FI61688B - PROCEDURE FOR THE FRAMEWORK OF THERAPEUTIC ANALYSIS - Google Patents

Description

r1 ADVERTISEMENT & Λ * θα jjgijft tBJ (11) UTLÄGGN I NGSSKRIFT OlOOö C (45) Patent aySnetty 10 09 1932 Patent meddelat (51) • Cv.tk.V.cu3 0 O? C 103/34 * 101/34, c O? D 213/75 * 239/49, 241/20 SUOM l — FI N LAND (21) p “* ntt, h, k ------——« · n »UU £ / (22) Hsktmtopllvl - AiMöknlngadsg 06.03.71 * (23) AlkupiM - GIWjh * ud «* 06.03.7 ^ (41) Tullut JulklMktl - Bllvit effamllg 2U.09.74

Patent and Registration Iti »/ 44) NthUvftkiipmon and moonLullullwn date. - 31.05.82

Patent and Registration Publications (32) (33) (31) Py / ditty «cuoikou' — HgM prtoritot 23.03.73 USA (US) 3UUU66 (71) American Home Products Corporation, 685 Third Avenue, New York, NY 10017, USA (72) John Hamilton Sellstedt, Pottstown, Pennsylvania, Charles John Guinosso,

King of Prussia, Pennsylvania, Albert John Begany, Perkiomenville,

The present invention relates to a process for the preparation of therapeutically useful oxamic acid derivatives, which has the following: Pennsylvania, USA (US) (7 * 0 Oy Kolster Ab (5M Process for the preparation of therapeutically useful oxamic acid derivatives) The present invention relates to a process for the preparation of therapeutically useful oxamic acid derivatives:

ANHC-C-R

wherein R is hydroxy, alkoxy of 1-1 + carbon atoms, cyclohexyloxy or amino, A is 3-pyridyl, 2-pyridyl when R is not ethoxy, 1 + -pyridyl, 2-pyrazinyl or 2-pyrimidinyl, 3-fluorophenyl, l -phenylazophenyl, 1 + -carbamoylphenyl, 2-nitro-1 + -trifluoromethylphenyl, 2-cyano-3-methoxyphenyl, 1 + -nitro-3-trifluoromethylphenyl, 5-chloro-2-sulfamoylphenyl or the group R 2 CONHo R 2 where R is hydrogen, alkoxy of 1-1 + carbon atoms, 2-phenoxyethoxy or chlorine, • 3. . 1ψ R is hydrogen, methoxy, chlorine or nitro, and R is hydrogen or methoxy, provided that ... 2 3-1 + such that one of R, R and R is other than hydrogen.

61 688 2

The compounds prepared by the method of the invention are used to treat allergic diseases in warm-blooded animals.

Atopic immediate sensitivity is the main cause of asthma, hay fever, allergic rhinitis, urticaria, etc. in animals. The substances that most commonly give clinical signs of sensitivity are plant pollen, animal feathers and hair dust, dust, milk and wheat.

Atopic hypersensitivity occurs in humans, dogs, and other animals.

It rarely occurs in lower animals.

The presence of antibodies in host serum associated with atopic reactions is demonstrated by passive sensitization of the skin of a healthy recipient by injecting serum from the sensitized host animal into the skin and then injecting the antigen into the same skin site 2 hours later, resulting in a local skin reaction. This is commonly referred to as the Prausnitz-Kuster reaction (P-K).

An antibody associated with atopic hypersensitivity is characterized by the fact that it does not precipitate with its antigen in all forms, cannot pass through the placenta from mother to fetus, has a special tendency to the skin, often lacks specificity against a single antigen in an individual sensitized to several antigens. it is generally unstable at about 56 ° C after 2 hours of wedging.

A homocytotropic antibody present in or induced in a rat is related in its function and reactions to immunoglobulin E (reagent or IgE) found in humans. The correlation between rat homocytotropic antibody and human IgE has been demonstrated by the general effects of chemical and immunological reactions and the effect of drugs on both hosts of these antibodies. In humans, a reagent is an antibody that causes atopic immediate hypersensitivity reactions. In rats, a homocytotropic antibody is responsible for atopic immediate hypersensitivity reactions.

