SE500849C2 - New 3-amino-2-oxo-azetidine-1-sulfonic acids, intermediates to the corresponding 3-amino-substituted-2-oxo-azetidine-1-sulfonic acids - Google Patents

Abstract

An azetidine of formula (I): or a salt thereof, in which R represents a hydrogen atom or a linear or branched, alkyl, alkenyl, or alkynyl radical having at most 12 carbon atoms, which radical is optionally substituted; R1 represents a radical -(CH2)n-X; in which n represents an integer from 1 to 4; and X represents a halogen atom; a cyano radical; a radical O-R'1 in which R'1 represents a hydrogen atom or an alkyl radical; or X represents a radical S-R''1 in which R''1 represents a hydrogen atom, an alkyl radical or a heterocyclic radical; or X represents a radical in which R' and R'' are the same or different and each represents a hydrogen atom or an alkyl radical having from 1 to 4 carbon atoms, or R' and R'' together with the nitrogen atom to which they are attached form a heterocyclic radical; or X represents an azido, a thiocyanato or an isothiocyanato radical; and the wavy line indicates that the compound is in its cis or transform or in the form of a cis-trans mixture; the oxime group in the compound being in the syn form, and the compound being in the racemic or an optically active form, is a new compound. The azetidine and its pharmaceutically acceptable salts are medicaments particularly antibiotics.

Description

10 15 20 25 30 35 500 849 2 amino, dimethylamino, diethylamino, halogen, alkoxy and methyl- thio or ethylthio, aryl, arylthio, tetrazolyl, pyridinyl, tetrazolylthio and thiadiazolylthio, R1 is - (CH2) n-X, n is an integer from 1 to 4, X represents fluorine and Al is selected from the group consisting of hydrogen and pharmaceutically acceptable only metal cations and their non-toxic pharmaceutically acceptable acid addition salts, the wavy line indicates the cis form, the trans form or the cis transforms.

The products of the general formula (I) have a lot good antibiotic activity against gram-negative bacteria, in particular coloform bacteria, klebsiella, salmonella and proteus.

These products can be used in particular as medicines in the treatment of colibacillosis and associated infections, in case of infections caused by proteus, by klebsiella and of salmonella and other ailments, caused of gram-negative bacteria. They can also be used for disinfection of surgical instruments.

The valuable end products of the general formula I, can be produced by reacting an association with u rum fl “W J S (II) gun racemic or optically active, in which formula Ra represents R1, wherein R1 has the meaning given above, or draws Ra R1, in which the reactive functions are protected, formula II and A represents a hydrogen atom or a sulfo group, with a product of formula III 10 15 20 25 30 35 3 500 849 Oh s N _ C021! (III) N \ oR ' b wherein R b represents a hydrogen atom or a protecting group for the amino group, and R'b represents a protecting group for the hydroxyl group or R'b represents R, wherein R has the meaning given above, or Rb denotes a group R, in which the reactive functions are protected, for position of a product of formula IV racemic or optically active, wherein Rb, R'b, Ra and A has the meaning given above, which product one, if required and, if desired, subject to which any one or more of the following reactions in any any arrangement: a) cleavage by hydrolysis, hydrogenolysis or by effect of thiourea on the protecting group or groups protecting groups, which Rb and R'b may represent or R'b and Ra may include; b) esterification or salting of the carboxy group, which the group R'b may comprise, and salting of the sulfo group; 10 15 20 25 30 BWO L; 849 4 c) salting of the amino group or groups with an acid; d) sulphonation of the products in which group A represents a hydrogen atom; e) cleavage of the molecule to obtain an optically active product.

Further details of this procedure are described in master application 8205870-2.

The novel intermediates of the invention of formula II, can be produced by reacting a product with a eln V, (- || (v) wherein Ra has the meaning given above, and Rp denotes a protecting group for the amino group, with a product eln VI R ' P \ _ N-CH // now 5) ~ V1 zum (l wherein one of R 'represents a hydrogen atom and the other and R "p a protecting group for the amino group, or denotes R'p and R "p together is a divalent protecting group, and B represents one hydroxyl or halogen group, to obtain a product with the formula VII 10 15 20 25 30 35 849 (VII) wherein Ra, Rp, R'p and R "p which product VII is subjected to the following reactions: has the meaning given above, a) cleavage by hydrolysis, hydrogenolysis or the effect of thiourea on the group Rp; b) possible sulfonation of the amine in the 1-position; c) cleavage by hydrolysis, hydrogenolysis or the action of and R "° thiourea of groups R'p P, d) possible cleavage of the molecule to obtain a optically active product.

