 15.
Moore, J. A.; Reed, D. E. "Organic Syntheses"; Wiley: New York, 1973; Collect. Vol. 5, p 351.
16.
Skinner, G. S.; J. Amer. Chem. Sot. 1924, 46, 738.
17.
Keshutine, N. V.; Ioffe, S. L.; Shitkin, V. M.; Cherskeya, A. 0.; Korenevskii,
Tertakovskii. V. A. J. Gen. Chem. SSSR lYK5, 43, 1699.
V. A.;
oo4a-w0/86 ss.oo+ .a0 Pcrgamon Journals Lld.
METAL-HYDRIDE
REDUCTION
OF
ISOXAZOLTNE-3-CARBOXYLATE
Patrizia
Csldirola,
Istituto
Marco
De
ESTERS
Amici,
Chimico-Farmaceutico Viale
Peter
A.
Abruszi,
Wade*,
Department
42
David of
and
-
T.
and
Micheli*
Milan0
-
Italy
James
Drexel PA
di
MILANO,
Trite,
Chemistry,
De
Universitd
20131,
Philadelphia,
Carlo
F.
Bereznak
University,
19104,
U.S.A.
(Received in USA 22 May 1986)
Abstract
The
sodium Reduction the
tro
by
with
Swern
cyclic
In
programs
acids3v4,
directed
two
following
Our approach
of the
isoxssoline-3-carboxylate
(in
Treatment
(Table
to
their
1).
There
apparently
because thus
protected
but
prepared
ethyl
by
particularly
suitable
base for
reduction
are
some
scattered
this
is
it
attached
is
high
the
reports
first
detailed
of
of
product
under
of
E-hydrory
can
in
be
the
the
genera
an excess
unusually
reaction. bond,
with
is
mild
of
ethoxyester
presence ted
recalcitrant
with
of
nitronic
or by thermal
preparations
double
have
acetals
reactions
the methyl
be used)
involving
similar
study
5267
from
can
to various
isoxazolines
of
from
isoxaeolines
conditions.
ethyl 9.
borohydride
in 34-989
The
acid
decomposition
of sodium
activated
of
dipolarophilesg.
3-(hydroxymethyl)isoxasolines
to a carbon-nitrogen
yields
cycloaddition
at room temperature
to the corresponding
3-(hy-
reodyavailabilityofethyl
methodology8)
cycloadditions
precursors
and nitroacetaldehyde
oxide
(Huisgen’s
of
antibiotics?,
advantageofthe
itself
derivatives
synthesis
3-a-oxygenated
can be generated
nitroacetate
the
isoxazoline-3-carboraldehydes.
to these
l,3-dipolar
oxide
active
for
aminosugars2,
nitroethanol
triol.
biologically
prepare
as
ethoxycarbonylformonitrile by using
permitting
of
are potential
such
takes
nitrile
either
smooth
’,
to
and the endo-
a monosilylated
methodology
approaches
of isoxazoline-3-carboxylates
isoxasoles’
esters,
compounds
procedure’.
for
prepared The
was silylated
synthesis
ways
suitably
This
Alternatively,
is
alsobe
produce
a general
Mukaiyama
some cases
chlorooximinoacetate, method
to
the
alternative
esters, oxide.
nitroacetate
The last
towards
to3-(hydrorymethyl)isoxazolines
carbonylformonitrile
catalysts7.
12
developed
Existing
with yield.
3-(hydroxymethyl)isoxezolines.
by ozonolysis
interesting
on the cycloaddition
74-98%
in 63 and 85% yields
and isoxszoline3-carboraldehydes
biologically
dipolarophiles
leads
corresponding
and +methylenelactones5.
centered
ethyl
the
, we have and
esters in
iaoxazoline-3-carboxaldehydes
was cleaved
3-(Hydroxymethyl)isoxazolines of
isoxazolinc-Fcarboxylate
3-(hydroxymethyl)isoxasoline
cycloaddition’
drorymethyl)isoxax.olines
of
3-(hydroxymethyl)isoxazolines
Isoxazoline-3-carboxaldehydescould
of
of bond
complementary
a series
studied.
oxidation group
double
1 ,%dipolar
classes
of gave
DIBAH gave
reactions
hydroryl
via
reduction
borohydride
ester
7*
yield ‘C
and
functionality,
compared
to simple
5268
P. C.uomot_4 et al. TABLE
i.
