FI79314B - PROCEDURE FOR THE PREPARATION OF THERAPEUTIC ANALYTICAL PRODUCTS 2-PHENYL-IMIDAZO / 1,2-A / QUINOLIN-1-ACETAMIDER. - Google Patents

Description

1 79314

The present invention relates to imidazo [1,2-a] quinoline derivatives represented by the general formula (I) represented by the following formula: The present invention relates to the imidazo [1,2-a] quinoline derivatives represented by the general formula (I) and to the preparation of therapeutically useful 2-phenylimidazo in the scheme below, wherein X represents hydrogen, halogen or a methyl, methoxy, thiomethyl or methylsulfonyl group, Y is hydrogen, halogen or a methyl group in the 6-, 7- or 8-position and and R 2 each independently represents hydrogen or methyl - or an ethyl group or R 1 and R 2 together with the nitrogen atom to which they are attached form a pyrrolidyl, piperidyl, 4-methyl-1-piperazinyl, 4-ethoxycarbonyl-1-piperazinyl or morpholino group.

Acid addition salts which may be formed with these compounds and acids are also part of the invention.

The compounds of the invention can be prepared according to the scheme on page 3.

The quinoline of formula III or the 2-aminoquinoline of formula IV is first reacted with a QE-bromoacetophenone having the aforementioned substituent X.

In the case of (III), the reaction is carried out in a hot solvent such as methylene chloride or 1,2-dichloro-ethane. There is thus obtained an ionic compound of formula III which is rendered ring-structured in the presence of ammonium acetate and ferric chloride to give a compound of formula V. In the case of 2-aminoquinoline (IV), the compound of formula V is obtained directly by carrying out the reaction in the presence of a base and in an alcoholic solvent.

The formylation of the compound of formula V thus obtained is then carried out, for example, by means of a reagent obtained by reacting oxalyl chloride with dimethylformamide 35; then this derivative is hydrolyzed.

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The aldehyde (IV) thus obtained is then reduced to the alcohol of formula VII in a manner known per se, for example by reaction with sodium or potassium borohydride.

The alcohol of formula (VII) is then tosylated, for example with paratoluenesulphonyl chloride, preferably pyridine (IV) 3 79314

Chart

n i jTrV-O

Ββ (V) (III) 1 '^ CHn (VI) N ^ ~ mm

/ OH

4 / 'fy \ j = \

0W

In the presence of 8 I (I) N 2 R 2 R 1 R 2 4 79314, and then by reaction of sodium or potassium cyanide in aqueous solution to give the nitrile of formula VIII.

This nitrile is then hydrolyzed to the carboxylic acid in a manner known per se, for example hot and in hydrochloric acid solution, to give a compound of formula IX. Finally, the corresponding amide is prepared by reacting an acid of formula (IX) first with a carbonyldiimidazole, then with an amine of formula R 1 -NH-R 2, wherein R 1 and R 2 are the same as above.

In the case of an unsubstituted amide of formula I (R 1 = R 2 = H), the final compound can be prepared directly by partial hydrolysis of the nitrile of formula (VIII) in basic aqueous solution.

Finally, it is self-evident that N, N-dimethylated amides can be prepared by methylation of an unsubstituted amide (Ti = R 2 = H) with iodomethane in the presence of sodium hydride.

The compounds of the invention have been subjected to pharmacological experiments which prove their importance as substances having a therapeutic effect.

Antagonism of cardiazol-induced convulsive seizures in mice.

The experiment has been inspired by experiments described by Goodman and colleagues J.Parm.Exp.Ther., 108, 168-176. Mice are administered test compounds or vehicle alone intraperitoneally 30 minutes before an intravenous injection of 36 mg / kg Cardiazo®. The animals are then observed for one hour and the percentage of mice with jerky seizures (100% jerky seizures and 10-20% continuous seizures in control animals) is calculated for each batch.

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For each dose, the percentage of seizure protection relative to control animals is calculated to determine graphically the dose that protects 50% of the animals from the anticonvulsant effects of Cardiazolin®. The DA values of the compounds of the invention are 0.1-30 mg / kg intraperitoneally and 0.1-30 mg / kg orally. "Burying test" This experiment has been given the subject of the method described by Pinel J.P.J., Treit D., Ladak F., and 10 MacLennan A.J. in Animal learning and behavior, 8, 447.451, (1980).

