CA1058160A - Cycloaliphatic thiones - Google Patents
Cycloaliphatic thionesInfo
- Publication number
- CA1058160A CA1058160A CA233,024A CA233024A CA1058160A CA 1058160 A CA1058160 A CA 1058160A CA 233024 A CA233024 A CA 233024A CA 1058160 A CA1058160 A CA 1058160A
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07J—STEROIDS
- C07J31/00—Normal steroids containing one or more sulfur atoms not belonging to a hetero ring
- C07J31/003—Normal steroids containing one or more sulfur atoms not belonging to a hetero ring the S atom directly linked to a ring carbon atom of the cyclopenta(a)hydrophenanthrene skeleton
-
- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07J—STEROIDS
- C07J33/00—Normal steroids having a sulfur-containing hetero ring spiro-condensed or not condensed with the cyclopenta(a)hydrophenanthrene skeleton
- C07J33/005—Normal steroids having a sulfur-containing hetero ring spiro-condensed or not condensed with the cyclopenta(a)hydrophenanthrene skeleton spiro-condensed
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- Organic Chemistry (AREA)
- Health & Medical Sciences (AREA)
- General Health & Medical Sciences (AREA)
- Steroid Compounds (AREA)
- Furan Compounds (AREA)
Abstract
ABSTRACT OF THE DISCLOSURE
Compounds of the general formula
Compounds of the general formula
Description
o This invention relates to cycloaliphatic thiones, in particular steroid thiones.
Compared with the aryl thiones, very few aliphatic thiones are known. Low molecular weight aliphatic thiones are known only to exist as trimeric species, i.e. 1~3,5 -trithianes. Higher molecular weight aliphatic thiones do exist in monomeric form, but tautomerisation to the corres-ponding enethiol occurs to a major extent unless the structure renders it unli~ely or impossible.
Steroid 1,4-diene-3-thiones would on theoretical grounds be considered to favour the enethiol form in view of the conjugation present but it has now been found however that, surprisingly,the cross-conjugated thione system found in a steroid 1,4-diene-3-thione or related compounds such as the thione analogue of santonin, exists in thione form as a stable entity.
The new compounds may be considered as cyclohexa-2,5-diene-l-thiones which may be substituted or form part of a poly-cyclic ring structure. However, in order to avoid isomerisation to tautomeric thiophenols, the 4-position of the cyclohexadiene ring should be disubstituted, i.e. should not carry a hydrogen atom . Such thiones can be represented, in general, by the formula
Compared with the aryl thiones, very few aliphatic thiones are known. Low molecular weight aliphatic thiones are known only to exist as trimeric species, i.e. 1~3,5 -trithianes. Higher molecular weight aliphatic thiones do exist in monomeric form, but tautomerisation to the corres-ponding enethiol occurs to a major extent unless the structure renders it unli~ely or impossible.
Steroid 1,4-diene-3-thiones would on theoretical grounds be considered to favour the enethiol form in view of the conjugation present but it has now been found however that, surprisingly,the cross-conjugated thione system found in a steroid 1,4-diene-3-thione or related compounds such as the thione analogue of santonin, exists in thione form as a stable entity.
The new compounds may be considered as cyclohexa-2,5-diene-l-thiones which may be substituted or form part of a poly-cyclic ring structure. However, in order to avoid isomerisation to tautomeric thiophenols, the 4-position of the cyclohexadiene ring should be disubstituted, i.e. should not carry a hydrogen atom . Such thiones can be represented, in general, by the formula
- 2 -1058~0 ~/
wherein the substituents R, which may be the same or different, represent hydrogen atoms or hydrocarbyl groups and the groups Rl represent hydrocarbyl groups or adjacent pairs of substituents R, or R and Rl together with the carbon atoms to which they are attached may constitute a non-aromatic ring structure, with the proviso that one of the ad;acent pairs of R and Rl forms part of a ring structure, said hydrocarbyl groups or ring structure if desired carrying one or more substituents.
- Where any of the groups R and Rl are hydrocarbyl groups, these may, for example~ be alkyl groups having 1-6 carbon atoms e.g. methyl groups as in santonin or in pregnanes. One of the adjacent pairs R and R represents a cyclic group, which may be monocyclic or, as in steroids or in santonin, polycyclic. In both the latter cases, one group Rl is alkyl while the other forms part of a ring structure. Such ring structures may be carbocyclic as in corticosteroids or may contain heterocyclic rings, e.g. the ~ ' .
lactone ring in santonin. Santonin has the formula:-_CH3
wherein the substituents R, which may be the same or different, represent hydrogen atoms or hydrocarbyl groups and the groups Rl represent hydrocarbyl groups or adjacent pairs of substituents R, or R and Rl together with the carbon atoms to which they are attached may constitute a non-aromatic ring structure, with the proviso that one of the ad;acent pairs of R and Rl forms part of a ring structure, said hydrocarbyl groups or ring structure if desired carrying one or more substituents.
- Where any of the groups R and Rl are hydrocarbyl groups, these may, for example~ be alkyl groups having 1-6 carbon atoms e.g. methyl groups as in santonin or in pregnanes. One of the adjacent pairs R and R represents a cyclic group, which may be monocyclic or, as in steroids or in santonin, polycyclic. In both the latter cases, one group Rl is alkyl while the other forms part of a ring structure. Such ring structures may be carbocyclic as in corticosteroids or may contain heterocyclic rings, e.g. the ~ ' .
lactone ring in santonin. Santonin has the formula:-_CH3
3 1 -The compounds of the invention may carry substituents~
e.g. oxo or hydroxy groups, protected oxo or hydroxy groups such as acetal, ketal, ester or ether groups ,carboxyl~
groups, esterified carboxyl groups, mercapto groups, halogen atoms, e.g. chlor~ne or fluorine atoms, or alkyl groups e.g.
having 1-6 carbon atoms. Acetal or ketal groups may be cyclic or acyclic groups derived from mono or dihydric alcohols having 1-5 carbon atoms. Ester groups may be derived from aliphatic, araliphatic or aromatic carboxylic acids, preferably having 1-8 carbon atoms. Ether groups may be alkoxy, aralkoxy or aryloxy groups, preferably having 1-8 carbon atoms, or silyloxy groups, e.g. having three hydro-carbon substituents which may be alkyl, aralkyl or arylgroups, preferably having 1-8 carbon atoms.
These compounds may be prepared by any conventional procedure which is suitable.
According to one feature of the present invention _ 4 _ '~, ^ .
~i ~058~0 there is provided a process for the prepaFation of a cot~pound of the formula:
R ~_R
R ~ R
wherein the s~bstituents ~ which may be the same or different, represent hydrogen atoms or hydrocarbyl groups and the groups R represent hydracarbyl groups or adjacent pairs of substituents R, or R and Rl together with the carbon atoms to which they are attached may constitute a non-aromatic ring structure, with the proviso that one of the adjacent pairs of R and R forms part of a ring structure~
said hydrocarbyl groups or ring structure if desired carrying one or more substituents, which process comprises reacting a corresponding cyclohexa-2,5-dien-1-one with a reagent serving to replace a keto group by a thione group. One reagent lS which serves to replace a keto-group by a thione group is hydrogen sulphide and an acid, but this reagent is not ideally suited to compounds in the corticosteroid field because of acid catalysed dienone-phenol rearrangement tot-the corres-ponding phenol or thiophenol, and because of sensitivity of.
the 17-side chain.