REDUCTION
ESTERS
R
R-COZEt
OF
ISOXAZOLINE-3-CARBOXYLATE
USING SODIUM BDROHYDRIDE
R-CH20H
YIELD
J,
Ph
9
IN
0.
“6-I
ml \
IN
a Preparation regioieomerg.
65-68’C (cyclohexane - EtOAc)
la
G!
81%
2a
-2b
18%
z!!
86%
eb
66%
Oil
‘“”
,b
78%
oil
6a
6b
83%
89-90°C (cyclohexane)
78
0
HP
oil
loo-102oc (Et20)
98%
129-31 oc (cyclohexane - EtOAc)
-8a
Ba
34%
oil
9”
s,b
52%
oil
66%
oil
89%
140.5-142’C (cc141
llb -
llab -
by 1,3-dipolar
cyoloaddition
b The methyl eater
gave a emall
xae employed.
amount of
the corresponding
Metal-hydride reduction of isoxaxoline-3-carboxylate esters The
methyl
ieorazoline-3-carboxylate
chlorooximinoacetate Ester I>
oxide.
89% yield. also
and triethylamine
out.
of the hydroxyl
Imidazole-catalyzed
reaction
ether 12 in 92% yield - dimethyl
sulfide
prepared12
(eq
by
generation
procedure
transformations
&butyldimethylsilyl aodium borohydride
was
the --in aitu
for
was reduced by the borohydrlde
Further
carried
12
5269
cycloeddition
with &-butyldimethylailyl
workup, gave the monosilylated
trio1
in
chloride
gave the
followed
by
13 in 62% yield. -
F O?iMe
12
double bond of IlJ were
Cleavage with one equivalentofozone,
1).
methyl
to the 3-(hydroxymethyl)iaoxaeoline
group and the endocyclic
of 12
using
of methorycarbonylformonitrile
Ye OSiMe
-
t-Bu
t- d u
OH
1)
(en
‘3
We have also
investigated
based on the direct
two alternative
reduction
of the corresponding
Direct
reduction
temperature. inmethylene
(Route
isoraeoline-3-carborylates
derived
Thiareactioniabestcarriedoutwithercesahydride
reagent
was observed.
In preliminary
Even at-78’C
due to the hi.gh reactivitn
3’
experimenta
asmallamount
lhs carbonpl
Route
R
(Scheme
(DIBAH) at low
(3-5 equivalents)
at-7S°C
in63%yieldandaldehyde
run at -20°C,
some overreduction
(<5% byNMRandTLC) ofalcoholuas
group attached
SCHEME
PhToh tt\v-
reduction
hydride
Undertheseconditions,thealdehyde14awaaobtained -
in 85% yield.
one
and the other
from sodium borohydride
di-iao-butglaluminum -
chloride.
A) was performed
isorazoline-3-carboraldehydes,
using
14b was obtained alcohol
ethyl
13 of the alcohols
indirectlythroughSwernoxidation 1).
ways to prepare
to the
produced,
to a carbon-nitrcweq
double
likely
bond.
1.
A
14a, -b,
DIBAH
CO,Et
R=H R =Ph
;CHO
\ Route
B
t
, Swern
NaBH, i=H20~
The second Swernoxidation the alcohol aldehyde
procedure
2_b to a DMSO-oxalyl chloride
12
in 82% yield.
In synthesizing
approach
for
is
preparation
of isoxazoline-3-carboxaldehydes
ofthecorresponding3-(hydroxymethyl)isorax.olines
DIBAH reduction reduction
investigated
or
Similar
at -6O’C
of alcohol
isorazoline-3-carboxaldehydes, the
two-step
somewhat quicker
requires
solution
reaction
less
stringent
borohydride
and givea control
(Scheme 1, Route B).
it reduction
a slightly
followed G
is necessary -
higher
of conditions.
by the addition
gave aldehyde
overall
yield.