The presence of foreign objects in the animal's normal environment causes an unpleasant situation to which the animal reacts by hiding the aggressive object 15 (glass balls) in the sawdust of its cage.

Anxiolytics reduce anxiety caused by a foreign situation: Animals hide less. The number of non-hidden glass beads is then calculated.

Test compounds are administered to male CD1 (Charles River) -20 male mice 30 minutes (intraperitoneally) or 60 minutes (orally) before being placed in cages with 25 glass beads. After 30 minutes: count the number of un hidden glass spheres. Calculate the percentage of processed and - * ’! 25 between control animals.

; ; This determines a DA, -0, 50% effective dose, which is the dose of compound (mg / kg) that halves the number of glass beads hidden compared to control animals. The DA 2 -q of the compounds of the invention is 0.1-30 mg / kg intraperitoneally.

Drinking conflict test in a rat.

This experiment has been described by Vogel J.R., Beer, B and Clody, D.E. in Psychopharmacologia, 21, 1-7, (1971). Male Wistar rats (IFFA 35 Credo) are used. Their drinking water is removed 24 hours before the experiment.

On the day of the experiment, 30 minutes after the animals have received the compound of the invention intraperitoneally, each rat is placed in a cage made of transparent plastic (24 x 20 x 21 cm) with an electric grate on the floor. Drinking water is dispensed using a pipette 2 cm from the wall of the cage and placed 3 cm from the floor of the cage.

After 10-90 seconds of examination, the animal finds a pipette and begins to drink. After the animal has skinned 20 times with its tongue (registered with an IMNITECH anisometer), it receives a 0.07 mA electric shock to the tongue (via an anxiometer), which ends 10 when the rat leaves the pipette. The 3-minute period begins after the first blow and the animal receives a continuous electric shock after every 20 tongue blows until it stops or until the period ends.

Under these conditions, control animals receive an average of 3 to 6 shocks. The number of electric shocks received by treated rats is recorded and compared to the shocks received by control animals using the Dunett experiment.

This determines the DEM, the lowest effective dose, which is the first dose to obtain a significant increase in the number of shocks received by the animals 20 compared to controls. The DEM is 3-100 mg / kg intraperitoneally.

Effect on the electrocorticogram in a curare-treated, artificially inhaled rat: The sedative or hypnotic effect of the compounds has been determined by observing their effect on the rat electrocorticogram by the method described by H. Depoorter, Rev. ELECTROENCEPHALOGRAM. Neurophysiol, 10, 3.207-214 (1980) and by the method described by H. Deporteren and M. Decobert, J. Pharmacol. (Paris), 14. 2, 195-265 (1983).

30 Test compounds are administered intraperitoneally in increasing doses of 1-30 mg / kg.

They cause sleep symptoms from doses of 3-30 mg / kg.

Effect on “sleep” duration induced by 4-35 hydroxysodium butyrate.

This effect has been determined by the effect of the compound on the "sleep" duration induced in 4-hydroxy-sodium butyrar (GBH) curare-treated rats.

v 79314 The animals used are moth rat rats of the Charles River strain weighing 200 + 2 g. Animals treated with alloferin 1 mg / kg intraperitoneally are given artificial respiration with a mask placed on the muzzle (ventilator speed = 50 / min; respiratory volume 14 ml). The esophagus is previously closed to prevent air from entering the stomach.

Cortical electrodes placed in the forehead and occiput are used to record an electrocorticographic effect on a Polygraph Grass Model 79 P at a speed of 6 mm / sec.

Preparation of the animal is performed under local anesthesia (xylocaine 2%). The rats are kept at a constant temperature (37.5 ° C) throughout the experiment. 10 minutes 15 after the preparation of the rat, a dose of 200 mg / kg of 4-hydroxysodium butyrate is injected intravenously at the tail.

The test compound is administered at a dose of 10 mg / kg intraperitoneally 3 minutes after administration of 4-hydroxysodium 20-butyrate. Symptom evaluation is performed in 15-minute increments for 75 minutes after GHB injection. During this analysis period, the total duration of "sleep" is determined. A series of 15 controls is used to determine the duration of "GHB sleep."

25 Statistical analysis of the results is performed

Using the Mann-Whitney U-test.