We have found that the treatment of a cyclohexa-2,5-_ 5_ . . .
lS~5B~tjO
diene-l-one with phosphorus pentasulphide or boron pentasulphide gives the corresponding thione in high yields. Any non-reactive solvent is appropriate for the reaction, for example tertiary amines such as triethylamine or pyridine; hydrocarbons such as alkanes, e.g. hexane, and light petroleum, or arenes e.g. benzene and toluene; ethers such as tetrahydrofuran and dioxan; nitriles such as acetonitrile and tertiary amides such as dialkyl formamides and acetamides. Tertiary amide solvents, however, react with the reagent, and are best used as co-solvents. Advantageously the solvent is a non-polar solvent, desirably an aryl hydrocarbon solvent, especially toluene.
The phosphorus or boror. polysulphide must of course be used in a molecular ratio of at ~ast 1:5 with the ketone substrate and preferably in excess, e.g. a ratio of 2 : 1 of more. The reaction is advantageously effected at a moderately elevated temperature, e.g. 60-100C.
Reactive groups in the substrate molecule, other than the keto group to be reacted must, of course, be protected.
In particular, reactive hydroxyl or mercapto groups should be protected as esters, e.g. acetyl, benzoyl, or trifluor-acetyl esters orethers~ ~ me~hyl,methyleDedioxy or silyl ethers.
In the steroids, 17,21-diol systems may be protected as 17,21-diacylates or 17,20:20,21-bismethylenedioxides. The A y ~os~o relatively hindered steroid ll~-hydroxy group needs no protection ~rom ~he polysulphide however, and keto groups other than the 3-keto react slowly with the reagent and thus may not need protection. Ester groups, amide groups and thioester groups are all less reactive than the ketones and thus similarly need no protection.
3-Thiones of steroid 1,4-dienes, possess interesting pharmacological activity of generally the same type as that of the parent 3-ones but characterised by particularly favourable assimilation into the body. Such steroids may be of the androstane, cholestane, oestrane or pregnane series. In particular, corticosteroid 3 thiones, especially when possessing an ll-oxygen function, e.g. a hydroxy or keto group, and a 17-oxygen function, e.g. a hydroxy or esterified hydroxy group, espeeially with a 17-aliphatic group as in the pregnane series, are noteworthy and the molecule should advantageously carry the typical corticoid 17,20,21 substituents, i.e. should be 20-keto-17,21-diols, mono-or diesters thereof, or ketalised derivatives such as acetonides and 17,20:20,21-bismethylenedioxy compounds.
Other advantageous substituents include a 16a- or ~- methyl group, a 7-mercapto group and a 9a-halo, especially fluoro, substituent.
Particular corticoid compounds of note according to ~ ,~1 ~.os~160 the present invention include the 3-thione analogues of dexamethasone, betamethasone and prednisone and acetonides, bismethylenedioxy derivatives and 17- and/or 21- acylates thereof.
; 5 Other noteworthy steroid 1,4-diene-3-thiones according to the invention include aldosterone inhibitors such as the thione analogue of 1(2)-dehydro-spironolactone, i.e. 17-hydroxy-7-mercapto-17a-pregna-1,4-diene-3-thione 21-carboxylic acid r- lactone, 7-acetate.
Apart from their interesting pharmacological activity, the cyclohexa-2,5-diene-1-thiones are useful active inter-mediates in the preparation of other compounds. Oxidation with peracids such as m-chloroperbenzoic acid yields the corresponding l-thione oxides (S-oxides) which comprise a further feature of this invention. The S-oxides are also surprisingly stable, but decompose when illuminated to form the corresponding l-one. This facility of returning to the parent l-one via the S-oxide makes the l-thiones particularly useful intermediates in reaction sequences for which the l-ones themselves are not well suited.
'~ ~
, . _ ~ _ 1~ 5~ 1 ~ 0 Thienol etherification may conveniently be achieved by treating the l-thione with an enol-alkylating agent such as trialkyloxonium hexafluorophophate or tetra-fluoroborate in an inert solvent such as a halogenated alkane, e.g. methylene chloride.
Thiones also react with 1,3-dipolar reagents to form heterocyclic derivatives. Thus, for example, reaction of a steroid-1,4-diene-3-thione with an aryl nitrile oxide, ; e.g. benzonitrile oxide yields a 3'-aryl-1',4',2'-oxathiazoline-5'-spiro-3-steroid. Thus, with prednisone BMD there is obtained 3'-phenyl-1',4',2'-oxathiazoline-5'-spiro-3-(17,20:20,21-bismethylenedioxypregna-1,4-dien-11-one). The aryl nitrile oxide may be prepared as described in Org.
Synth. 49 by treatment of the appropriate a-chloro aldoxime with a tertiary amine such as triethylamine.
The androstane derivatives according to the invention eg. 17-keto-, 17~-hydroxy- and 17~-hydroxy-17~-alkyl-androsta-1,4-dien-3-thiones have been found useful as anabolic agents and may advantageously be used to replace conventional agents.
They have been found of particular use in the treatment of ostçoporosis, whether sterile,post menopausal or steroid induced. A dosage of from 0.5 to 50 mg/day, preferably from _ ,,~ ._ ,, ,_ q 1~581~
1.0 to 15 mg/day, is desirable.
The corticoid derivatives according to the invention, eg. the 3-thione analogues of betamethasone,dexamethasone, prednisone, prednisolone,16a- and 16~-methyl prednisolone and triamcinolone and their 17 and/or 21-esters and acetonides, have been found to be anti-inflammatory agents which are longer acting than the corresponding ketones and have good topical activity with few side-effects. They may be used in low concentration topically for the treatment of e.g. rheumatoid arthritis and bursitis or may be ~ administered orally or parenterally in dosages similar to ; the parent oxygenated steroids. In this manner they are especially suited to alternate day therapy.
The spironolactone compounds according to the invention are aldosterone antagonists and may be used alone or in combination with diuretics for the management of hypertensi3n, congestive heart failure or chinosis. They may be administered at a rate of 10-1000 mgfday, preferably from 40-400 mg/day and ar~ both orally active and good for alternate day therapy.
The S-oxide deratives of the above compounds are generally similar but are preferred for alternate day therapy.
They may be used for both intramuscular and topical applications.
,~
~ ~o ~j _ ,~ _ ~0S8160 The compounds of the invention may be formulated in compositions using any of the conventional pharmaceutical carriers or excipients. The compounds may be administered parenterally in combination with an injectable liquid carrier such as sterile pyrogen-free water, sterile peroxide-free ethyl oleate, dehydrated alcohol, propylene glycol or a dehydrated alcohol/propylene glycol mixture.
Such compositions may be injected intravenously, intramuscularly or intraperitoneally.
The compounds may be made up into orally administrable compositions containing one or more physiologically compatible car~iers and/or excipients, and may be solid or liquid.
The compositions may take any convenient form including, for example, tablets, coated tablets, capsules, lozenges, aqueous or oily suspensions, solutions, emulsions, syrups, elixirs and dry products suitable for reconstitution with water or another suitable liquid vehicle before use.
Tablets and capsules containing the new compounds may, if desired, contain conventional ingredients such as binding agents, for example syrup, acacia, gelatin, sorbitol, tragacanth or polyvinyl-pyrollidone; fillers, for example lactose, sugar, maize-starch, calcium phosphate, sorbitol or r ~ _ J/ _ ~058i~0 glycine; lubricants, for example magnesium stearate, talc, polyethylene glycol or silica; disintegrants, for example potato starch; or acceptable wetting agents such as sodium lauryl sulphate. Tablets may be coated according to methods well known in the art.
Liquid compositions may contain conventional additives such as suspending agents, for example sorbitol syrup, methyl cellulose, glucose/sugar syrup, gelatin, hydroxymethylcellulose, carboxymethylcellulose, aluminium stearate gel or hydrogenated edible fats, emulsifying agents, for example lecithin, sorbitan monooleate or acacia; non-aqueous vehicles, which may include edible oils, for example ; vegetable oils such as arachis oil~ almond oil, fractionated coconut oil, fish-liver oils, oily esters such as polysorbate 80, propylene glycol, or ethyl alcohol; and preservatives, for example methyl or propyl p-hydroxybenzoates or sorbic acid. Liquid compositions may conveniently be encapsulated in, for example, gelatin to give a product in dosage unit form.