Addition
of
of base gave the
14a in SO% yield. -
to choose
Swern oxidation
involved
either
the one-step
sequence.
The direct
However,
the two-step
P. CALDIROLAel al.
5270
Experimsntal
‘H-NER spectra
GeneralHethode.
otherwise
noted)
Infrared
spectrawere
were obtained
were recorded
on Hitachi-Perkin
out on Merck and Analtech
0.25
was carried
in toluene
(10
AfterlShatreflux,
mL).
approximately
2 h to a stirred
portions
of ether.
pressure.
Prooedlue solution
residue
in this
solution
stripped
(‘Baker
solution
(final
ex@osives!).
Analyzed’
Hetbyl
acid
g. 0.017
kugelrohr
silica
distillation
gel,
60-200
[Lit’7
Anal. Calcd forC3H4ClNO3:
The procedure
acetate)
C, 26.20;
followed
~orr],
nithonic
U&U
(16.5
was reflured
g, 0.16 for 2 h,
Na2S04). concentration
and column chromatography
gave 2.32
g (66% yield)
was analagous
of pure &.
to the preparation
from CC14 giving
N,l0.18;
of ethyl
a 34% yield
Found:
C1.25.78.
ProcsdureB8usedinpreparingthe
C, 26.23:
attack
4.50 (dt,
of the ester until
gave an 85:15
on the fulvene
1 H, J - 7.92,
mixture,
Of white
H, 2.97:
N,
(15 mL) and extracted concentrated
chromatography
at
of the starting
1J: 6 7.4 (m, 5H. aryl),
- 18 Hz, H-4),
2a: 6 7.43 (a, lOH, aryl)
(dd,
H, 2 H-7 and OH), 1.9
(m, 2 H. 2 H-6). aryl),
alcohols
2.3
J4’,5 (8.
4.25 (s,
6.06 (dd,
1 H, J-5.64,
2.17Hs,
excess ofNaBH4wasadded h).
R-6),
and 3.88 (s, 3 H); ES m/e 331 (E+). The reaction
portionwise
was stirred
at room
The mixture was then poured into
(Table
were dried
1)
were
(snhyd.
purified
Na2SC4)
by column
-8Hs,
H-5), 4.5 (8, 2H, C&OH), 3.5 (dd,
1 H,
1 H, OH). H-5).
4.45 (a, 2H, Cl&OH),3.25
(m, 3 H, 2 H-7 and OH), 1.7-2.2
52: 6 7.25 (m, 4H. sryl).
(3-4
J1,5=9.0Hz,H-1),4.5
42: 6 7.0-7.8(m,4H,
of NER
NMRspectra.
1 H. H-4’).
(d,lH,
bond. Recrystallization
The combined extracts
5.52 (d, 1 H, J4,5 =6.8Hs,
32: 6 7.3(m,4H,aryl),5.5
3 H. Me).
material
5.7 (dd, 1 H, J4,5=1OHs,
3.1
H-7).
or CH2C12 (10 mL).
The crude
pressure.
and gave characteristic
double
(95:5
(NMR) of 1111and the
mp 160-161 OC; IR (CHC13 1720 cm-l (C-0);
2.17 Hz, H-5),
with CHCl3 (3 X 20 mL).
reduced
ethyl esters
Column chromatography
respectively,
endocyclic
Aten-fold
(1 .O mmol) in ethanol
disappearance
analogous
and w,w-diphenylfulvens.
EeductionofEthyl Ieo-lime-3-carboxylatea.
(a.
solution
added
The resulting
by styrene
Drying(anhyd.
recrystallized
H, 2.93;
on the crude product
formed from reverse
to a solution
2.5-2.9
and I&
25.83.
