DE2438120A1 - 5-Phenylsulphonyl and -sulphinyl benzimidazol-2-yl-carbamates - with anthelmintic activity - Google Patents

Abstract

Benzimidazol-2-ylcarbamates of formula (I) are new: (where R and R1 are H, opt. substd. alkyl, haloalkyl, halogen, opt. substd. alkoxy, NO2, opt. substd. amino, opt. substd. alkoxycarbonyl or CN; R2 is H, opt. substd. alkyl or halogen; R3 is opt. substd. alkyl, alkenyl or alkynyl; n = 1 or 2). (I) are anthelmintics active against nematodes and cestodes.

Description

Substituted benzimidazolyl carbamic acid esters, process for it he production and their use as pharmaceuticals The present invention relates to new benzimidazolylcarbamic acid esters, processes for their preparation as well their use as medicaments, in particular as anthelmintics.

It has already become known that certain benzimidazolylcarbarnidic acid esters have an anthelmintic effect (see DT-OS 2 o29 637, French patent specification 1 56 824, DT-OS 2 164 690, P. Actor et al. Nature 215, 321 (1967)) . So the benzimidazolyl carbamic acid esters parbendazole (A) and mebendazole (B) are commercial products for the same indication.

R = = C4H9 = Parbendazole (A) K = COC6H5 = Mebendazole (B) the However, the aforementioned compounds show a less pronounced anthelmintic Effect as the compounds according to the invention of the present application.

It has been found that the new substituted benzimidazolylcarbamic acid esters of the formula in which R and R1 can be the same or different and represent hydrogen, optionally substituted alkyl, haloalkyl, halogen, optionally substituted alkoxy, vitro, optionally substituted amino, optionally substituted carbalkoxy or cyano and represent hydrogen, optionally substituted alkyl, halogen and R3 represents optionally substituted alkyl, optionally substituted alkenyl, optionally substituted alkynyl and n represents 1 or 2, have very good antithelial activity.

It has also been found that substituted benzimidazolylcarbamic acid esters of the formula (I) are obtained if a) o-phenylene-diamine derivatives of the formula in which R, R1, R² and n have the meaning given above, with acid derivatives of the formula Y-COOR (III) in which has the meaning given above and Y stands for one of the following radicals: where R3 has the meaning given above and Hal stands for halogen, or that b) 2-aminobenzimidazole derivatives of the formula are reacted in which R, R1, R2 and n have the meaning given above, with a carbonic acid derivative of the formula in which has the meaning given above and Z is halogen, optionally substituted alkoxy or the radical OCOOR3, optionally reacted in the presence of acid binders, or that c) arylthiobenzimidazolylcarbamic acid esters of the formula in which R, R¹, R² and R³ have the meaning given above, reacted with a suitable oxidizing agent.

The substituted benzimidazolylcarbamic acid esters according to the invention surprisingly show of formula (I) a much more pronounced anthelmintic effect than that Commercial products known from the prior art parbendazole and mebendazole. The substances according to the invention thus represent an enrichment for pharmacy.

The compounds of the formula (I) according to the invention can exist in tautomeric forms, as the following example is intended to show: In the registration text, the respective structural formulas are formulated in the same way in all cases for reasons of consistency.

If, in process variant a), 4-phenylsulfonyl-1,2-phenylenediamine and methyl N - [(bis-chloro) -methylene] carbamic acid are used as starting materials, the course of the reaction can be represented by the following equation: If in process variant b) 2-amino-5-phenylsulfonyl-benzimidazole and methyl chloroformate are used as starting materials, the course of the reaction can be represented by the following equation: If, in process variant c), 5-phenylmercaptobenzimidazole-2-carbamic acid methyl ester and 1 equivalent of hydrogen peroxide are used as starting materials, the course of the reaction can be represented by the following equation: If 2 equivalents of hydrogen peroxide are used in process variant c), the corresponding sulfonyl compound is formed: The optionally substituted alkyl R, R1, R2 and R3 in the formulas I, II, III, IV, V, VI is straight-chain or branched alkyl having preferably 1 to 6, in particular 1 to 4, carbon atoms. Optionally substituted methyl, ethyl, n- and i-propyl, n-, i- and t-butyl may be mentioned as examples.

As optionally substituted alkenyl R3 in the formulas I, III, V, VI is straight-chain or branched alkenyl with preferably 2 to 6, in particular 2 to 4 carbon atoms.

Examples are optionally substituted ethenyl, Propenyl- (1), Propenyl- (2) and butenyl- (3) called.

As optionally substituted alkynyl R3 in the formulas I, III, V, VI is straight-chain or branched alkynyl with preferably 2 to 6, in particular 2 to 4 carbon atoms.

