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Prostagland1ns:total synthesis of pgd2 “via” 1,3 cyclopentanedione.
m404020/85 s3.m+ .m 0 1985Rrpmon Ptus Ltd.
TctrW,m Vol. 41. No. 7. pp. 1385to 1392.1985 Printedin Great Britain.
PROSTAGLANDINS:TOTAL
GIANFRANCO CAINELLla* GlORGlO
1,3
CYCLOPENTANEDIONE.
, DARIA GIACOMINla,MAURO
MARTELLlb
and
GIUSEPPE
PANUNZIOa*,
SPUNTAb.
Universita and C.S.F.M.-C.N.R. Chimico “G.Ciamician” Via Selmi 2 1 40126 Bologna (Italy) Composts de1 Carbonio Contenenti Eteroatomt e Loro Appltcazioni 1 4006.4 Ozzano Emilta Italy Via Tolara di Sotto 89
Istituto
a) lstituto
b)
OF PGD2 “via”
SYNTHESIS
dei C.N.R.
(Received ia LIK I2 February 1985) Abstract: precursor
A practtcal is reported.
z?trtp,sy;sat;esf;=;epd
ProstaRlandins was
(PGs)
little
ability
to
them
inhtbit
blood
avotd
parttcular
an
proper
stde
interest,
at
much
step
for
from
this
which
chains
their
recently la aggregation
platelet lc,d . Although
y-keto-esters
and
the
the
drawback
of
discrimtnattng solution system
between
to this as
this
in
this
The
synthetic
readtly
3
. The
a)
by
deprotection
the by
the
rtnq
been
introduction
of
of
position
was
followtnq exposure
to for
ttle
the in
C
our
siqntficance
of
their
potent
, and other
unique
to their
synthests2,
carbonyl 11 opinion, the
tnto
few
function.
Of
base-induced
suitably
elaboration
reliable
Recently
synthesis
proposed
of
includes
a
(5). of
functtonalized PGD
2’
chemoselecttve
we the
have
reported
highly
sequenttal
We wish
to
methods an
substituted
of
attracttve
cyclopentane
bis-acetaltzation-selective report
here
an
from
y-ketoester
application
PGD2. easily
(21,
easily
view lb
activtty
devoted
is,
of
carbonyls.
synthests
in
cyclopentanones
further
lack
cyclopentanedione to the
view,
bioloqtcal
.
the
allowed
antitumor
has
directly
cyclopentanedione
p-toluenesulfonic of
is
solution the
cyclrzation3c.
yteld
of
two
which
procedure
acetahzation
amount
of
avatlable
base-induced overall
the
problem (A)
mono-de-acetalizatton of
method
whose
revaluated
, thetr
potnt
lead
destred
been
effort
baas
The
metabolites.
have
oxidattve
synthetic of
D series
earlier.
properties
cyclizatton wtth
the
apprectated
physioloRica1 of
of
starting from an acycltc total syntheses of PGD A novel effictent tnve?sion of stereochemtstry at by tetrabutylammontum %a” a SN2 dtsplacement
converted
obtained
to
the
monoethylene
acttal
(1) (3)
tn
via 70%
sequence: to acid
Cg carbonyl
an
excess (PTSA)
RrouP
of in
by
ethylene
glycol
benzene
at
stirring
the
tn
reflux product
the for with
presence 8
of
hours,
St0
2
a catalytic b)
selective
and. a catalytic
1386
G. CAINELLIet al.
amount The
of aqueous
9-keto
group
selectrvely the
the
below
1.
of
(3)
produce
the
alcohol
(4)
desired
from
H2SO4 tn methylene
attack
tn
An alternative
route
to
the
of
reduction
of
fl-alcohol
13
the
in
C NMR spectra
Indeed
the
corresponding showed 9
numbertng) tosylate
($1
by
products
the
pentane
(DMF))‘l,
the
catalytic
(9)
amount
acetate next
purpose exposure
key
further
of
starting
was
then
Completton
of
borohydride and
of the In now (2)
to
Cti,Cl,
solution
of
the
at
to
then
synthesis of
was
the
a-8
of
in
(5)
Its
the
80
from
CL) and (Prostane
correspondtng tosylate
the
($1
nitric that
ester
by
to
ester
no
comparison
from
(1)
trace
of
Zn/Cll3COOH
wtth
authentic
(3).
lithium
an
oil
in
anydride
for
2 h,
the
alumtnum
hydride
90% yteld.
Finally
in
pyridlnc
furnished
and
a
quantitatively
with
Zn/CH3COOH.
to
the
practical formation
by
synthesis and of
of
efficient the
f+)
react
tn 12
of
a by
t.1.c.
of
ephedrtne
afford to
aldehyde
of
with
treatment
with
the
(3)
of
ester aldehyde
the
alcohol;
In (2)
sodium
salt
procedure.
procedure: epimeric
polar
the
to mild
standard
step
/CH3CN1’. aq from optically
The
by was
subjected
the
means
known
most
by
was
led by
mi.xture
the
obtained
(g1
three
(2)
solutton
a) C(15) c)
sodium alcohols
hydrolyses
to HF
PGD2 purely method
a
blue
dimethylsulfoxide
to
well a
deep
which
(16)
ketone
afforded
exposure
(12) -
To thts
aldehyde
ozontde
dlazomethane
effected
the
a
oxidation
preparative
Into
appendages.
until
product
by
which
ring
-78°C
bromide
coupled
unsaturated
then
necessary
converted at
following
15-ketone
ester
a
oy
as
0“C
allowed
Cr03/Pyridtne the
to PGD2 methyl complete
of
a -nitric
acetic
the
resultin
esteriflcatlon
by
the
of
of
oxtdattvely
give
separation
developed “via”
attack
was
sequential (2).
b)
(18);
latter
order
In
to
from
the
than Into
with
(2)
excess
was
reduction
converted
reduction
9-
reduction
(DMAP)
(2-oxohepthyl)phosphonate
dimethyl
(17) -
and
to FT
ppm upfleld
NMR spectra
mcnttoning
starting
(4-carboxybutyl)trtphenyl-phosphontum
hydrolysis
0.3
afforded
conformed
alcohol
slight
the
(10) -
purtficatton,
salt
yteld
a
is
ozone
the
methylsulfinylmethtde,
whtch
upon the
pyridine
synthesis
sodium
43%
was
stereospecifically
(4)
converted
the
Thus
oil.
of
by
In
Exposure
70% yield
In
,
whtch
with
dimethylamtne
stream
3c
of
for
~t-butyld~methylsilylchloride--in~~dazole--d~methylformamide-
treatment
sodium basic
group
intermediate
followed
structure
route
(8)
the
of
whose
afforded
an
wtthout
(A),
Reduction
ether
of
a
detected.
ether
as
to
be
procedure
MHz ‘H NMR and
90
13C
the
pyrtdtne.
‘H NMW (see
laboratories.
approx.
tube for 5 hours 10 yield. It is worth
silyl
(10) -
in
conventent
of
resulttng
alcohol.
at
was
13C and
proceeds
shielded
obtained
whtch
formation
group,
these
the
9 - a-
more
exclusive
by
tn
of
condtttons
hydroxyl
a
borohydrtde
to occur
-78’C,
shown
sealed
ethyl by
of
a
give
tnvolves
Moreover
be
chloride
alternattve
phase the
obtained, CG,,
the
of
The
an
anhydrous
acetylatton
thus
in
(3)
known
to
to the
was
Analysis
PG’s8.