5.42 (d, 1 H, J = 7.92 He, H-l),
54.4’
several
at reduced
62, 72, 2,
conceded
The resulting
this mixture from methanol gave lla (51% yield) as a solid: d 7.3-8.0 (m, lOH, aryl), 6.41 (dd, 1 H, J-5.64, 2.17Hs,
and
(2
with
oc].
lIethylIsoxasoli.n~J-Carborylatel&.
rater
over
chlorooximinoacetate
12, 214,
tide
(bp 140-16OoC [0.025
was repeated with methyl chlorooximinoacetate
temperature
fashion.
dropwise
(60 mL, 0.024 x101) was cautiously
mesh; CH2C12 elution)
mp 57-60
regioisomer
in this
and extracted
(30 mL) was sdded followed mol).
solid:
cc14 - ethyl
esters
ethyl
(5 mmol)
Na2SO4) and concentrated
(5OmL) and water.
The product was twice
Cl,
of
pressure and the resulting
(2.11 g, 0.016 mol) in CH2C12 (10 mL).
chlorooximinoacetate16.
10.23;
(anhyd.
noted. (5aL)
mL) was added
water,
volume was 10 mL; caution!
(3.0
Chlorooximinoacetate.
mp 61-620C
into
of diasomethanel5
Methylene chloride
andwashed successivelyxith5%NaOH
at reduced pressure,
poured
Column
of the dipolarophile
(10 mmol) and ethyl
were dried
of ethyl nitroacetate
and ptoluenesulfonic
cooled,
3 h,
otherwise solution
at reduced (10
was carried
plates.
GF254
and 82 were prepared
ether
Massspectra
fashion.
was partially
Me potem
for
solution
52,
diethyl
gel
toluene
A
was column chromatographed:
A 0.4 I etheral
c.
to a cold (0-50~)
was stirred
silica
stripped 42,
of dipolarophile
The combined extracts
The resulting
were prepared
mmol) in
(3
in CDC13, unless
HFT-80 instruments.
chromatography
mesh, unless
A.
to a refluxing
volatileswere
solution
slurry
60-200
Proeedw
Compounds 2,
Triethylamine
Bs.
The resulting
mmol).
mol)
1clOa.
was column chromatographed.
Procedure
gel,
_(5 mmol) was added dropwise
chlorooximinoacetate
Thin-layer
1 mm precoated
out on Merck silica
standard
and Varian
and137 spectrophotometers.
spectrometers.
mm and Analtech
IXthFl Isoxasolime-3-carboxylatee
residue
Me4Si as internal
JEOL FX-300,
obtainedusingPerkinElmerl3l0,457,
on Finnegan 4023 CC-ES orA.E.1.
chromatography
(vith
Elmer R-600FT.
(s,2H, (dd.
(m, 2 H, 2 H-6),
2H, C&OH), 4.15 (a.
4.38 (d,
1
H, H-4),4.0-4.5
C&OH), 3.7 (m.
1 H, J5,6’6.OHs. 1.6
(s,
(m,3H,
Cl&O&.
1 if, H-5), 2.7 (m, 3
55,6”9*OHs,R-5)s
3 H, Ee).
1 H, H-l), 2.0-3.0
(m, 4H, 2H-6 and2R-7).
1.5
Metal-hydride reduction of isoxazoline-3-carboxylate
(;_a: 6 4.55
1 H, +,6 -8.OHs.
(d,
5271
4.4 ( s, 2H, C&OH), 3.2 (d, 1 H, H-6).
2.5 (ba,3H,
H-l, H-7and
.8 (m, 6 H, 2 H-8, 2 H-9 and 2 H-10).
OH), 0.9-l
7b: 6 7.1-7.8 3.2
H-2).
esters
(ba,
(m, 6 H, aryl).
(d, 1 H. J1.5 - 9.0Hs, H-l ), 5.2 (d, 1 H, H-5).