In theory, the reagent acts on the cell membrane of the mast cell, initiating the reaction or reactions in the mast cell, resulting in the release of a mediator such as bradykinin, SRS-A (slow reactant A), histamine, and other unknowns. The mediator causes a change in the permeability of the surrounding cell wall, allowing a rapid change in the flow or seepage of the mediator or agents from the cell, resulting in symptoms of an allergic seizure. The various methods commonly used to alleviate an allergic seizure, none of which can be considered completely acceptable, are 1) avoidance of antigenic action, 2) inhibition of antibody formation by immunosuppressant, 3) prevention of neurotransmitters during cell seizure by administration of antihistamines, anti-5-hydroxytryptamine (5 -HT) or anti-inflammatory agents or 3 61688 1+) cell stimulation during a seizure to nullify the effect of a neurotransmitter with bronchodilators such as Isoprei® or xanthines.

The only currently known compound that acts as an antiallergic through mast cell blockade reaction or reactions, and thus to inhibit the production and release of mediators, is disodium cromoglycate (intai ^).

Oxamic acid derivatives have previously been used as intermediates in the formation of polymers and as reagents in chemical research.

All of the compounds of the invention have been found to alleviate allergic symptoms when administered intraperitoneally to sensitized rats. Several compounds were found to be effective antiallergic agents in experiments when administered orally to sensitized animals.

The technique used to demonstrate the antiallergic activity of the compounds of the invention is described in Immunology, Vol.

16, pages 7-9-760 (1969), and uses groups of a male Charles River rat (200-25Ο g body weight) as controls, recipients of a standard antiallergic compound (disodium cromoglycate), and recipients of a test compound. Serum from rats immunized with egg albumin and pertussis vaccine was injected intracutaneously into the neck of rats. 2k hours after the first injections, test compounds were administered intraperitoneally or orally at a dose level of 200 mg / kg body weight. 5 minutes later, 1 ml of 0.5-¾ Evans-blue dye solution and 8 mg of albumin were injected intravenously. After 1 + 0 minutes, the animal is killed and the size of the blister on its back is measured. The mean bladder size in animals given the test compound is calculated and the # of prevention is determined by comparison with a control animal. A representative amount of the compounds were tested at a dose of 200 mg / kg of the recipient's body weight to determine the activity of the compounds.

The studies are presented in the following table.

Table

Antiallergic activity of the compounds.

Compound Contraception% Contraception% i.p. 200 mg / kg p.o. 200 mg / kg

Disodium cromoglycate 86

Example 1 82 "2 100" 3 96 81+ "1+ 100 83" 5 77 100 "6 58 77." 7 100 100 "8 100 ____________ continued.

k 616 8 8

Table .continued

Compound Contraception% Contraception%

Example i.p. 200 mg / kg p.o. 200 mg / kg 9 53 10 100 11 78 12 55 13 iti lU 100 91 15 80 71 17 75 18 9 6 19 96 20 57 21 U8 23 58 2 it 59 26 91 27 70 28 100 73 29 91 30 98 31 100 70 32 8θ 33 52 3 it 60 35 75

Thus, the new compounds are effective antiallergic agents even when administered orally. Particularly valuable compounds are lower alkylpyridyloxamates (methyl, ethyl and propyl 2-pyridyloxamates, ethyl-k-pyridyloxamate, ethyl 3-pyridyloxamate), lower alkylpyrazinyloxamates (ethyl-2-pyrazinyloxamate), -carbamoyl 3'-methoxyoxanilate and ethyl 1'-nitro-3 '- (trifluoromethyl) oxanilate.

Although the mechanism by which the compounds prepared by the method of this invention work is not fully known, it has now been found that the compounds block the reaction or reactions leading to the production of the mediator in the feeder cell in a manner presumed to be the same as the disodium cromoglyc. However, disodium cromoglycate is not orally active.

5,61688 The compounds prepared by the method of this invention allow for the occurrence of a non-producing antigen-antibody interaction. They effectively block the IgE-type reaction and have little or no effect on other immunoglobulins such as IgG, IgM, IgA and IgD.

These compounds do not have any pharmacological mode of action of known antiallergics: they do not have antihypertensive activity (no cardiovascular effect, etc.), they do not have analgesic activity, they do not have central nervous system activity, they do not have the activity of histamine, serotonin, serotonin. and have no endocrinological activity.