Examples are optionally substituted ethynyl, priopynyl- (1), Propynyl (2) and butynyl (3) called.

As optionally substituted alkoxy R and R1 in the formulas I, II, IV, VI is straight-chain or branched alkoxy with preferably 1 to 4 Carbon atoms. Examples are optionally substituted methoxy, ethoxy, called n- and i-propoxy and n-, i- and t-butoxy.

Haloalkyl R and R1 in the formulas I, II, IV, VI preferably contain 1 to 4, especially 1 or 2 carbon atoms and preferably 1 to 5, especially 1 to 3 identical or different halogen atoms, the preferred halogen atoms being Fluorine, chlorine and bromine, especially fluorine and chlorine.

Examples include trifluoromethyl, chloro-di-fluoromethyl, bromomethyl, 2,2,2-tri-fluoroethyl and pentafluoroethyl called.

As optionally substituted carbalkoxy R and R in the formulas I, II, IV, VI is straight-chain or branched carbalkoxy with preferably 2 up to 7, in particular 2 to 5 carbon atoms. Examples may be substituted carbomethoxy, carboethoxy, carbo-n- and -i-propyloxy and carbo-n-, -i- and -t-butyloxy called.

Halogen R and R in the formulas I, II, IV, VI preferably represent Chlorine, bromine and fluorine.

The optionally substituted radicals R, R1, R2 and. R3 in the formulas I to VI can be one or more, preferably 1 to 3, in particular 1 or 2 same or different Carry substituents. As a substituent are listed by way of example: Alkyl with preferably 1 to 4, in particular 1 or 2 carbon atoms, such as methyl, ethyl, n- and i-propyl and n-, i- and t-butyl; Alkoxy with preferably 1 to 4, in particular 1 or 2 carbon atoms, such as methoxy, Ethoxy, n- and i-propyloxy and n-, i- and t-butyloxy; Alkylthio with preferably 1 to 4, especially 1 or 2 carbon atoms, such as methylthio, ethylthio, n- and i-propylthio and n-, i- and t-butylthio; Haloalkyl with preferably 1 to 4, especially 1 or 2 carbon atoms and preferably 1 to 5, especially 1 to 3 halogen atoms, the halogen atoms being identical or different and as Halogen atoms, preferably fluorine, chlorine or bromine, especially fluorine, are like Trifluoromethyl; Hydroxy; Halogen, preferably fluorine, chlorine, bromine and iodine, in particular Chlorine and bromine; Cyano; Nitro; Amino; Monoalkyl and dialkylamino with preferably 1 to 4, in particular 1 or 2 carbon atoms per alkyl group, such as methylamino, Methyl-ethylamino, n- and i-propylamino and methyl-n-butylamino; Carboxyl; Carbalkoxy with preferably 2 to 4, in particular 2 or 3 carbon atoms, such as carbomethoxy and carboethoxy; Alkylsulfonyl with preferably 1 to 4, in particular 1 or 2 carbon atoms, such as methylsulfonyl and ethylsulfonyl.

Some of the 0-phenylenediamine derivatives of the formula (II) which can be used according to the invention are not yet known. But you can easily, as shown in the following example, by reacting optionally substituted sodium benzene sulfinate with optionally substituted 5-chloro-2-nitroaniline and subsequent reduction with z. B. (Raney Ni / H2); (Pd-C catalyst / H2); 02-cat. / H2): Other routes to the abovementioned compounds of the formula (ii) are also possible. For example, 2-nitro-5-phenylmercaptoanilides are oxidized with an oxidizing agent to 2-nitro-5-phenylsulfinyl- or 2-nitro-5-phenylsulfonyl-anilides, then saponified to the corresponding anilines and to the 4-phenylsulfinyl- or 4-phenylsulfonyl -1,2-phenylenediamines reduced, as shown in the following examples: Most of the acid derivatives of the formula (III) used as starting materials are known.

As starting materials of the formula (III) are mentioned by way of example: N "Methoxyearbonylcyanamid, N methoxy carbonylisothiourea methyl ether, N-methoxycarbonylischurea methyl ether, N-methoxycarbonylguanidine, N - [(bis-methoxy) methylene] -carbamic acid methyl ester, N- / (Bis-methylmercapto) methylene 7-carbamic acid methyl ester, N- [methoxy- (methylmercapto) -methylene] -carbamic acid methyl ester.

Some of the 2-aminobenzimidazole derivatives of the formula (IV) are still not known, but they can easily be prepared by using phenylenediamine derivatives of formula (II) with cyanogen chloride in an inert solvent, optionally under Addition of a tertiary base such as triethylamine or an aqueous / alcoholic base Solution with the addition of a base, such as. B.