6.35
4.4 (bs,
2 H, C&OH),
1 H, OH).
a_b: (pyridlna-D5)
6 5.22
92: 6 6.3(d,lH,
J~,5-6.0Hz,H-l),4.4(s,2H,C~OH),3.3-4.3(mr4H,H-5,2H-7andOH),2.2(m,2
(d,
2.7-4.8
1 H, H-l),
(m, 7 H, C&OH, H-5,
2 H-6 and 2 H-8).
H, 2 H-6).
lob: 6 4.90 (m, 1 H, H-51, 4.5 (s, 2 H, C&OH) 3.60 (d, 2 H, CH_$l,J = 5.0Hs), 3.20 (m, 2 H, 2 H-4). ?l_b:6 7.3-8(m,lOH, aryl),6.29 (dd.1 H, J-5.20, 2.28Hz,H-7), 5.95 (dd, 1 H, H-6). 5.20 (d, 1 H, J = 7.49Hz, 5.82
H-l),
4.41 (d, 2H, J-5.82Hz,
C&OH), 4.27 (dt,
1 H, J-7.49,
2.28Hz,
H-5),
DILUIImhction (1.4 mL of an 0.79
solution
of
Btbl t~.5-D~~.5-dipbenjllsoraMl~Fcarbo~late
I cyclohexane
1 .l mmol) was added dropxiae
solution;
of & (103 mg, 0.3 mmol) in CH2C12 (5 mL) under N2.
min and then water (10 mL) was added, the mixture was allowed The organic
products
were extracted
1 H. J-
Preparative
to an oil.
mg, 85% yield)
Kugelrohrdistillationofthe
as an oil.
(0.025 Torr);
IR (neat)
J = 6.1 Hz, H-5). A satisfactory
(d,
elemental
sample was converted Anal.
1690 cm-l (C-O);
and 4.5
Calcd
analysis
C22H17N505:
were washed (water),
outanalogouslyto
1 H, CHO). 7.1-7.5
(63% yield)
Torr);
as an oil.
IR (neat)
Kugelrohr
1690 cm-1 (C-O);
(m, lOH, aryl),
in several
Found:
11.4Hz,H-5),3.55
(dd, 1 H, J-11.4,
attempts
C, 61.12;
for aldehyde 12.
A
H. 4.03.
TLC (CH2C12) gave pure (NMR, TLC) aldehyde
gave the analytical
1 H, CHO), 7.2-7.5
17.6Hz,H-41,
1 H,
The reductionof
Preparative
distillation
5.68 (d,
mp 194-95OC.
H, 3.97.
NHR 6 9.97 (s,
(74
MS m/e 251 CM+).
could not be obtained
reductionof&.
(anhyd.
bp140-145°C
DI~BeductionofBt~l4,5-Dihyd~5_pha~lis~~I~~~rbo~late(l~~. was carried
for 50
dried
oilgavetheanalyticalsample:
Hz, H-4);
C, 61.21;
(-780C)
was stirred
to warm and 1% aqueous HCl (3 mL) was added.
to the 2,4-dinitrophenylhydrazone:
for
solution
TLC (CH2C12) gave pure (NHE, TLC) aldehyde 1s
NKR d 9.91 (8,
1 H, J = 6.1
(22). DIBAH
over 1 qin to a cold
The resulting
with CH2C12 and the extracts
Na2SO4). and concentrated
l&
1.86 (t,
Hz, OH).
and3.11
sample:
(m, 5 H, aryl),
(dd.1
H, J-9,
bp 90-loO°C 5.81 (dd,
(3.025
1 H, J = 9,
17.6Hz.H_4’);MSm/el75
CM+). Anal.
Calcd
for
C8HgN02:
8ve~rn Oxidation13 sol.ution
of DWSO(0.1
solution
of oxalyl
of
C, 68.57;
g, 1.3 zmol)
chloride
H, 5.14.
Found:
C, 68.76;
H, 5.36.
trans_4,5-D~~J-(hJd~~e~l)-4.5-dipbenjlisoxasole (0.07
in CH2C12 (1 mL) was added dropwise
g, 0.6 mmol) in CH2C12 (2 mL) under N2.
After
The resulting
solution
mixture was then allowed
was stirred
to warm to OoC and water was added.
phase was washed (water),
dried
(anhyd.
procedure
Oxidation13 was repeated
(CH2C12) to give Silylation dimethylsilyl
of
12.
using 51mg of alcohol
of aldehyde
of Alcoholl&2.
A solution
(111 mg; 0.74 mol), The resulting
solution
- sodium acetate
mL acetic
acid
(CH2C12), washing (water), silyl
ether 12.
(128 mg; 92% yield) (dd,l
H, J-5.51,
4.45 (s. 2H),
drying
(anhyd.
