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Stereospecific total synthesis of ajugarin-IV
Tetrahedron Letters,Vol.23,No.l7,pp Printed in Creat Britain
STEREOSPECIFIC
TOTAL
Andrew Department
1751-1754,1982
S.
SYNTHESIS
Kende
and
0040-4039/82/171751-04$03.00/O 01982 Pergamon Press Ltd.
OF AJUCARIN-IV
Bruce
Roth
of Chemistry, Untversity of Rochester Rochester, New York 14627 lsao Kubo
Diviston
Summary
of Entomology and Parasitology, Colleqe of Natural Resources University of Californta, Berkeley, Caltfornla 94720
A stereospecific
lnsecttcrde
sequence Formation
ajuqarin-IV.
-21 by successive
use of the
from the octalindlone of the
reaqents
butenohde
2 leads
portion
In 21 steps
is conveniently
trts(tr~methylsiloxy)ethylene
and
to the new achteved
from acid
ketenyhdenetrtphenyl-
phosphorane.
Current
efforts
the antifeedant clerodane plant
remota
epoxlde
the total
Insecticidal
antifeedants
Ajuqa
C-4
toward
and
recently
We now describe
a stereospecific
synthesis
natural
of any
regio-
and
stereoselective
more
hiqhly
oxygenated
Our
starting
the dithioketal
methylene verted
to Its Me3SI
minatlon NMR
6 7.12
(d,
that
was the octalindione was converted
enol ether
IS
serve
been
stimulated
class.
Among
unique
uttllzes
that
both the 3
ajuqarlns.
comprises
an lnterestlnq
as prototypes
for
by the
medicinal
In lacklnq
described
by a route
sequence
could
J=lOHr,
reflux,
lH),
6.93
(d,
the first
series
synthesis
was now set for the two-step
enone
MeLt gave
transposition a single 1751
transformed 90°,
of
of the
(NBS,
the conjugated (s,
1H).
developed tertiary
I) to by
2 was con-
O”I and dehydrobro-
(s,
by Dauben
alcohol
followed
ketone
ketone
4.60
(Scheme
70% of the AB trans
numberlnq),
brominatlon
4.63
12 hrs)
of 4 qave
(ajugarin
gave
lH1,
DMSO,
allylatlon
C-7
This
J=lOHz,
the
5 with
C-6
by selective 3 hrs).
was selectively
(4 eqt,
Reductive
staqe
of ketone
z4 which
To functionallze
followed
DMF,
5.
Thus
reaction
(l_12
of the previously
by Ph3P=CH2
to the enone
5, mp 47-49°.6
(LIBr-L12C03,
This
have of this
of the East African
of ajuqarin-IV
tnsecttcrde.
transformations
hydrolyses
ketone
leaves
aJugarlrrlV
characteristic
synthesis
members
ajuqarlns.
This
3.5
total
ajuqarin
material
HgC12-Cd Co3
component
substituent
dlterpenes’
for certain
from the bitter
the trace
oxygen
of clerodane
noted
Isolated
(Lablatae)
and C-16
synthesis
properties
6 [ IR 1H).
1670 C-II-‘,
90%1.
The
and Michno.’
tn nearly
quantitative
yield.
1752
Scheme
I
2 X=Y=O 2 X=S(CH2) 4 X=0,
Scheme
3S, Y=O
Y=CH2
II
y$$y& lJ
R’=R*=O
12 R’=H,
z R*=OH
13 R’=OH,
R*=H
14 R’=H,
Is
R*=OMOM
_.jLj?
R’=H,
R2=CH20H,
16 R’=H,
R*=CHO,
lJ R1=R3=C02CH3, 18 R’=H,
CH302k
’ &tl
19 R’=MOM, g
R’=H,
U
R’=COCH3,
R*=H
R*=H R*=H
R*=H
R2=R3=C02CH3
;!j!Lj?P”
CH,O&
R3=CH20H R3=C02H
&OCH, -22
1753
Unfortunately, drnium
treatment
chlorochromate
of the
desired
enone
be suppressed
25O, 2 hrs)
5.00
lH),
metal
the
ll_,
rn which
”
shown.
the
Reaction
the equatorial
stereochemistry ketone
with
Rf for 12 = 0.15,
6 3.89
1lHz.