In summary, the compounds of the present invention block the release of a mediator that usually results from an antigen-antibody reaction, exemplified by a passive skin anaphylaxis (PCA) assay using a rat homocytotropic antibody, a known human reagent-antibody correlate.

Warm-blooded animals whose allergic symptoms can be alleviated by the compounds of the invention include domestic animals such as mouse, rat, hamster, jump rat, dog, cat, sheep, goat, horse, cow, etc. A therapeutically active amount of one or more of the present compounds is used. orally, topically, intraperitoneally, intramucularly or intravenously. Because the compounds do not have a similar or opposite pharmacological pattern to conventional antiallergics, they can be administered in conjunction with known compounds having antihistamine, antihypertensive, analgesic, CNS depressant, immunosuppressive, antiserotonin, antibraquinine or endocrine activity. In addition, known conventional excipients may be included in the antiallergics of this invention to provide compositions and solutions for drug delivery, although it is considered desirable and possible to use as antiallergic and immiscible and pure compounds without additives other than those necessary to provide suitable pharmaceutical solutions or liquids or vapor suspensions.

Experimental animals in the effective dose range have been shown to range from about 1.5 mg / kg to a dose that causes 100-? inhibition of an allergic reaction, and which is 5 mg per kilogram of body weight of the recipient when administered intraperitoneally. Orally, the dose range is from about 1.5 mg / kg to a dose of $ 90 to prevent an allergic reaction, which is 200 mg per kilogram of body weight. As an inhaler, the dose is 1 to 20/20 of the dose corresponding to the dose of Intal®, given as needed before the attack. Thus, a dosage based on the potency of the compounds for humans is from about 100 mg to 1 mg, preferably from about 250 to 750 mg in unit dosage form as needed and to the extent desired to be effective, in one or more doses as prescribed by a physician.

β 616 8 8 The compounds of this invention have not been shown to be toxic to mice, which are standard experimental animals of this type of toxicity study, at doses greater than 2 g / kg body weight. No level of toxicity has been observed in other standard dikoe animals. These new compounds do not appear to have the side effects commonly found with other antiallergics (such as fatigue, dizziness, and depression).

The process according to the invention is characterized in that the amine of the formula ANH4 is coupled to the reactive compound CICOCO2, in which A is as defined above and X is alkyl or cyclohexyl, and that the ester formed is optionally saponified to the corresponding salt, if desired hydrolyzed to the corresponding acid; optionally reacted with ammonia to give the corresponding amide.

Coupling of the amine to an appropriately substituted oxalyl chloride is performed in the presence of an acid scavenger such as pyridine at room temperature.

The course of the reaction is as follows:

ANH2 + C1C-C-0X -6 --—> ANHCOCOgX

The process used in the preparation of each of the separately mentioned compounds is set forth in the following Preparation Examples, either in detail or with reference to the appropriate literature, the latter being incorporated herein by reference. The following examples have the following references: CA (Chemical Abstracts), Zh, Obshch. Khim. (The Journal of General Chemistry - Soviet Union), Rec. Trav. Chim. (Recueil des Travaux Chimique des Pays-Bas - Netherlands), Heilbron (Dictionary of Organic Compounds), Ber. Devrt. Chem. (Berichte der Deutschen Chemischen Gesellschaft), J.

Org. Chem. (Journal of Organic Chem.), J.A.C.S (Jouinai of the American Chem. Society) and Farmaco, Ed. Sci. (Il Farmaco Scientifica Edition - Italy).

Example 1 (2-Pyrimidyl) oxamic acid ethyl ester.

2-Aminopyrimidine (2.85 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in 100 ml of dichloromethane with stirring at 10 ° C for pyridine (1 +, 83 ml, 0.06 mol). moles) to give 2.0 g of the title compound, m.p. 9β ~ 99 ° 0 crystallized from ethanol.

Elemental analysis for C 9 H 8 N 2 O 2:

Calculated: C * + 9.23, H h, 65, N 21.53 Found: C 1 + 9.05, H 1 +, 68, N 21.57.

Example 2 (1 + -pyridyl) oxamic acid ethyl ester.

1 + - Aminopyridine (2.82 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 1.26 g of the title compound, m.p. 100-113 ° C crystallized from diethyl ether.

7 61688

Elemental analysis for C 9 H 8 N 2 O 2:

Calculated: C 55.66, H 5.19, N 11 +, 1 + 3 Found: C 55.88, H 5.15, N 11 +, 61 +.