ITaHC03. Or NaOH reacts with one another. E.g.

Examples of starting compounds of the formula IV) include: 2-amino-5-phenylsulfonylbenzimidazole, 2-amino-6-phenylsulfonylbenzimidazole, 2-amino-5- (4-methylphenylsulfonyl) -benzimidazole, 2-amino-5- (3-chlorophenylsulfonyl) -benzimidazole, 2-amino-5-phenylsulfinylbenzimidazole, 2-amino-6-phenylsulfinylbenzimidazole.

Most of the carbonic acid derivatives of the formula (V) are known. Examples of carbonic acid derivatives of the formula (V) include: dimethyl carbonate, Diethyl carbonate, dimethyl pyrocarbonate, diethyl pyrocarbonate, methyl carbonate chloride, Allyl carbonate chloride, propargyl carbonate chloride.

Some of the arylthiobenzimidazolylcarbamic acid esters of the formula VI are not yet known. But they can easily be prepared by adding compounds of the formula with compounds of formula (III), e.g. B.

implements.

As examples of arylthiobenzimidazolylcarbamic acid esters of the formula VI are: 5-phenylthio-benzimidazolyl-2-carbamic acid methyl ester, 5-phenylthio-benzimidazolyl-2-carbamic acid ethyl ester, Propyl 5-phenylthio-benzimidazolyl-5-carbamic acid.

Those used as starting product in process variant c) Oxidizing agents are already known.

Examples include: Organic peracids, such as peracetic acid, Performic acid, perbenzoic acid, m-chloroperbenzoic acid, monoperphthalic acid, inorganic Peroxides, such as hydrogen peroxide, dissolved in water or dilute organic acids, inorganic oxidizing agents such as chromic acid, nitric acid, potassium permanganate, Chlorine, bromine, halogenated oxygen acids, such as hypochlorous, chlorous, chloric or hyperchloric acid, tert-butyl hypochlorite, methyl hypochlorite, tert-butyl chromate, organic N-halogen compounds, such as N-chlorosuccinimide, N-bromosuccinimide and N-halogenosulfonamides or N-halocarboxamides.

By appropriate selection of the reaction conditions known from the literature the oxidation potential can be adjusted accordingly and the reaction to manufacture the sulfoxides or

sulfone are directed.

Of the acid derivatives of the formula (III) are N-Nethoxycarbonylcyanamid, N-methoxycarbonylisoureaalkyl ethers, N-methoxycarbonylisoureaalkyl ethers, N-methoxycarbonylguanidine, N - [(bisalkoxy) methylene] carbamic acid ester, N- / (bisalkylmercapto) methylene 7-carbamic acid esters and N- / alkoxy- (alkylmercapto) -methylene 7-carbamic acid esters with the phenylenediamine derivatives of the formula (II) at 0 to 1500C, preferably at 3c to 12o0C, if necessary in a solvent such as alcohol, dilute acetic acid, Ethylene glycol, tetrahydrofuran, dioxane, benzene, toluene or water reacted.

It is advantageous to work in solvents that contain water and in which a pH range of 2 to 7, preferably 2 to 5, by adding a organic acid such as acetic acid or lactic acid or p-toluenesulfonic acid or an alkali salt of an organic acid is complied with.

The N-L (bis-halogen) -methylene] carbamic acid esters become advantageous in the presence of a base 9 such as triethylamine, pyridine, sodium hydroxide solution, sodium bicarbonate or sodium carbonate with the phenylenediamine derivatives of the formula II at 0 to 100 ° C, preferably 0 to 50 ° C condensed.

The N- [alkoxy- (halogen) -methylene] -carbamic acid esters and N-L-alkylmercapto- (halogen) -methylene 7-carbamic acid esters are advantageous first in the presence of a base such as triethylamine9 Pyridine, sodium hydroxide solution or sodium carbonate reacted at room temperature and then by heating, preferably in a pH range of 2 to 5 by adding a organic acid, such as acetic acid or lactic acid at 0 to 150C, preferably condensed at 20 - 120 ° C.

In the case of process variant b), the system is optionally present an organic base such as triethylamine, pyridine or an inorganic base, such as an alkali, alkaline earth alcoholate, e.g. B. sodium methylate or alkali or alkaline earth metal hydroxide, z. B. sodium hydroxide, at temperatures between about 20 and about 150 ° C, preferably between 60 and 120 ° C in an organic solvent that is indifferent to this reaction, such as B. tetrahydrofuran, dioxane, benzene, toluene, chlorobenzene, acetonitrile, acetone, Methyl ethyl ketone, diethylene glycol dimethyl ether, methanol and ethanol or mixtures the aforementioned diluents.