The protection group Rp can be selected from the previously mentioned list of substituents for the amines.

However, for reasons explained below, it is preferred that use the benzyl group or the 2,4-dimethoxybenzyl group or an equivalent.

In addition, the protecting group Rp may contain an asymmetric the carbon atom, and thus the invention has in particular to purpose a method as defined above, characterized by first reacting a product of formula (V), wherein Rp represents a protecting group for the imino group, which carries an asymmetric group, and isolates a product of formula (VII) in optically active form. 10 15 20 25 30 35 500 849 6 These optically active products of formula (VII) lead to optically active products of formula (I) according to previously described procedure.

As a protecting group, mention may be made in particular of 1-phenyl-ethyl- the group.

An example of the preparation of an optically active product of formula (VII) is reproduced below in the experimental mental part.

The groups R'p and R "p can be selected from the same list of protection groups, as mentioned above. It is preferred to use the phthaloyl group.

Group B may represent a halogen atom. You prefer the acid chloride.

When B represents a halogen atom, the reaction is carried out by product V with product VI in the presence of a base such as triethylamine or a metal such as zinc.

When B represents a hydroxyl group, being a dehydrating agent such as an anhydride, preferably trifluoroacetic anhydride.

The turnover of the products of formula V with product the compounds of formula VI preferably give the cis products.

The trans products are obtained by isomerization in alkaline environment.

The primary reaction to remove protecting groups has the purpose, when one wants to perform the sulfonation of the resulting products, to selectively remove the group Rp. 10 15 20 25 30 7 500 849 Thus, it is preferably used as indicated above, a benzyl or dimethoxybenzyl group such as man preferably unblocked by means of an oxidation agents such as potassium peroxodisulfate.

One preferably works in a solvent such as the mixture of water-acetic acid or acetonitrile.

The possible sulfonation of the products, whose secondary amine in the 1-position is free, is performed as indicated above.

The possible second operation to remove the protective groups aim to release the amine in the 3-position one by eliminating the groups R'p and R "p. When, as stated above, one works with a phthalimido group, the elimination is carried out as indicated above with hydrazine, preferably a hydrazine hydrate in a solvent such as dimethylformamide.

Of course, especially in the case when not performs the sulfonation of the products of formula IV, and R "p are eliminated simultaneously. k R R ' to the groups p, p The cleavage is performed, as indicated above, as usual way.

The products of formula (V), which are not known, can prepared by reacting an aldehyde of the formula RaCHO optionally in the form of hydrate Ra-CH (OH) 2 on a protected amine of the formula RPNHZ. 10 15 20 25 30 500 849 8 Example 1; 4-fluoromethyl-3-: 2- (2-amino-4-thiazolyl) -2- methoxyimino-acetamido] -2-oxo-azetidine-1-sulfonic acid cis, sight, racemic.

0.915 g of 2- (2-tritylamino-4-thiazolyl) -2- methoxyimino-acetic acid, syn-isomer, 7 cm 3 of acetone and 0.319 g tosyl chloride. Stir for 50 minutes 200 ° C, filter and add a solution containing 0.216 g of 4-fluoromethyl-3-amino-2-oxo-azetidine chlorohydrate cis, 7 cm 3 of methylene chloride and 0.42 cm 3 of triethylamine.

Stir for 45 minutes, evaporate to dryness, add water, shake, spin, then stir acetone and centrifuges. The product is purified by stirring in ethyl acetate. 0.654 g of the desired the product.

Analysis: C 29 H 26 O 3 N 5 SF 543.62 calculated: C% 64.07 H% 4.82 N% 12.88 S% 5.90 F% 3.49 Found: 64.0 4.9 12.4 5.9 3.4 a) Preparation_§y_pyridinium sulfonate.