; 20 The compounds may also be administered topically, Such topical applications may, for example, be formulated in hydrophobic or hydrophilic bases as ointments, creams, lotions, paints and powders.
.. . ..
~.ossl~
The invention will now be more particularly described in thefollowing Examples which should not be interpreted as limiting the invention Example 1 9~-Fluoro-16a-methyl-11,17~21-trihydroxypregna-1,4-diene-20-one-3-thione 17,20;20~ 21-bismethvlene dioxide Dexamethasone-BMD (l.Og), phosphoxus pentasulphide (150 mg) and pyridine (15 ml) were stirred at 90C under argon for 1 ho~r. The solution was cooled, filtered and diluted with methylene chloride (100 ml). The purple solution was washed in turn with dilute hydrochloric acid (2 x 100 ml) and aqueous sodium bicarbonate, dried over MgS04 and evaporated to dryness~ The residue was filtered through activated magnesium silicate in methylene chloride to give a purple product (290 mg) which was recrystallised from methylene chloride/hexane to yield the ~itle product (dexamethasone BMD-3-thione), m.p. 212C (dec.); ~1.0 (3H,d,J=6Hz,C-16 methyl protons); 1.2(3H,s,C-18 protons);
1.6(3H,s,C-l9 protons); 4.0(2H,s,C-21 protons); 4.3 (lH,broad d,J=lOHz,C-ll proton); 4.9-5.3(4H,m,BMD protons);
6.9(1H, broad s,C-4 proton); 7.0(2H,s,C-1,2 protons);
3500 cm ,(m),(OH), 1630 cm ,(s),(C=C). AmaX 331 nm ( 17900), 580 nm ( 25). Mass spectrum, M ,450. (Found C,63.84%; H, 6.66%; S, 7.27%. C24H31F05S requires C, 63.97%; H,6.94%; S, 7.18%.).
Further elution of the column gave dexamethasone-~A~
~3 _ ~ _ 105~}~60 BMD (205 mg).
Example 2 9a-Fluoro-16~-methyl-llJ17,21-trihYdroxYpre~na-1,4-dien-20-one-3-thione 17,21-dipropionate Betamethasone 17,21-dipropionate (1.0 g), phosphorus pentasulfide ~100 mg) and pyridine (15 ml) were stirred at 80C for 45 minutes under an atmosphere of argon. A further aliquot of phosphorus pentasulphide (100 mg) was then added and the mixture was stirred for another 90 minutes. The product (200 mg) was isolated in the same manner as described in Example 1 and recrystallised from methylene chloride/hexane to give blue plates of the title product (betamethasone 17,21-dipropionate-3-thione), m.p. 113C; 6 l.o (s,C-18 protons); 1.6 (s,C-l9 protons); 4.5 (lH,broad,C-ll proton); 4.6 (2H,AB-q,J=16Hz, C-21 protons); 6.9 (lH,broad s, C-4 proton); 7.0 (2H,s, C-1,2 protons). Y max 3570 cm , (m), (OH), 1735 cm , (vs), (C=O), 1635 cm 1, (s),(C=C)- ~ 330 nm (E 19000), 575 nm (e 24). Mass spectrum, M ,498. (Found: C, 64.74%;
H, 7.19%; S, 6.02%. C24H31F05S requires C, 64-59%;
H, 7.16%; S, 6.16%.).
Example 3 17,21-dihydroxypregna-1,4-dien-11,20-dione-3-thione 17,20;
_ ,~ _ ~ss~o 20,21-bismethylenedioxide Prednisone-BMD (4.0 g), phosphorus pentasulfide (4.0 g) and toluene (40 ml) were stirred at 70C under argon for 4 hours. The solution was cooled, filtered and the residue was washed with toluene (15 ml). The filtrate was evaporated to low vo~ume and chromatographed on activated magnesium silicate with methylene chloride. The fractions which were blue in colour were collected and evaporated to dryness to give a blue solid (3.0 g, 72%), which on recrystallisation from methylene chloride/hexane yielded the title product (prednisone-BMD-3-thione) m.p.
184-187C. ~0.9(3H,s,C-18 protons); 1.5(3H,s,C-l9 protons);
e.g. oxo or hydroxy groups, protected oxo or hydroxy groups such as acetal, ketal, ester or ether groups ,carboxyl~
groups, esterified carboxyl groups, mercapto groups, halogen atoms, e.g. chlor~ne or fluorine atoms, or alkyl groups e.g.
having 1-6 carbon atoms. Acetal or ketal groups may be cyclic or acyclic groups derived from mono or dihydric alcohols having 1-5 carbon atoms. Ester groups may be derived from aliphatic, araliphatic or aromatic carboxylic acids, preferably having 1-8 carbon atoms. Ether groups may be alkoxy, aralkoxy or aryloxy groups, preferably having 1-8 carbon atoms, or silyloxy groups, e.g. having three hydro-carbon substituents which may be alkyl, aralkyl or arylgroups, preferably having 1-8 carbon atoms.
These compounds may be prepared by any conventional procedure which is suitable.
According to one feature of the present invention _ 4 _ '~, ^ .
~i ~058~0 there is provided a process for the prepaFation of a cot~pound of the formula:
R ~_R
R ~ R
wherein the s~bstituents ~ which may be the same or different, represent hydrogen atoms or hydrocarbyl groups and the groups R represent hydracarbyl groups or adjacent pairs of substituents R, or R and Rl together with the carbon atoms to which they are attached may constitute a non-aromatic ring structure, with the proviso that one of the adjacent pairs of R and R forms part of a ring structure~
said hydrocarbyl groups or ring structure if desired carrying one or more substituents, which process comprises reacting a corresponding cyclohexa-2,5-dien-1-one with a reagent serving to replace a keto group by a thione group. One reagent lS which serves to replace a keto-group by a thione group is hydrogen sulphide and an acid, but this reagent is not ideally suited to compounds in the corticosteroid field because of acid catalysed dienone-phenol rearrangement tot-the corres-ponding phenol or thiophenol, and because of sensitivity of.
the 17-side chain.
We have found that the treatment of a cyclohexa-2,5-_ 5_ . . .
lS~5B~tjO
diene-l-one with phosphorus pentasulphide or boron pentasulphide gives the corresponding thione in high yields. Any non-reactive solvent is appropriate for the reaction, for example tertiary amines such as triethylamine or pyridine; hydrocarbons such as alkanes, e.g. hexane, and light petroleum, or arenes e.g. benzene and toluene; ethers such as tetrahydrofuran and dioxan; nitriles such as acetonitrile and tertiary amides such as dialkyl formamides and acetamides. Tertiary amide solvents, however, react with the reagent, and are best used as co-solvents. Advantageously the solvent is a non-polar solvent, desirably an aryl hydrocarbon solvent, especially toluene.
The phosphorus or boror. polysulphide must of course be used in a molecular ratio of at ~ast 1:5 with the ketone substrate and preferably in excess, e.g. a ratio of 2 : 1 of more. The reaction is advantageously effected at a moderately elevated temperature, e.g. 60-100C.
Reactive groups in the substrate molecule, other than the keto group to be reacted must, of course, be protected.
In particular, reactive hydroxyl or mercapto groups should be protected as esters, e.g. acetyl, benzoyl, or trifluor-acetyl esters orethers~ ~ me~hyl,methyleDedioxy or silyl ethers.
