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Synthesis of (±) Fredericamycin A
lllwdo39/93 $6.00 + .oo Pcrgamm Press Ltd
Tcmhedmn Lexus. Vol. 34. No. 16. pp. 26652668.1993 Pdcd in Gnat Britain
SYNTHESIS
OF ($
FREDERICAMYCW
A
AVRamaRao+,AshokKSingh,BatchuVenkateswaraRaoandKomandlaMallaReddy Indian Institute of Chemical Technology, Hyderabad 500 007, India
Abstract : The synthesis of Fredericamycin A (1) has been achieved by subjecting the 1,3-dione (II) to an unusual 5-etrigonal radical cyclization followed by reductive elimination of the halogen in 15 and subsequent demethylation.
Fredericamycln been
the
also
target
because
A
of
of
its
(I)
much
CliveSb.
We wish to report
the
of
main
segments, segment
interest
the 3)7
3 were protected
our
earlier
total
leading
model
pentamethoxy were
in the form
Two
good
elegant
were
process
approaches
for
However,
we
condensing of two polyketide Isocoumarine
The two
lized
for
separately
this
purpose Oxidation
methanol, lowed
building
segment
goal.
All
I,
of
afforded
by oxidative
the
ABC
in which
synthesis
of 3 have
a simplified
converted
6
was
compound
7,
to
the
groups at C-3 of’ pentadienyl treated after
with
(2)
the
been
phenolic
in scheme pivotal
and radical
give
exclusively
derivative
(8).
Condensation
of olefinic
group
the
two
isoquinoline
hydroxyls
part
in 2 and
furnished
2665
been but
the
took
6a,b
established overall
advantage
.
yields of
the
1.
of isoqulnoline
side chain to
which
intermediate
and C-6
NBS
developed,
approach
resultant
cleavage
the key step
Spiro system,
has already
the
acetal
by
convenience.
treating
dimethyl
the
1
segment
units as summarized
methyl
but
cyclisation.
2J6 and the
the
ethers for operational
preferred
introduction
compound
for
the
(418 was
set of reactions.
(7).
for
of
radical
1 yielding
10~~~‘~.
trigonal
(ABC the
1 A
to its antitumor properties* approaches 394 have been devised for 5a syntheses, first by Kelly and recently
reactions3
completing
of methyl
has
griseusl
only .due
to the synthesis
benzphthalide
chosen for
by Streptomyces
Various
two
our findings
not
produced
the Spiro system by an unusual 5endo
basis of
(DEF
antibiotic
complexity.
1, including
construction
On
antitumor
synthetic
structural
skeletal
involves building
an
the
aldehyde
(6)
trap
a standard
respectively.
monobromo with
of 8 with
required
through
have to be functiona-
acidic
derivative solution
benzaldehyde
aldehyde
For
(91 which
of folwas
later
transformed
treatment
with
to the styrene
(12) as a mixture form
under
derivative
(IO). Regeneration
crotyltriphenylphosphoniumchloride of geometrical
iodine
catalysed
isomers9. conditions
of aldehyde
and butyllithium
Compound (cis-trans
12 was isomerized
and
at C-3 and further
in THF gave
trans-trans
diene
ester
to a more trans-trans
forms,
16:8+
from
HPLC
and NMR).
Scheme-1
a) NaOH(2N),
24 h (65%), b) DMS, K2C03,
24 h (70%), d) POC13, reflux
aq, 45’C, Benzoyl
MeOH, rt,
peroxide
min (65%),
(cat),
h) MeOH,
6 h, light PPTS,
Mel, 12 h (82%), j) 0s04,
5 h (87%), e) NaOMe,
(95%),
reflux
acetone,
g) Hexamine,
1 h (98%),
Na104, buffer
reflux
Buli,
3.5 days (98%), c) NH3 6 h (80%), f) NBS, CC14,
acid-H20
PhCHO,
V/V),
(I:l,
HMPA,
rt,
pH 7, O°C, 5 h (60%), k) Ph3P+CH3Br-,
THF (20~1, v/v), O°C, 10 min (78%), 1) DDQ, CH3CN-HZ0 CH2-CHXH-MeCI-,
reflux
acetic
i) NaNH2,
reflux
45 min, -45“C,
THF, -78”C,
45 min (93%), o) DIBAL, CH2C12,
80%
30
8 h; K2C03, NaNH2, ether-
(9:l v/v), 1.5 h, rt (95%), m) Ph3P+-
45 min (78%), n) PTS, NaBr, 12, MeOH,
I h, -78“C (92%), p) PDC, CH2C12, molecular
seives,
45 min, rt (70%). Aldol 2). Sodium careful 3 under carried
reaction
experimental Shapiro’s as
(II) acetate
between
methoxide
per
our
2 and 3 in presence
mediated conditions. 10
conditions earlier
and chloroform
rearrangement Model were
approach in acetic
of LDA furnished
to the
experiments
1,3-dione to
the adduct
(13) (Scheme
(14a) was accomplished
synthesize
l4a
directly
from
unsuccessful. Spiro annulation of dione (I4a) was 3c wherein 14a was treated with Mn (III) acetate, , acid
at room
temperature
for 30 min, resulting
under 2 and first Cu in the
2667
formation
of
chloro
Bu3SnH gave
ether
derivative
a mixture
of the
bromo
in 60% which
and acetic
Reductive
10% yield.