J=4.5,
lH),
fi
with
tempt
problems
to direct
the bulky
(6 eqt Jones ing dlester having
E
dicating
C-4
for
C-4
CH20H kinetic
transformed
(1.5
qave
25”,
stlrrlng
12 h). with
IV was accomplished 2 hrs)
followed
dlester
diester
the
saponification
90% of the monoester
brief
t-BuOH,
lo,
aq HCO3
H202
By this
18.
side chain. ester
(3 eqt Ac20, gave
of all volatiles
core now assured, An interesting KOH,
hydrolyzed Et3N,
DMAP,
to the CH2C12,
in 95% yield.
of 21 with
at reduced
solution
excess
pressure
Sla2BH
dlol asslqned
hydroxy
then
reaction -14 was
remaining
24 hrs) ester
10 hr)
Conversion (5 eqt,
and addition
in the
acid Is,
was developed reflux,
CICOCOCI
possl-
the
equlllbratlnq
5 eqt
the dlolefin
25”,
in-
to the desired
the principal
CH30H,
1H)
the desired
pH 5, 24 hrs) and sequence
eqt
asslqned
under
yield.
in
dlester
2Hz.
we explored
with
In 53% overall
(1.1
The
to the aldehyde
2S”,
gave
the correspond-
J=4.5,
was a single
at-
by use of
H202)
to qlve
reactlon
stereo-
to the diaclds
completely
stereospecific
s
alk.
(dd,
to react
oxldatlon
and
respectively.
qroup
25O, 12 hrs)
the acetate2l_
Reaction
CH2N2
convert-
An initial
substituent
In hand,
was allowed
DMF,
was quantitatively
In two steps.
by removal
from
2
reqio-
II).
was therefore
vlnyl
2-methyl-2-butene,
unhindered
Acetylatlon dilute
when
in the ahcycllc
which
(g)
(NMR
2 da).
the
then
6 2.71
out the dlslamylborane
stereolsomer
butenollde
of the
C-4
2S”,
of
(SI qel,
mp 51-52O
was oxldlzed
assignments
of the exocyclrc
(7 eqt PDC,
stereochemistry
Isomer
at
a 20 1 mixture
be quantitatively
2 hrs,
LI.
ketone,
separated
(Scheme
with
(10 eqt
confiquratlon
2,
CH20H
0“+25’,
slqnal
With these
sole product
eqt,
the slnqle
blem was to construct
aq THF,
the
sites
When how-
saturated
gave
we examined
dlol mixture
‘H-nmr
Rf = 0.28
by carrylnq 12 Indeed,
was oxidized
to the desired
With correct
selective
series
CH2C12,
3.1 hexane-EtOAc)
(SI gel,
The
proton.
at reflux
oxidation
2 CH2N2
0.28
stereochemistry.
conditions.
This
Is.
NaClO
and
12 could
30%) and esterlfled
at 400 MHz a clean
the hydroboratlon
5 hours
structure
with
Rf = 0.37
COOCH3
equatorial than
12 hrs,
Alcohol
THF,
source
20 mln)
the equatorial
This
at C-4.
proton
IPr2NEt,
established,
to yield
mixture
83% of pure
at the olefinic
(4 eqt Sia2BH, epimeric
O”+2So,
exhibited
an equatorial
of driving
rather --THF
and 3,
C-4
of 14 at C-4
of dlols
Me2C0,
Rf = 0.37
equatorial bility
rgt,
3 eqt
thus
inseparable
was reduced.
was readily
to qive
3H)l.