Example 3 (3-Pyridyl) oxamic acid ethyl ester.

3-Aminopyridine (2.82 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 2.36 g of the title compound, m.p. 98-100 ° C crystallized from diethyl ether. Elemental analysis for C.H.J 0: y 1U d. 3

Calculated: C 55.66, H 5.19, N 11 +, 1 + 3 Found: C 55.1 + 0, H 5.13, N 11 +, 71.

Example 1+ (2-Pyrazinyl) oxamic acid ethyl ester.

Aminopyrazine (2.88 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 3.63 g of the title compound, m.p. 13 * + ~ 137 ° C crystallized from ethanol.

Elemental analysis for the compound: C 9 H 2 N 2 O 2:

Calculated: C 1 + 9.23, H 1 +, 65, N 21.53 Found: C 1 * 8.99, H 1 +, 58, N 21.56.

Example 5 (2-Pyridyl) oxamic acid methyl ester.

2-Aminopyridine (2.82 g, 0.03 mol) is condensed with methyl oxalyl chloride (3.0 L + mL, 0.033 mol) in the same manner as in Example 1 to give 3.18 g of the title compound, m.p. 102-106 ° C after crystallization from diethyl ether.

Elemental analysis for C 9 H 9 N 2 O 2:

Calculated: C 53.33, H 1 +, 1 + 8, N 15.55 Found: C 53.51+, H 1 +, 1 + 7, N 15.76.

Example 6 (2-Pyridyl) oxamic acid n-propyl ester.

2-Aminopyridine (2.82 g, 0.03 mol) is condensed with n-propyloxalyl chloride (1+, 26 ml, 0.033 mol) in the same manner as in Example 1 to give 2.2 g of the title compound m.p. 56-59 ° crystallized from diethyl ether. Elemental analysis for c ^ q ^ 12 ^ 2 ^ 3:

Calculated: C 57.68, H 5.81, N 13.36 Found: C 57.72, H 5.81+, N 13.1 + 8.

8 61688

Example 7 (2-Pyridyl) oxamic acid isopropyl ester.

2-Aminopyridine is condensed with isopropyloxalyl chloride in the same manner as in Example 1 to give the title compound as a liquid. Elemental analysis for C ^ H ^ N ^ O:

Calculated: C 57.68, H 5.81, N 13, U 6 Found: C 57.15, H 6.0 * +, N 13.51.

Example 8 (2-Pyridyl) oxamic acid n-butyl ester.

2-Aminopyridine is condensed with n-butyloxalyl chloride in the same manner as in Example 1 to give the title compound, m.p. 33 ~ 37 ° C. Elemental analysis for C ^ H ^ N ^ O ^:

Calculated: C 59, * + 5, H 6.35, N 12.60 Found: C 59.16, H 6.72, N 12.1 + 5-

Example 9 (2-Pyridyl) oxamic acid cyclohexyl ester.

2-Aminopyridine is condensed with cyclohexyloxalyl chloride in the same manner as in Example 1 to give the title compound, m.p. + 62-61 ° C.

Elemental analysis for C 11 H 14 N 2 O 3

Calculated: C 62.89, H 6.50, N 11.28 Found: C 63.22, H 7.00, N 11.08.

Example 10 (2-Pyridyl) oxamic acid sec-butyl ester.

2-Aminopyridine is condensed with secondary butyloxalyl chloride in the same manner as in Example 1 to give the title compound as a liquid, b.p. 112-116 ° C / 0.05 mmHg.

Elemental analysis for the compound: CH 2 Cl 2:

Calculated: C 59.5, H 6.35, N 12.60 Found: C 59.1 + 8, H 6.62, N 12.6θ.

Example 11 3'-Fluorooxanilic acid ethyl ester.

m-Fluoroaniline (5.55 g, 0.05 mol) is condensed with ethyl oxalyl chloride (6.16 ml, 0.055 mol) in the same manner as in Example 1 to give 9.26 g of the title compound, m.p. 85-89 ° C crystallized from ethanol.

9 61688

Elemental analysis for C 1 H 2 FNO 2:

Calculated: C 57.00, H 4.78, N 6.64 Found: C 56.45, H 4.8 ?, N 6.61.