C-9
quantitative
hydroxy
gave in
the
in could
by
of
and
12O’C
a-hydroxyacetal
obtained
(LAH)
at
displacement
Protectton
9-p-hydroxy C-8
p-toluenesulfonyl
eltmination
sample
in of
is
at
of
correspondtng
PG’s
THF
developed
sodium 6
of the
9-a-hydroxy
from
yteld.
fl-hydroxy-.acetal
tn
gave
0°C
in
stde,
recently
9 with
.
compounds5,
hindered
C
4
5 hours
configuration
starttng
at
absence
signal
But4N+NO 3 “via” SN2
similar
less
(L)
for
K-Selectride
The
quantitative
the
signals
The
.
the
at
tn
H tn
the
from
ethanol (5)
(C-9)
(5)
yield.
compound
shows
the
tn
70%
stereochemistry
(3)
with
9 a-hydroxyl
hydride
give
reduced
was
of
tnverston
dichloride
for
resolving
salt
of
acttve
precursors,,
cyclopentanedione the
correspondtng
we have
bis-acetal acid
(2)
3c and
1387
Prostaglandins
conversion into
the
Details
to
the
optIcally of
this
optIcally active
process
active natural
~111 be
intermediate PGD2
following
reported
shortly
SCHEME
(23) the
(SCHEME II), route
reported
which
can
in this
11
/ v
r
0
OG
3) CH$J,
(22):
O
‘-‘C02Me
2) H+
:
transformed
elsewhere.
1) (+I Ephedrine
(21)
be
paper.
Cal;’
R = C,H,
(c
R = H
[al;=
= tw.1
-16.5
(c 1.2 CHCI,)
1.2 Cl-ICI,)
(23)
EXPERIMENTAL 1 H and l3C 1.r. spectra were recorded as film on a Perkin-Elmer 710 B spectrophotometer or C6D6 solutions on Varlan Eh: 390 and Varian FT n.m.r. spectra were determlned In CDCl In p.p.m. from as d-values 80 Instruments respectively; chemical 3Shlfts are expressed Internal standard Sthie . Yass spectra were taken on a Varlan Mat 112 S instrument (70 eV). was perfo+med on silica T.1.c. gel sheets (Kirselgel 60 F2 ~ chromatography on a Chromatospac Prep. 10 (JobIn-Ivan instrument? uTinyr~~:lcaan$l cT:iuG h;erck). prior pur~flcatlon, Materials.--Commercially avallable starting materials were used without unless otherwise stated. THF was obtaIned anhydrous and oxye,en-free by dlstlllatlon over sodium benzophenone ketyl under argon. Methylene dlchlorlde was distilled over P 0 . Dllsopropylamlne was refluxed over molecolar sieves (Type /+A, Flukal and cllstllle b 5,t atmospheric pressure. Dlmethyl sulfoxide (DhlSO) was distilled at reduced pressure over Call . bromide and dimethyl-(2-oxo-heptyll(L-Carboxybutyl) triphenyl-phosphonlum phoz?phonatc were purchased from Aldrich. Preparation
of
compounds.
2,3-trans-3,L-trans-2-Ethoxycarbonyl-3-(prop-2-~)-l-hydroxy-cyclopentanone Acetal (5)
Ethylene
--A solution of ketone (3) (lg. 3.9 mmol) in ethanol (5 ml) was added dropwlse at O’C to a stIrred suspension of NaBH (0.6 g,15 mmol) In ethanol (20 ml., 95% solution). The resulting solution was stirredLat this temperature for 1 h, then the excess of the reagent was destroyed with 1% HCl. The mixture was extracted with ether (3 x 30 ml). The combined extracts were dried (MgSO ) and evaporated in vacua to qiv quantitatively the crude acetal (5) as an oil whose iurity was estimated by t.1.c. and 93C n.m . r . analysis to be 100%. m/z 256 (hl+), 238 CM+-H 0). _1 (film) 3 500 and 12735s cm bym&b MHz; CDCl 1 6.0-L.9 Cm 3 HI, L.2 (q 2 HI, 3.9 (m 5 H), 2.8 (bs 1 H 0111, 2.7-2 rcomplex pattern3 6 HI, 1.3 (t 3 H). 2,3-trans-3,L-trans-2-Ethoxycarbonyl-3-(prop-2-~)-l-p-toluen-sulfonyloxy Ethylene Acetal (6).
cyclopentanone
--To a solution of hydroxy ketone (5) (0.6g, 2.3 mmol) in dry methylene dichloride (10 ml) was added at 0°C triethyl amIne (1 ml, 3.5 mmol), p-toluenesulfonyl chloride (0.5g. 2.6 mmol), L-dlmethylamlnopyridyne (DMAP) (0.03Og). The mixture was stlrred overnight at room temperature. After filtration, the reaction mixture was quenched with cold dll. HCl and extracted with methylene dichloride. The organic layers were washed several times with residue was removed in vacua and the water, the solvent was dried ( Na2SOL),
1388
G. CAINELLI
at medium chromatographed (2) (0.99 95%). m/z 410 (M+), 369, 365.
pressure
er
01.
(Cyclohexane/ethyl
(m 5 H),
2.3-1.65
(m 6 H),
l/l)
to
give
the
tosylate
-1
;&%I (film) hiHZ, 1CDCl 73Os,) 17.85 600, (d 1 2370, H), 1 7.35 180. (d 1 090 2 HI, cm 5.45 . g.9
acetate
2.4
(s
3 HI,
1.2
(t
(m 1 H), 3 H).
4.85
(m 2 H),
2,3-trans-3,4-cls-2-Ethoxycarbonyl-3-(prop-2-~)-4-nitroxy-cyclopentanone
4.2
Ethylene
(q
2 H),
Acetal
(1).
tetrabutylammonium nitrate (1 .lg 3.6 solution of tosylate (6) (0.5g, 1.2 mmol) and in pentane was heated In sealed tube at 12O’C for 5 h. The pentane solution was and the solvent removed in vacua to give essentially pure (1) separated from oily-residue (0.35g 97%). m/z 301 (MC), 260, 256, 255. -1 (film) 1 730s. 1 630, 1 280 cm . sVmHz CDCl ) 5.75 (m 1 It), 5.4 (bs 1 II), 5.15 (m 2 HI, 4.2 (q 2 HI, 3.9 (m 4 HI, 2.9 4 HI, 1.2 (t 3 H). r m 2 HI, 2.33(m
--A
mmol)
2,3-trans-3,4-cis-2-Ethoxycarbonyl-3-(prop-2-~)-l-hydroxy (I) (From reduction of nitric ester). --A solution of nitric ester (1) (0.359 1.16 powder in small portions, at room temperature, The reaction mixture was filtered, by t.1.c. washed several times with aq. (5%) NaHC03, stripped off and the residue chromatographed l/l) to give (2) (0.22~ 74%) ldentlc$ in reduction of ketone (3) with K-Selectride . m/z 256 (M+), 238 (M*-tl 0) -1 (film) 3 500 and I2735 cm . 6ymf% MHz C D ) 5.8 (m 1 HI, 5.15 (m 2 7 II), 1.3 (t 3 HI. y-. 1.5 (comp16ex6 pattern
cyclopentanone
Ethylene
Acetal
mmol) in C113COOH (5 ml) was treated with Zn until no more starting material was detected diluted with ether and the organic layers were brine, and dried (Na2S0 ). The solvent was at medium pressure (cycle k exane/ethyl acetate all respects to the product obtalned from
Ii),
4.2
(m
1 H),
4.1
(q
2 HI,
3.9
(m 4 ii),
cyclopentanone
2,3-trans-3,4-cls-2-Ethoxycarbonyl-3-(prop-2-~)-l-t-butyldlmethylsllyloxy Ethylene Acetal (8).