In reaction variant c), 1 mol of compound (VI) is added one or at least 1 mole of the oxidizing agent according to process conditions known per se in an inert organic solvent or solvent mixture, for example in water, acetic acid, formic acid, acetic anhydride, propionic anhydride, at Temperatures between about 0 and 100 ° C, preferably between 0 and 80 ° C. the Working up is done by customary methods.

The following are listed as active ingredients according to the invention: 5-phenylsulfonyl-benzimidazolyl-2-carbamic acid methyl ester, 5-Phenylsulfinyl-benzimidazolyl-2-carbamic acid methyl ester, 5- (3-chlorophenylsulfonyl ) -benzimidazolyl-2-carbamic acid methyl ester, 5- 14-chlorophenylsulfonylJ -benzimidazolyl-2-carbamic acid methyl ester 5- (4-methylphenylsulfonyl) -benzimidazolyl-2-carbamic acid methyl ester and the in Examples 1-7 on pages 23-31 listed compounds of the general Formula I.

Reference is also made to the active ingredients listed in Example 7.

The compounds shown according to the invention are shown individually for example a surprisingly good and broad action against the following nematodes and cestodes: 1. Hookworms (e.g., E3unostomum trigonocephalum, Incinaria senocephala); 2. Trichostrongylids (e.g. haemonchus contoruts, Trichostrongylus colubriformis, Ostertagia circurncinc-ta, Nippostrongylus urins, Cooperia curticei); 3. Strongyles (e.g. 3. Oesophagostomum columbianum); 4. Rhoabditids (e.g. Strongyloides ratti); 5. roundworms (e.g. 3. Toxocara canis, Toxascaris leonina, Ascaris suum); G. Pinworms (e.g. 3. Aspiculuris tetraptera); 7. T-leterakids (e.g. 3. Heterakis spumosa); 3. Flukes (e.g. Trichuris muris); 9. Filaria (e.g. Litomosoides carinii, Dipetalonema witei); 10. Tapeworms (e.g. Taenia pisiformis, Hymenolepis nana).

The effect was demonstrated in animal experiments after oral and parenteral application tested in test animals heavily infested with parasites. The dosages used were tolerated very well by the test animals.

The new active ingredients can be used as anthelmintics in human as well as used in veterinary medicine.

The new active ingredients can be converted into the customary formulations in a known manner be transferred.

The new compounds can either be used as such or in combination use pharmaceutically acceptable carriers. As dosage forms in combination with various inert carriers come tablets, capsules, I, ranlate, aqueous suspensions, injectable solutions, emulsions and suspensions, elixirs, Syrups, pastes and the like. Such carriers include solid diluents or fillers, a sterile, aqueous medium, as well as various non-toxic ones organic solvents and the like. Of course they can work for a oral administration tablets and the like with added sweeteners and the like. The therapeutically effective compound should be mentioned in the above Case present in a concentration of about 0.5 to 90% by weight of the total mixture be, d. H. in amounts sufficient to cover the above dosage range to reach.

The formulations are prepared in a known manner, e.g. B, through Extension of the active ingredients with solvents or carriers, if appropriate using emulsifiers and / or dispersants, where z. B. in In the case of the use of water as a diluent, optionally organic solvents can be used as co-solvents.

The following are examples of auxiliary substances: water, non-toxic organic solvents such as paraffins (e.g.

Petroleum fractions), vegetable oils (e.g. peanut / sesame oil), alcohols (e.g. ethyl alcohol, glycerine), glycols (e.g.

Propylene glycol, polyethylene glycol) and water; solid carriers, such as B. natural rock flour (e.g. kaolins, clays, talc, chalk), synthetic Rock flour (e.g.

highly dispersed silica, silicates), sugar (e.g. raw, milk and Glucose); Emulsifiers, such as non-ionic and anionic Emulsifiers (e.g. polyoxyethylene fatty acid esters, polyoxyethylene fatty alcohol ethers, Alkyl sulfonates and aryl sulfonates), dispersants (e.g. lignin, sulfite waste liquors, Ethyl cellulose, starch and polyvinylpyrrolidone) and lubricants (e.g. magnesium stearate, Talc, stearic acid and sodium lauryl sulfate).

In the case of oral use, tablets can of course except the carrier substances mentioned, also additives such as sodium citrate, calcium carbonate and Dicalcium phosphate, along with various additives such as starch, preferably Potato starch, gelatin and the like can also contain lubricants, such as magnesium stearate, sodium lauryl sulfate and talc, are also used for tableting will.

In the case of aqueous suspensions and / or elixirs intended for oral Applications are intended, the active ingredients can except with the abovementioned auxiliaries can be mixed with various flavor enhancers or colorings.