A mixture of 0.564 g is stirred at 200 DEG C. for 88 hours 10 l5 20 25 30 35 9,500,849 of the product obtained in step A, 0.410 g of pyridine sulfate and 4.1 cm 3 of dimethylformamide. You pour in 200 cm3 ether, centrifuge the product, add methanol, stir, centrifuges and dries the obtained crystals. MAN obtains 0.473 g of the desired product. b) Detritylation 0.470 g of the product obtained above are suspended. in 1.87 cm3 of formic acid, containing 33% water, after which one heats at 55 - 600 C for 5 minutes then at 700 C der l3 minutes, add 1.2 cm3 new at 700 C for 15 minutes. It is cooled to 200 C, filters, add ethanol to the filtrate and concentrate formic acid and heats up then dries to dryness. The residue is added with water. and ethanol and then concentrate again to dryness.

The residue is dissolved in water, added 1.6 cm3 10% sodium bicarbonate. You filter, add 2N hydrochloric acid to pH 2, evaporate the water, stir out the residue it into a dough in water, filters, washes with water, then with ether, dries and obtains 0.140 g of the desired the product. M.p. (decomposition) Q = 240O C.

Analysis: C 10 H 12 O 6 N 5 S 2 F = 381.36 calculated: C% 31.50 H% 3.17 N% 18.36 S% 16.8l F% 4.98 found: 31.6 3.2 l8.5 l6.5 5, l Preparation of 4-fluoromethyl-3-amino-2-oxo-azetidine hydrochloride cis 1) N-methyl-N-methoxy-fluoroacetamide.

27.2 g of fluoroacetyl chloride are mixed in 120 cm 3 of methylene chloride, cools to +50 C under inert gas and invests in and SO cm3 methoxymethylamine while maintaining the temperature read below 200 C, after which stir for 2 hours at 200 C. Filter, drive off the solvent while immersed 10 l5 20 25 30 35 500 849 10 pressure, redistills the residue under reduced pressure and obtains 30.9 g of the desired product.

Boiling point23 = 930 ° C. 2) Fluoroacetaldehyde hydrate.

7.8 g of the product obtained in the previous reaction are dissolved. the step, in 133 cm 3 of tetrahydrofuran, cools to 0, +20 C and slowly charges 74 cm 3 of a 1M solution of diisobutyl- aluminum hydride and hexane. The temperature is allowed to slowly return go to room temperature, pour in a mixture of 28 cm3 concentrated hydrochloric acid and 56 cm3 of water under cooling, stir about and then distills under atmospheric pressure. One obtained 38 cm3 of the desired product, diluted in water (boiling point = 75 to loo, 5 ° c). 3) 4-Fluoromethyl-3-phthalimido-2-oxo-1- (1-phenyl-ethyl) - azetidine, cis.

Dilute 69 cm 3 of solution as obtained in the previous walking step in 100 cm3 of water. You cool in an ice bath under l5 Ü 3 minutes and then add 8.8 cm DL <3-phenyl-ethylamine, stir for 10 minutes, filter, wash with water and add 130 cm3 of methylene chloride to the filtrate. Man reflux- boil to complete dissolution, cool, decant, dry the organic phase, it then cools under inert gas to -5 ° C. Slowly add 15.4 g of phthalomlaoacetyl- chloride in 60 cm3 of methylene chloride and 10.4 cm3 of triethylamine in methylene chlorides. The temperature is allowed to return to 200 C and stir for 1 hour. 25 cm3 of 10% are added. sodium bicarbonate and 60 cm3 of water, stir, decanate extracts with methylene chloride, they dry organically combined phases, concentrating them on dryness, chromatography graphs the residue on silica eluting with methylene chloride containing 10% ethyl ether and receiving 13.7 g of the desired product. l0 15 20 25 30 35 11 500 849 5ggly§ = C20H17O3N2 F = 352.37 calculated: C% 68.17 H% 4.86 N% 7.95 F% 5.39 found: 68.2 4.9 7.8 5.6 4) 4-fluoromethyl-3-phthalimido-2-oxo-azetidine, cis, race- misk.

The 13.7 g of the product obtained in the previous procedure are dissolved. step step, in 200 cm3 acetonitrile and add 3 130 cm a solution of 22.2 g of ammonium persulphate in 52 cm 3 of water water. Boil at reflux, strain for 15 minutes. and reflux for 1 hour and 25 minutes. MAN cools, saturates with sodium chloride, decants, washes with a saturated aqueous solution of sodium chloride, extracted with ethyl acetate, dries the combined organic phases and evaporates the solvent. The residue is chromatographed on silica eluting with the methylene mixture chloride-ethyl acetate (75-25), wash the obtained crystalline with ethyl ether to give 3.756 g of the desired the duct.