at room
acid
yield.
separation
However,
temperature
for
(14b) in 80% yield’ ‘. Radical
derivative
elimination
on chromatographic
A (16) in less than
of fredericamycin
Mn (III) acetate
(15a)
of products,
of
treatment
with
of l4a with CuBr2,
15 min resulted
cyclitation
chlorine
gave the hexamethyl in the
of 14b with
formation
slow addition
Scheme-2
c
I@
c
llo
X=tl
Ub
X=CIorBr
x =Cl
l>b X - Br a) LDA, 3, THF, HMPA, (58%),
c) CuBr2,
benzene,
-78OC, 3 h (54%), b) NaOMe,
Mn(lII)acetate,
slow addition
AcOH,
12 h, 50°C,
I5 min,
e) Ph3SnH
ethylpropionate,
MeOH,
reflux
1.5 h
rt (SO%), d) Ph3SnH (1 eq), AIBN (0.03 eq), (1.1 eq), benzene,
reflux
2 h (55%), f) BBr3,
CH2C12, -78“C, 30 min, OOC, 10 min. of Ph3SnH (I eq), AIBN (0.03 eq) in benzene of
bromine
additional
in 15b (not
isolated)
graphic
2 h gave the hexamethyl ether I1 separation . The NMR spectrum
ture12.
Subjecting
ricamycin
16 with
at 50°C for
by adding
Ph3SnH
12 h followed
(1.1 eq) and
of fredericamycin
of 16 is fully in agreement and bringing 13 sample .
with the natural
the
elimination mixture
A (16) in 55% yield after
BBr3 in CH2C12, -78“C,
A (1) which is identical
by reductive
refluxing with
it slowly
for
chromato-
the assigned
struc-
to 0°C gave
Frede-
Referencess 1.
Isolation
- Pandey,
R.C.;
Toussaint,
Garretson,
A.L.;
1981,
34,
1389; Structure
sot.,
1982,
104,
Wei, T.T.; Byrne,
4478;
-
Misra,
M.W.; Stroshane, K.M.;
Misra,
R.;
R.;
Pandey,
J.V. .I. Anlibiot,
1987, 44
Misra, R.; Pandey,
R.C. Biochemistry,
R.M.; Kalita,
Geoghegan, Pandey,
786; Biosynthesis
R.C.;
R.C.;
B.D.;
KM.;
C.C.;
White,
Silverton,
Hilton,
- Byrne,
1985, 24, 478.
R.F.;
Jr.
XV. Roller,
Hilton,
Aszalos,
A.A.;
R.J. .I. Antibiot., J.
Am.
P.P.;
Chem.
Silverton,
B.D.; White,
R.J.;
2668
2.
Warnick-Pickle, Latham,
Byrne,
a) Rama
K.M.; Pandey,
R.C.;
1988, 41, 976; Dalal,
King,
M.D.;
Pharmacol., 3.
D.J.;
R. J. Antibiot.,
Misra,
C.K.;
Gorycki,
R.J. J. Antibiot.
1981, 34, 1402;
N.S.8 Shi, X. Biochemistry,
White,
1989, 28, 748;
P.; Macdonald,
T.L.;
Ross,
(Bemother.
W.E. Cancer
1989, 24, 167. Rao,
Reddy,
D.R.;
1119; b) Rama
Rao,
A.V.;
Reddy,
1065; c)
Rama
Rao,
A.V.;
Rao,
Comrtun,
1989, 400; d) Rama
A.V.;
Deshpande, D.R.;
D.R.;
Rao,
A.V.;
J.