(2 eqt,
functlonallzatlon
dlslamylborane
a 1 1 mixture
J=7Hz,
of the B-ring
hydroboratlon
reaqent
80% yield
(d,
a nearly
equatorial
-42O.
mixture
Rf for 13 = 0.40)
0.87
of selective
Et20,
s,
of
to a single
the expected
This
5.
lH),
(br
55% yield. conversion
of added
transformed
(4 eqt,
epimer
6 5.92
for direct
the ally1 qroup
absence
IS asslqned
CICH20CH3
With the stereochemistry chemical
In which
LiAIH4
12 and the axial
ed to the MOM ether
THF,
lo,
1 was quantltatlvely
3 1 hexane-EtOAc, (dd,
NH3,
authors,
py,
NMR
condltlons 10 afforded EtOH)
with 40% 8 could
(6 eqt Cr03*2
in approximately
standard
wrth pyn-
8 toqether
by other
condrtions
1660 cm -‘,
(IR
out in the complete
enone
of this
alcohol
LI,
the latter
was obtained
1 using
byproduct
was carried
E-methyl
3H)]
condltlons
compound
not mentioned
Under
mp 59-61”
s,
of enone (e.g.,
Dauben-Michno
exo-methylene
srde reaction,
z,
(br
2 and the
90 mln),
-33’,
standard
reagent.’
enone
1.97
alcohols
alcohol
reduction
THF,
NH3,
1H).
reduction
to saturated
of the desired ever
(s,
under
unexpected
crystalllne
4.75
Drssolvinq enones
This
1.
alcohol
ZO-30% of the undesired
by use of the Collins
CH2C12, (s,
of this
gave
g
through to give (6N
followed
of c
pro-
HCI. by
to a]ugarln
CH2C12,
25O,
of 15 eqt of neat
tris-
1754
(trtmethylslloxylethylene, of the crystalhne (m.
Reaction
1Hll.
superior
(+)-ajugarin-lV
Into
(1).
to those
12 hrs of heatinq
ketone
of this
to alternative
Identical e
l3 then
hydroxy
22,
hydroxy
reagents
ketone
for our
mp 175-176°.16
of the
(+I-ajugarln-I
natural
at 90’ followed
[ NMR .
mp 128 131 o
series)
Our
product.
by appropriate
with
6 4.27 (s,
ketenylldene
l5 for
by actd hydrolyses 2H1,
(m,
lH1,
triphenylphosphorane
1 hr at 25’ qave
racemtc
aluqarin
Studies
are in proqress
functionalizatlon
2.30
IV had
IR,
UV,
of the C-18
angular
56%
2.15
l4 (vastly
In 86% yteld
crystalline
‘H-NMR
to convert
qave
and MS
our
IntermedIate 17 group.
methyl
References 1.
The first total synthesis of trans-clerodane, (?I-annonene, was achieved by Takahashl, S., Kusumi, T., Kaklsawa, H. ChamistrY Lett. m 515. Other recent approaches include (al Luteijn, J. M., deGrcot, A. Tetrahedron Lett. m 789, Ibid. 1980, 4129 (b) ColdsmIth D. J., SrouJi, C., Kwonq, C. J. Orq. Chem.m, 5, 3182. Seelszference 8.
2.
Kubo,
I.,
3.
Kubo. U.-W.,
I., Kldo. M., Balogh-Nalr,
4.
Kltahara,
5.
WIlllams, J. R., Sarkislan, G. M. Synthesis 1974, 32. R. A. J., Hannah, D. J. Synth. Comm. 1979, 2, 301.
6.
Ardon-Jlmlnez,
7.
Dauben,
a.
For a related allylic enone transposition In an approach deCroot, A. J. Orq. Chem. 1981. 46, 3448.
9.
Collins,
10.
DJerassl,
11.
Stork, G., Darling, D. W., Walshaw, K.
12.
Krublner,
13.
Wissner,
14.
Nlcklsch,
15.
(a) Donovan, Frltsch, W.,
16.
All Intermediates In our synthetic had mp 119-120.5°C. and 400 MHz lH-NMR spectra In agreement with the Synthetic (+I-ajuqarin-IV had mp 175-6’C. UV (CH30H) vmax 212nm. assigned structures. 400 MHz 1H-NMR (CDCl3) 6 5.84 (br s, e 16,000. IR (CH Cl21 1785, 1750, 1730, 1635 cm-l. llHz, 1H). 1.97 (s, 3H). 1.21 (s, 3H). 0.82 (d, 1H). 4.74 (br s, 2?-l 1, 4.60 (dd, J=4.5, J=7Hz, 3H), 0 78 (s, 3H). Synthetic aluqarln-IV exhibited lnsectlcldal actlvltv aaalnst the silkworm. Bombyx marl. at 1500 ppm (LD951, but only qrowth inhibitory actlvlty against the pink bollworm. Pectlnophora qossyplella at 1500 ppm (ED50) with artlflclal diet feedlnq bloassay. This activity IS about one third of natural ajugarln-IV. Natural
to be published. Fukuyama, Y. V., Nakanlshl,
Y.,Yoshikoshl,
A.,
W. G.,
J. C., C.,
A. A. K.,
A.,
Halsall,
Mtchno,
Hess, Gals,
M.,
Klose, S. F., Stache,
Chem. Comm. 1980, A. ibid 3, 9r
S. Tetrahedron
G.