IR spectrum (CHCl3) Absorbances at 3430 cm -1 (-NH) and 1790, 1770 and 1725 cm'l (c === o p-iakcam and fcaiimiao). 5) 4-fluoromethyl-3-amino-2-oxo-azetidine hydrochloride, cis.

1.24 g of the product obtained therein are suspended the previous step, in 1.2 cm3 of dioxane, then add 3 3 l4 cm dioxane. Hold for 45 minutes at room temperature, 1N hydrochloric acid and lasts of a solution of 1 cm 3 of hydrazine hydrate for 50 cm n 3 after which add 5 cm stirring 15 hours. The focus is on dryness, add water and 2.3 cm3 lN hydrochloric acid, stir and filter rar. Ethanol is added to the filtrate and concentrated 10 15 20 25 30 35 500 849 12 to dryness. Methanol is added to the residue, then ethanol and concentrate again to dryness. MAN recrystallizes the crystals in methanol.

0.391 g of the desired product is obtained. M.p. (Sun- derfaii) z 22ø ° c.

Example 2: 4-Fluoromethyl-3- [2- (2-amino-4-thiazolyl) -2- (1-carboxy-1-methyl-ethoxy) -imino-acetamido] -2-oxo-azetidine- 1-sulfonic acid cis, syn, racemic.

0.686 g of 2- (2-tritylamino-4-thiazolyl) -2- (1- t-Butoxycarbonyl-1-methyl-ethoxy) -imino-acetic acid, syn- isomer, 5 cm 3 of acetone and 0.17 cm 3 of triethylamine and then 0.229 g of tosyl chloride, stir for 50 minutes, filters and puts the filtrate while stirring with a solution of 0.155 g of 4-fluoromethyl-3-amino-2-oxo-azetidine chlorohydrate ethylamine. Stir for 55 minutes at 200 ° C, evaporate cis, in 5 cm 3 of methylene chloride and 0.3 cm 3 of tri- solvents, add methylene chloride and water, add 2 cm3 of 10% sodium bicarbonate, stir, de- edging, extracting with methylene chloride, drying the compounds the organic phases and concentrates to dryness. MAN chromatographs the residue on silica eluting with ethyl ether to give 0.613 g of the desired product.

The thiazole compound used as a starting product is described French Patent Application 2,421,906. 10 15 20 25 30 35 13 a) Preparation of pyridinium sulphate.

Dissolve the product obtained in step A and 0.36 g pyridine sulfane in 3.6 cm 3 of dimethylformamide.

Stir at 200 C for 62 hours, pour in water, stir if, centrifuges and dries the precipitate obtained. MAN obtains 0.518 g of the desired product. b) Detritylation: The product obtained in the previous step is dissolved. in 2.9 cm 3 of trifluoroacetic acid and maintains at 200 ° C 15 minutes.

29 cm3 of isopropyl ether are added, filtered and stirred the product in ethyl acetate for 15 minutes. You filter, dries, dissolves the product in some water, containing 1 cm3 10% sodium bicarbonate, filters, additives 2N hydrochloric acid to the filtrate to pH 2, filters, evaporates the water in batches, cools, centrifuges crystalline , wash them with ether to give 0.094 g of it ~ desired product. M.p. (decomposition) 2 2300 C.

NMR spectrum (DMSO - 90 MHz) Peaks at 1.5 ppm (CH3), 3.78 to 4.94 ppm (H4 and CHZF) 5.22 - 5.27 - 5.32 and 5.37 ppm (H4), 6.88 ppm (H5 thiazole syn), 9.21 and 9.31 ppm (NHCO).

Example 3: 4-Fluoromethyl-3- [2- (2-amino-4-thiazolyl) -2- difluoromethoxyimino-acetamidol-2-oxo-azetidine-1-sulfonic acid acid, cis, syn, racemic. 849 10 15 20 25 30 35 sun 849 ut 0.914 g of 2- (2-tritylamino-4-thiazolyl) -2-di- fluoromethoxyimino-acetic acid, syn isomer, 7 cm acetone and 0.25 cm 3 of triethylamine and then add 0.339 g of tosyl chloride and stir for 50 minutes. You then add a solution of 0.23 g of 4-fluoromethyl-3-amino-2-oxo-azetidine chlorohydrate cis in 7 cm 3 of methylene chloride and 0.45 cm 3 of triethyl amin. Stir for 1 hour and 30 minutes, evaporate solvents, then add methylene chloride and water 3 cm3 10% sodium bicarbonate, stir, decant, extracts the aqueous phase with methylene chloride, dries the the organic phases, evaporates the solvent, recycles absorbs the residue in ethanol, cools, centrifuges crystalline , wash them with ethanol then with ethyl ether and dry kar dem. 0.537 g of the desired product are obtained.