In the case of parenteral use, solutions of the active ingredients can be used be used using suitable liquid carrier materials.

The active ingredients can be found in capsules, tablets, lozenges, Dargees, Ampoules etc. can also be contained in the form of dosage units, with each dosage unit is adapted to deliver a single dose of the active ingredient.

The new compounds can also be used in the formulations in mixtures with other known active ingredients.

The new active ingredients can be used in the usual way. the Application is preferably carried out orally, a parenteral, especially subcutaneous, however, dermal application is also possible.

In general, it has been found to be advantageous to narrow around 1 to about 100 mg of the new compounds per kg of body weight per day to achieve deliver more effective results.

Even so, it may be necessary to use the above narrow, depending on the body weight of the test animal or the rrt of the application route, but also due to the species and their individual Behavior towards the drug or the type, its formulation and the Time or interval at which the administration takes place. So it may in some In some cases it is sufficient to manage with less than the aforementioned minimum amount, while in other cases the upper limit mentioned must be exceeded. in the If larger amounts are to be applied, it may be advisable to split them up in several To distribute individual items over the day. For use in human and veterinary medicine the same dosage range is provided. The others also apply mutatis mutandis above.

The anthelmintic effect of the active ingredients according to the invention is based on explained in more detail in the following application examples.

Example A Gastric and intestinal worm test / sheep Experimental with Haemonchus contortus or Trichostrongylus colubriformis infected shafts become after expiration the prepatent period of the parasites treated. The amount of active ingredient was considered pure active ingredient administered orally in gelatin capsules.

The efficiency is determined by the fact that one with the> ot excreted worm eggs before and after treatment quantitatively.

Complete cessation of egg excretion after treatment means that the warmer ones have been aborted or are so damaged that they no longer have eggs can produce (dose effectiva).

Tested active ingredients and effective dosages (dose effectiva minima) can be seen in Table 1 below.

In the table below, in addition to the formula of the active ingredient the type of parasite controlled and the minimum effective dose in mg of active ingredient per kg body weight indicated at which 90% of the worms have been aborted ("dose effectiva minima (red. 90) in mg / kg ").

T abe 1 1 e 1 (for example A) Active ingredient according to the invention, parasite dose effectiva minimum (lieduk tion > 90% in mR / kg Haemonchus / \ 1N cont. 1 -NH-CO-OCH Trichostrong. o, 5 O 3 col. N H 0 O -S- + g Haemonchus o, 5 N 3 Trichostrong. II col.

Related preparations for comparison Parbendazole Haemonchus cont. 5 Trichostrong.

col. 2.5 Mebendazole Haemonchus cont. 5 Trichostrong.

col. 2.5 Example 1 5-Phenylsulfonyl-benzimidazolyl-2-carbamic acid methyl ester To 6.6 g (0.03 mol) of 4-phenylsulfonyl-1,2-phenylenediamine, dissolved in 100 ml of chloroform, 1o ml of triethylamine and 5.6 g (0.031 mol) of N - [(bis-chloro) methylene] carbamic acid methyl ester added dropwise at 2o0C. The mixture is refluxed for 30 minutes. After distilling off of the solvent in vacuo, the residue is triturated several times with water, filtered off with suction, Triturated again well with n-hexane and again suctioned off.

Yield: 9 g of 5-phenylsulfonyl-benzimidazolyl-2-carbamic acid methyl ester (M.p. 3080C).

The 4-phenylsulfonyl-1,2-phenylenediamine used as starting material, Mp. 115 ° C, is obtained by catalitic hydrogenation of 2-Nitzro-5-phenylsulfonyl-aniline, Mp. 184-185 ° C, or obtained from 2-nitro-4-phenylsulfonyl-aniline, m.p. 172-1760C.

The 2-nitro-5-phenyl-sulfonyl-aniline in turn is made by reaction of sodium benzenesulfinate with 5-chloro-2-nitroaniline in dimethylformamide 130C manufactured.

