Synthesis of steroids

First obtained from Physosligma venenosum (Calabar bean) and is readily isolated from many plant sources where it often co-occurs with sitosterol. It has served as a starting substance for the synthesis of steroid hormones. 

Methyl vinyl ketone is used as a comonomer in photodegradable plastics, and is an intermediate in the synthesis of steroids and vitamin A. It is highly toxic and faciUties handling over a threshold of 100 lbs (45.5 kg) are subject to special OSHA documentation regulations (273). 

The pharmaceutical industry employs ozone in organic reactions to produce peroxides as germicides in skin lotions, for the oxidation of intermediates for bacteriostats, and in the synthesis of steroids (qv) such as cortisone (see Disinfectants and antiseptics). Vitamin E can be prepared by ozonation of trimethyUiydroquinone. 

During this period of intense synthetic research, a search for inexpensive raw materials for the partial synthesis of steroids was initiated. Abundant quantities of the sapogenin diosgenin [512-04-9] were isolated from plant sources and used for the industrial preparation of steroids (9). 

The 1950s and 1960s saw the development of orally active progestins based on the synthesis of steroids that lack the C19-angular methyl substituent (19-norsteroids). The commercial production of these compounds for the regulation of menstmal disorders began in 1957, and for oral contraception in 1960. 

The stereocontroUed syntheses of steroid side chains for ecdysone, cmstecdysone, brassinoHde, withanoHde, and vitamin D have been reviewed (185). Also, other manuscripts, including reviews on the partial synthesis of steroids (186), steroid dmgs (187—189), biologically active steroids (190), heterocychc steroids (191), vitamin D (192), novel oxidations of steroids (193), and template-directed functionali2ation of steroids (194), have been pubhshed. 

Estranes. Investigations into the total synthesis of steroids began in the 1930s shordy after the precise formula for cholesterol was estabUshed. The eadiest studies focused on equilenin (5) because of its relative stereochemical simplicity when compared to other steroid nuclei Initially, equilenin was synthesi2ed in 20 chemical steps with an overall yield of 2.7%. This synthesis helped to confirm the perhydro-l,2-cyclopentenophenanthrene ring system of... 

A more recent ring annulation strategy for the total synthesis of steroids from the Stork group is shown in the following equation (210 — 211 — ... 

D. Lednicer and L. A. Mitscher, The Organic Chemistry of Drug Synthesis Vols. 1—4, John Wiley and Sons, Inc., New York, 1977,1980, 1984,1990, for general references of partial synthesis of steroid dmgs. 

A. A. Akhrem and Y. A. Titov, Total Steroid Synthesis, Plenum Press, New York, 1970, for total synthesis of steroids before 1970. 

Synthesis of steroidal diazirines has led to some biologically active compounds (65JA2665). The observation that diazirines and their parent ketones are identical in smell (B-67MI50800), points to the possibility that a diazirine group may stand for a keto group vis-d-vis a receptor. 

This chapter will deal exclusively with three-membered rings containing the hetero atoms O, S and N, and fused to the steroid skeleton. Because of the conformational requirements in steroids, not all of the usual methods of synthesis of three-membered rings are applicable to the fused ring system. For the synthesis of steroids to which an aziridine, oxirane or thiirane is attached either in the side chain or at a ring position but not directly fused to the nucleus, the methods discussed in this chapter, as well as others, are applicable. 

The high degree of stereoselectivity associated with most syntheses and reactions of oxiranes accounts for the enormous utility of these systems in steroid syntheses. Individual selectivity at various positions in the steroid nucleus necessitates the discussion of a collection of uniquely specific reactions used in the synthesis of steroidal epoxides. The most convenient and generally applicable methods involve the peracid, the alkaline hydrogen peroxide and the halohydrin reactions. Several additional but more limited techniques are also available. 

Few procedures are available for the synthesis of steroid thiiranes because the rigidity of the steroid nucleus prohibits the application of many methods of thiirane synthesis. The only general methods involve the con-... 

Recent improvements in the total synthesis of steroids which give as the first tetracyclic products 19-norsteroids bearing a hydroxyl or keto group at C-17 have revived interest in the conversion of androstanes to pregnanes. 