Certain compounds reduce the effects of GHB (up to 24% reduction in sleep duration at 10 mg / kg), while others potentiate these effects by 30 (up to 18% increase at 10 mg / kg or 30% at 30 mg / kg). It is also noted that the effects may be opposite depending on whether the compounds are administered in high or low doses.

. ·· *. The results of these various tests show that the compounds of the invention have anxiolytic, sleep-inducing, hypnotic and anticonvulsant effects; The compounds of the invention are useful in the treatment of pain, sleep disorders and other neurological and psychiatric disorders, in the treatment of insomnia, in particular in the treatment of behavioral disorders due to cerebrovascular injury and cerebral calcification in the elderly, and in the treatment of memory disorders. .

The compounds of the invention may be in any form suitable for oral or parenteral administration, for example as tablets, coated pills, capsules, drinkable or injectable solutions mixed with suitable excipients.

The daily dose may be 1-100 mg.

Therapeutic Comparative Experiments The anti-jerking effect of the new compounds on Cardiazol® in mice (ACS test) was compared with that of known compounds and the sedative effect of the new compounds by monitoring the rat electrocorticogram (ECOG test) was compared with that of known compounds. Both experiments are described above.

Compounds 1, 2 and 5 known from FI patent 71,143 were used as reference compounds. In addition, an imidazo [1,2-a] pyridine derivative having a fused benzene ring in position 7-8 and imidazo [1,2-a] pyridine derivative was synthesized. the isoquinoline isomer is not disclosed in the present specification. The chemical structure of this isomer can be derived from known compounds in the same manner as the compounds of the invention.

30 The results of the experiments are shown in the following table.

9 79314 nr1r2 \ NR1R2

Compound of the invention Known compound [Oi> Synthetic-N (CH 2) -isomer of the compound of the invention: · 0Αςη Dose ,,. Mg / kg mg / kg ι.ρ.

vuj · „. Base _ mouse rat

Compound,. NR-R0 _ or 1 2 ACS-ECoG- __salt___test__test _test _

New 2 00 0.15 10 - 30

Comparison 1 00__NHCH3__2 .__ 1_

New 3 00 _N (CH, 1 30

Comparison 2 15 J z 0.7 10 _____1: New 6 15 nu 1 10 - 30 -N N-CH.,

Comparison 5 00 \ _ / 0 11 10

Isomer 15 -NiCH 2> 30> 30 1-1- * - 10 7931 4

The results show that both the new and known compounds are potent anticonvulsants, with a magnitude of one mg / kg in the DA5q ACS test (with the exception of reference compound 5, which is less active). From this single experiment, it could be assumed that the properties of the new compounds are obvious.

In contrast, looking at the results of the ECoG test, it is observed that known compounds cause experimental animals to sleep at low doses (1 to 10 mg / kg), while new compounds require a higher dose (10 to 30 mg / kg).

The differences are even more pronounced if the results are considered compound by compound, i.e., each known compound is compared to its new homologue. In addition to the axiolytic effect, the former have a sedative effect, even a hyp-15 effect, while the latter have no sedative effect. This is such a significant difference in activity that the two groups of compounds can be considered to have different effect profiles. Thus, the known compounds are anxiolytics which have the side-effect of sleep-20, or they are hypnotic substances which also have anxiolytic effect.

In contrast, the new compounds are anxiolytics with little or no sedative effect.

The isomeric compound is the structural isomer of the new compound B. This compound was synthesized to prove that it is not sufficient to attach a benzene group to the heterocyclic ring of a known compound to obtain a compound having the same properties as the compound to which the benzene group is attached.

Examples A and B below illustrate two other four for the preparation of compounds of formula V. The following examples illustrate the preparation of some of the compounds of the invention.

Microanalyses and IR-NMR spectra confirm their structure.

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Example A

2- (4-chloro) phenyl-imidazo / 1,2-a7kinoliini. 17.7 g (0.123 mol) of 2-aminoquinoline, 28.7 g (1 equivalent) of Φ-bromo-p-chloroacetophenone and 20.6 g (2 equivalents) of sodium carbonate are mixed with 180 ml of n-propanol and heated under reflux 20 hours.

The precipitate obtained is filtered off, washed with ethanol, water and dried. This gives a white solid which is recrystallized from nitromethane.