This was purified
and the organic
at reduced pressure.
which crystallized 1 H, J-7.42,
(I?).
The crude product
containing
solution
Preparative
was purified
The preceding by preparative
alcohol
TLC
12 (101 mg: 0.33 mmol), t-butyl-
(118 mg; 1 .70 mmol) in DMF(0.3
was poured into
buffer
concentrate,
TLC (60:40
on standing:
water containing diluted
Na$30,+), and concentration
by preparative
2.12Hz,H-7),6.02(dd.
4.32 (dt,
were separated
at
The reaction
l&.
and imidazole
for 8 h at 40-450C under Ar. (5.0
mL) was added.
4.5-Di~-3-(~~~eth~l)-5-phenjli~~sole
41 mg (80% yield)
chloride
The layers
Na2SO4), and concentrated
of
the temperature
of pure (NME, TLC) 14b.
TLC (CH2C12) gave 56 mg (82% yield) Slrern
for 15 min and Et3N (0.35
(-65OC)
10 min, a solution
2b14 (66 mg, 0.26 mmol) In CH2C12 (1 mL) was added dropwise over 1 min maintaining <-600~.
(22). A
over 1 min to a cold
(s,9H,
acetate)
NHE 6 7.3-8.0
1 H, J=5.51,2.12Hz.H-6),5.20(d. 2.12Hz,H-5),0.90
pH 7.0 buffer
to 25 mL).
Extraction
at reduced pressure
hexanes - ethyl
mp 108-lll°C;
mL) was heated
CHgC).andO.lO
gave crude
to give
an oil
(m. 10 H, aryl),
6.31
1 H. J-7.42Hz.H-1). (8.6H.Ke2Si);
MSm/e
of 12 (128 mg; 0.31 mmol) in absolute
methanol
417 (n+).
Osonolymsis ofally1ether1212.
A cloudy
solution
P. CALDIROLA
5272
(25 mL) and CH2C12 (2OmL) was cooled in aDry
et
al.
ice bath for15 min.
wes carefully stenderdieed iodometricelly to deliver0.0262
An02 streamconteiningce.
mm01 ! min of 03.
of delivered 03).
passed through the solution for12 min (0.31 mm01
for20 min et -780C end ves then elloved to verm to -250C.
The reactionmixture was stirred
After 5 min NaBH4 (0.21 g; 5.52 mmol) was
added end stirring et -20 to -250C was continued for en additional25 min. wes added end the reactionwas allowed to vew
to 1OoC over 5 h.
pressure and the residue was taken up in CH2C12.
3% oeone
This stream was then
Dimethyl sulfide (0.3 mL)
Voletiles were removed under reduced
The resulting solution was washed (water), dried
(enhyd. Na2SO4). and concentrated to en oil containing one major end five minor products (TLC). Preparative
TLC (80:20 hexanes- ethyl
enoff-whiteeolid:mp113.5-114.5°C;
acetate)
gevethemonosilylated
triol1_2(86.6mg; 62%yield) es
IR(CHC13) 2.95 (b, OH) cm-l; NNB 6 7.3-8.0 (m, IOH, eryl), 5.75
(d, 1 H, J - 11.2 Hz, 5-H),4.80 (dd, 2H),4.62
(dd, 2H).4.22
(dd, 2 H, J-3.75
11.2, 3.75 Hz, 4-H), 1.6 ( 8, 2 H, 2 OH), 0.86 (a, 9 H), and 0.11 (d, 6 H, J -
Achowld&ment.
Hz), 3.45 (dt, 1 H, J 1 He); MS m/s 453 (a').
FlnencielsupportfromtheMiniaterodellePubbliceIatruzione(Italy)
end IBN
Corporation Is gratefully acknowledged.
Eeferemces
1.
DeNicheli, C.; DeAmici,N.;
1983,2,
817.
and
?ootmotes
SantagoatinoBerbone, M.G.; Zonta, F.;Grene,
E. I1 Fermeco Ed. Sci.
(b) Wade, P. A.; Pilley, H. K.; Singh, S. W. Tetrahedron Lett. 19e2.3,
Micheli, C.; De Amici, !I.;Scelfi, M. 11 Fermeco Ed. Sci.1984,2,487.