19.5 mmol) In dry dimethylformamide (10 ml) t-butyl--To a solution of alcohol (2) (Sg, 23.6 mmol) and freshly crystallized imldazole (3.54 51 mmol) dlmethylsilyl chloride (3.45g, The mixture was stirred overnight at room temperature, poured Into ice-water were added. The extracts were washed with water, dried over MgSO4 and extracted with ethylacetate. 97%) with a good degree of purity for and concentrated in vacua to give (2, (7.03g, further elaboration. m/z
370 (M+) , 325, (film) 1 750,
tjYPtjb”MHz #,,
0.9
CDCI
1
(s 9 H?,
313 -1 1 650, 1 250, 1 100, 1 040 cm . 6.0-4.7 (m 3 H), 4.05 (q 2 tl), 3.8 0.08 (s 6 HI.
(m 5 H),
3.1-1.9
(m 6 II),
2,3-trans-3,4-cis-2-(~lydroxy-methyl)-3-(~-2-~)-4-t-butyldimethylsi~yloxy Ethylene Acetal (9). (0.759g 20 mmol) was added in small portions --LiAIH After (60 ml) at O’C. mmol) f;, anhydrous ethyl ether solution of NH,+Cl and treated with saturated aqueous Usual work-up gave (2) (5.6g, 90.3%) homogeneous acetate l/l). m/z 328 (M+), 271. -1 (film) 3 530, 1 650 and 1 250 cm . 4.15 (m 1 HI, 3.85 dVw MHz CDCl 1 6.0-4.8 (m 3 Ii) 8H). 2.4-1.8 (2 6 H), 0.88 (s 9 t;,, 0.05 (s 6 HI.
1.3
(t
3
cyclopentanone
to a solution of ester (i) (7g. 18.9 stlrrlng for 1 h, the mixture was extracted with ether (3 x 150 ml). on t.1.c. (silica gel, Hexane/Ethyl
(bs
4
HI, 3.7
(d
2 H),
2.65
(bs
1 H
2,3-trans-3,~-cis-2-(Methyl-acetyloxy)-3-(prop-2-~~-4-t-butyldimethyls~lyloxy-cyclopentanone Ethylene
Acetal
(IO).
-A mixture of alcohol (2) (5.4g, 16.4 mmol), pyridine (5 ml), acetic anhydride The solution is partitioned and OhlAP (0.2q) is allowed to stand for 1 h at O’C. ethylacetate and cold HCl (30 ml 1 NJ, the organic phase IS washed with saturated
(5 ml), between NaHC03,
1389
Rostaglandins dried over MgSO,,, and yield (64). m/z 370 (hi+), 313, 253 dv?&? u ).
the
solvent
removed
3 ~),~0.88
(s
vacua.
Was
obtained
(10) -
as
an
oil
in
96%
-1
(film) MHz CDCl 1 750, 1 6.0-4.7 1 650 and (m 31 2.40 H) cm 4.25 2 (s
in
9 Ii).
0.05’(s
(m
1 HI,
4.15
(d
2 It),
3.8
(bs
4 HI,
2.5-1.6
(m 6
6 11).
2,3-trans-3,4-c~s-2-~Methyl-acetyloxy~-3-(methyl-formyl~-4-t-butyldimethylsililoxy-cyclopentanone Ethylene Acetal (11). --A solution of (10) (6~ 16.1 mmol) in methylene dichloride (50 ml) was cooled to -78°C. Ozone was passed through the solution at the rate of 0.5 ml/mln until deep blue solution. the system was flushed with nitrogen until colourless solution, the While still at -78°C temperature was then allowed to rise to O’C and acetic acid (10 ml) was added, followed by Zn powder In small portlons at room temperature monitorlnq by t.1.c. (S102, Hexane/EthylThe resulting mixture was fIltered, acetate 6/4) until the reduction of ozonide was complete. washed several times with water. The organic layer the pll adjusted at 7 with NaHC03 (5%). solvent removed In vacua to give the 011~ aldehyde (5.3g 88.5%) which was employed as such in successive step. m/z
372 (M+), 315, 313 -1 (film) 2 700, 1 740, 1 725, 1 250, 1 040 cm . 4.2 (m 1 H), 4.15 (d 2 It), bvw MHz CDCI ) 9.8 (s 1 II CHO) #,, 2.05 (s 3 ?i,, 0.9 (s 9 H), 0.d5 (s 3 HI, 0.025 (s 3 HI.
3.9
(s
4 H),
2.7-2.2
(m 6
2,3-trans-3,4-c~s-2-O~ydroxy-methyl)-3-~6-methoxycarbonyl-hex-2~Z)-enyl~-4-t-butyld~methylsllyloxy-cyclopentanone Ethylene Acetal (14). (4.2~) and dimethylsulfoxide (50 ml --A rnlxture of 50% sodium hydride-dlsperslon-in-oil freshly distilled over calcium hydride) was stirred under argoIt at 75°C until gas evolution ceased (1 h). To the resulting solution (33.6 ml, 67 mmol, 2 M in sodium methylsulflnylmethide) cooled to room temperature, (4-carboxybutyl)-triphenyl-phosphonlum bromide (15.64, 35 mmol) in DMSO (40 ml) was added dropwise. After the deep red liquid had been stirred for a further 20 min, 14 mnol) in DMSO (40 ml) was added. The a solution of the aldehyde (11) (5.3g. temperature was raised to 5O”C, and stlrring continued for 1 h. The mixture was poured into Ice-water and extracted with ethyl acetate. The cooled aqueous layer was acidified with dll. HCl and extracted with ethyl acetate (3 x 100 ml). The combined organic extracts were washed with water, dried (MgS04) and concentrated. The resulting crude product (5~) was dissolved in methanol (100 ml) and treated with K2CO3 (3!33 at reflux for 1 h. The methanol was stripped off and the mixture was poured Into ice-water, acidified with dil. HCl, extracted with ethyl acetate, washed with brine, dried and concentrated. To the oil-residue ethereal dlazomethane was added and the solution stlrred at 0°C for 1 h. To this solution were added few drops of acetlc acid In order to destroy the excess of reagent and the solvent was removed In vacua. The final product was purified by chromatography at medium pressure on silica gel elutlng with ethyl acetate/hexane l/l to yield the alcohol (g) as colourless oil (2.69, 43% from 2). m/z 428 (M+), 410, 397, 371. -1 3 530, 1 735, 1 250, 1 080, 1 040 cm . CDCl_) 5.3 (m 2 tl), 4.02 (m 1 HI, 3.75 (m 7 Ii), 3.5 (s 3 HI, 2.4(bs 1 H OH), 11 d), 0.8 (s 9 II), 0.05 (s 6 HI. 2,3-trans-3,4-c~s-2-Formyl-3-/6-methoxycarbonyl-hex-2~Z~-~/-4-t-butyldimethylsilyloxy-~ pentanone Ethylene Acetal (15). --To a solution of chromium trioxide (0.87q)-pyridine (1.5 ml)-complex in anhydrous methylene dichloride (20 ml), was added at O’C with stirring under argon, a solution of alcohol (14) (0.5g 1.2 mmol) In methylene dichloride (10 ml). After 20 mln the mixture was filtered on dry diatomaceous earth (Celite 2Og0, washed with ice-cooled HCl (1 N) and the solvent removed in vacua to give the aldehyde (15) (0.45g 90%). m/z 426 CM+), 395, 369. -1 dyw 2.0-1.5 (film) MHz (m CDCl 12 2 710, d),1 9.7 0.8 1 735, (s (d 9H), 11 720, HIA.05 15.4250. (s (m 6 1 HI. 2100HI,and4.25 1 040 (m cm 1 HI, .