In the steroids, 17,21-diol systems may be protected as 17,21-diacylates or 17,20:20,21-bismethylenedioxides. The A y ~os~o relatively hindered steroid ll~-hydroxy group needs no protection ~rom ~he polysulphide however, and keto groups other than the 3-keto react slowly with the reagent and thus may not need protection. Ester groups, amide groups and thioester groups are all less reactive than the ketones and thus similarly need no protection.
3-Thiones of steroid 1,4-dienes, possess interesting pharmacological activity of generally the same type as that of the parent 3-ones but characterised by particularly favourable assimilation into the body. Such steroids may be of the androstane, cholestane, oestrane or pregnane series. In particular, corticosteroid 3 thiones, especially when possessing an ll-oxygen function, e.g. a hydroxy or keto group, and a 17-oxygen function, e.g. a hydroxy or esterified hydroxy group, espeeially with a 17-aliphatic group as in the pregnane series, are noteworthy and the molecule should advantageously carry the typical corticoid 17,20,21 substituents, i.e. should be 20-keto-17,21-diols, mono-or diesters thereof, or ketalised derivatives such as acetonides and 17,20:20,21-bismethylenedioxy compounds.
Other advantageous substituents include a 16a- or ~- methyl group, a 7-mercapto group and a 9a-halo, especially fluoro, substituent.
Particular corticoid compounds of note according to ~ ,~1 ~.os~160 the present invention include the 3-thione analogues of dexamethasone, betamethasone and prednisone and acetonides, bismethylenedioxy derivatives and 17- and/or 21- acylates thereof.
; 5 Other noteworthy steroid 1,4-diene-3-thiones according to the invention include aldosterone inhibitors such as the thione analogue of 1(2)-dehydro-spironolactone, i.e. 17-hydroxy-7-mercapto-17a-pregna-1,4-diene-3-thione 21-carboxylic acid r- lactone, 7-acetate.
Apart from their interesting pharmacological activity, the cyclohexa-2,5-diene-1-thiones are useful active inter-mediates in the preparation of other compounds. Oxidation with peracids such as m-chloroperbenzoic acid yields the corresponding l-thione oxides (S-oxides) which comprise a further feature of this invention. The S-oxides are also surprisingly stable, but decompose when illuminated to form the corresponding l-one. This facility of returning to the parent l-one via the S-oxide makes the l-thiones particularly useful intermediates in reaction sequences for which the l-ones themselves are not well suited.
'~ ~
, . _ ~ _ 1~ 5~ 1 ~ 0 Thienol etherification may conveniently be achieved by treating the l-thione with an enol-alkylating agent such as trialkyloxonium hexafluorophophate or tetra-fluoroborate in an inert solvent such as a halogenated alkane, e.g. methylene chloride.
Thiones also react with 1,3-dipolar reagents to form heterocyclic derivatives. Thus, for example, reaction of a steroid-1,4-diene-3-thione with an aryl nitrile oxide, ; e.g. benzonitrile oxide yields a 3'-aryl-1',4',2'-oxathiazoline-5'-spiro-3-steroid. Thus, with prednisone BMD there is obtained 3'-phenyl-1',4',2'-oxathiazoline-5'-spiro-3-(17,20:20,21-bismethylenedioxypregna-1,4-dien-11-one). The aryl nitrile oxide may be prepared as described in Org.
Synth. 49 by treatment of the appropriate a-chloro aldoxime with a tertiary amine such as triethylamine.
The androstane derivatives according to the invention eg. 17-keto-, 17~-hydroxy- and 17~-hydroxy-17~-alkyl-androsta-1,4-dien-3-thiones have been found useful as anabolic agents and may advantageously be used to replace conventional agents.
They have been found of particular use in the treatment of ostçoporosis, whether sterile,post menopausal or steroid induced. A dosage of from 0.5 to 50 mg/day, preferably from _ ,,~ ._ ,, ,_ q 1~581~
1.0 to 15 mg/day, is desirable.
The corticoid derivatives according to the invention, eg. the 3-thione analogues of betamethasone,dexamethasone, prednisone, prednisolone,16a- and 16~-methyl prednisolone and triamcinolone and their 17 and/or 21-esters and acetonides, have been found to be anti-inflammatory agents which are longer acting than the corresponding ketones and have good topical activity with few side-effects. They may be used in low concentration topically for the treatment of e.g. rheumatoid arthritis and bursitis or may be ~ administered orally or parenterally in dosages similar to ; the parent oxygenated steroids. In this manner they are especially suited to alternate day therapy.
The spironolactone compounds according to the invention are aldosterone antagonists and may be used alone or in combination with diuretics for the management of hypertensi3n, congestive heart failure or chinosis. They may be administered at a rate of 10-1000 mgfday, preferably from 40-400 mg/day and ar~ both orally active and good for alternate day therapy.
The S-oxide deratives of the above compounds are generally similar but are preferred for alternate day therapy.
They may be used for both intramuscular and topical applications.
,~
~ ~o ~j _ ,~ _ ~0S8160 The compounds of the invention may be formulated in compositions using any of the conventional pharmaceutical carriers or excipients. The compounds may be administered parenterally in combination with an injectable liquid carrier such as sterile pyrogen-free water, sterile peroxide-free ethyl oleate, dehydrated alcohol, propylene glycol or a dehydrated alcohol/propylene glycol mixture.
Such compositions may be injected intravenously, intramuscularly or intraperitoneally.
The compounds may be made up into orally administrable compositions containing one or more physiologically compatible car~iers and/or excipients, and may be solid or liquid.
The compositions may take any convenient form including, for example, tablets, coated tablets, capsules, lozenges, aqueous or oily suspensions, solutions, emulsions, syrups, elixirs and dry products suitable for reconstitution with water or another suitable liquid vehicle before use.
Tablets and capsules containing the new compounds may, if desired, contain conventional ingredients such as binding agents, for example syrup, acacia, gelatin, sorbitol, tragacanth or polyvinyl-pyrollidone; fillers, for example lactose, sugar, maize-starch, calcium phosphate, sorbitol or r ~ _ J/ _ ~058i~0 glycine; lubricants, for example magnesium stearate, talc, polyethylene glycol or silica; disintegrants, for example potato starch; or acceptable wetting agents such as sodium lauryl sulphate. Tablets may be coated according to methods well known in the art.
Liquid compositions may contain conventional additives such as suspending agents, for example sorbitol syrup, methyl cellulose, glucose/sugar syrup, gelatin, hydroxymethylcellulose, carboxymethylcellulose, aluminium stearate gel or hydrogenated edible fats, emulsifying agents, for example lecithin, sorbitan monooleate or acacia; non-aqueous vehicles, which may include edible oils, for example ; vegetable oils such as arachis oil~ almond oil, fractionated coconut oil, fish-liver oils, oily esters such as polysorbate 80, propylene glycol, or ethyl alcohol; and preservatives, for example methyl or propyl p-hydroxybenzoates or sorbic acid. Liquid compositions may conveniently be encapsulated in, for example, gelatin to give a product in dosage unit form.
; 20 The compounds may also be administered topically, Such topical applications may, for example, be formulated in hydrophobic or hydrophilic bases as ointments, creams, lotions, paints and powders.
.. . ..