An ingenious approach to the synthesis of steroids incorporating a tropone A ring has been developed by Birch and co-workers. Addition of dibromocarbene to 3-methoxyestra-2,5(10)-dien-17-one 17-ethylene ketal (42) gives a monodibromocarbene adduct formulated as (43) accompanied by a minor amount of a bisadduct. This confirms earlier observations that electrophilic halocarbenes add mainly to 2,3- or 2,5-dihydroanisoles at the double bond bearing the methoxyl group. 

Alkylation of dienamines with alkyl halides has been found to take place at the oc carbon (288-290). The reaction was used in the synthesis of steroid analogs (291). 

The rearrangement with ring contraction probably is the most important synthetic application of the Favorskii reaction it is for example used in the synthesis of steroids. Yields can vary from good to moderate. As solvents diethyl ether or alcohols are often used. With acyclic a-halo ketones bearing voluminous substituents in a -position, yields can be low a tcrt-butyl substituent will prevent the rearrangement. 

Hydrogenolysis of methylenediisoxazoles have been useful in preparing substituted resorcinols and aminophenols (7). The isoxazole annelation reaction (71,89,90,91,103) is well suited to the synthesis of steroids and other complex molecules. 

The so-called Wieland-Miescher ketone is a valuable starting materia) used in the synthesis of steroid hormones. How might you prepare it hom 1,3-cycio-hexanedione ... 

Intermolecular [4C+2S] cycloaddition reactions where the diene moiety is contained in the carbene complex are less frequent than the [4S+2C] cycloadditions summarised in the previous section. However, 2-butadienylcarbene complexes, generated by a [2+2]/cyclobutene ring opening sequence, undergo Diels-Alder reactions with typical dienophiles [34,35] (Scheme 59). Also, Wulff et al. have described the application of pyranylidene complexes, obtained by a [3+3] cycloaddition reaction (see Sect. 2.8.1), in the inverse-electron-demand Diels-Alder reaction with enol ethers and enamines [87a]. Later, this strategy was applied to the synthesis of steroid-like ring skeletons [87b] (Scheme 59). 

Dihydro-1-vinylnaphthalene (67) as well as 3,4-dihydro-2-vinylnaphtha-lene (68) are more reactive than the corresponding aromatic dienes. Therefore they may also undergo cycloaddition reactions with low reactive dienophiles, thus showing a wider range of applications in organic synthesis. The cycloadditions of dienes 67 and 68 and of the 6-methoxy-2,4-dihydro-1-vinylnaphthalene 69 have been used extensively in the synthesis of steroids, heterocyclic compounds and polycyclic aromatic compounds. Some of the reactions of dienes 67-69 are summarized in Schemes 2.24, 2.25 and 2.26. In order to synthesize indeno[c]phenanthrenones, the cycloaddition of diene 67 with 3-bromoindan-l-one, which is a precursor of inden-l-one, was studied. Bromoindanone was prepared by treating commercially available indanone with NBS [64]. 

Winterfeldt E. Enantiomerically Pure Cyclopentadienes Chem. Rev. 199393 827 843 Keywords synthesis of steroid cyclopentadienes, hydrindan dienes and their kinetic resolution... 

Blickenstaff, R.T. Ghosh, A.C. Wolf, G.C. Total Synthesis of Steroids (Organic Chemistry Vol, 30) p. 187 ff Academic Press, New York, London 1974. 

Some representative Claisen rearrangements are shown in Scheme 6.14. Entry 1 illustrates the application of the Claisen rearrangement in the introduction of a substituent at the junction of two six-membered rings. Introduction of a substituent at this type of position is frequently necessary in the synthesis of steroids and terpenes. In Entry 2, formation and rearrangement of a 2-propenyl ether leads to formation of a methyl ketone. Entry 3 illustrates the use of 3-methoxyisoprene to form the allylic ether. The rearrangement of this type of ether leads to introduction of isoprene structural units into the reaction product. Entry 4 involves an allylic ether prepared by O-alkylation of a (3-keto enolate. Entry 5 was used in the course of synthesis of a diterpene lactone. Entry 6 is a case in which PdCl2 catalyzes both the formation and rearrangement of the reactant. 

A combination of a Sakurai reaction [447] as the first step with an ene reaction has been developed by Tietze and coworkers for the synthesis of steroids [448]. These studies are discussed in Chapter 4. 

---