B.V. Indian
Reddy,
B.V.;
Rao,
J. Chem. Sot.
V.H.
Rao,
Singh,
Chem. Comrmn.,
CRem. Sec.
A.K.
B.V.; Reddy,
J.
Chem.
D.R. lrriian
1982,
B, 1988, 27, Sot.
Chem.
J. Chem.
Sec.
Khodabocus,
A.;
B, 1991, 30, 723. 4.
Other
approaches
Vernon, D. J.
P.G.;
for
constructing
Angoh,
Chem.
Sot.
Spiro system,
Bordeleau,
A&.;
Trans. 1, 1991,
Perkin
see
L.; (in part)
a) Clive,
D.L.J.;
Middleton,
1443; b) Boger,
D.S.;
D.L.;
Lowe,
C.; Kellner, I.C. J. Org.
Jacobson,
Chem., 1991, 56, 2115. 5.
a) Kelly,
T.R.;
Bell,
S.H.; Ohashi,
110, 6471; b) Clive, S.M.; 6.
Boddy,
C.J.;
Richardson,
ABC
Segment
Tetrahedron J.
- a) Rama 1987,
Chem.,
DEF Segment 574; b) Pulla
ault,
G.A.
Rao, 28,
1987, 52,
Reddy,
Rao,
A.; Wu, Y.-J.; Kleiner,
D.R.; Rao,
Thesis,
Chem., 1987, 24, 509. S.H. Synthesis, 1980, 708.
9.
a) Bohlmann, Schmid,
H. HeIv. Chim. Acta.,
10.
Shapiro,
S.L.; Geiger,
11.
Details
12.
Spectroscopic
F.; Mannhardt,
Reddy,
D.R. J. Chem.
Pune University,
H.-J.
of this methodology
will be published
India,
Deshpande, N.;
V.H.
Reddy,
D.R.;
K.A.; Spero,
D.M.; Koziski,
A.; Tsuboi,
T.; Hayashida,
Sot.
Chem.
1m
D.L.J.;
Comrmn,
c) Parker,
Sedgeworth,
1987,
K.A.; Bre-
J. J. Hetero-
H.-J.:
L. J. Org. Chem.
l%l,
26, 3580.
separa-tely.
of 16: ‘H NMR (200 MHz, CDC13):
data
6 1.87, 1.95 (3H, d, J = 7.0 Hz,
2.55 (2H, t, J = 7.5 Hz), 3.40 (2H, t, J = 7.5 Hz), 3.49, 3.52 (3H, s, CH3, 3.96 (3H, s, CH3,
two
sets),
4.05-4.15
(ISH,
s, 5CH3),
5.95 (IH,
6.95, 6.98 (IH, s, two sets),
7.35 (IH, dd, J = 15.0, 10.0 Hz), 7.60, 7.65 (IH, s, two sets),
at 2.55 ppm resulted
singlet
at 3.40 ppm and vice
versa;
IR vmax
(CHC13):
MS m/z : 625 (M+).
We thank Dr Ven L Narayanan,
IICT Communication
G.S.;
1972, 55, 1828.
6.30 (IH, m), 6.50, 6.55 (IH, d, J = 15.0 Hz, two sets),
1700 cm-‘;
Bennett, Nicholas,
Ber. 1956, 89, 1307; b) Hug, R.; Hansen,
Chem.
K.; Youlus, 3.; Freedman,
7.15 (IH, s, two sets),
13.
A&.; D.S.;
1992, 1489.
Sreenivasan,
Y.; Terada,
183; d) Tanoue,
Angoh,
Middleton,
Annapurnq,
A.V.;
1986, 27, 3835; d) Clive,
Lett.,
Bertz,
diation
C.;
1987, 28, 455; c) Parker,
A.V.;
S. Ph.D.
Tetrahedron
3.95,
Reddy,
b) Rama
Lett.,
cyclic.
sets),
A.V.;
451;
8.
two
D.;
1988,
Chem. Sot. Jpn, 1987, 60, 2927.
- a) Rama
CH3, two sets),
Kellner,
J. Am. Chem. Sot.,
R.J.
P.G. J. Chem. Sot. Chem. Comnun.
V.H. Tetrahedron Org.