Example 2 N-methoxycarbonyl-isothiourea methyl ether, which by Reaction of 7.8 g of S-methylisothiourea sulfate with 4.5 g of methyl chloroformate and 17 g of 25% sodium hydroxide solution was obtained, is increased with acetic acid (CV 5-6 ml) pH 5 brought. 6.6 g of 4-phenylsulfonyl-1,2-phenylenediamine, dissolved in alcohol, are used to, heated for 1 hour to 80-850C, cooled, the reaction product filtered off and obtained after washing with water and alcohol 8.5 g of 5-phenylsulfonyl-benzimidazolylcarbamic acid methyl ester of melting point 3080C, the same compound is obtained analogously by condensation with N-methylcarbonyl-isourea methyl ether in a crowd of 4.7 g or by condensation of 4-phenylsulfonyl-1,2-phenylenediamine (0.03 mol) with 0.03 mol of N - [(bis-ethoxy) -methylene] -carbamic acid methyl ester 110 to 140 ° C in glycol (yield 5.6 g) or with 0.03 moles of If- / (bis-alkylmercapto) -methylene] carbamido acid methyl ester (Yield 4.7 g) or with 0.03 mol of N- [ethoxy- (methylmercapto) -methylene] -carbamic acid methyl ester (Yield 3.8 g) or with 0.03 mol of N-methoxycarbonylguanidine at 140 to 160 ° C (yield 5.4 g) or with 0.03 ol methoxycarbonylcyanamide in water at 80 to 100 ° C, whereby a pH of 2 to 4 is adjusted with hydrochloric acid (yield 3.5 g).

Example 3 To 24.8 g (0.1 mol) of 4-phenylsulfonyl-1,2-phenylenediamine and 1o, 1 g (0.1 mol) of triethylamine in 300 ml of dry chloroform are stirred with stirring at 0 ° C. 16.7 g (0.1 mol) -L-chloro- (methylmercapto) -methylene] -carbamic acid methyl ester in a little chloroform, added dropwise. The mixture is stirred for 2 to 3 hours at 25 to 30 ° C, evaporates in vacuo, adds 200 ml of alcohol, 10 ml of water and 0.5 g of p-toluenesulfonic acid and heated to 9o0C for 2 hours. After evaporation, the residue is stirred with water, filtered off and the reaction product was washed with alcohol. Yield 26.2 g of 5-phenylsulfonylbenzimidazolyl-2-carbamic acid methyl ester. One condenses analogously o, 1 mol of N- [chloro (methoxy) methylene] carbamic acid methyl ester with 4-phenylsulfonyl-1,2-phenylenediamine, a yield of 21.3 g is obtained.

Example 4 27.3 g (0.1 mol) of 2-amino-5-phenylsulfonyl-benzimidazole if one adds to a solution of 2.4 g of sodium in 200 ml of methanol, 5.6 g of dimethyl carbonate are added dropwise and refluxed for one hour. It is evaporated in a vacuum, washed the The residue is successively mixed with water, dilute acetic acid and alcohol and obtained after drying 27.3 g of 5-phenylsulfonyl-benzimidazolyl-2-carbamic acid methyl ester, M.p. 3080C.

The same compound is formed by reacting 2-amino-5-phenylsulfonyl-benzimidazole with an equivalent amount of dimethyl pyrocarbonate in chloroform at 40 ° C.

The same compound is also produced by reacting 0.1 mol 2-Amino-5-phenylsulfonyl-benzimidazole, dissolved in chloroform, with 0.1 mol of methyl chloroformate in the presence of 0.1 mol of triethylamine. After the end of the dropping in, the mixture is still heated 5 to 6 hours under reflux. Yield: 26.5 g.

The 2-amino-5-phenylsulfonylbenzimidazole used as the starting material arises from the reaction of 4-phenyl-sulfonyl-1,2-phenylenediamine with chlorine or Cyanogen bromide in tetrahydrofuran, alcohol or water.

Example 5 Obtained according to the preparation described in Example 1 from 6.5 g of 4-phenylsulfinyl-1,2-phenylenediamine and 5.6 g of N- (bis-chloro) -methylene7-carbamic acid methyl ester 8.4 g of 5-phenylsulfynyl-benzimidazolyl-carbamic acid methyl ester, melting point 2870C (decomposition).

The 4-phenylsulfinyl-1,2-phenylenediamine used as the starting material is obtained in the following way: 2-nitro-5-phenylmercapto-propionanilide is in Acetic anhydride with one equivalent of H202 to 2-nitro-5-phenylsulfinyl-propionanilide, Mp. 62-64 ° C, oxidized, then saponified to 2-nitro-5-phenylsulfinyl-aniline and catalytically reduced to 4-phenylsulfinyl-1,2-phenylenediamine.

Example 6 12 g of 5-phenylmercapto-benzimidazole-2-carbamic acid methyl ester are dissolved in 500 ml of acetic anhydride. 4.7 g of 30% hydrogen peroxide solution are added dropwise, stir for 3 hours and evaporate in vacuo. The residue becomes with a mixture rubbed with petroleum ether / ethyl acetate. After filtering off, 5-phenylsulfinyl-benzimidazolyl-2-carbamic acid methyl ester is obtained of m.p. 2870C (decomposition).