3.9
(m 4 HI,
3.65
(s
3 H),
1391
Prostaglandins
Table--
4 CInf 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 1% 19 20
46.8 71.0 47.1 117.5 57.8 171.2
13
5
48.7 73.5 45.7 116.5 58.2 171.7
C N.m.r.
chemical
8
115.7 137.3 33.3 47.1 71.6 47.9 117.0 57.8 170.8
2
115.5 137.9 32.6 44.8 71.3 47.1 117.7 51.3 59.3
shifts
and
for
Compounds 11 14
10
115.7 137.6 32.7 47.2 71.1 67.2 116.1 68.8 63.0
asslgnements
200.3 63.3 61.8 71.0 47.2 115.8 48.6 63.1
Chemical shifts in p.p,m. downfleld from Me4Sl. fourier mode with a Varian FT 80 spectrometer. b) Prostane numbering. c) Assignements may be
173.3 25.1 c 26.0 i 27.0 129.7 129.7 33.4 45.6 71.5 47.1 117.6 51.6 60.0
Spectra
were
cyclopentanoids
15
16
qz;;
+;
128.6 130.6 33.3 45.8 71.9 47.8 117.5 63.0 200.1
taken
17 173.1
173.1
173.1
+zi 129.1 129.8
tn
33.3 50.4 71.5 68.3 117.7 55.1 146.3 132.9 198.3 60.14 31.8
129.4 128.0 33.1 50.9 71.0 48.3 117.6 55.0 138.1 130.0 72.9 37.9 32.3
16.1
14.3
C6D6
a,b
derivative
at
20.00
1% 173.1 27.0 c 25.6 t 25.2 129.4 128.5 33.3 50.6 71.0 48.2 117.5 56.9 137.5 129.8 72.4 37.9 32.3
IL.2 MHz in
reversed.
References and notes. and W.L.killler, j.Aied.Chem., D.R.Yorton, D.C.Petersen, E.E.Nlehlzawa, 1. (a) G.L.Bundy, 26, 790. (1983); (b) M.Fukushima, T.Kato, R.Ueda, K.Ota, S.Narumiya, and O.Havalshl, Ic) R.Ueno, K.Ifonda, S.lno&, and ~ochem.Biophys.Res.~ommun., 9, 956, (1982). O.Hayaishl, Proc.Natl.Acad.Scl.USA, 80, 1735, (1983): (d) E.J.Corey, K.Shlnoli. J.Am.Chem. 105, 1662, (1983) and references cited hereln. s0c.E chemical synthesis of PGDs: PGD (a) t:,tIayashi and T.Tanouchi, j.Org.Chem., 2. Previoz W.L.&ller, R.R.Gorman, and G.L.Bundy, Prostaglan2, 2115, (1973); (b) E.E.Nishizawa, dins. 2, 109, (1975); (cl N.H.Andersen, S.lmamoto, and D.H.Plcker, Prostaglandtns, G, 61,(1977). See also reference la. (d) E.F.Jenny, P.Schaublin, H.Fritz, and H.Fuhrer, Tetrahedron Lett., te) E.W.Collinston, C.J.Wallis, and I.Waterhouse, 2235, (1974); Tetrahedron Lett., 26, 3125, (1983): (f) D.P.Reynolds, R.F.Newton, and S.M.Roberts, j.Chem.Soc.,Chem.Comyun., 1150, (1979); (g) R.F.Newton, D.P.Reynold, C.F.Webb, and S.hi.Roberts, j.Chem.Soc.,Perkin Trans.1, 2055, 11981); (h) T.W.iIart, D.A.hletcalfe and F.Scheinmann, j.Chem.Soc.,Chem.Commun., 156, (1979); (if A.G.Cameron, A.T.Hewson and A.H. Wadsworth, Tetrahedron Lett., 2, 561, (19821; (1) M.Suzuki, A.Yanagisawa, and R.Noyori, Tetrahedron Lett., 1383, (1984). G.Catnelll, M.Panunzlo, L.Plessi, G.Martelll, G,Spunta, Gazz.Ch~m.ltal.,ll4, 327, 3. (a) (b) A.Bonginl, G.Cainelll, D.Giacomlni, M.Panunzio, R.Danleli, Gxrtellt, (1984); G.Spunta, j.Chem.Soc.; Perkin Trans. 1, 000, (cl A.Bonqini, G.Cainelli, 1985 : D.Slacomlni, M.Panunzio, G.Martelll, G.Spunta, Tetrahedron, lo, 2861 (1984) A.Lechevallier, kl.Pellet, J.ht.Conia, Synthesis, 63, (197%). 6. F.Huet, H.C.Brown, S.Krlshmamurty, Tetrahedron, 35, 567, (19791; (bf E.J.Corey, R.K.Varma, 5. (a) J.Am.Chem.Soc., 93, 7319, (1971). stereospeclflcally reductton 6. This is rather surprisingly sance NaBH 1s known to g’ve a 47 mixture of diastereomerlc alcohols in molecules of similar structure . However previous studies in prostaglandins field have shown that the same stereospe yf;c l$gductlon takes place when the C-11 carbonyl group 1s protected by a dlthiane ring . The reason of remarkable this stereospecific reduction is currently u.~der investigation in our laboratory. E.G.Daniels, F.H.Lincoln, J.E.Pike. j.Am.Chem.Soc., 2, 2124, 11972) and 7. G.L.Bundy, references cited thereln. (a) F.H.Lincoln, 8. W.P.Schneider, and J.E.Pike, J.Org.Chem., 951, 3&, i 1973). H.J.Schnelder, N.Nguyan-Ba, and F.Thomas, Tetrahedron, 23, 2327, (1982). 9. 10. G.Catnelli, F.Manescalchl, G,Martelli, M.Panunzio, L.Plessi, Work in preparation. 11. E.J.Corey, A.Venkateswarlu, j.Am.Chem.Soc., 94, 6190, (19721. 12. (a) E.J.Corey, G.T.Kwlatkowski, j.Am.Chem.Soc., 88, 5654, (1966): (b) E.J.Corey,
the
G. CNNELLIet al.
1392 E.Hamanaka,
Ibid,,
g,
2758,
(1967);
(c)
A.p.Grieco,
Ch.Pogonowskt, x,
95. 3071,
(1973). (1979); (b) A.G.Cameron, 13, (a) R.F.Newton and D.P.Rcynolds, Tetrahedron Latt-9 3981, A_T.Hewwn, A.H.Wadsworth, J.Chem.Soc.Perkin 1, 2337, (1984).
SCHEME
1
(2)
(4): R = OH;
R’ = H
4s) : R = H
(5): R = l-4;
R’ = OH
(10) : R = COCH,
IS): R = H;
R’ = OTs
(7): R =ONO,;
R’ = H
(8): R = OSiMe,;
R’ = H
ill):
R = COW,
4
(121:R = COW,;
R’= H
(13): R=
H;
R=N
(14): R=
H;
R’= Me
0
(I@):
117): R=H;
R’ =OH
120): ~~014
(18):
R’=H
(16):
R=R’=
R=OH;
R=H;
R’=OH R*=H
TctrW,m Vol. 41. No. 7. pp. 1385to 1392.1985 Printedin Great Britain.