J. Chem.
Frank, L.
Sot.,
Chem.
N., 1979.
1977,
J. Tetrahedron
A.
J. Am.
Bohlmann,
E.
1964,
Kubo,
I.,
Lee,
1763.
For a related
Trans,
example,
I 1978,
Chem.
to alugarln-I
Lett.
see Smith,
1461.
Sot.
86,
P. J. Orq.
see LutelJn,
1968, 1959.
J. M.,
3363. 81,
1761,
Halsall,
Chem.
1968,
2386. T.
33,
G.,
Theobald,
1715.
4617. F.
Chem.
Ber.
1980,
113,
J. E. Tetrahedron Avery, M. A., McMurry, V., Ruschiq, H. Ann. 1966, 669, 195. -= [aD]
897.
‘12, 682.
F.
Okveto, 44,
Lett.
Perkln
D. J. Am. Chem. Sot. 196y, J. Chem. Sot. 1964, 1029.
Chem. W.,
T.
Mitscher,
Gottfrled,
J. Orq.
aJugarln-IV
S. B.
Olda,
D. M. J. Orq.
W. W.,
M.,
J. Chem. Sot. K., Chapya.
2038. Lett.
1979,
3287.
(b)
= -57.5’.
sequencehad IR, MS or mlcroanalysls
17.
Partial supoort of thts work by grant USPHS, IS gratefully acknowledqed.
(Received in USA 26 January
CA-18846,
1982)
awarded
by the
National
Cancer
lnstttute,
STEREOSPECIFIC
TOTAL
Andrew Department
1751-1754,1982
S.
SYNTHESIS
Kende
and
0040-4039/82/171751-04$03.00/O 01982 Pergamon Press Ltd.
OF AJUCARIN-IV
Bruce
Roth
of Chemistry, Untversity of Rochester Rochester, New York 14627 lsao Kubo
Diviston
Summary
of Entomology and Parasitology, Colleqe of Natural Resources University of Californta, Berkeley, Caltfornla 94720
A stereospecific
lnsecttcrde
sequence Formation
ajuqarin-IV.
-21 by successive
use of the
from the octalindlone of the
reaqents
butenohde
2 leads
portion
In 21 steps
is conveniently
trts(tr~methylsiloxy)ethylene
and
to the new achteved
from acid
ketenyhdenetrtphenyl-
phosphorane.
Current
efforts
the antifeedant clerodane plant
remota
epoxlde
the total
Insecticidal
antifeedants
Ajuqa
C-4
toward
and
recently
We now describe
a stereospecific
synthesis
natural
of any
regio-
and
stereoselective
more
hiqhly
oxygenated
Our
starting
the dithioketal
methylene verted
to Its Me3SI
minatlon NMR
6 7.12
(d,
that
was the octalindione was converted
enol ether
IS
serve
been
stimulated
class.
Among
unique
uttllzes
that
both the 3
ajuqarlns.
comprises
an lnterestlnq
as prototypes
for
by the
medicinal
In lacklnq
described
by a route
sequence
could
J=lOHr,
reflux,
lH),
6.93
(d,
the first
series
synthesis
was now set for the two-step
enone
MeLt gave
transposition a single 1751
transformed 90°,
of
of the
(NBS,
the conjugated (s,
1H).
developed tertiary
I) to by
2 was con-
O”I and dehydrobro-
(s,
by Dauben
alcohol
followed
ketone
ketone
4.60
(Scheme
70% of the AB trans
numberlnq),
brominatlon
4.63
12 hrs)
of 4 qave
(ajugarin
gave
lH1,
DMSO,
allylatlon
C-7
This
J=lOHz,
the
5 with
C-6
by selective 3 hrs).
was selectively
(4 eqt,
Reductive
staqe
of ketone
z4 which
To functionallze
followed
DMF,
5.