Sp. 206-208 ° C.

Example B

2- (4-chloro) phenyl-imidazo / 1,2-a / quinoline. 23.3 g (0.1 mol) of N-bromo-p-chloro-15-acetophenone and 13 ml (1.1 equivalents) of quinoline are mixed with 100 ml of methylene chloride. Heat under a condenser for 1 hour, then add 100 ml of ether to the reaction mixture and cool. The resulting yellow precipitate is filtered off and dried.

In a 20 L autoclave, 38.3 g (0.105 moles) of the quaternary ammonium obtained above, 48.6 g (0.63 moles) of ammonium acetate are stirred; 55 g (0.34 mol) of ferric chloride in 270 ml of acetic acid and the mixture are heated at 140 ° C for 13 hours. The resulting solid is filtered, washed with acetic acid, then water; the precipitate is dried, recrystallized from ethanol and then from nitromethane.

Example 1 2- (4-Chloro) phenylimidazo [1,2-a] quinoline-1-30 acetamide a) -2- (4-chloro) phenylimidazo [1,2-a] quinoline-1-carboxaldehyde.

Cool to 150 ml of anhydrous dimethylformamide at -20 ° C and add dropwise 17.4 ml (0.2 mol) of oxalyl chloride. 13.6 g (0.05 mol) of the compound obtained according to Example A or B are then added and the mixture is stirred for 15 hours at room temperature and for 15 hours at 55 ° C.

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The mixture is then poured into 1 liter of water, the precipitate is filtered off and basified, washed with water until the pH is neutral and dried. It is recrystallized from nitromethane.

5 Sp. 199-200 ° C.

b) 1-Hydroxymethyl-2- (4-chloro) phenylimidazo [1H] quinoline.

The aldehyde obtained above is suspended in 13.3 g (0.043 mol) of 300 ml of dry absolute ethanol.

To this is added 825 mg (0.5 equivalents) of sodium borohydride and stirred for 18 hours at room temperature. It is then evaporated to dryness, the residue is dissolved in water, the pH is adjusted to 8 with dilute hydrochloric acid, filtered, the precipitate is washed with water, acetone, then with ether and dried.

Sp. 236-237 ° C (decomposition temperature).

E-1-cyanomethyl-2- (4-chloro) phenylimidazo [1,2-a] quinoline.

7.8 g (0.025 mol) of the above alcohol and 5.3 g (1.1 equivalents) of p-toluenesulfonyl chloride are mixed with 100 ml of pyridine. The reaction mixture is heated at 40 ° C for 8 hours, then stirred for 60 hours at room temperature. The residue is then dissolved in 700 ml of water and 300 ml of methylene chloride, the precipitate between the two phases is filtered and the mixture is poured into 400 ml of water containing 3.7 g (0.075 mol) of sodium cyanide and 2.1 g. (0.025 mol) sodium bicarbonate. The mixture is refluxed for 15 hours, then cooled and filtered. The precipitate is washed with water, extracted with methylene chloride and the extract is dried over sodium sulfate. The nitrile is purified by chromatography on silica gel. After crystallization from ether and filtration, a white solid is obtained, m.p. 221-223 ° C.

13 7931 4 d) 2- (4-Chlorophenyl) imidazo [2,2-a] quinolirt-1-acetamide 7 g (0.022 mol) of the nitrile obtained above and 6 g (5 eq.) Of potassium hydroxide in 200 ml of ethanol and 50 ml of 5 water is mixed together and boiled at reflux for 3 hours. The mixture is then evaporated to dryness, the residue is taken up in water, filtered, washed with water until neutral and dried; mp. 298-300 ° C.

Example 2 2- (4-Chloro-phenyl) -N-methyl-imidazo [1,2-a] quinoline-1-acetamide a) 2- (4-chloro-phenyl) -imidazo [1,2-a] quinolin-1- acetic acid 3.5 g (0.011 mol) of the nitrile-15 obtained in Example 1 c) are poured into a mixture of 1 ml of concentrated hydrochloric acid and 20 ml of acetic acid. The reaction mixture is refluxed for 8 hours, then a further 10 ml of concentrated hydrochloric acid are added and the mixture is refluxed for 8 hours. The reaction mixture is evaporated to dryness, the residue is taken up in water and the precipitate is filtered off. The precipitate is suspended in water, the pH is adjusted to 5 with dilute sodium hydroxide, the suspension is filtered, washed with ethanol, acetone and ether and dried; mp. 246-248 ° C (decomposes).

b) 2- (4-Chloro) phenyl-N-methylimidazo-25 [1,2-a] quinoline-1-acetamide.