PROSTAGLANDINS:TOTAL
GIANFRANCO CAINELLla* GlORGlO
1,3
CYCLOPENTANEDIONE.
, DARIA GIACOMINla,MAURO
MARTELLlb
and
GIUSEPPE
PANUNZIOa*,
SPUNTAb.
Universita and C.S.F.M.-C.N.R. Chimico “G.Ciamician” Via Selmi 2 1 40126 Bologna (Italy) Composts de1 Carbonio Contenenti Eteroatomt e Loro Appltcazioni 1 4006.4 Ozzano Emilta Italy Via Tolara di Sotto 89
Istituto
a) lstituto
b)
OF PGD2 “via”
SYNTHESIS
dei C.N.R.
(Received ia LIK I2 February 1985) Abstract: precursor
A practtcal is reported.
z?trtp,sy;sat;esf;=;epd
ProstaRlandins was
(PGs)
little
ability
to
them
inhtbit
blood
avotd
parttcular
an
proper
stde
interest,
at
much
step
for
from
this
which
chains
their
recently la aggregation
platelet lc,d . Although
y-keto-esters
and
the
the
drawback
of
discrimtnattng solution system
between
to this as
this
in
this
The
synthetic
readtly
3
. The
a)
by
deprotection
the by
the
rtnq
been
introduction
of
of
position
was
followtnq exposure
to for
ttle
the in
C
our
siqntficance
of
their
potent
, and other
unique
to their
synthests2,
carbonyl 11 opinion, the
tnto
few
function.
Of
base-induced
suitably
elaboration
reliable
Recently
synthesis
proposed
of
includes
a
(5). of
functtonalized PGD
2’
chemoselecttve
we the
have
reported
highly
sequenttal
We wish
to
methods an
substituted
of
attracttve
cyclopentane
bis-acetaltzation-selective report
here
an
from
y-ketoester
application
PGD2. easily
(21,
easily
view lb
activtty
devoted
is,
of
carbonyls.
synthests
in
cyclopentanones
further
lack
cyclopentanedione to the
view,
bioloqtcal
.
the
allowed
antitumor
has
directly
cyclopentanedione
p-toluenesulfonic of
is
solution the
cyclrzation3c.
yteld
of
two
which
procedure
acetahzation
amount
of
avatlable
base-induced overall
the
problem (A)
mono-de-acetalizatton of
method
whose
revaluated
, thetr
potnt
lead
destred
been
effort
baas
The
metabolites.
have
oxidattve
synthetic of
D series
earlier.
properties
cyclizatton wtth
the
apprectated
physioloRica1 of
of
starting from an acycltc total syntheses of PGD A novel effictent tnve?sion of stereochemtstry at by tetrabutylammontum %a” a SN2 dtsplacement
converted
obtained
to
the
monoethylene
acttal
(1) (3)
tn
via 70%
sequence: to acid
Cg carbonyl
an
excess (PTSA)
RrouP
of in
by
ethylene
glycol
benzene
at
stirring
the
tn
reflux product
the for with
presence 8
of
hours,
St0
2
a catalytic b)
selective
and. a catalytic
1386
G. CAINELLIet al.
amount The
of aqueous
9-keto
group
selectrvely the
the
below
1.
of
(3)
produce
the
alcohol
(4)
desired
from
H2SO4 tn methylene
attack
tn
An alternative
route
to
the
of
reduction
of
fl-alcohol
13
the
in
C NMR spectra
Indeed
the
corresponding showed 9
numbertng) tosylate
($1
by
products
the
pentane
(DMF))‘l,
the
catalytic
(9)
amount
acetate next
purpose exposure
key
further
of
starting
was
then
Completton
of
borohydride and
of the In now (2)
to
Cti,Cl,
solution
of
the
at
to
then
synthesis of
was
the
a-8
of
in
(5)
Its
the
80
from
CL) and (Prostane
correspondtng tosylate
the
($1
nitric that
ester
by
to
ester
no
comparison
from
(1)
trace
of
Zn/Cll3COOH
wtth
authentic
(3).
lithium
an
oil
in
anydride
for
2 h,
the
alumtnum
hydride
90% yteld.
Finally
in
pyridlnc
furnished
and
a
quantitatively
with
Zn/CH3COOH.
to
the
practical formation
by
synthesis and of
of
efficient the
f+)
react
tn 12
of
a by
t.1.c.
of
ephedrtne
afford to
aldehyde
of
with
treatment
with
the
(3)
of
ester aldehyde
the
alcohol;
In (2)
sodium
salt
procedure.
procedure: epimeric
polar
the
to mild
standard
step
/CH3CN1’. aq from optically
The
by was
subjected
the
means
known
most
by
was
led by
mi.xture
the
obtained
(g1
three
(2)
solutton
a) C(15) c)
sodium alcohols
hydrolyses
to HF
PGD2 purely method
a
blue
dimethylsulfoxide
to
well a
deep
which
(16)
ketone
afforded
exposure
(12) -
To thts
aldehyde
ozontde
dlazomethane
effected
the
a
oxidation
preparative
Into
appendages.
until
product
by
which
ring
-78°C
bromide
coupled
unsaturated
then
necessary
converted at
following
15-ketone
ester
a
oy
as
0“C
allowed
Cr03/Pyridtne the
to PGD2 methyl complete
of
a -nitric
acetic
the
resultin
esteriflcatlon
by
the
of
of
oxtdattvely
give
separation
developed “via”
attack
was
sequential (2).
b)
(18);
latter
order
In
to
from
the
than Into
with
(2)
excess
was
reduction
converted
reduction
9-
reduction
(DMAP)
(2-oxohepthyl)phosphonate
dimethyl
(17) -
and
to FT
ppm upfleld
NMR spectra
mcnttoning
starting
(4-carboxybutyl)trtphenyl-phosphontum
hydrolysis
0.3
afforded
conformed
alcohol
slight
the
(10) -
purtficatton,
salt
yteld
a
is
ozone
the
methylsulfinylmethtde,
whtch
upon the
pyridine
synthesis
sodium
43%
was
stereospecifically
(4)
converted
the
Thus
oil.
of
by
In
Exposure
70% yield
In
,
whtch
with
dimethylamtne
stream
3c
of
for
~t-butyld~methylsilylchloride--in~~dazole--d~methylformamide-
treatment
sodium basic
group
intermediate
followed
structure
route
(8)
the
of
whose
afforded
an
wtthout
(A),
Reduction
ether
of
a
detected.
ether
as
to
be
procedure
MHz ‘H NMR and
90
13C
the
pyrtdtne.
‘H NMW (see
laboratories.
approx.
tube for 5 hours 10 yield. It is worth
silyl
(10) -
in
conventent
of
resulttng
alcohol.
at
was
13C and
proceeds
shielded
obtained
whtch
formation
group,
these
the
9 - a-
more
exclusive
by
tn
of
condtttons
hydroxyl
a
borohydrtde
to occur
-78’C,
shown
sealed
ethyl by
of
a
give
tnvolves
Moreover
be
chloride
alternattve
phase the
obtained, CG,,
the
of
The
an
anhydrous
acetylatton
thus
in
(3)
known
to
to the
was
Analysis
PG’s8.