Example 12 4'-Carbamoyloxanilic acid ethyl ester. .

p-Aminobenzamide (4.08 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 2.85 g of the title compound, m.p. 259-264 ° C (decomposes) crystallized from N, N-dimethylformamide.

Elemental analysis for c- 1H12N2 ^ 4

Calculated: C 55.93, H 5.12, N 11.86 Found: C 56.01, H 5.24, N 11.92.

Example 13 1''-Phenylazo-oxanilic acid ethyl ester.

p-Phenylazoaniline (5.92 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 7.36 g of the title compound, m.p. 157-160 ° C crystallized from ethanol. Elemental analysis for C ^ H ^ N ^ O ^:

Calculated: C 64.63, H 5.09, N 14.14 Found: C 64.61, H 5.13, N 14.04.

Example 14 2'-Carbamoyl-3'-methoxy-oxanilic acid ethyl ester.

6-Amino-o-anisamide (8.75 g, 0.0527 mol) is condensed with ethyl oxalyl chloride (6.2 ml, 0.0554 mol) in the same manner as in Example 1 to give 8.35 g of the title compound, m.p. . 170-173 ° C crystallized from ethanol. Elemental analysis for C

Calculated: C 54.13, H 5.30, N 10.52 Found: C 54.36, H 5.20, N 10.66.

Example 15 2, -Cyano-3'-methoxy-oxanilic acid ethyl ester.

2-Amino-6-methoxybenzonitrile (4.67 g, 0.0315 mol) is condensed with ethyl oxalyl chloride (3.88 ml, 0.0346 mol) in the same manner as in Example 1 to give 5.0 g of the title compound, m.p. . 142-145 ° C, crystallized from toluene.

Elemental analysis for C ^ H ^ N ^ O ^:

Calculated: C 58.06, H 4.87, N 11.29 Found: C 58.21, H 4.93, N 11.02.

, 0 61 688

Example 16 2'-Carbamoyl-3'-chloro-oxanilic acid ethyl ester.

2-Amino-6-chlorobenzamide (4.26 g, 0.025 mol) is condensed with ethyl oxalyl chloride (3.1 ml, 0.0275 mol) in the same manner as in Example 1 to give 5.2% of the title compound, m.p. 190-193 ° C crystallized from ethanol. Elemental analysis for ^ ^ CIN ^ O ^:

Calculated: C U 8.8, H it .10, N 10.35 Found: C 49.08, H it .05, N 10.72.

Example 17 2 "-Carbamoyl-3'-12-phenoxyethoxy) -oxanilic acid ethyl ester 2-Amino-6- (2-phenoxy-ethoxy) -benzamide (2.8 g, 0.0103 mol) is condensed with ethyl oxalyl chloride (1.26 mL, 0.0113 moles) in the same manner as in Precursor 1 to give 1.26 g of the title compound, mp 1U2-1U5 ° C, crystallized from ethanol.

Elemental analysis for C 19 H 20 N 2 O 2 Calculated: C 61.28, H 5.41, N 7.52 Found: C 6.1 H, H 5.57, N 7.50.

Example 18 2'-Carbamoyl-3'-methoxy-oxanilic acid methyl ester.

6-Amino-o-anisamide (4.98 g, 0.03 mol) is condensed with methyl oxalyl chloride (3.04 ml, 0.033 mol) in the same manner as in Example 1 to give 2 g of the title compound, m.p. 195-198 ° C crystallized from methanol. Elemental analysis for Ο ^ Η ^ Ν ^ Ο ^:

Calculated: C 52.38, H 4.80, N 11.11 Found: C 52.30, H M 2 *, H 11.4o.

Example 19 2'-Carbamoyl-3'-methoxyoxanilic acid n-propyl ester. . .

6-Amino-o-anisamide (4.98 g, 0.03 mol) is condensed with n-propyloxalyl chloride (4.25 ml, 0.033 mol) in the same manner as in Example 1 to give U.31 g of the title compound, m.p. . 158-161 ° C crystallized from acetonitrile. Elemental analysis for the compound Calculated: C 55.71, H 5.75, N 10.00 Found: C 55.92, H 5.93, N 10.34.

Example 20 2'-Carbamoyl-3'-methoxyoxanilic acid isopropyl ester.

6-Amino-o-anisamide (4.98 g, 0.03 mol) is condensed with isopropyloxa-11,61683 yl chloride (4.25 ml, 0.033 mol) in the same manner as in Example 1 to give 4.74 g of the title compound, m.p. . 12-132 ° C crystallized from benzene.