Suspend 2.5 g (0.0074 mol) of the above acid in 50 ml of dry tetrahydrofuran, add 1 to 4 g (1.2 equivalents) of carbonyldiimidazole and heat the mixture at about 40 ° C for 2 hours.

Methylamine is then bubbled for 30 minutes and stirring is continued for 15 hours.

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The mixture is evaporated to dryness, the residue is dissolved in water and methylene chloride, the organic phase is separated and washed with water, dried and evaporated.

The residue is purified by chromatography and allowed to crystallize from ether.

Mp 289-293 ° C (decomposition temperature).

Example 3 2- (4-Chloro) phenyl-N, N-dimethylimidazo [1,2-a] quinoline-1-acetamide.

To a suspension of 3.35 g (0.01 mol) of the compound obtained in Example Id) in 200 ml of tetrahydrofuran is added 1.05 g (0.022 mol) of 50% sodium hydride in oil, 0.1 ml of dimethylformamide, then rapidly 1.9 ml (3 equivalents) of iodomethane.

After stirring for 15 hours under argon at room temperature, the mixture is then evaporated to dryness, the residue is dissolved in water and methylene chloride, the organic phase is washed with water, dried and evaporated. The residue is purified by chromatography.

20 Sp. 190 to 191.5 ° C.

Example 4: 2- (4-Chloro) phenyl-N, N-tetramethyleneimidazo [1,2-a] quinolin-1.

2.5 g (0.0074 mol) of the acid prepared according to Example 2a) are suspended in 50 ml of dry tetrahydrofuran, 1.4 g (1.2 equivalents) of carbonyldiimidazole are added and the mixture is heated to about 40 ° C. at 2 hours.

0.63 g (1.2 equivalents) of pyrrolidine is then added and stirring is continued at room temperature for 15 hours. The mixture is evaporated to dryness, the residue is dissolved in water and methylene chloride, the organic phase is separated and washed with water, dried and evaporated. The residue is chromatographed and allowed to crystallize from ether.

Sp. 217-218 ° C.

The tables below describe the structures and properties of the compounds of the invention.

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Table 4

5 "VVQ

8 (1) βΓ "ν - κζ

Compound YX R1 R2 Base / Sp (° C) salt (1) 1 (Example 1) H 4 -Cl HH 00 298-300 2 (Example 2) H. · 4-C1 H CH 3 00 289-292 3 ( Ex.3) H 4 -Cl CH 3 CH 3 00 190-191.5 4 (Ex. 4) H 4 -Cl - (CH 2 - 00 217 ^ -218 5 (Ex. 5) H 4 -Cl - (CH 2) 5- 00 163-164 6 (Ex.6) H 4 -Cl - (CH 2) 2 -N- (CH 2) 2 - 15 162-165 CH 3 7 (Ex.7) H 4 -Cl - (CH 2) 2-N- (CH2) 2-00 188-190 C00C2H5 8 (Ex.8) H4 "cl - (CH2) 2-0- (CH2) 2-00 228-232 9 (Ex.9) ^ 4- C1 H ^ 2 ^ 5 268-270: 0 0 = free base 15 = methanesulfonate ie 7931 4

Table (continued)

Compound YX R1 R2 Bnäs / Sp (° C) salt (*) 10 8-C1 4-C1 H CH3 00 290.5-291 11 8-C1 4-C1 CH3 CH3 00 259-260 12 7-C1 4-C1 H CH3 00 300-302 15 7-C1 4-C1 CH3 CH3 00 248-250 14 6-C1 4-C1 H CH3 00 306-307 15 6-Cl 4-C1 CH3 CH3 00 243-249 16 7-F 4 -C1 H CH3 00 304-305 17 7-CH3 4-C1 H CH3 00 269-271 18 H 4-CH3 H CH3 00 265-266 19 H 4-CH3 CH3 CH3 00 181-182.5 20 H 4 -CHCH3 H CH3 00 264-265 21 H 4-0CH3 CH3 CH3 00 194-196 22 H 4-SCH3 M CH3 00 284-287 23 H 4-SCH3 CH3 CH3 00 172-173 24 H 3-Cl H CH3 00 261-262 {* ): 00 = free base i7 7931 4