C-9
quantitative
hydroxy
gave in
the
in could
by
of
and
12O’C
a-hydroxyacetal
obtained
(LAH)
at
displacement
Protectton
9-p-hydroxy C-8
p-toluenesulfonyl
eltmination
sample
in of
is
at
of
correspondtng
PG’s
THF
developed
sodium 6
of the
9-a-hydroxy
from
yteld.
fl-hydroxy-.acetal
tn
gave
0°C
in
stde,
recently
9 with
.
compounds5,
hindered
C
4
5 hours
configuration
starttng
at
absence
signal
But4N+NO 3 “via” SN2
similar
less
(L)
for
K-Selectride
The
quantitative
the
signals
The
.
the
at
tn
H tn
the
from
ethanol (5)
(C-9)
(5)
yield.
compound
shows
the
tn
70%
stereochemistry
(3)
with
9 a-hydroxyl
hydride
give
reduced
was
of
tnverston
dichloride
for
resolving
salt
of
acttve
precursors,,
cyclopentanedione the
correspondtng
we have
bis-acetal acid
(2)
3c and
1387
Prostaglandins
conversion into
the
Details
to
the
optIcally of
this
optIcally active
process
active natural
~111 be
intermediate PGD2
following
reported
shortly
SCHEME
(23) the
(SCHEME II), route
reported
which
can
in this
11
/ v
r
0
OG
3) CH$J,
(22):
O
‘-‘C02Me
2) H+
:
transformed
elsewhere.
1) (+I Ephedrine
(21)
be
paper.
Cal;’
R = C,H,
(c
R = H
[al;=
= tw.1
-16.5
(c 1.2 CHCI,)
1.2 Cl-ICI,)
(23)
EXPERIMENTAL 1 H and l3C 1.r. spectra were recorded as film on a Perkin-Elmer 710 B spectrophotometer or C6D6 solutions on Varlan Eh: 390 and Varian FT n.m.r. spectra were determlned In CDCl In p.p.m. from as d-values 80 Instruments respectively; chemical 3Shlfts are expressed Internal standard Sthie . Yass spectra were taken on a Varlan Mat 112 S instrument (70 eV). was perfo+med on silica T.1.c. gel sheets (Kirselgel 60 F2 ~ chromatography on a Chromatospac Prep. 10 (JobIn-Ivan instrument? uTinyr~~:lcaan$l cT:iuG h;erck). prior pur~flcatlon, Materials.--Commercially avallable starting materials were used without unless otherwise stated. THF was obtaIned anhydrous and oxye,en-free by dlstlllatlon over sodium benzophenone ketyl under argon. Methylene dlchlorlde was distilled over P 0 . Dllsopropylamlne was refluxed over molecolar sieves (Type /+A, Flukal and cllstllle b 5,t atmospheric pressure. Dlmethyl sulfoxide (DhlSO) was distilled at reduced pressure over Call . bromide and dimethyl-(2-oxo-heptyll(L-Carboxybutyl) triphenyl-phosphonlum phoz?phonatc were purchased from Aldrich. Preparation
of
compounds.
2,3-trans-3,L-trans-2-Ethoxycarbonyl-3-(prop-2-~)-l-hydroxy-cyclopentanone Acetal (5)
Ethylene
--A solution of ketone (3) (lg. 3.9 mmol) in ethanol (5 ml) was added dropwlse at O’C to a stIrred suspension of NaBH (0.6 g,15 mmol) In ethanol (20 ml., 95% solution). The resulting solution was stirredLat this temperature for 1 h, then the excess of the reagent was destroyed with 1% HCl. The mixture was extracted with ether (3 x 30 ml). The combined extracts were dried (MgSO ) and evaporated in vacua to qiv quantitatively the crude acetal (5) as an oil whose iurity was estimated by t.1.c. and 93C n.m . r . analysis to be 100%. m/z 256 (hl+), 238 CM+-H 0). _1 (film) 3 500 and 12735s cm bym&b MHz; CDCl 1 6.0-L.9 Cm 3 HI, L.2 (q 2 HI, 3.9 (m 5 H), 2.8 (bs 1 H 0111, 2.7-2 rcomplex pattern3 6 HI, 1.3 (t 3 H). 2,3-trans-3,L-trans-2-Ethoxycarbonyl-3-(prop-2-~)-l-p-toluen-sulfonyloxy Ethylene Acetal (6).
cyclopentanone
--To a solution of hydroxy ketone (5) (0.6g, 2.3 mmol) in dry methylene dichloride (10 ml) was added at 0°C triethyl amIne (1 ml, 3.5 mmol), p-toluenesulfonyl chloride (0.5g. 2.6 mmol), L-dlmethylamlnopyridyne (DMAP) (0.03Og). The mixture was stlrred overnight at room temperature. After filtration, the reaction mixture was quenched with cold dll. HCl and extracted with methylene dichloride. The organic layers were washed several times with residue was removed in vacua and the water, the solvent was dried ( Na2SOL),
1388
G. CAINELLI
at medium chromatographed (2) (0.99 95%). m/z 410 (M+), 369, 365.
pressure
er
01.
(Cyclohexane/ethyl
(m 5 H),
2.3-1.65
(m 6 H),
l/l)
to
give
the
tosylate
-1
;&%I (film) hiHZ, 1CDCl 73Os,) 17.85 600, (d 1 2370, H), 1 7.35 180. (d 1 090 2 HI, cm 5.45 . g.9
acetate
2.4
(s
3 HI,
1.2
(t
(m 1 H), 3 H).
4.85
(m 2 H),
2,3-trans-3,4-cls-2-Ethoxycarbonyl-3-(prop-2-~)-4-nitroxy-cyclopentanone
4.2
Ethylene
(q
2 H),
Acetal
(1).
tetrabutylammonium nitrate (1 .lg 3.6 solution of tosylate (6) (0.5g, 1.2 mmol) and in pentane was heated In sealed tube at 12O’C for 5 h. The pentane solution was and the solvent removed in vacua to give essentially pure (1) separated from oily-residue (0.35g 97%). m/z 301 (MC), 260, 256, 255. -1 (film) 1 730s. 1 630, 1 280 cm . sVmHz CDCl ) 5.75 (m 1 It), 5.4 (bs 1 II), 5.15 (m 2 HI, 4.2 (q 2 HI, 3.9 (m 4 HI, 2.9 4 HI, 1.2 (t 3 H). r m 2 HI, 2.33(m
--A
mmol)
2,3-trans-3,4-cis-2-Ethoxycarbonyl-3-(prop-2-~)-l-hydroxy (I) (From reduction of nitric ester). --A solution of nitric ester (1) (0.359 1.16 powder in small portions, at room temperature, The reaction mixture was filtered, by t.1.c. washed several times with aq. (5%) NaHC03, stripped off and the residue chromatographed l/l) to give (2) (0.22~ 74%) ldentlc$ in reduction of ketone (3) with K-Selectride . m/z 256 (M+), 238 (M*-tl 0) -1 (film) 3 500 and I2735 cm . 6ymf% MHz C D ) 5.8 (m 1 HI, 5.15 (m 2 7 II), 1.3 (t 3 HI. y-. 1.5 (comp16ex6 pattern
cyclopentanone
Ethylene
Acetal
mmol) in C113COOH (5 ml) was treated with Zn until no more starting material was detected diluted with ether and the organic layers were brine, and dried (Na2S0 ). The solvent was at medium pressure (cycle k exane/ethyl acetate all respects to the product obtalned from
Ii),
4.2
(m
1 H),
4.1
(q
2 HI,
3.9
(m 4 ii),
cyclopentanone
2,3-trans-3,4-cls-2-Ethoxycarbonyl-3-(prop-2-~)-l-t-butyldlmethylsllyloxy Ethylene Acetal (8).