Si§f_sXn¿ šaåeßiâki a) Preparation of pyridinium sulfonate.

Dissolve the product obtained in step A and 0.37 g pyridine sulfane in 3.7 cm 3 of dimethylformamide. You move under 72 hours at 200 ° C, pour in 150 cm3 of ether, filter, wash take ether and dissolve the product in ethanol. It is about, filters the crystals formed, washing with ethyl ether and dries them. 0.506 g of the desired product are obtained. the duct. b) Detritylation: 0.76 g of the product obtained above is mixed with 4 cm3 formic acid containing 33% water. You warm up 600 C for 15 minutes, dilute with water, filter, add adds ethanol to the filtrate, brings to dryness, absorbs with a mixture of water and ethanol, brings to dry again, resume with water and add 2 cm 3 10-rocentict sodium bicarbonate, filters an insoluble P, 10 15 20 25 30 35 16 500 8¿9 substance, add 2N hydrochloric acid to the filtrate pH 2, concentrates and allows to crystallize. You filter crystals, wash them with water and then with ethyl ether and dries. 0.312 g of the desired product are obtained. the duct. ë fl ëíïï * C10H10 ° 6Nss2F3 calculated; c% 26.78 H6 2.41 N% 16.78 sæ 13.66 P3 15.36 found: 28.9 2.5 16.6 13.4 15.3 NMR spectrum (DMSO) 90 MHz Peaks at 4.39 and 4.94 ppm (-CH2-F) Peaks at 5.21 - 5.26 - 5.3 and 5.35 ppm (H3 cis) Peaks at 6.38 - 7.15 and 7.93 ppa (-CHF2) Peaks at 7.01 ppm (H5 thiazole) Peaks at 9.66 and 9.76 ppm (-CONH) IR spectrum (CHCl 3) Absorbances at 1770 cm -1 (C = O lactam), 1675 cm -1 (amide), 1640 cm-1 (amide II), 1585 cm-1 (conjugated system), 1530 cm -1 (thiazole), 1280 - 1270 cm -1 (-sO 3 H) and _ I 1052 cm -1 (-c = N-o-).

Example 4: 4-Fluoromethyl-3- [2- (2-amino-4-thiazolyl) -2- hydroxyimino-acetamido} -2-oxo-azetidine-1-sulfonic acid cis, sight, racemic.

Step A: 4-Fluoromethyl-3-C2- (2-tritylamation-on-thiazolyl-2- Efåtïl9Xši¶iE ° Z¿EeEaEïÉ ° l'Ä "9X9'â2Étldln_ ° lS¿ §YEf ragemic.

0.806 g of 2- (2-tritylamino-4-thiazolyl) -2-trityl- oxy-imino-acetic acid, syn isomer, 5 cm 3 of acetone and 0.17 cm 3 of triethylamine and then add 0.228 g of tosyl chloride.

Stir for 1 hour, then add 0.155 g 4-Fluoromethyl-3-amino-2-oxo-azetidine hydrochloride in 5 cm 3 methylene chloride and 0.31 cm 3 of triethylamine. You stir under 10 15 20 25 30 35 BÜÛ 849 m 20 minutes, add methylene chloride, stirring again under l hour and 30 minutes, bring to dryness, add methylene chloride and water, stir, decant, dry it organic phase, evaporates the solvent and chromatograph graphs the residue on silica eluting with ethyl ether. 0.598 g of the desired product are obtained. ragemiåk. a) Preparation of pyridinium sulfonate.

The procedure is as indicated in step B of Example 4, starting from from the product obtained in step A above and receiving the desired product. b) Detritylation The procedure is as follows in step B of Example 4 from the product obtained above and obtains the desired the product.

Example 5 (3S, 4S) Z 4-Fluoromethyl-3- [2- (2-amino + 4-thiazolyl] -2-methyl] imino-acetamido] -2-oxo-acetidine-1-sulfonic acid Example 4: 4-Fluoromethyl-3-phthalimido-2-oxo-1- (1-phenylethyl) - -acetidine.