In a corresponding procedure, 12 g of 5-phenylmercapto-benzimidazolyl-2-carbamic acid methyl ester are obtained, dissolved in 250 ml of acetic acid with 12 g of 30% hydrogen peroxide and 8 g of 5-phenylsulfonyl-benzimmidazolyl-2-carbamic acid methyl ester of m.p. 308 ° C.

EXAMPLE 7 The method described in Example 1 gives the following benzimidazolyl-2-carbamic acid esters from substituted phenylenediamine derivatives: Starting materials Compounds prepared according to the invention R1 'R2' n F. ° C R1 'R2' n R3 'F. ° C C6H5 H 2 C6H5 H 2 C2H5 C6H5 H 2 C6H5 H 2 CH2-CH = CH2 C6H5 H 2 C6H5 H 2 CH2-C # CH C6H5 CH3 2 C6H5 CH3 2 CH3 C6H5 Cl 2 C6H5 Cl 2 CH3 4- (3-CH3O-C6H4) H 2 4- (3-CH3O-C6H5) H 2 CH3 4- (4-Cl-C6H4) H 2 126 4- (4-Cl-C6H5) H 2 CH3 317 oc

4- (4-CH3-C6H4) H 2 183 4- (4-CH3-C6H5) H 2 CH3 330 u.

4- (3-CH3-C6H4) H 2 4- (3-CH3-C6H5) H 2 CH3 4- (2-CH3-C6H4) H 2 4- (2-CH3-C6H5) H 2 CH3 4- (3-Cl-C6H4) H 2 160 4- (3-Cl-C6H5) H 2 CH3 317 ET

4- (2-Cl-C6H4) H 2 160 4- (2-Cl-C6H5) H 2 CH3 317 ET

Starting materials Compounds produced according to the invention R1 'R2' n R1 'R2' n R3 '4- (4-Br-C6H4) H 2 4- (2-Br-C6H4) H 2 CH3 4- (3,4-Cl-C6H4) H 2 4- (3.4 -Cl-C6H3) H 2 CH3 4- (4-C4H9-C6H4) H 2 4- (2-C4H9-C6H4) H 2 CH3 4- (4-C2H5-C6H4) H 2 4- (2-C2H5-C6H4) H 2 CH3 4- [3.5 (CH3) 2C6H3] H 2 4- [3.5 (CH3) 2C6H3] H 2 CH3 4- [2.4 (CH3) 2C6H3] H 2 4- [2.4 ( CH3) 2C6H3] H2 CH3 4- (3-C2H5O-C6H4) H2 4- (3-C2H5O-C6H4) H2 CH3 4- (4-CH3-CONH-C6H4) H2 4- (2-CH3-CONH-C6H4 H 2 CH3 4- (4-CH3O-C6H4) H 2 4- (2-CH3O-C6H4) H 2 CH3 4- (4-CH3S-C6H4) H 2 4- (2-CH3S-C6H4) H 2 CH3 4- (3-CF3-C6H4) H 2 4- (3-CF3-C6H4) H 2 CH3 4- (4-F-C6H4) H 2 4- (2-F-C6H4) H 2 CH3 4- (4- (CH3) 3C-C6H4) H 2 4- (4- (CH3) 3C-C6H4) H 2 CH3 4- (4-CH3CO-C6H4) H 2 4- (4-CH3CO- C6H4) H 2 CH3 Starting materials Compounds prepared according to the invention R1 'R2' N R1 'R2' n R3 '4- (3-CH3CO-C6H4) H 2 4- (3-CH3CO-C6H4) H 2 CH3 4- (3-C3C7-CO-C6H4) H 2 4- (3-C3C7-C6H4) H 2 CH3 4- (4-H3CO-CO-NH-C6H4) H 2 4- (3-H3CO-CO-NH-C6H4) H 2 CH3 4- (4-CN-C6H4) H 2 4- (4-CN-C6H4) H 2 CH3 4- (3-CN-C6H4) H 2 4- (3-CN-C6H4) H 2 CH3 C6H5 H 1 C6H5 H 1 C2H5 C6H5 H 1 C6H5 H 1 CH2-CH = CH2 C6H5 H 1 C6H5 H 1 CH2-C # CH C6H5 CH3 1 C6H5 CH3 1 CH3 C6H5 Cl 1 C6H5 Cl 1 CH3 4- (3-CH3O-C6H4) H 2 4- (3-CH3O-C6H4) H 1 CH3 4- (3-Cl-C6H4) H 2 4- (3-Cl-C6H4) H 1 CH3 4- (3-CH3-C6H4) H 2 4- (3-CH3-C6H4) H 1 CH3 Starting materials Compounds prepared according to the invention R1 'R2' N R1 'R2' n R3 '4- (3-CH3-C6H4) H 1 4- (3-CH3-C6H4) H 1 CH3 4- (2-CH3-C6H4) H 1 4- (2-CH3-C6H4) H 1 CH3 4- (3-Cl-C6H4) H 1 4- (3-Cl-C6H4) H 1 CH3 4- (2-Cl-C6H4) H 1 4- (2-Cl-C6H4) H 1 CH3 4- (4-Br-C6H4) H 1 4- (4-Br-C6H4) H 1 CH3 4- (3,4-Cl2-C6H3) H 1 4- (3,4-Cl2-C6H3) H 1 CH3 4- (4-C4H9-C6H4) H 1 4- (4-C4H9-C6H4) H 1 CH3 4- (4-C2H5-C6H4) H 1 4- (4-C2H5-C6H4) H 1 CH3 4- [3,5- (CH3) 2C6H3) H 1 4- [3,5 (CH3) 2C6H3) H 1 CH3 4- [2,4- ( CH3) 2C6H3) H 1 4- [2,4 (CH3) 2C6H3) H 1 CH3 4- (3-C2H5O-C6H4) H 1 4- (3-C2H5O-C6H4) H 1 CH3 4- (4-CH3-CONH-C6H4) H 1 4- (CH3-CONH-C6H4) H 1 CH3 4- (4-CH3O-C6H4) H 1 4- (4-CH3O-C6H4) H 1 CH3 4- (4-CH3S-C6H4) H 1 4- (4-CH 3 S-C 6 H 4) H 1 CH 3 Starting materials produced according to the invention Compounds R1 'R2' n R1 'R2' n R3 '4- (3-CF3-C6H4) H 1 4- (3-CF3-C6H4) H 1 CH3 4- (4-F-C6H4) H 1 4- (4-F-C6H4) H 1 CH3 4- (4- (CH3) C-C6H4) H 1 4- (4- (CH3) C-C6H4) H 1 CH3 4- (4-CH3CO- C6H4) H 1 4- (4-CH3CO-C6H4) H 1 CH3 4- (3-CH3CO-C6H4) H 1 4- (3-CH3CO-C6H4) H 1 CH3 4- (4-C3H7-CO-C6H4) H 1 4- (4-C3H7-CO-C6H4) H 1 CH3 4- (4-H3CO-CO-NH-C6H4) H 1 4- (4-H3CO-CO-NH-C6H4) H 1 CH3 4- (4-CN-C6H4) H 1 4- (4-CN-C6H4) H 1 CH3 4- (3-CN-C6H4) H 1 4- (3-CN-C6H4) H 1 CH3