~.ossl~
The invention will now be more particularly described in thefollowing Examples which should not be interpreted as limiting the invention Example 1 9~-Fluoro-16a-methyl-11,17~21-trihydroxypregna-1,4-diene-20-one-3-thione 17,20;20~ 21-bismethvlene dioxide Dexamethasone-BMD (l.Og), phosphoxus pentasulphide (150 mg) and pyridine (15 ml) were stirred at 90C under argon for 1 ho~r. The solution was cooled, filtered and diluted with methylene chloride (100 ml). The purple solution was washed in turn with dilute hydrochloric acid (2 x 100 ml) and aqueous sodium bicarbonate, dried over MgS04 and evaporated to dryness~ The residue was filtered through activated magnesium silicate in methylene chloride to give a purple product (290 mg) which was recrystallised from methylene chloride/hexane to yield the ~itle product (dexamethasone BMD-3-thione), m.p. 212C (dec.); ~1.0 (3H,d,J=6Hz,C-16 methyl protons); 1.2(3H,s,C-18 protons);
1.6(3H,s,C-l9 protons); 4.0(2H,s,C-21 protons); 4.3 (lH,broad d,J=lOHz,C-ll proton); 4.9-5.3(4H,m,BMD protons);
6.9(1H, broad s,C-4 proton); 7.0(2H,s,C-1,2 protons);
3500 cm ,(m),(OH), 1630 cm ,(s),(C=C). AmaX 331 nm ( 17900), 580 nm ( 25). Mass spectrum, M ,450. (Found C,63.84%; H, 6.66%; S, 7.27%. C24H31F05S requires C, 63.97%; H,6.94%; S, 7.18%.).
Further elution of the column gave dexamethasone-~A~
~3 _ ~ _ 105~}~60 BMD (205 mg).
Example 2 9a-Fluoro-16~-methyl-llJ17,21-trihYdroxYpre~na-1,4-dien-20-one-3-thione 17,21-dipropionate Betamethasone 17,21-dipropionate (1.0 g), phosphorus pentasulfide ~100 mg) and pyridine (15 ml) were stirred at 80C for 45 minutes under an atmosphere of argon. A further aliquot of phosphorus pentasulphide (100 mg) was then added and the mixture was stirred for another 90 minutes. The product (200 mg) was isolated in the same manner as described in Example 1 and recrystallised from methylene chloride/hexane to give blue plates of the title product (betamethasone 17,21-dipropionate-3-thione), m.p. 113C; 6 l.o (s,C-18 protons); 1.6 (s,C-l9 protons); 4.5 (lH,broad,C-ll proton); 4.6 (2H,AB-q,J=16Hz, C-21 protons); 6.9 (lH,broad s, C-4 proton); 7.0 (2H,s, C-1,2 protons). Y max 3570 cm , (m), (OH), 1735 cm , (vs), (C=O), 1635 cm 1, (s),(C=C)- ~ 330 nm (E 19000), 575 nm (e 24). Mass spectrum, M ,498. (Found: C, 64.74%;
H, 7.19%; S, 6.02%. C24H31F05S requires C, 64-59%;
H, 7.16%; S, 6.16%.).
Example 3 17,21-dihydroxypregna-1,4-dien-11,20-dione-3-thione 17,20;
_ ,~ _ ~ss~o 20,21-bismethylenedioxide Prednisone-BMD (4.0 g), phosphorus pentasulfide (4.0 g) and toluene (40 ml) were stirred at 70C under argon for 4 hours. The solution was cooled, filtered and the residue was washed with toluene (15 ml). The filtrate was evaporated to low vo~ume and chromatographed on activated magnesium silicate with methylene chloride. The fractions which were blue in colour were collected and evaporated to dryness to give a blue solid (3.0 g, 72%), which on recrystallisation from methylene chloride/hexane yielded the title product (prednisone-BMD-3-thione) m.p.
184-187C. ~0.9(3H,s,C-18 protons); 1.5(3H,s,C-l9 protons);
4.0(2H,s,C-21 protons); 5.0-5.4(4H,m,BMD protons);
6.8-7.0(2H,m,C-2,4 protons); 7.5(1H,d,J=lOHz,C-l proton).
V 1710 cm ,(s),(C=O), 1630 cm ,(s),(C=C). AmaX 330 nm (E 19500), 565 nm (s 20). Mass spectrum, M ,416. (Found:
C, 66.42%; H, 6.69%; S, 7.44%. C23H2805S requires C, 66.32%; H, 6.78%; S, 7.70%.). m-Chloroperbenzoic acid oxidation of this diene-thione gave the yellow syn-anti thione-S-oxide derivatives, m.p. 203-204, [a~DH2C12 + 130, a 358 nm (s 16000). Although the syn-anti isomers were sep~rable by p.l.c. they rapidly interconverted on standing.
On irradiation (tungsten lamp) the S-oxidesin dichloromethane gave the l,4-dien 3-one starting material.
7 . . .~
'-A~ ,5 ~-o~ o Using the above procedure (but with benzene as solvent and reaction temperature 20C) androsta-1,4-dien-3,17 dione was converted into androsta-1,4-dien-17-one-3-thione Yield 70%; m.p. 163-5C; AmaX 330 nm (E ~ 19 ,000) This thione was then reacted with diphenyl diazomethane at room temperature to yield 3(diphenylmethylene)-androst-1,4-dien-17-one.
Example 4 9~-Fluoro-16~-methyl-11,17,21-trihydroxypregna-1,4-dien-20-one-3-thione 17,21-dipropionate Betamethasone 17,21-dipropionate (2.3 g) in toluene (60 ml) with P2S5 (2.0 g) was stirred at 75-80C for 4 hours.
., .2, )~
~. - ~ _ , ..
~05~ ;0 The mixture was then cooled and filtered through an activated magnesium silicate CH2C12 column. Elution with further CH2C12gave the 3-thione (1.45 g, 60%).
By the foregoing prccedure, the following compounds were also prepared:
17-keto androsta-1,4-diene-3-thione, m.pt 163-5C, Found C 75.9,H 8.0, S 10.4, Calcd. C 76.0, H 8.1, S 10.7, 17~-hydroxyandrosta-1,4-diene-3-thione 17~-hydroxy-17a-alkyl androsta-1,4-diene-3-thione and the 17,21-diesters-3-thiones of prednisone, prednisolone, ;~ 16a-methylprednisolone, 16~-methylprednisolone, dexamethasone, triamcinolone acetonide and other 17,21-diesters of betamethasone.
Example 5 9a-Fluoro-16~-methyl-11,17-21-trihydroxypregna-lt4-dien-20-one-3-thione The product of Example 4 (500 mg~ in methanol (100 ml) was deoxygenated and stirred at 0C under argon.
N/10 Na0H (20 ml, 2 equiv.) was added and the solution was stirred at 0C for 2 hours. Acetic acid (1 drop) was added and the mixture partitioned between CH2C13 and water. The organic layer was dried, evaporated to dryness and recrystallised from acetone/hexane to give blue microneedles m.pt. 170-4C.
i ,~ _ ~os8~6~
Analysis: Calc. E'ound C 64.68 64.72%
H 7.16 7.03%
S 7.85 7.38%
PMR: ~ HAssi~nment H
1.1-1.3 6H (m)C-16 and C-18 methyls lo 6 3H (S) C-l9 4.2-4.5 3H(m) C-21 and C-ll 6.7-7.2 3H(m) vinyl K~ .
lR: ~' cm : 3500 (vs). 1710 (m), 1640 (vs).
max.
By the foregoing procedure were also prepared the 3-thiones of prednisone, prednisolone, 16~-methylprednis~one, 16~-methylprednisolone, and dexamethasone.
Example 6 9~-Fluoro-16r~-meth~1-11,17,21-trihy~oxypregna-1,4-dien-20-one-3-thione 17,21-dipropionate S-oxide The product of Example 4 (100 mg) in CH Cl was stirred in the dark and m-chloroperbenzoic acid (50 mg) was added.
The solution was washed with aqueous sodium bicarbonate, dried and evapo$~ted to dryness. Recrystallization of the residue from CH2C12/hexane gave yellow crystals, m.pt. 110-115 C.
~0 5~ ~ ~ 0 NMR: ~ H Assignment 1.0-1.4 multiple methyl C-18, C-16 and ester resonances 1.6 3H (s) C-19 4.55 2H (AB quart.) C-21 protons 6.2-7.3 3~ (m) vinyl protons lR:~ 3500 (m). 1730 (vs). 1190 (vs) cm max.