Thus
reaction
(l_12
of the previously
by Ph3P=CH2
to the enone
5, mp 47-49°.6
(LIBr-L12C03,
This
have of this
of the East African
of ajuqarin-IV
tnsecttcrde.
transformations
hydrolyses
ketone
leaves
aJugarlrrlV
characteristic
synthesis
members
ajuqarlns.
This
3.5
total
ajuqarin
material
HgC12-Cd Co3
component
substituent
dlterpenes’
for certain
from the bitter
the trace
oxygen
of clerodane
noted
Isolated
(Lablatae)
and C-16
synthesis
properties
6 [ IR 1H).
1670 C-II-‘,
90%1.
The
and Michno.’
tn nearly
quantitative
yield.
1752
Scheme
I
2 X=Y=O 2 X=S(CH2) 4 X=0,
Scheme
3S, Y=O
Y=CH2
II
y$$y& lJ
R’=R*=O
12 R’=H,
z R*=OH
13 R’=OH,
R*=H
14 R’=H,
Is
R*=OMOM
_.jLj?
R’=H,
R2=CH20H,
16 R’=H,
R*=CHO,
lJ R1=R3=C02CH3, 18 R’=H,
CH302k
’ &tl
19 R’=MOM, g
R’=H,
U
R’=COCH3,
R*=H
R*=H R*=H
R*=H
R2=R3=C02CH3
;!j!Lj?P”
CH,O&
R3=CH20H R3=C02H
&OCH, -22
1753
Unfortunately, drnium
treatment
chlorochromate
of the
desired
enone
be suppressed
25O, 2 hrs)
5.00
lH),
metal
the
ll_,
rn which
”
shown.
the
Reaction
the equatorial
stereochemistry ketone
with
Rf for 12 = 0.15,
6 3.89
1lHz.
J=4.5,
lH),
fi
with
tempt
problems
to direct
the bulky
(6 eqt Jones ing dlester having
E
dicating
C-4
for
C-4
CH20H kinetic
transformed
(1.5
qave
25”,
stlrrlng
12 h). with
IV was accomplished 2 hrs)
followed
dlester
diester
the
saponification
90% of the monoester
brief
t-BuOH,
lo,
aq HCO3
H202
By this
18.
side chain. ester
(3 eqt Ac20, gave
of all volatiles
core now assured, An interesting KOH,
hydrolyzed Et3N,
DMAP,
to the CH2C12,
in 95% yield.
of 21 with
at reduced
solution
excess
pressure
Sla2BH
dlol asslqned
hydroxy
then
reaction -14 was
remaining
24 hrs) ester
10 hr)
Conversion (5 eqt,
and addition
in the
acid Is,
was developed reflux,
CICOCOCI
possl-
the
equlllbratlnq
5 eqt
the dlolefin
25”,
in-
to the desired
the principal
CH30H,
1H)
the desired
pH 5, 24 hrs) and sequence
eqt
asslqned
under
yield.
in
dlester
2Hz.
we explored
with
In 53% overall
(1.1
The
to the aldehyde
2S”,
gave
the correspond-
J=4.5,
was a single
at-
by use of
H202)
to qlve
reactlon
stereo-
to the diaclds
completely
stereospecific
s
alk.
(dd,
to react
oxldatlon
and
respectively.
qroup
25O, 12 hrs)
the acetate2l_
Reaction
CH2N2
convert-
An initial
substituent
In hand,
was allowed
DMF,
was quantitatively
In two steps.
by removal
from
2
reqio-
II).
was therefore
vlnyl
2-methyl-2-butene,
unhindered
Acetylatlon dilute
when
in the ahcycllc
which
(g)
(NMR
2 da).
the
then
6 2.71
out the dlslamylborane
stereolsomer
butenollde
of the
C-4
2S”,
of
(SI qel,
mp 51-52O
was oxldlzed
assignments
of the exocyclrc
(7 eqt PDC,
stereochemistry
Isomer
at
a 20 1 mixture
be quantitatively
2 hrs,
LI.