Elemental analysis for C

Calculated: C 55.71, H 5.75, N 10.00 Found: C 55.66, H 5.93, N 10.38.

Example 21 2'-Carbamoyl-3'-methoxyoxanilic acid.

2'-Carbamoyl-3'-methoxy-oxanilic acid ethyl ester (1.33 g, 0.005 mol) is mixed with water (50 ml), 5.0 ml of 1N NaOH are slowly added to give a solution. After 1/2 hour, the solution is filtered, the filtrate is acidified to pH 2 with 1N HCl to give 0.71 g of the title compound, m.p. 214-215 ° C crystallized from ethanol.

Elemental analysis for c- | qH10 ^ 5N2:

Calculated: C 50.42, H 4.23, N 11.76 Found: C 50.60, H 4.35, N 11.80.

Example 22 N- (2-carbamoyl-3-methoxyphenyl) oxamide.

2'-Carbamoyl-3'-methoxy-oxanilic acid ethyl ester (5.0 g, 0.0188 mol) is added to 50 ml of ammonia-saturated ethanol at 0-5 ° C, and the mixture is stirred in an ice bath for 2 hours, then filtered. The precipitate is washed with ethanol to give 1.41 g of the title compound, m.p. 252-255 ° C crystallized from water. Elemental analysis for C ^ H ^ N ^ O ^:

Calculated: C 50.63, H 4.67, N 17.72 Found: C 50.1 + 5, H 4.70, N 17.65-Example 23 2'-Carbamoyl-4'-chloro-oxanilic acid ethyl ester.

2-Amino-5-chlorobenzamide (3.41 g, 0.02 mol) is condensed with ethyl oxalyl chloride (2.46 ml, 0.022 mol) in the same manner as in Example 1 to give 4.57 g of the title compound, m.p. 204-210 ° C crystallized from acetonitrile.

Elemental analysis for C ^ H ^ CIN ^ O ^:

Calculated: C 48.8, H 4.10, N 10.35, Cl 13.10 Found: C 48.65, H 3.98, N 10.26, Cl 12.84.

Example 24 2'-Carbamoyl-4'-nitro-oxanilic acid ethyl ester.

2-Amino-5-nitrobenzamide (5.43 g, 0.03 mol) is condensed with ethyl octane-2 61 688 yl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 6.5 ** g. the title compound, m.p. 206-209 ° C crystallized from ethanol.

Elemental analysis for the compound C

Calculated: C 1 + 6.98, H 3.1 + 9, N 11+, 9U

Found: C 1 + 6.68, H 3.96, N 15.12.

Example 25 2'-Nitro-1 '' - (trifluoromethyl; oxanilic acid ethyl ester.

1 + -amino - + »- nitrobenzotrifluoride (3.21 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 7.01 g of the title compound, m.p. 12l + -126 ° C crystallized from ethanol.

Elemental analysis for C ^ H ^ F ^ N ^ O ^:

Calculated: C 1 + 3.1, H 2.96, N 9.16 Found: C 1 + 2.97, H 3.02, N 9.28.

Example 26 2'-Carbamoyl-51-methoxy-oxanilic acid ethyl ester.

2-Amino-p-anisamide (1+, 99 g, 0.03 mol) is condensed with ethyl oxalyl chloride (3.68 ml, 0.033 mol) in the same manner as in Example 1 to give 3.81+ g of the title compound, m.p. . 186-188 ° C crystallized from ethanol.

Elemental analysis for C.0H, ι N_0, _: 12 14 2 5

Calculated: C 5 H 13, H 5.3 L +, N 10.52 Found: C 5 * 1.29, H 5.50, N 10.89.

Example 27 5'-Chloro-2'-sulfamoyloxanilic acid ethyl ester.

2-Amino-1 + -chlorobenzenesulfonamide (1 +, 13 g, 0.02 mol) is condensed with ethyl oxalyl chloride (2.1 + 6 ml, 0.022 mol) in the same manner as in Example 1 to give 3.0 * + g of the title compound, mp. 183-187 ° C crystallized from ethanol.

Elemental analysis for C 18 H 28 ClN 2 O 2 S:

Calculated: C 39.2, H 3.65, N 9.1 U, S 10.1 + 5 Found: C 38.95, H 3.65, N 9.1 * +, S 10.86.