4563.
(c) De
(d)Hede,P. A.;Singh, S.M.;
Pilley, M. K. Tetrahedron 1964, 40, 601. 2.
(a) Jliger,V.; Grund, H.; Buss, V. Schwab, Y.; Mllller, I. Schohe, R.; Franz, R.; Ehler, R. Bull.
Sot. Chim. Belg. 1983,92, 1039.
(b)Jiiger, V.; Schohe, R. Tetrahedron lW,g,
cited therein. (c) JAiger,V.; Hillier,I. Tetrahedron Lett. 1985.26, 2997.
2199 end references
(d) Wade, P. A.: Price, D.
T.; Bereenek, J. F.; unpublished studies. 3.
Kosikowski, A. P.; Ghoah, A. K. J. Org. Chem. 14,
4.
Curren, D. P.; Scange, S. A.: Fenk, C. J. J. Org. Chem. 1984, 49, 3474.
2,
2762.
5.
Kozikowski, A. P.; Ghosh, A. K. Tetrahedron Lett. 1983, 3,
6.
Mukeiyeme, T.; Hoshino, T. J. Am. Chem. Sot. 1960, g,
2623.
5339.
7.
Wade, P. A.: Amin, N. V.; Yen, H.-K.; Price, D. T.; Huhn, G. F. J. Org. Chem. 1984. 49, 4595.
8.
Chriatl, N.; Huiagen, R. Chem. Ber. 1973, 106, 3345.
9.
Celdirole, P.; De Amici, M.; De Micheli, C. Heterocyclea 1985, 2J, 2479.
IO. The isorasoline-3-cerborylete ester obtained from reaction of ethoxycerbonylformonitrile oxide
withexcesacycloherenehesbeenreducedwithsodiumborohydride:
Lee,V.; Yoodwerd, R. B.; unpublished
studies performed et Harvard University, 1975-1976 [Personal communication from V. Lee (Lederle Laboratories)].
This is apparently the first example of the transformation of an isoxezoline-3-
cerboxylete ester to a 3-(hydroxymethyl)ieoxesoline. 11. (a) Barco, A.; Benetti, S.; Bereldi,P.G.; Chem. Commun. 1981, 599.
Guemeri,M.;Pollini,G.P.;
Simoni, D.; J. Chem. SoC.,
(b) Bereldi, P. G.; Simonl, D.; Moroder, F.; Menfredlni, S.; Mucchi. L.;
DelleVecchie, F.; Orsolini, P. J. Heterocyclic Chem. 1982,fi, 557.
(c) Beraldi, P.G.;Moroder,
Pollini, G. P.; Simoni, D. Berco, A.: Benetti, S. J. Chem. Sot., Chem. Commun. 1982. 2983.
F.; (d)
Bereldi, P. G.; Berco, A.; Benetti, D.; Menfredini. S.; Polllni, G. P.; Simoni, D. Tetrahedron Lett. 1984,2,4313.
(e) Forthereleted
reductionofethylthieeolidine-4-cerboxylete,
aee:Hebermehl,G.
G.; Ecsy, W. Heterocyclea 1977, 1, 1027. 12. This work was Performed in the Converse Research Laboratories, Harvard University, 1975-1976. 13. Omure, K.; Swern, D. Tetrahedron 1978, 74, 1651.
14.
Ester 2~ used in the eldehyde studies was prepared directly from ethyl nitroecetete by TSA-
catalyzed reaction with stilbene7. 15.
Moore, J. A.; Reed, D. E. "Organic Syntheses"; Wiley: New York, 1973; Collect. Vol. 5, p 351.
16.
Skinner, G. S.; J. Amer. Chem. Sot. 1924, 46, 738.
17.
Keshutine, N. V.; Ioffe, S. L.; Shitkin, V. M.; Cherskeya, A. 0.; Korenevskii,
Tertakovskii. V. A. J. Gen. Chem. SSSR lYK5, 43, 1699.
V. A.;