ketone,
separated
(Scheme
with
(10 eqt
confiquratlon
2,
CH20H
0“+25’,
slqnal
With these
sole product
eqt,
the slnqle
blem was to construct
aq THF,
the
sites
When how-
saturated
gave
we examined
dlol mixture
‘H-nmr
Rf = 0.28
by carrylnq 12 Indeed,
was oxidized
to the desired
With correct
selective
series
CH2C12,
3.1 hexane-EtOAc)
(SI gel,
The
proton.
at reflux
oxidation
2 CH2N2
0.28
stereochemistry.
conditions.
This
Is.
NaClO
and
12 could
30%) and esterlfled
at 400 MHz a clean
the hydroboratlon
5 hours
structure
with
Rf = 0.37
COOCH3
equatorial than
12 hrs,
Alcohol
THF,
source
20 mln)
the equatorial
This
at C-4.
proton
IPr2NEt,
established,
to yield
mixture
83% of pure
at the olefinic
(4 eqt Sia2BH, epimeric
O”+2So,
exhibited
an equatorial
of driving
rather --THF
and 3,
C-4
of 14 at C-4
of dlols
Me2C0,
Rf = 0.37
equatorial bility
rgt,
3 eqt
thus
inseparable
was reduced.
was readily
to qive
3H)l.
(2 eqt,
functlonallzatlon
dlslamylborane
a 1 1 mixture
J=7Hz,
of the B-ring
hydroboratlon
reaqent
80% yield
(d,
a nearly
equatorial
-42O.
mixture
Rf for 13 = 0.40)
0.87
of selective
Et20,
s,
of
to a single
the expected
This
5.
lH),
(br
55% yield. conversion
of added
transformed
(4 eqt,
epimer
6 5.92
for direct
the ally1 qroup
absence
IS asslqned
CICH20CH3
With the stereochemistry chemical
In which
LiAIH4
12 and the axial
ed to the MOM ether
THF,
lo,
1 was quantltatlvely
3 1 hexane-EtOAc, (dd,
NH3,
authors,
py,
NMR
condltlons 10 afforded EtOH)
with 40% 8 could
(6 eqt Cr03*2
in approximately
standard
wrth pyn-
8 toqether
by other
condrtions
1660 cm -‘,
(IR
out in the complete
enone
of this
alcohol
LI,
the latter
was obtained
1 using
byproduct
was carried
E-methyl
3H)]
condltlons
compound
not mentioned
Under
mp 59-61”
s,
of enone (e.g.,
Dauben-Michno
exo-methylene
srde reaction,
z,
(br
2 and the
90 mln),
-33’,
standard
reagent.’
enone
1.97
alcohols
alcohol
reduction
THF,
NH3,
1H).
reduction
to saturated
of the desired ever
(s,
under
unexpected
crystalllne
4.75
Drssolvinq enones
This
1.
alcohol
ZO-30% of the undesired
by use of the Collins
CH2C12, (s,
of this
gave
g
through to give (6N
followed
of c
pro-
HCI. by
to a]ugarln
CH2C12,
25O,
of 15 eqt of neat
tris-
1754
(trtmethylslloxylethylene, of the crystalhne (m.
Reaction
1Hll.
superior
(+)-ajugarin-lV
Into
(1).
to those
12 hrs of heatinq
ketone
of this
to alternative
Identical e
l3 then
hydroxy
22,
hydroxy
reagents
ketone
for our
mp 175-176°.16
of the
(+I-ajugarln-I
natural
at 90’ followed
[ NMR .
mp 128 131 o
series)
Our
product.
by appropriate
with
6 4.27 (s,
ketenylldene
l5 for
by actd hydrolyses 2H1,
(m,
lH1,
triphenylphosphorane
1 hr at 25’ qave
racemtc
aluqarin
Studies
are in proqress
functionalizatlon
2.30
IV had
IR,
UV,
of the C-18
angular
56%
2.15
l4 (vastly
In 86% yteld
crystalline
‘H-NMR
to convert
qave
and MS
our
IntermedIate 17 group.
methyl
References 1.