Example 28 1+ '-Nitro-3' - (trifluoromethyl) oxanilic acid ethyl ester.

5-Amino-2-nitrobenzotrifluoride (6.18 g, 0.08 mol) is condensed with ethyl oxalyl chloride (3.7 ml, 0.033 mol) in the same manner as in Example 1 to give 6.07 g of the title compound, m.p. 106-110 ° C crystallized from ethanol.

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Elemental analysis for C ^ H F ^ N ^ O:

Calculated: C 1 + 3.1, H 2.96, N 9.16 Found: C 1 + 3.26, H 2.95, N 9.18.

Example 29 2'-Carbamoyl-3'-methoxyoxanilic acid cyclohexyl ester.

6-Amino-o-anisamide is condensed with cyclohexyloxalyl chloride to give the title compound, m.p. 166-169 ° C.

Elemental analysis for C ^ H ^ N ^ O ^:

Calculated: C 59.99, H 6.29, N 8.75 Found: C 60.17, H 6.33, N 8.69.

Example 30 21-Carbamoyl-S'-methoxyoxanilic acid butyl ester.

6-Amino-o-anisamide is condensed with n-butyloxalyl chloride to give the title compound, m.p. 126-129 ° C.

Elemental analysis for C

Calculated: C 57.13, H 6.17, N 9.52 Found: C 57.1 + 3, H 6.1 + 6, N 9.38.

Example 31 2'-Carbamoyl-3'-methoxyoxanilic acid sec-butyl ester, 6-amino-o-anisamide is condensed with secondary butyloxalyl chloride to give the title compound, m.p. 119-122 ° C.

Elemental analysis for C 18 H 19 N 2 O 2:

Calculated: C 57.13, H 6.17, N 9.52 Found: C 56.91+, H 6.1 + 1 +, n 9.50.

Example 32 2'-Carbamoyl-3'-ethoxy-oxanilic acid ethyl ester.

2-Amino-6-ethoxy-benzoic acid amide is condensed with ethyl oxalyl chloride to give the title compound, m.p. II + II-2 + 5 ° C.

Example 33 2'-Carbamoyl-3'-propoxy-oxanilic acid ethyl ester.

2-Amino-6-propoxy-benzoic acid amide is condensed with ethyl oxalyl chloride to give the title compound, m.p. 130-133 ° C.

Example 31 + 2'-Carbamoyl-3'-isopropoxy-oxanilic acid ethyl ester.

2-Amino-6-isopropoxy-benzoic acid amide is condensed with ethyl oxalyl chloride to give the title compound, m.p. 123 ~ 125 ° C.

Example 35 2'-Carbaraoyl-3'-n-butoxy-oxanilic acid ethyl ester.

2-Amino-6-n-butoxy-benzoic acid amide is condensed with ethyl oxalyl chloride to give the title compound, m.p. 120-123 ° C.

Claims (1)

1h 61683 A process for the preparation of therapeutically useful oxamic acid derivatives of the formula: O ANHC-CR wherein R is hydroxy, alkoxy containing 1-1 + carbon atoms, cyclohexyloxy or amino, A is 3-pyridyl, 2-pyridyl when R does not denote ethoxy, U-pyridyl, 2-pyrazinyl or 2-pyrimidinyl, 3-fluorophenyl, 1 + -phenylazophenyl, 1 + -carbamoylphenyl, 2-nitro-1 + trifluoromethylphenyl, 2-cyano-3-methoxyphenyl, U-nitro-3- trifluoromethylphenyl, 5-chloro-2-sulfamoylphenyl or a group R 2 CONH 2 R 10 O wherein R is hydrogen, alkoxy containing 1-1 + carbon atoms, 2-phenoxyethoxy or chlorine, R 0 is hydrogen, methoxy, chloro or nitro, and R ** is hydrogen or methoxy, provided 2 1-1 +. that one of R, R and R is other than hydrogen, characterized in that the amine of the formula ANH2 is coupled to the reactive compound CICOCO2, in which A is as defined above and X is alkyl or cyclohexyl, and that the ester formed is optionally saponified to the corresponding salt , which is optionally hydrolyzed to the corresponding acid, or optionally reacted with ammonia to give the corresponding amide.