Y.; Khodabocus,
L.;
S.R.; Vernon,
T.; Tsuge, 0. &II. 7.
Tao,
Bardeleau,
Lett.,
Deshpande, K.A.
D.L.J.;
C.N.;
N.; Armstrong-Chong,
No. 3153
(Received in UK 7 December
1992)
NCI, USA, for providing
natural
Fredericamycin-A.
m), 7.10, irra1730,
Tcmhedmn Lexus. Vol. 34. No. 16. pp. 26652668.1993 Pdcd in Gnat Britain
SYNTHESIS
OF ($
FREDERICAMYCW
A
AVRamaRao+,AshokKSingh,BatchuVenkateswaraRaoandKomandlaMallaReddy Indian Institute of Chemical Technology, Hyderabad 500 007, India
Abstract : The synthesis of Fredericamycin A (1) has been achieved by subjecting the 1,3-dione (II) to an unusual 5-etrigonal radical cyclization followed by reductive elimination of the halogen in 15 and subsequent demethylation.
Fredericamycln been
the
also
target
because
A
of
of
its
(I)
much
CliveSb.
We wish to report
the
of
main
segments, segment
interest
the 3)7
3 were protected
our
earlier
total
leading
model
pentamethoxy were
in the form
Two
good
elegant
were
process
approaches
for
However,
we
condensing of two polyketide Isocoumarine
The two
lized
for
separately
this
purpose Oxidation
methanol, lowed
building
segment
goal.
All
I,
of
afforded
by oxidative
the
ABC
in which
synthesis
of 3 have
a simplified
converted
6
was
compound
7,
to
the
groups at C-3 of’ pentadienyl treated after
with
(2)
the
been
phenolic
in scheme pivotal
and radical
give
exclusively
derivative
(8).
Condensation
of olefinic
group
the
two
isoquinoline
hydroxyls
part
in 2 and
furnished
2665
been but
the
took
6a,b
established overall
advantage
.
yields of
the
1.
of isoqulnoline
side chain to
which
intermediate
and C-6
NBS
developed,
approach
resultant
cleavage
the key step
Spiro system,
has already
the
acetal
by
convenience.
treating
dimethyl
the
1
segment
units as summarized
methyl
but
cyclisation.
2J6 and the
the
ethers for operational
preferred
introduction
compound
for
the
(418 was
set of reactions.
(7).
for
of
radical
1 yielding
10~~~‘~.
trigonal
(ABC the
1 A
to its antitumor properties* approaches 394 have been devised for 5a syntheses, first by Kelly and recently
reactions3
completing
of methyl
has
griseusl
only .due
to the synthesis
benzphthalide
chosen for
by Streptomyces
Various
two
our findings
not
produced
the Spiro system by an unusual 5endo
basis of
(DEF
antibiotic
complexity.
1, including
construction
On
antitumor
synthetic
structural
skeletal
involves building
an
the
aldehyde
(6)
trap
a standard
respectively.
monobromo with
of 8 with
required
through
have to be functiona-
acidic
derivative solution
benzaldehyde
aldehyde
For
(91 which
of folwas
later
transformed
treatment
with
to the styrene
(12) as a mixture form
under
derivative
(IO). Regeneration
crotyltriphenylphosphoniumchloride of geometrical
iodine
catalysed
isomers9. conditions
of aldehyde
and butyllithium
Compound (cis-trans
12 was isomerized
and
at C-3 and further
in THF gave
trans-trans
diene
ester
to a more trans-trans
forms,
16:8+
from
HPLC
and NMR).