The first total synthesis of trans-clerodane, (?I-annonene, was achieved by Takahashl, S., Kusumi, T., Kaklsawa, H. ChamistrY Lett. m 515. Other recent approaches include (al Luteijn, J. M., deGrcot, A. Tetrahedron Lett. m 789, Ibid. 1980, 4129 (b) ColdsmIth D. J., SrouJi, C., Kwonq, C. J. Orq. Chem.m, 5, 3182. Seelszference 8.
2.
Kubo,
I.,
3.
Kubo. U.-W.,
I., Kldo. M., Balogh-Nalr,
4.
Kltahara,
5.
WIlllams, J. R., Sarkislan, G. M. Synthesis 1974, 32. R. A. J., Hannah, D. J. Synth. Comm. 1979, 2, 301.
6.
Ardon-Jlmlnez,
7.
Dauben,
a.
For a related allylic enone transposition In an approach deCroot, A. J. Orq. Chem. 1981. 46, 3448.
9.
Collins,
10.
DJerassl,
11.
Stork, G., Darling, D. W., Walshaw, K.
12.
Krublner,
13.
Wissner,
14.
Nlcklsch,
15.
(a) Donovan, Frltsch, W.,
16.
All Intermediates In our synthetic had mp 119-120.5°C. and 400 MHz lH-NMR spectra In agreement with the Synthetic (+I-ajuqarin-IV had mp 175-6’C. UV (CH30H) vmax 212nm. assigned structures. 400 MHz 1H-NMR (CDCl3) 6 5.84 (br s, e 16,000. IR (CH Cl21 1785, 1750, 1730, 1635 cm-l. llHz, 1H). 1.97 (s, 3H). 1.21 (s, 3H). 0.82 (d, 1H). 4.74 (br s, 2?-l 1, 4.60 (dd, J=4.5, J=7Hz, 3H), 0 78 (s, 3H). Synthetic aluqarln-IV exhibited lnsectlcldal actlvltv aaalnst the silkworm. Bombyx marl. at 1500 ppm (LD951, but only qrowth inhibitory actlvlty against the pink bollworm. Pectlnophora qossyplella at 1500 ppm (ED50) with artlflclal diet feedlnq bloassay. This activity IS about one third of natural ajugarln-IV. Natural
to be published. Fukuyama, Y. V., Nakanlshl,
Y.,Yoshikoshl,
A.,
W. G.,
J. C., C.,
A. A. K.,
A.,
Halsall,
Mtchno,
Hess, Gals,
M.,
Klose, S. F., Stache,
Chem. Comm. 1980, A. ibid 3, 9r
S. Tetrahedron
G.
J. Chem.
Frank, L.
Sot.,
Chem.
N., 1979.
1977,
J. Tetrahedron
A.
J. Am.
Bohlmann,
E.
1964,
Kubo,
I.,
Lee,
1763.
For a related
Trans,
example,
I 1978,
Chem.
to alugarln-I
Lett.
see Smith,
1461.
Sot.
86,
P. J. Orq.
see LutelJn,
1968, 1959.
J. M.,
3363. 81,
1761,
Halsall,
Chem.
1968,
2386. T.
33,
G.,
Theobald,
1715.
4617. F.
Chem.
Ber.
1980,
113,
J. E. Tetrahedron Avery, M. A., McMurry, V., Ruschiq, H. Ann. 1966, 669, 195. -= [aD]
897.
‘12, 682.
F.
Okveto, 44,
Lett.
Perkln
D. J. Am. Chem. Sot. 196y, J. Chem. Sot. 1964, 1029.
Chem. W.,
T.
Mitscher,
Gottfrled,
J. Orq.
aJugarln-IV
S. B.
Olda,
D. M. J. Orq.
W. W.,
M.,
J. Chem. Sot. K., Chapya.
2038. Lett.
1979,
3287.
(b)
= -57.5’.
sequencehad IR, MS or mlcroanalysls
17.
Partial supoort of thts work by grant USPHS, IS gratefully acknowledqed.
(Received in USA 26 January
CA-18846,
1982)
awarded
by the
National
Cancer
lnstttute,