5a acetate

The exchange of alkoxy groups for the cyanide function can also be achieved in acetals (cyclic types like dioxolanes and 1,3-dioxane derivatives included), 5A -acetals and ortho esters with the combination of TMS-CN/Lewis acids, or under neutral conditions with transition metal salts as catalysts (Scheme 16). Furanose derivatives may be treated with TMS-CN in a similar way. ... 

Beside the above-mentioned hydroxylation steps, oxygenation at C-9 is also presumed to occur fairly early in the pathway. A clone for the cytochrome P450 taxoid 9a-hydroxylase was tentatively identified, but testing the 5a,13a-diol, the 5a,10p-diol, and the corresponding 5a-acetates as substrates could not provide sufficient biosynthetic products to permit NMR-based confirmation of structures [251]. 

Markedly branched alkyl 3,3,3-trialkylpropanedithioates (69) can be prepared by 1,4-addition of or-ganometallics to a,p-unsaturated imidothioates and subsequent sulfhydrolysis of the ketene 5A( acetals according to equation (65). 

Since the expression of some of the genes originating from plants requires specialized environments or compartments, the host strain E. coli alone is not competent to produce subsequent metabolites after taxadiene in the paclitaxel pathway. The production of taxadine-5 -ol and taxadien-5a-acetate-lO -ol in E. coli and S. cerevisiae consortium brings some inspirations in the heterologous production of natural products (i) we can take full usage of the properties in different species And (ii) spatial segregation the whole pathway into different microbes helps to prevent some internal regulation in the pathway, and pathway modules can be separately optimized. 

As first demonstrated by Stork,the metal enolate formed by metal-ammoni reduction of a conjugated enone or a ketol acetate can be alkylated in liquic ammonia. The reductive alkylation reaction is synthetically useful since ii permits alkylation of a ketone at the a-position other than the one at whicf thermodynamically controlled enolate salt formation occurs. Direct methyl-ation of 5a-androstan-17-ol-3-one occurs at C-2 whereas reductive methyl-... 

The presence of an a-bromo substituent may cause anomalies. With NaBH4, 2a-bromo-5a-cholestan-3-one gives a mixture of epimers, in which the 3p-o predominates. 4 -Bromo-17)5-hydroxy-5)5-androstan-3-one acetate gives 25% of the 315,4 -bromohydrin and 34% of the 3a,4)5-compound. Reduction of 7a-bromo-3)5,5a-diacetoxycholestan-6-one gives exclusively 7a-bromocholestane-3)5,5a,6a-triol 3,5-diacetate,whereas reduc-... 

Zinc dust (35 mg) is added to a solution of 9a-bromo-5a-androstan-ll-one (225, 13 mg) in anhydrous ether (2 ml) and acetic acid-OD (0.5 ml, prepared by heating an equimolar mixture of acetic anhydride and deuterium oxide) and the resulting suspension is stirred at room temperature for 4 hr. (The progress of the reaction can be checked by thin layer chromatography.) The... 

A solution of 6a,7 x-oxido-5a-cholestan-3j8-ol acetate (232, 3.07 g) in anhydrous ether (100 ml) is treated with lithium aluminum deuteride (0.88 g) and... 

In the absence of steric factors e.g. 5 ), the attack is antiparallel (A) (to the adjacent axial bond) and gives the axially substituted chair form (12). In the presence of steric hindrance to attack in the preferred fashion, approach is parallel (P), from the opposite side, and the true kinetic product is the axially substituted boat form (13). This normally undergoes an immediate conformational flip to the equatorial chair form (14) which is isolated as the kinetic product. The effect of such factors is exemplified in the behavior of 3-ketones. Thus, kinetically controlled bromination of 5a-cholestan-3-one (enol acetate) yields the 2a-epimer, (15), which is also the stable form. The presence of a 5a-substituent counteracts the steric effect of the 10-methyl group and results in the formation of the unstable 2l5-(axial)halo ketone... 

The reaction of A -bromosuccinimide with 5a-cholestan-3-one enol acetate in aprotic conditions, described by Green and Long, is probably free radical in character cf. ref. 69). 

The scope of this reaction was investigated by Djerassi, °° who showed that 4-bromo ketones in the series and 2-bromo ketones in the 5a series give unsaturated 2,4-dinitrophenylhydrazones in 80-90% yield on warming under nitrogen with 1.1 moles of 2,4-dinitrophenylhydrazine in acetic acid. Cleavage with pyruvic acid affords the pure unsaturated ketones in 60-70 % yield. 

Acetoxy-17a-hydroxy-5a-pregnane-3,l 1,20-trione (40) is brominated in acetic acid under equilibrating conditions to give a solution of the 2a,4a-di-bromo compound (41). This is reduced by chromous chloride without further treatment, to the 4a-bromo compound (42). The recrystallized bromo compound (42) is then dehydrobrominated via the semicarbazone (43) which is converted without isolation into cortisone acetate (44) by treatment with pyruvic acid ... 

Thionyl chloride behaves in some circumstances as though it dehydrates by tran -diaxial elimination, as described for phosphorous oxychloride. For example, the 5a-alcohol (102) undergoes anti-Saytzelf elimination to give the A" -olefin. In this particular example, phosphorous oxychloride-pyridine does not work, and acetic anhydride-sulfuric acid gives the A -isomer (ref. 185, p. 199). 

Hydroboration affords an efficient preparation of the 5a-A -system (141, for example) from A" -3-ketones. Reaction with diborane followed by decomposition of the organoboron intermediate with refluxing acetic anhydride gives good yields of olefins. Ketones must be protected, and alcohols are transformed to acetates. A -7-Ketones yield 5oc-A -olefins (for example, 138). 

Selectivity in formation of protective groups may also be achieved by a proper choice of reaction conditions and catalyst. Thus formation of the 3-monothioketal from 3,6-diketones is achieved by dilution of the ethane-dithiol-boron trifluoride reaction mixture with acetic acid. 3-Monocyanohydrins are obtained in good yield from 3,20-diketo-(5a)-pregnanes by diluting the exchange reaction with ethanol. Similarly, dilution of the... 

Beta- and 3a-alcohols of the 5)5- and 5a-series respectively also form tetrahydropyranyl ethers, cycloalkenyl ethers and mixed acetals. ... 

Cyano-3 -hydroxy-5a-pregnan-20-one A suspension of 5a-pregnane-3, 20-dione (2 g) in ethanol (90 ml) is treated with acetone cyanohydrin (4 ml) and three drops of triethylamine and stirred at room temperature until complete dissolution. After 3 hr, the solution is diluted with 200 ml of water, acidified with acetic acid and the crystalline precipitate is thoroughly washed with water and dried under vacuum to give 2.1 g (97%) of product mp 172-178° (dec). A sample recrystallized from ethyl acetate melts at 176-179° (dec) [a]p 86° (ethyl acetate). 

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