Analysis Found C,62,42; H, 7.21; S, 5.81 %
Reg C,62,66; H, 6.95; S, 5.98 %
By the foregoing procedure, the S-oxides of the 3-thiones of 17,21-diesters of prednisone, prednisolone, 16a-methylprednisolone, 16~-methylprednisolone and dexamethasone and of triamcinolone acetonide were also prepared.
Example 7 9~-Fluoro-16g-methyl-11,12-21-trihydroxypregna-1,4-dien-20-one-3-thione S-oxide The procedure and scale of Example 6 was used to prepare the title product from the product of Example 5.
Recrystallization from ethyl acetate/hexane gave yellow crystals m.pt. 170-4 C.
- ,l~B'-~5~S~l~O
PMR: ~ H Assignment H
1.1 3H (d)J=7Hz) C-16 methyl 1.1 3H (s) C-18 1.6 3H (s) C-l9 4.0 3H (bm) OH
4.4 2H (AB quartet) C-21 4.4 lH (bm) C-ll 6.5-7.1 3H (m) vinyl lR:~aX ~m 3500 (vs), 1110 (m). Analysis Found C 61,85;
Reg C,62,24;H,6, 89;S,7,55 %
By the foregoing procedure, the S-oxides of the 3-thiones of prednisone, prednisolone, 16a-methylprednisolone, 16~-methylprednisolone, and dexamethasone were also prepared.
Example 8 _-phenyl-1',4'~2'-oxathiazoline-5'-spiro-3-(17,20:20~21-bismethylenedioxypregna-1,4-dien-11-one The product of Example 3 (416 mg) and PhCCl=NOH
(400mg) in dry benzene (10 ml) were treated with anhydrous triethylamine (1 ml). The residue after evaporation was passed through ac~ivated magnesium silicate and the product was eluted with 70% CH2C12 in hexane.
_... -...
~OS81~0 : Recrystallization from CH2C12/hexane gave colorlessplates m.pt. 134 C UV:~ 246nm ( 20000), 300 nm ( 1700).
lR: ~ cm : 1700 (vs), 1660 (w).
PMR: ~ H Assignment H
0.9 3H (s) C-18 1.4 3H (two peaks) C-l9 4.0 2H (s) C-21 4.S-S.1 4H (m) BMD
0.0_7,0 3H (m) vinyl 7.3-7.7 5H (m) aryl _ ~ _ A~
lOS8160 Example 9 3-Ethoxy-17.21-dihydroxypregna-1 3.5-triene-11 20-dione 17,~0-20 21-bismethylene dioxide Prednisone BMD 3 thione (from Example 3) (1 0 g) in dry CH2C12 (25 ml) over 4A molecular sieve and under an atmosphere of argon, was treated with 1 equiv (2.5 ml) of triethyloxonium tetrafluoroborate in CH2C12 solution The mixture was stirred for 2 5 hrs and then quenched with 1.4 equiv. (643 mg) of 1,8-bis-(dimethylamino)naphthalene.
The solution was filtered to remove sieves and amine tetrafluoro-borate and the fitra~e applied to 9, 20cm x 20cm preparative chromatography plates. The band corresponding to the desired product was removed from each plate and extracted with CH2C12 The extracts on evaporation gave 0 38 g of product;
recrystallization ex hexane/CH2C12 gave off white crystals, m.p.178-180 C
PMR: ~ H Assi~nment 0.8 3(s) C-18 1.25 3(t, J=7Hz) CH3-CH2-S
1.30 3(s) C-l9 2.75 2(q, J=7Hz) CH3-CH2-S
4.0 2(s) C-21
6.8-7.0(2H,m,C-2,4 protons); 7.5(1H,d,J=lOHz,C-l proton).
V 1710 cm ,(s),(C=O), 1630 cm ,(s),(C=C). AmaX 330 nm (E 19500), 565 nm (s 20). Mass spectrum, M ,416. (Found:
C, 66.42%; H, 6.69%; S, 7.44%. C23H2805S requires C, 66.32%; H, 6.78%; S, 7.70%.). m-Chloroperbenzoic acid oxidation of this diene-thione gave the yellow syn-anti thione-S-oxide derivatives, m.p. 203-204, [a~DH2C12 + 130, a 358 nm (s 16000). Although the syn-anti isomers were sep~rable by p.l.c. they rapidly interconverted on standing.
On irradiation (tungsten lamp) the S-oxidesin dichloromethane gave the l,4-dien 3-one starting material.
7 . . .~
'-A~ ,5 ~-o~ o Using the above procedure (but with benzene as solvent and reaction temperature 20C) androsta-1,4-dien-3,17 dione was converted into androsta-1,4-dien-17-one-3-thione Yield 70%; m.p. 163-5C; AmaX 330 nm (E ~ 19 ,000) This thione was then reacted with diphenyl diazomethane at room temperature to yield 3(diphenylmethylene)-androst-1,4-dien-17-one.
Example 4 9~-Fluoro-16~-methyl-11,17,21-trihydroxypregna-1,4-dien-20-one-3-thione 17,21-dipropionate Betamethasone 17,21-dipropionate (2.3 g) in toluene (60 ml) with P2S5 (2.0 g) was stirred at 75-80C for 4 hours.
., .2, )~
~. - ~ _ , ..
~05~ ;0 The mixture was then cooled and filtered through an activated magnesium silicate CH2C12 column. Elution with further CH2C12gave the 3-thione (1.45 g, 60%).
By the foregoing prccedure, the following compounds were also prepared:
17-keto androsta-1,4-diene-3-thione, m.pt 163-5C, Found C 75.9,H 8.0, S 10.4, Calcd. C 76.0, H 8.1, S 10.7, 17~-hydroxyandrosta-1,4-diene-3-thione 17~-hydroxy-17a-alkyl androsta-1,4-diene-3-thione and the 17,21-diesters-3-thiones of prednisone, prednisolone, ;~ 16a-methylprednisolone, 16~-methylprednisolone, dexamethasone, triamcinolone acetonide and other 17,21-diesters of betamethasone.
Example 5 9a-Fluoro-16~-methyl-11,17-21-trihydroxypregna-lt4-dien-20-one-3-thione The product of Example 4 (500 mg~ in methanol (100 ml) was deoxygenated and stirred at 0C under argon.
N/10 Na0H (20 ml, 2 equiv.) was added and the solution was stirred at 0C for 2 hours. Acetic acid (1 drop) was added and the mixture partitioned between CH2C13 and water. The organic layer was dried, evaporated to dryness and recrystallised from acetone/hexane to give blue microneedles m.pt. 170-4C.
i ,~ _ ~os8~6~
Analysis: Calc. E'ound C 64.68 64.72%
H 7.16 7.03%
S 7.85 7.38%
PMR: ~ HAssi~nment H
1.1-1.3 6H (m)C-16 and C-18 methyls lo 6 3H (S) C-l9 4.2-4.5 3H(m) C-21 and C-ll 6.7-7.2 3H(m) vinyl K~ .
lR: ~' cm : 3500 (vs). 1710 (m), 1640 (vs).
max.
By the foregoing procedure were also prepared the 3-thiones of prednisone, prednisolone, 16~-methylprednis~one, 16~-methylprednisolone, and dexamethasone.
Example 6 9~-Fluoro-16r~-meth~1-11,17,21-trihy~oxypregna-1,4-dien-20-one-3-thione 17,21-dipropionate S-oxide The product of Example 4 (100 mg) in CH Cl was stirred in the dark and m-chloroperbenzoic acid (50 mg) was added.