He stirs for 96 minutes 96.6 cm3 of an aqueous solution of f1uoroaceta1aenyanyafat 0.797 M / 1, iøo cm3 aqueous solution of ice-cold sodium chloride and 9.8 cm 3 R (+) chloroform, dries of a saturated phenylethylamine. It is extracted with 192 cm3 and cools to -70 ° C under an inert atmosphere. You invest together early for 15 minutes while maintaining the temperature at -50 ° C 2 ° C 16.8 g of phthalimidoacetyl chloride 1 77 cm 3 of chloro- form, then 7.8 g of triethylamine in 77 cm 3 of chloroform. Man vär- more back to room temperature and let rest for 1 hour. 10 15 20 25 30 35 17 500 849 He adds 46 cm3 of a 10% aqueous solution of sodium bicarbonate, then 77 cm 3 of water. You move strongly, decant, re-extract with methylene chloride, wash it organic phase with water, dries and concentrates dryness under reduced pressure. The residue is chromatographed on silica eluting with a mixture of benzene-acetone (95: 5). He recovers 10.3 g of the 35.48 isomer and 2.5 g of 3R.4R isomers.

Molecular Weight Analysis 352.37 Calculated C% 68.2 H% 4.86 N% 7.95 Ft 5.40 Found (isomer 35.48) 68.4 4.9 8.0 5.3 (isomer 3R.4R) 67.1 4.8 7.4 5.1 Iain: lsomer 38.48 = -29 ° C ¿1.5 ° c (C = 1 x cH 30 H) isomer 3R, 4R = + 50 ° C ¿1.5 ° C (C = 1 x CHCl 3) §Tgg_§: (3S, 4S) 4-fluoromethyl-3-phthalimido-2-oxo-1-acetidine.

9.8 g of the previously obtained (3S, 4S) isomer are boiled in 150 cm 3 of acetonitrile and 96.5 cm 3 for 15 minutes add 15.9 g of ammonium peroxide disulfate in 3 39 cm of water and reflux for 1 hour and 30 hours linuter. After cooling, saturate the reaction mixture water. after which one sodium chloride, decant, wash with water saturated with sodium chloride and extract with ethyl acetate. You wash it the organic phase with 100 cm3 of a solution containing 20 g sodium thiosulfate per 100 cm of water saturated with sodium chloride. The organic phase is dried and concentrated dryness under reduced pressure, chromatographs the residue on silica, eluting with a mixture of methylene chloride-ethyl acetate (75-25) and obtained after crystallization from ether 2.33 g of the desired product. Mp = 160 ° C-162 ° C. [α] D = + 7 ° 11 ° (C = 1 X CH 3 OH) Step C: Hydrochloride of (3S, 4S) 4-fluoromethyl-3-amino-2-oxo- -acetidine.

He mixes 2.3 g of that product. obtained in step B, and dioxane, add for 20 minutes 26 cm of a 3 hydrazine hydrate supplemented 2.3 cms solution prepared with 1 cm 10 15 20 25 30 som 849 18 3. . with 50 cm of dioxane. After 45 minutes at room temperature 9.3 cm3 of 1N hydrochloric acid are added. You stir for 16 hours room temperature under inert atmosphere, concentrates to dry under reduced pressure, resume with anhydrous ethanol, then brings to dryness. dissolves the residue in a minimum of methanol, add ethanol and concentrate again Dryness. He dissolves the residue in a minimum of methanol below reflux, ice-cool, centrifuge, wash with cold methanol, then with ether. 1.10 g of it are obtained in several yields desired product.

Analysis: C H ON ClF: 154.57 4 8 2 Calculated C% 31.08 H% 5.22 Ni 18.12 Cl% 22.24 F% 12.29 Found 6 32.1 5.2 17.0 20.8 11.4 [α] D = -25 ° ¿1 ° (C = 1% CH 3 OH) Step D: (3S, 4S) Z 4-Fluoromethyl-3- [2- (2-tritylamino-4-thiazole) -yl) -2-methoxyimino-acetamido1-2-oxo-8-acetidine 2.85 g of 2-tritylamino-triazole-4- are stirred for 40 minutes. -yl-2-methoxyiminoacetic acid, 0.92 cm 3 triethylamine, 33 cm 3 acetone and 1.23 g of tosyl chloride. He adds 0.95 g of it - 3 the product obtained above in 33 cm 3 of methylene chloride and 1.85 cm 3 of triethylamine. You concentrate on dryness. re- occupy with ethyl acetate, wash with water. then with one 10% solution of bicarbonate, dries and concentrates to dryness. The residue is chromatographed on silica, elutes with a mixture of methylene chloride-acetone (8-2), after crystallization in ethyl acetate, 1.36 g of it desired product. Mp> 220 ° C (dec.).