Scheme-1
a) NaOH(2N),
24 h (65%), b) DMS, K2C03,
24 h (70%), d) POC13, reflux
aq, 45’C, Benzoyl
MeOH, rt,
peroxide
min (65%),
(cat),
h) MeOH,
6 h, light PPTS,
Mel, 12 h (82%), j) 0s04,
5 h (87%), e) NaOMe,
(95%),
reflux
acetone,
g) Hexamine,
1 h (98%),
Na104, buffer
reflux
Buli,
3.5 days (98%), c) NH3 6 h (80%), f) NBS, CC14,
acid-H20
PhCHO,
V/V),
(I:l,
HMPA,
rt,
pH 7, O°C, 5 h (60%), k) Ph3P+CH3Br-,
THF (20~1, v/v), O°C, 10 min (78%), 1) DDQ, CH3CN-HZ0 CH2-CHXH-MeCI-,
reflux
acetic
i) NaNH2,
reflux
45 min, -45“C,
THF, -78”C,
45 min (93%), o) DIBAL, CH2C12,
80%
30
8 h; K2C03, NaNH2, ether-
(9:l v/v), 1.5 h, rt (95%), m) Ph3P+-
45 min (78%), n) PTS, NaBr, 12, MeOH,
I h, -78“C (92%), p) PDC, CH2C12, molecular
seives,
45 min, rt (70%). Aldol 2). Sodium careful 3 under carried
reaction
experimental Shapiro’s as
(II) acetate
between
methoxide
per
our
2 and 3 in presence
mediated conditions. 10
conditions earlier
and chloroform
rearrangement Model were
approach in acetic
of LDA furnished
to the
experiments
1,3-dione to
the adduct
(13) (Scheme
(14a) was accomplished
synthesize
l4a
directly
from
unsuccessful. Spiro annulation of dione (I4a) was 3c wherein 14a was treated with Mn (III) acetate, , acid
at room
temperature
for 30 min, resulting
under 2 and first Cu in the
2667
formation
of
chloro
Bu3SnH gave
ether
derivative
a mixture
of the
bromo
in 60% which
and acetic
Reductive
10% yield.
at room
acid
yield.
separation
However,
temperature
for
(14b) in 80% yield’ ‘. Radical
derivative
elimination
on chromatographic
A (16) in less than
of fredericamycin
Mn (III) acetate
(15a)
of products,
of
treatment
with
of l4a with CuBr2,
15 min resulted
cyclitation
chlorine
gave the hexamethyl in the
of 14b with
formation
slow addition
Scheme-2
c
I@
c
llo
X=tl
Ub
X=CIorBr
x =Cl
l>b X - Br a) LDA, 3, THF, HMPA, (58%),
c) CuBr2,
benzene,
-78OC, 3 h (54%), b) NaOMe,
Mn(lII)acetate,
slow addition
AcOH,
12 h, 50°C,
I5 min,
e) Ph3SnH
ethylpropionate,
MeOH,
reflux
1.5 h
rt (SO%), d) Ph3SnH (1 eq), AIBN (0.03 eq), (1.1 eq), benzene,
reflux
2 h (55%), f) BBr3,
CH2C12, -78“C, 30 min, OOC, 10 min. of Ph3SnH (I eq), AIBN (0.03 eq) in benzene of
bromine
additional
in 15b (not
isolated)
graphic
2 h gave the hexamethyl ether I1 separation . The NMR spectrum
ture12.
Subjecting
ricamycin
16 with
at 50°C for
by adding
Ph3SnH
12 h followed
(1.1 eq) and
of fredericamycin
of 16 is fully in agreement and bringing 13 sample .
with the natural
the
elimination mixture
A (16) in 55% yield after
BBr3 in CH2C12, -78“C,
A (1) which is identical
by reductive
refluxing with
it slowly
for
chromato-
the assigned
struc-
to 0°C gave
Frede-
Referencess 1.
Isolation
- Pandey,
R.C.;
Toussaint,
Garretson,
A.L.;
1981,
34,
1389; Structure
sot.,
1982,
104,
Wei, T.T.; Byrne,
4478;
-
Misra,
M.W.; Stroshane, K.M.;
Misra,
R.;
R.;
Pandey,
J.V. .I. Anlibiot,
1987, 44
Misra, R.; Pandey,
R.C. Biochemistry,
R.M.; Kalita,
Geoghegan, Pandey,
786; Biosynthesis
R.C.;
R.C.;
B.D.;
KM.;
C.C.;
White,
Silverton,
Hilton,
- Byrne,
1985, 24, 478.
R.F.;
Jr.
XV. Roller,
Hilton,
Aszalos,
A.A.;
R.J. .I. Antibiot., J.
Am.
P.P.;
Chem.
Silverton,
B.D.; White,
R.J.;
2668
2.
Warnick-Pickle, Latham,
Byrne,
a) Rama
K.M.; Pandey,
R.C.;
1988, 41, 976; Dalal,
King,
M.D.;
Pharmacol., 3.
D.J.;
R. J. Antibiot.,
Misra,
C.K.;
Gorycki,
R.J. J. Antibiot.
1981, 34, 1402;
N.S.8 Shi, X. Biochemistry,
White,
1989, 28, 748;
P.; Macdonald,
T.L.;
Ross,
(Bemother.