Table (continued)

Compound 'YX R1 R2 Base / Mp (° C) suQla ______n__ 25 H 3 -Cl CH 2 CH 3 00 138-140 26 H 2 -Cl H CH 3 00 222-224 27 H 2 -Cl CH 3 CH 3 00 165-167 28 HHH CH3 00 264-266 29 HHCH, CH00 173-175 30 H 4-502CH3'H CH3 00 2 ^ 9-280 31 H 4 -SO2CH3 CH3 CH300 244-245 (*): 00 =: \. u u - free base

Claims (4)

A process for the preparation of therapeutically useful 2-phenylimidazol-2, 2-α7-quinoline-1-acetamides of the formula (I) X6-Q, io Y_Π Y λ ^ (I) Xr2 wherein X is a hydrogen or halogen atom or a methyl, methoxy, methylthio or methylsulfonyl group, Y is a hydrogen or halogen atom or a methyl group in position 6, 7 or 8, and R 1 and R 2 independently represent a hydrogen atom or a methyl or ethyl group, and and R 2 together form a nitrogen atom thereof, to which they are attached, for the preparation of pyrrolidyl, piperidyl, 4-methyl-1-piperazinyl, 4-ethoxycarbonyl-1-piperazinyl or morpholino groups, and their pharmacologically acceptable acid addition salts, characterized in that a) quinoline of formula (II) aj di) wherein Y is as defined above is reacted with f 1 -bromoacetophenone of formula (X) [Y * V-CO-CH 2 Br 35 X-fr I (X) 19 7931 4 wherein X is as defined above, to give an ionic compound of formula (III) Y {! -) - x am 10 which compound is cyclized by heating in the presence of ammonium acetate and ferric chloride, or b) 2-aminoquinoline of formula (IV) γ OCX N xnh2 wherein Y is as defined above is reacted with 0 (-) of formula (X) with bromoacetophenone to give a compound of formula (V) 25. A compound which is formylated to give an aldehyde of formula (VI) which is reduced to give an alcohol of formula (VII) ^ (VII) ) HO 10 which alcohol is converted into a nitrile of formula (VIII) 15 V (VIII) ϊ-ίΤ Λ x NC 20 which nitrile is hydrolysed to give an acid of formula (IX); »OH 30 which acid is reacted with an amine which the formula is R 1 -NH-I 1 in which and R 2 have the same meaning as above, and that the compound of formula (I) thus obtained is, if desired, converted into a pharmacologically acceptable acid addition salt 21 7931 4 For the preparation of therapeutically active 2-phenylimidazo E, 2-α7-quinoline-1-acetamide with 5 forms of (I) and 15 * 2 color X is a substance or a halogen atom or a methyl, methoxy, methylthio or methylsulfonyl group, Y is a compound -20 or a halogen atom or en methyl group 6-, 7- or 8-membered and R2 is used in the form of an enantiomer or methyl or ethyl or R 2 and R 2 may be added with the same substituents as pyrrolidyl, piperidyl, 4-methyl-1-piperazinyl, 4-ethoxycarbonyl-1-piperazinyl or morpholino. , as the case may be, pharmacologically active compound, in which case the quinoline with the formulation -CO color Y is anhydrous formulation, with the addition of Δ-bromoacetophenone with the formulation (X) 22 7931 4 r ^^ | -CO-CH2Br (X) 5 color X is an anhydrous process, for which a mixture of the ammonium acetate and ferric chloride is used in the form of (III) 10. l) y— —x (iii) 15 en 2-aminoquinoline with formula (IV) 20 Y Γ jJ / 1 (IV) n ^ nh2 color Y is an anhydrous compound, the same as ol-Bromo-25 acetophenone with formula (X), for a mixture of the formulation (V) --CX 35 for the preparation of aldehydes with the formula (VI) 23 79314 * ί ^ CH0 for the reduction of aldehydes or alcohol in the form of alcohol (VIII) 25 Y / wk nitrile hydrolysers for the Netherlands to give 30 formulas (IX) OH ^ (IX)