Analysis C 29 H 26 O 3 N 5 SF: 543.62 Calculated CX 64.07 H% 4.82 Nä 12.9 5% 5.9 F% 3.49 Found 63.7 4.9 12.6 5.9 3.3 [QJD = -2 ° _ + _ o, s ° (c = 1% om) 10 15 20 25 “9 590 S49 Step E: (3S, 4S) Z 4-Fluoromethyl-3- [2- (2-aminothiazol-4-yl) -2- -methoxyimino-acetamido1-2-oxo-1-acetidine-1-sulfonic acid.

660 mg of it are stirred under an inert atmosphere for 90 minutes product. obtained in step D. 600 mg of the SO 3 complex, pyridine and 5 cm 3 of dimethylformamide. He brings to dry- under reduced pressure, add 600 mg of the SO3 complex, pyridine. 3 cm 3 of dimethylformamide and stir another 48 tinnar. He pours the reaction mixture into 250 cm 3 of ether. decanting. eliminates the ether phase and adds acetone, filters the excess of the complex. He evaporates dimethyl- the formamide from the filtrate and dissolves the residue in methanol, chromatographs under reduced pressure on silica, eluting with methanol and bring the eluate to dryness. Tlll the received the residue is added 3 cm3 of formic acid. 33% in water, bring to 50 ° C with stirring for 30 minutes and filter rerar. Ethanol is added to the filtrate, evaporated dryness and repeat this procedure several times until the product crystallizes. You spin and receive 150 mg of product, which is purified by passing on HP20 resin Mitsubishi to obtain 55 mg of the desired pure product ten. Mp> 220 ° C (dec.).

Analysis C10H1206N5S2F: 381.36 C% 31.5 Ht 3.17 Nt 18.35 Found 31.6 3.1 17.9 [α] D = -14.5 ° + 2 ° (c = 0.3% water) 5% 16.8 FX 4.98 16.0 4.8 Calculated

Claims (4)

10 15 20 "25 30 35 590 849" x 20 Patent claims 1. Associations. intended to be used as intermediates for the preparation of 3-amino-2-oxo-azetldine-1-sulfonic acids, characterized by the formula (II) in that they consist of the compounds (II) wherein Ra represents - (CH 2) n 1-4 and X = F and A represent a hydrogen atom or a sulfo group. A process for the preparation of compounds of formula (II) (II) wherein Ra represents - (CH 2) n -X, n = 1-4 and X = F and A represents a hydrogen atom or a sulfo group. k ä n n e t e c k n a t formula (V): by reacting a compound with n wherein Ra has the meaning given in claim 1 and RP denotes a protecting group for the amino group. Formula I (VI): with a compound of (VI) wherein one of R 'represents a hydrogen atom and the other a protecting group for the amino group, or R'P and R'P together represent a divalent protection group. and B represents a hydroxyl group or a halogen group. to prepare a compound of formula (VII) and R 'P R'p \ N Ra / \ 3 4 RI! P (v11) f? 1N \ 0 R P vari Ra. R. R 'and R' have the meaning given above, which compound of formula (VII) is subjected to the following reactions: a) cleavage of the group RP by hydrolysis, hydrogenolysis or action of thiourea; b) possible sulfonation of the amino group 1 l position; c) cleavage of the groups R 'and R'P by hydrolysis, hydrogenolysis or the action of thiourea; d) possible cleavage of the molecule to obtain an optically active product. A process according to claim 2, carrying out the process according to claim 2 starting from a compound of formula (V), wherein RP represents a protecting group for the imino group having an asymmetric carbon and isolates a product of formula (VII) 1 optically active form. k ä n n e t e c k n a t av att man 4. A method according to any one of claims 1-3, characterized in that the group Ra represents a fluoromethyl group.