Claims (4)

Claims, 1.3 Substituted benzimidazolylcarbamic acid esters of the formula in which R and R1 can be the same or different and represent hydrogen, optionally substituted alkyl, haloalkyl, halogen, optionally substituted alkoxy, nitro, optionally substituted amino, optionally substituted carbalkoxy or cyano and R2 represents hydrogen, optionally substituted alkyl, halogen and optionally substituted alkyl, optionally substituted alkenyl, optionally substituted alkynyl and n is 1 or 2. 2.) Process for the preparation of substituted benzimidazolyl carbamic acid esters of the formula in which R and R¹ can be the same or different and represent hydrogen, optionally substituted alkyl, haloalkyl, halogen, optionally substituted alkoxy, nitro, optionally substituted amino, optionally substituted carbalkoxy or cyano and R2 represents hydrogen, optionally substituted alkyl, halogen and R3 represents optionally substituted alkyl, optionally substituted alkenyl, optionally substituted alkynyl and n represents 1 or 2, characterized in that a) o-phenylene-diamine derivatives of the formula in which R, R1, R2 and n have the meaning given above, with acid derivatives of the formula Y-COOR³ (III) in which R3 has the meaning given above and Y stands for one of the following radicals: where R3 has the meaning given above and Hal stands for halogen, or that b) 2-aminobenzimidazole derivatives of the formula are reacted in which R, R1, R2 and n have the meaning given above, with a carbonic acid derivative of the formula in which has the meaning given above and Z is halogen, optionally substituted alkoxy or the radical OCOOR3, optionally reacted in the presence of acid binders, or that c) arylthiobenzimidazolylcarbamic acid esters of the formula in which R, R1, R2 and R3 have the meaning given above, is reacted with a suitable oxidizing agent. 3.) Medicines, characterized by a content of at least a substituted benzimidazolyl carbamic acid ester according to claim 1. 4.) Process for the production of anthelmintic means, thereby characterized in that substituted benzimidazolyl carbamic acid esters according to claim 1 mixed with inert, non-toxic, pharmaceutically suitable carriers.