19.5 mmol) In dry dimethylformamide (10 ml) t-butyl--To a solution of alcohol (2) (Sg, 23.6 mmol) and freshly crystallized imldazole (3.54 51 mmol) dlmethylsilyl chloride (3.45g, The mixture was stirred overnight at room temperature, poured Into ice-water were added. The extracts were washed with water, dried over MgSO4 and extracted with ethylacetate. 97%) with a good degree of purity for and concentrated in vacua to give (2, (7.03g, further elaboration. m/z
370 (M+) , 325, (film) 1 750,
tjYPtjb”MHz #,,
0.9
CDCI
1
(s 9 H?,
313 -1 1 650, 1 250, 1 100, 1 040 cm . 6.0-4.7 (m 3 H), 4.05 (q 2 tl), 3.8 0.08 (s 6 HI.
(m 5 H),
3.1-1.9
(m 6 II),
2,3-trans-3,4-cis-2-(~lydroxy-methyl)-3-(~-2-~)-4-t-butyldimethylsi~yloxy Ethylene Acetal (9). (0.759g 20 mmol) was added in small portions --LiAIH After (60 ml) at O’C. mmol) f;, anhydrous ethyl ether solution of NH,+Cl and treated with saturated aqueous Usual work-up gave (2) (5.6g, 90.3%) homogeneous acetate l/l). m/z 328 (M+), 271. -1 (film) 3 530, 1 650 and 1 250 cm . 4.15 (m 1 HI, 3.85 dVw MHz CDCl 1 6.0-4.8 (m 3 Ii) 8H). 2.4-1.8 (2 6 H), 0.88 (s 9 t;,, 0.05 (s 6 HI.
1.3
(t
3
cyclopentanone
to a solution of ester (i) (7g. 18.9 stlrrlng for 1 h, the mixture was extracted with ether (3 x 150 ml). on t.1.c. (silica gel, Hexane/Ethyl
(bs
4
HI, 3.7
(d
2 H),
2.65
(bs
1 H
2,3-trans-3,~-cis-2-(Methyl-acetyloxy)-3-(prop-2-~~-4-t-butyldimethyls~lyloxy-cyclopentanone Ethylene
Acetal
(IO).
-A mixture of alcohol (2) (5.4g, 16.4 mmol), pyridine (5 ml), acetic anhydride The solution is partitioned and OhlAP (0.2q) is allowed to stand for 1 h at O’C. ethylacetate and cold HCl (30 ml 1 NJ, the organic phase IS washed with saturated
(5 ml), between NaHC03,
1389
Rostaglandins dried over MgSO,,, and yield (64). m/z 370 (hi+), 313, 253 dv?&? u ).
the
solvent
removed
3 ~),~0.88
(s
vacua.
Was
obtained
(10) -
as
an
oil
in
96%
-1
(film) MHz CDCl 1 750, 1 6.0-4.7 1 650 and (m 31 2.40 H) cm 4.25 2 (s
in
9 Ii).
0.05’(s
(m
1 HI,
4.15
(d
2 It),
3.8
(bs
4 HI,
2.5-1.6
(m 6
6 11).
2,3-trans-3,4-c~s-2-~Methyl-acetyloxy~-3-(methyl-formyl~-4-t-butyldimethylsililoxy-cyclopentanone Ethylene Acetal (11). --A solution of (10) (6~ 16.1 mmol) in methylene dichloride (50 ml) was cooled to -78°C. Ozone was passed through the solution at the rate of 0.5 ml/mln until deep blue solution. the system was flushed with nitrogen until colourless solution, the While still at -78°C temperature was then allowed to rise to O’C and acetic acid (10 ml) was added, followed by Zn powder In small portlons at room temperature monitorlnq by t.1.c. (S102, Hexane/EthylThe resulting mixture was fIltered, acetate 6/4) until the reduction of ozonide was complete. washed several times with water. The organic layer the pll adjusted at 7 with NaHC03 (5%). solvent removed In vacua to give the 011~ aldehyde (5.3g 88.5%) which was employed as such in successive step. m/z
372 (M+), 315, 313 -1 (film) 2 700, 1 740, 1 725, 1 250, 1 040 cm . 4.2 (m 1 H), 4.15 (d 2 It), bvw MHz CDCI ) 9.8 (s 1 II CHO) #,, 2.05 (s 3 ?i,, 0.9 (s 9 H), 0.d5 (s 3 HI, 0.025 (s 3 HI.
3.9
(s
4 H),
2.7-2.2
(m 6
2,3-trans-3,4-c~s-2-O~ydroxy-methyl)-3-~6-methoxycarbonyl-hex-2~Z)-enyl~-4-t-butyld~methylsllyloxy-cyclopentanone Ethylene Acetal (14). (4.2~) and dimethylsulfoxide (50 ml --A rnlxture of 50% sodium hydride-dlsperslon-in-oil freshly distilled over calcium hydride) was stirred under argoIt at 75°C until gas evolution ceased (1 h). To the resulting solution (33.6 ml, 67 mmol, 2 M in sodium methylsulflnylmethide) cooled to room temperature, (4-carboxybutyl)-triphenyl-phosphonlum bromide (15.64, 35 mmol) in DMSO (40 ml) was added dropwise. After the deep red liquid had been stirred for a further 20 min, 14 mnol) in DMSO (40 ml) was added. The a solution of the aldehyde (11) (5.3g. temperature was raised to 5O”C, and stlrring continued for 1 h. The mixture was poured into Ice-water and extracted with ethyl acetate. The cooled aqueous layer was acidified with dll. HCl and extracted with ethyl acetate (3 x 100 ml). The combined organic extracts were washed with water, dried (MgS04) and concentrated. The resulting crude product (5~) was dissolved in methanol (100 ml) and treated with K2CO3 (3!33 at reflux for 1 h. The methanol was stripped off and the mixture was poured Into ice-water, acidified with dil. HCl, extracted with ethyl acetate, washed with brine, dried and concentrated. To the oil-residue ethereal dlazomethane was added and the solution stlrred at 0°C for 1 h. To this solution were added few drops of acetlc acid In order to destroy the excess of reagent and the solvent was removed In vacua. The final product was purified by chromatography at medium pressure on silica gel elutlng with ethyl acetate/hexane l/l to yield the alcohol (g) as colourless oil (2.69, 43% from 2). m/z 428 (M+), 410, 397, 371. -1 3 530, 1 735, 1 250, 1 080, 1 040 cm . CDCl_) 5.3 (m 2 tl), 4.02 (m 1 HI, 3.75 (m 7 Ii), 3.5 (s 3 HI, 2.4(bs 1 H OH), 11 d), 0.8 (s 9 II), 0.05 (s 6 HI. 2,3-trans-3,4-c~s-2-Formyl-3-/6-methoxycarbonyl-hex-2~Z~-~/-4-t-butyldimethylsilyloxy-~ pentanone Ethylene Acetal (15). --To a solution of chromium trioxide (0.87q)-pyridine (1.5 ml)-complex in anhydrous methylene dichloride (20 ml), was added at O’C with stirring under argon, a solution of alcohol (14) (0.5g 1.2 mmol) In methylene dichloride (10 ml). After 20 mln the mixture was filtered on dry diatomaceous earth (Celite 2Og0, washed with ice-cooled HCl (1 N) and the solvent removed in vacua to give the aldehyde (15) (0.45g 90%). m/z 426 CM+), 395, 369. -1 dyw 2.0-1.5 (film) MHz (m CDCl 12 2 710, d),1 9.7 0.8 1 735, (s (d 9H), 11 720, HIA.05 15.4250. (s (m 6 1 HI. 2100HI,and4.25 1 040 (m cm 1 HI, .