W.E. Cancer
1989, 24, 167. Rao,
Reddy,
D.R.;
1119; b) Rama
Rao,
A.V.;
Reddy,
1065; c)
Rama
Rao,
A.V.;
Rao,
Comrtun,
1989, 400; d) Rama
A.V.;
Deshpande, D.R.;
D.R.;
Rao,
A.V.;
J.
B.V. Indian
Reddy,
B.V.;
Rao,
J. Chem. Sot.
V.H.
Rao,
Singh,
Chem. Comrmn.,
CRem. Sec.
A.K.
B.V.; Reddy,
J.
Chem.
D.R. lrriian
1982,
B, 1988, 27, Sot.
Chem.
J. Chem.
Sec.
Khodabocus,
A.;
B, 1991, 30, 723. 4.
Other
approaches
Vernon, D. J.
P.G.;
for
constructing
Angoh,
Chem.
Sot.
Spiro system,
Bordeleau,
A&.;
Trans. 1, 1991,
Perkin
see
L.; (in part)
a) Clive,
D.L.J.;
Middleton,
1443; b) Boger,
D.S.;
D.L.;
Lowe,
C.; Kellner, I.C. J. Org.
Jacobson,
Chem., 1991, 56, 2115. 5.
a) Kelly,
T.R.;
Bell,
S.H.; Ohashi,
110, 6471; b) Clive, S.M.; 6.
Boddy,
C.J.;
Richardson,
ABC
Segment
Tetrahedron J.
- a) Rama 1987,
Chem.,
DEF Segment 574; b) Pulla
ault,
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a) Bohlmann, Schmid,
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Details
12.
Spectroscopic
F.; Mannhardt,
Reddy,
D.R. J. Chem.
Pune University,
H.-J.
of this methodology
will be published
India,
Deshpande, N.;
V.H.
Reddy,
D.R.;
K.A.; Spero,
D.M.; Koziski,
A.; Tsuboi,
T.; Hayashida,
Sot.
Chem.
1m
D.L.J.;
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J. J. Hetero-
H.-J.:
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l%l,
26, 3580.
separa-tely.
of 16: ‘H NMR (200 MHz, CDC13):
data
6 1.87, 1.95 (3H, d, J = 7.0 Hz,
2.55 (2H, t, J = 7.5 Hz), 3.40 (2H, t, J = 7.5 Hz), 3.49, 3.52 (3H, s, CH3, 3.96 (3H, s, CH3,
two
sets),
4.05-4.15
(ISH,
s, 5CH3),
5.95 (IH,
6.95, 6.98 (IH, s, two sets),
7.35 (IH, dd, J = 15.0, 10.0 Hz), 7.60, 7.65 (IH, s, two sets),
at 2.55 ppm resulted
singlet
at 3.40 ppm and vice
versa;
IR vmax
(CHC13):
MS m/z : 625 (M+).
We thank Dr Ven L Narayanan,
IICT Communication
G.S.;
1972, 55, 1828.
6.30 (IH, m), 6.50, 6.55 (IH, d, J = 15.0 Hz, two sets),
1700 cm-‘;
Bennett, Nicholas,
Ber. 1956, 89, 1307; b) Hug, R.; Hansen,
Chem.
K.; Youlus, 3.; Freedman,
7.15 (IH, s, two sets),
13.
A&.; D.S.;
1992, 1489.
Sreenivasan,
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Angoh,
Middleton,
Annapurnq,
A.V.;
1986, 27, 3835; d) Clive,
Lett.,
Bertz,
diation
C.;
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A.V.;
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Tetrahedron
3.95,
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b) Rama
Lett.,
cyclic.
sets),
A.V.;
451;
8.
two
D.;
1988,
Chem. Sot. Jpn, 1987, 60, 2927.
- a) Rama
CH3, two sets),
Kellner,
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R.J.
P.G. J. Chem. Sot. Chem. Comnun.
V.H. Tetrahedron Org.
Y.; Khodabocus,
L.;
S.R.; Vernon,
T.; Tsuge, 0. &II. 7.
Tao,
Bardeleau,
Lett.,
Deshpande, K.A.
D.L.J.;
C.N.;
N.; Armstrong-Chong,
No. 3153
(Received in UK 7 December
1992)
NCI, USA, for providing
natural
Fredericamycin-A.
m), 7.10, irra1730,