The solution was washed with aqueous sodium bicarbonate, dried and evapo$~ted to dryness. Recrystallization of the residue from CH2C12/hexane gave yellow crystals, m.pt. 110-115 C.
~0 5~ ~ ~ 0 NMR: ~ H Assignment 1.0-1.4 multiple methyl C-18, C-16 and ester resonances 1.6 3H (s) C-19 4.55 2H (AB quart.) C-21 protons 6.2-7.3 3~ (m) vinyl protons lR:~ 3500 (m). 1730 (vs). 1190 (vs) cm max.
Analysis Found C,62,42; H, 7.21; S, 5.81 %
Reg C,62,66; H, 6.95; S, 5.98 %
By the foregoing procedure, the S-oxides of the 3-thiones of 17,21-diesters of prednisone, prednisolone, 16a-methylprednisolone, 16~-methylprednisolone and dexamethasone and of triamcinolone acetonide were also prepared.
Example 7 9~-Fluoro-16g-methyl-11,12-21-trihydroxypregna-1,4-dien-20-one-3-thione S-oxide The procedure and scale of Example 6 was used to prepare the title product from the product of Example 5.
Recrystallization from ethyl acetate/hexane gave yellow crystals m.pt. 170-4 C.
- ,l~B'-~5~S~l~O
PMR: ~ H Assignment H
1.1 3H (d)J=7Hz) C-16 methyl 1.1 3H (s) C-18 1.6 3H (s) C-l9 4.0 3H (bm) OH
4.4 2H (AB quartet) C-21 4.4 lH (bm) C-ll 6.5-7.1 3H (m) vinyl lR:~aX ~m 3500 (vs), 1110 (m). Analysis Found C 61,85;
Reg C,62,24;H,6, 89;S,7,55 %
By the foregoing procedure, the S-oxides of the 3-thiones of prednisone, prednisolone, 16a-methylprednisolone, 16~-methylprednisolone, and dexamethasone were also prepared.
Example 8 _-phenyl-1',4'~2'-oxathiazoline-5'-spiro-3-(17,20:20~21-bismethylenedioxypregna-1,4-dien-11-one The product of Example 3 (416 mg) and PhCCl=NOH
(400mg) in dry benzene (10 ml) were treated with anhydrous triethylamine (1 ml). The residue after evaporation was passed through ac~ivated magnesium silicate and the product was eluted with 70% CH2C12 in hexane.
_... -...
~OS81~0 : Recrystallization from CH2C12/hexane gave colorlessplates m.pt. 134 C UV:~ 246nm ( 20000), 300 nm ( 1700).
lR: ~ cm : 1700 (vs), 1660 (w).
PMR: ~ H Assignment H
0.9 3H (s) C-18 1.4 3H (two peaks) C-l9 4.0 2H (s) C-21 4.S-S.1 4H (m) BMD
0.0_7,0 3H (m) vinyl 7.3-7.7 5H (m) aryl _ ~ _ A~
lOS8160 Example 9 3-Ethoxy-17.21-dihydroxypregna-1 3.5-triene-11 20-dione 17,~0-20 21-bismethylene dioxide Prednisone BMD 3 thione (from Example 3) (1 0 g) in dry CH2C12 (25 ml) over 4A molecular sieve and under an atmosphere of argon, was treated with 1 equiv (2.5 ml) of triethyloxonium tetrafluoroborate in CH2C12 solution The mixture was stirred for 2 5 hrs and then quenched with 1.4 equiv. (643 mg) of 1,8-bis-(dimethylamino)naphthalene.
The solution was filtered to remove sieves and amine tetrafluoro-borate and the fitra~e applied to 9, 20cm x 20cm preparative chromatography plates. The band corresponding to the desired product was removed from each plate and extracted with CH2C12 The extracts on evaporation gave 0 38 g of product;
recrystallization ex hexane/CH2C12 gave off white crystals, m.p.178-180 C
PMR: ~ H Assi~nment 0.8 3(s) C-18 1.25 3(t, J=7Hz) CH3-CH2-S
1.30 3(s) C-l9 2.75 2(q, J=7Hz) CH3-CH2-S
4.0 2(s) C-21
5~0-5.2 4(m) BMD-methylenes 5.3-5.8 3(m) C-2,4,6
6.45 l(d,J=lOHz) C-l _ ~ _ lOS816i0 IR: (KBr~ 2950 (m), 1700 (s), 1100 (s), 1080 (s), 945 (s), 745 (m) cm [a]D = -216 C (c=1,20, CH2C12), UV A 3 = 326 nm ( E = 6400) max Example 10 Preparation of 17-hydrox~-7-mercapto-17~-pregna-1l4-diene-3-thione-21-carboxylic acid ~ -lactone~ 7-ac t _ To 17-hydroxy-7-mercapto-3-oxo-17a -pregn-1,4-diene-21-carboxylic acid ~-lactone, 7-acetate (207 mg, 0,5 m,moles) in toluene (6 ml), was added phosphorus pentasulfide (200 mg, 0.9 m.moles) in a flask fitted with a reflux condenser and a gas inlet tube. The mixture under an argon atmosphere, o + O
was heated to 70 - 5 with constant stirring until t,l,c, revealed the onset of formation of undesired by-products (4 hrs.) The mixture was filtered, the insoluble material being washed with methylene chloride and directly applied to an activated magnesium silicatecolumn, Elution with methylene chloride gave the product as a dark blue glass after solvent removal under vacuum, The crude product was recrystallized from acetone/hexane to yield 90 mg of pure thione as deep blue micro needles (m,p, ~240 , loss of color and dec,).
UV: ~maX:330 m~ (E = 24,700) in MeOH
IR: vmax cm :3000 (m), 1775 (vs), 1690 (s), 1630 (s), 1180 (s), 1135 (s), 1025 (m), 805 (m), ~` A i 3 ~ _ ~05E~O
PMR: o H Assi~nment H
1.0 3 (s) C-18 1.3 ~ (s) C-19 2.35 3 (s) -S-~-Me 4.0 1 (m) C-1
was heated to 70 - 5 with constant stirring until t,l,c, revealed the onset of formation of undesired by-products (4 hrs.) The mixture was filtered, the insoluble material being washed with methylene chloride and directly applied to an activated magnesium silicatecolumn, Elution with methylene chloride gave the product as a dark blue glass after solvent removal under vacuum, The crude product was recrystallized from acetone/hexane to yield 90 mg of pure thione as deep blue micro needles (m,p, ~240 , loss of color and dec,).
UV: ~maX:330 m~ (E = 24,700) in MeOH
IR: vmax cm :3000 (m), 1775 (vs), 1690 (s), 1630 (s), 1180 (s), 1135 (s), 1025 (m), 805 (m), ~` A i 3 ~ _ ~05E~O
PMR: o H Assi~nment H
1.0 3 (s) C-18 1.3 ~ (s) C-19 2.35 3 (s) -S-~-Me 4.0 1 (m) C-1
7.5 2 (m~ C-2, C-4 Example 11 Reaction of Santonin with P2S5/tuluene Santonin (2.0 g) and P2S5 (3 g) in toluene (40 ml) were stirred at 70 C for 4 hrs. The reaction was then found to be about 50% complete and the t.l.c~ showed that the less polar product was blue in color. Further reaction resultedin som~ decomposition products forming. Isolation of the blue fraction on activated magnesium silicate gave a blue crystalline s~lid. mp 143-144 Analysis: Found C,680~7; H,6095; S,12.22%
Reg C,68.67; H,6.91; S,12~22 %
lOS~l~O
Example 12 Pharmaceutical Compositions Compositions containing the various classes of compounds of the invention may be formulated as follows:-a) 12,5g or 0.5g androstane steroid 8g methyl stearate up to 200g lactose The mixture is pressed after mixing and 1000 tablets are prepared, A suitable dose could be from 1-4 per day b) lOg or lOOg or 250g spironolactone steroid 5g methyl stearate up to 500g lactose The mixture may be pressed to provide 1000 tablets, with a suitable dose rate of 1-4 per day.
c) 0.3 or 0.8g betamethasone derivative or 3 or 7g prednisolone derivative 8g methyl stearate up to 250g lactose The mixture may be pressed to yield 1000 tablets, with a suitable dose rate of 1-4 per day or 1-4 on alternate days.