3.9
(m 4 HI,
3.65
(s
3 H),
1391
Prostaglandins
Table--
4 CInf 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 1% 19 20
46.8 71.0 47.1 117.5 57.8 171.2
13
5
48.7 73.5 45.7 116.5 58.2 171.7
C N.m.r.
chemical
8
115.7 137.3 33.3 47.1 71.6 47.9 117.0 57.8 170.8
2
115.5 137.9 32.6 44.8 71.3 47.1 117.7 51.3 59.3
shifts
and
for
Compounds 11 14
10
115.7 137.6 32.7 47.2 71.1 67.2 116.1 68.8 63.0
asslgnements
200.3 63.3 61.8 71.0 47.2 115.8 48.6 63.1
Chemical shifts in p.p,m. downfleld from Me4Sl. fourier mode with a Varian FT 80 spectrometer. b) Prostane numbering. c) Assignements may be
173.3 25.1 c 26.0 i 27.0 129.7 129.7 33.4 45.6 71.5 47.1 117.6 51.6 60.0
Spectra
were
cyclopentanoids
15
16
qz;;
+;
128.6 130.6 33.3 45.8 71.9 47.8 117.5 63.0 200.1
taken
17 173.1
173.1
173.1
+zi 129.1 129.8
tn
33.3 50.4 71.5 68.3 117.7 55.1 146.3 132.9 198.3 60.14 31.8
129.4 128.0 33.1 50.9 71.0 48.3 117.6 55.0 138.1 130.0 72.9 37.9 32.3
16.1
14.3
C6D6
a,b
derivative
at
20.00
1% 173.1 27.0 c 25.6 t 25.2 129.4 128.5 33.3 50.6 71.0 48.2 117.5 56.9 137.5 129.8 72.4 37.9 32.3
IL.2 MHz in
reversed.
References and notes. and W.L.killler, j.Aied.Chem., D.R.Yorton, D.C.Petersen, E.E.Nlehlzawa, 1. (a) G.L.Bundy, 26, 790. (1983); (b) M.Fukushima, T.Kato, R.Ueda, K.Ota, S.Narumiya, and O.Havalshl, Ic) R.Ueno, K.Ifonda, S.lno&, and ~ochem.Biophys.Res.~ommun., 9, 956, (1982). O.Hayaishl, Proc.Natl.Acad.Scl.USA, 80, 1735, (1983): (d) E.J.Corey, K.Shlnoli. J.Am.Chem. 105, 1662, (1983) and references cited hereln. s0c.E chemical synthesis of PGDs: PGD (a) t:,tIayashi and T.Tanouchi, j.Org.Chem., 2. Previoz W.L.&ller, R.R.Gorman, and G.L.Bundy, Prostaglan2, 2115, (1973); (b) E.E.Nishizawa, dins. 2, 109, (1975); (cl N.H.Andersen, S.lmamoto, and D.H.Plcker, Prostaglandtns, G, 61,(1977). See also reference la. (d) E.F.Jenny, P.Schaublin, H.Fritz, and H.Fuhrer, Tetrahedron Lett., te) E.W.Collinston, C.J.Wallis, and I.Waterhouse, 2235, (1974); Tetrahedron Lett., 26, 3125, (1983): (f) D.P.Reynolds, R.F.Newton, and S.M.Roberts, j.Chem.Soc.,Chem.Comyun., 1150, (1979); (g) R.F.Newton, D.P.Reynold, C.F.Webb, and S.hi.Roberts, j.Chem.Soc.,Perkin Trans.1, 2055, 11981); (h) T.W.iIart, D.A.hletcalfe and F.Scheinmann, j.Chem.Soc.,Chem.Commun., 156, (1979); (if A.G.Cameron, A.T.Hewson and A.H. Wadsworth, Tetrahedron Lett., 2, 561, (19821; (1) M.Suzuki, A.Yanagisawa, and R.Noyori, Tetrahedron Lett., 1383, (1984). G.Catnelll, M.Panunzlo, L.Plessi, G.Martelll, G,Spunta, Gazz.Ch~m.ltal.,ll4, 327, 3. (a) (b) A.Bonginl, G.Cainelll, D.Giacomlni, M.Panunzio, R.Danleli, Gxrtellt, (1984); G.Spunta, j.Chem.Soc.; Perkin Trans. 1, 000, (cl A.Bonqini, G.Cainelli, 1985 : D.Slacomlni, M.Panunzio, G.Martelll, G.Spunta, Tetrahedron, lo, 2861 (1984) A.Lechevallier, kl.Pellet, J.ht.Conia, Synthesis, 63, (197%). 6. F.Huet, H.C.Brown, S.Krlshmamurty, Tetrahedron, 35, 567, (19791; (bf E.J.Corey, R.K.Varma, 5. (a) J.Am.Chem.Soc., 93, 7319, (1971). stereospeclflcally reductton 6. This is rather surprisingly sance NaBH 1s known to g’ve a 47 mixture of diastereomerlc alcohols in molecules of similar structure . However previous studies in prostaglandins field have shown that the same stereospe yf;c l$gductlon takes place when the C-11 carbonyl group 1s protected by a dlthiane ring . The reason of remarkable this stereospecific reduction is currently u.~der investigation in our laboratory. E.G.Daniels, F.H.Lincoln, J.E.Pike. j.Am.Chem.Soc., 2, 2124, 11972) and 7. G.L.Bundy, references cited thereln. (a) F.H.Lincoln, 8. W.P.Schneider, and J.E.Pike, J.Org.Chem., 951, 3&, i 1973). H.J.Schnelder, N.Nguyan-Ba, and F.Thomas, Tetrahedron, 23, 2327, (1982). 9. 10. G.Catnelli, F.Manescalchl, G,Martelli, M.Panunzio, L.Plessi, Work in preparation. 11. E.J.Corey, A.Venkateswarlu, j.Am.Chem.Soc., 94, 6190, (19721. 12. (a) E.J.Corey, G.T.Kwlatkowski, j.Am.Chem.Soc., 88, 5654, (1966): (b) E.J.Corey,
the
G. CNNELLIet al.
1392 E.Hamanaka,
Ibid,,
g,
2758,
(1967);
(c)
A.p.Grieco,
Ch.Pogonowskt, x,
95. 3071,
(1973). (1979); (b) A.G.Cameron, 13, (a) R.F.Newton and D.P.Rcynolds, Tetrahedron Latt-9 3981, A_T.Hewwn, A.H.Wadsworth, J.Chem.Soc.Perkin 1, 2337, (1984).
SCHEME
1
(2)
(4): R = OH;
R’ = H
4s) : R = H
(5): R = l-4;
R’ = OH
(10) : R = COCH,
IS): R = H;
R’ = OTs
(7): R =ONO,;
R’ = H
(8): R = OSiMe,;
R’ = H
ill):
R = COW,
4
(121:R = COW,;
R’= H
(13): R=
H;
R=N
(14): R=
H;
R’= Me
0
(I@):
117): R=H;
R’ =OH
120): ~~014
(18):
R’=H
(16):
R=R’=
R=OH;
R=H;
R’=OH R*=H