,~ 2~
~ ~S -~0581f~0 Example 13 Compositions for topical application a) For the preparation of an ointment are throughly mixed 30g propylene glycol monostearate 30g sorbitol monostearate O.Sg 4-chloro m-cresol or methyl paraben.
Add polyethylene glycol/propylene glycol to 1 kg.
Into this ointment are stirred betamethasone derivative lg or 2g or betamethasone dipropionate derivative O.Sg or lg or prednisolone derivative 2g or 5g The ointment is applied to the affected area 1-4 times daily. The area under treatment may, in the case of arthritis or bursitis, be covered with a plastic film and sealed at the edges with adhesive.
b) For the preparation of a cream, The cream may be prepared in the same manner as the ointment, except that the polyethylene glycol/poly-propylene glycol are replaced by a mixture of liquid and white petrol~t~m containing hydrogenated lanolin.
Reg C,68.67; H,6.91; S,12~22 %
lOS~l~O
Example 12 Pharmaceutical Compositions Compositions containing the various classes of compounds of the invention may be formulated as follows:-a) 12,5g or 0.5g androstane steroid 8g methyl stearate up to 200g lactose The mixture is pressed after mixing and 1000 tablets are prepared, A suitable dose could be from 1-4 per day b) lOg or lOOg or 250g spironolactone steroid 5g methyl stearate up to 500g lactose The mixture may be pressed to provide 1000 tablets, with a suitable dose rate of 1-4 per day.
c) 0.3 or 0.8g betamethasone derivative or 3 or 7g prednisolone derivative 8g methyl stearate up to 250g lactose The mixture may be pressed to yield 1000 tablets, with a suitable dose rate of 1-4 per day or 1-4 on alternate days.
,~ 2~
~ ~S -~0581f~0 Example 13 Compositions for topical application a) For the preparation of an ointment are throughly mixed 30g propylene glycol monostearate 30g sorbitol monostearate O.Sg 4-chloro m-cresol or methyl paraben.
Add polyethylene glycol/propylene glycol to 1 kg.
Into this ointment are stirred betamethasone derivative lg or 2g or betamethasone dipropionate derivative O.Sg or lg or prednisolone derivative 2g or 5g The ointment is applied to the affected area 1-4 times daily. The area under treatment may, in the case of arthritis or bursitis, be covered with a plastic film and sealed at the edges with adhesive.
b) For the preparation of a cream, The cream may be prepared in the same manner as the ointment, except that the polyethylene glycol/poly-propylene glycol are replaced by a mixture of liquid and white petrol~t~m containing hydrogenated lanolin.
Claims (14)
PROPERTY OR PRIVILEGE IS CLAIMED ARE DEFINED AS FOLLOWS:-
1. A process for the preparation of a compound of the formula:
wherein the substituents R, which may be the same or different, represent hydrogen atoms or hydrocarbyl groups and the groups R1 represent hydrocarbyl groups or adjacent pairs of substituents R, or R and R1 together with the carbon atoms to which they are attached may constitute a non-aromatic ring structure, with the proviso that one of the adjacent pairs of R and R1 forms part of a ring structure, said hydrocarbyl groups or ring structure if desired carrying one or more substituents, which process comprises reacting a corres-ponding cyclohexa-2,5-dien-1-one with a reagent serving to replace a keto group by a thione group.
wherein the substituents R, which may be the same or different, represent hydrogen atoms or hydrocarbyl groups and the groups R1 represent hydrocarbyl groups or adjacent pairs of substituents R, or R and R1 together with the carbon atoms to which they are attached may constitute a non-aromatic ring structure, with the proviso that one of the adjacent pairs of R and R1 forms part of a ring structure, said hydrocarbyl groups or ring structure if desired carrying one or more substituents, which process comprises reacting a corres-ponding cyclohexa-2,5-dien-1-one with a reagent serving to replace a keto group by a thione group.
2. A process as claimed in claim 1 wherein the cyclohexa-2,5-dien-1-one is reacted with hydrogen sulphide and an acid.
3. A process as claimed in claim 1 in which the cyclohexa-2,5-dien-1-one is reacted with phosphorus pentasulphide.
4. A process as claimed in claim 3 in which the ratio of phosphorus pentasulphide to ketone is at least 1:5.
5. A process as claimed in claim 4 in which said ratio is 2:1 or more.
6. A process as claimed in claim 3 in which the reaction temperature is 60-100°C.
7. A process as claimed in claim 1 in which the cyclohexa-2,5-dien-1-one is reacted with boron pentasulphide.
8. A process as claimed in claim 1 wherein the cyclo-hexa-2,5-dien-1-one is a steroid 1,4-dien-3-one of the pregnane series.
9. A process as claimed in claim 1 in which the thione formed is subsequently oxidised to the corres-ponding S-oxide.
10. A process as claimed in claim 1 in which the thione formed is reacted with an enol-alkylating agent to form the corresponding thienol ether.
11. A process as claimed in claim 1 in which the thione formed is reacted with an aryl nitrile oxide to form a 3-aryl-1,4,2-oxathiazoline-5-spiro-grouping.
12. Compounds as defined in claim 1 whenever prepared by the process of claim 1 or an obvious chemical equivalent thereof.
13. S-oxides of the compounds defined in claim 1 whenever prepared by the process of claim 9 or an obvious chemical equivalent thereof.
14. Steroid 1,4-dien-3-thiones of the pregnane series whenever prepared by the process of claim 8 or an obvious chemical equivalent thereof.
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| GB3808274A GB1522136A (en) | 1974-08-30 | 1974-08-30 | Conjugated cyclic thiones and their s-oxides |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| CA1058160A true CA1058160A (en) | 1979-07-10 |
Family
ID=10401055
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA233,024A Expired CA1058160A (en) | 1974-08-30 | 1975-08-07 | Cycloaliphatic thiones |
Country Status (6)
| Country | Link |
|---|---|
| JP (1) | JPS5163156A (en) |
| AU (1) | AU504398B2 (en) |
| CA (1) | CA1058160A (en) |
| GB (1) | GB1522136A (en) |
| NZ (1) | NZ178323A (en) |
| PH (1) | PH13535A (en) |
Families Citing this family (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US4903862A (en) * | 1987-10-13 | 1990-02-27 | Abc/Sebrn Tech. Corp., Inc. | Soft drink dispenser |
-
1974
- 1974-08-30 GB GB3808274A patent/GB1522136A/en not_active Expired
-
1975
- 1975-02-25 PH PH16853A patent/PH13535A/en unknown
- 1975-08-07 NZ NZ17832375A patent/NZ178323A/en unknown
- 1975-08-07 JP JP9546375A patent/JPS5163156A/en active Granted
- 1975-08-07 CA CA233,024A patent/CA1058160A/en not_active Expired
- 1975-08-08 AU AU83796/75A patent/AU504398B2/en not_active Expired
Also Published As
| Publication number | Publication date |
|---|---|
| AU8379675A (en) | 1977-02-10 |
| JPS5163156A (en) | 1976-06-01 |
| NZ178323A (en) | 1978-06-02 |
| PH13535A (en) | 1980-06-19 |
| AU504398B2 (en) | 1979-10-11 |
| GB1522136A (en) | 1978-08-23 |
| JPS6222998B2 (en) | 1987-05-20 |
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