DE2029185A1 - 2-azaquinolizidine derivs and salts neurotropic and anti - -histamine agents synthesis - Google Patents

Abstract

2-Azaquinolizidine derivs. of formula (I): (where X is H, halogen, halomethyl or methoxy; Z is S or -CH=CH- or -CH2-CH2- and n is 1-5, pref. 2 or 3) and their non-toxic acid addn. salts have neurotropic and antihistamine effects and are used as active ingredients in medicinal prepns.

Description

New 2-azaquinolizidine derivatives, their acid addition salts and processes for their production and their use.

Hokuriku Seiyaku Co. Ltd. in Tatekawa, Katsuyama, Japan The present Invention relates to new 2-azaquinolizidine derivatives and their acid addition salts, which have neurotropic and antihistamine effects and as valuable drugs can be used as well as a process for the preparation of these compounds.

The present invention relates to new 2-azaquinolizidine derivatives of the general formula wherein X represents a hydrogen atom, a halogen atom, a halomethyl group or methoxy group, Z represents a sulfur atom or a radical -CH = CH- or -CH2-CH2- and n represents a number from 1 to 5 and their acid addition salts as well as a method for the Preparation of these compounds and the use of these new compounds as active ingredients in pharmaceuticals.

The 2-azaquinolizidine derivatives and their acid addition salts are everything new compounds not previously described in the literature.

These compounds have and are neurotropic and antihistamine effects accordingly usable as valuable medicaments.

The method of this invention is represented by the following equation: wherein X, Z and n have the same meaning as already explained above, and X 'represents a halogen atom.

The process comprises the following three stages: (1) the stage of Reaction of l- (ß-chloroethyl) -2-chloromethylpiperidine of the formula (I) with a hydroxyalkylamine of the general formula (II) to give a 2-hydroxyalkyl-2-azaquinolizidine of the general Formula (III) to form (2) the step of halogenating 2-hydroxyalkyl-2-azaquinolizidine of the general formula (AS) in its hydroxyl group eva a 2-haloalkyl-2-azaquinolizidine of the general formula (1V), and (3) the step of condensing 2-haloalkyl-2-azaquinolizidine with of the general formula (IV) with a phenothiazine derivative or a 5H-dibenzo (b , f) -azepine derivative of the general formula (V) to a 2-azaquinolizidine derivative of the general formula (VI).

In stage (I) is l- (ß-chloroethyl) -2-chloromethyl-piperidine with for example monoethanolamine or 3-aminol-propanol in the presence of a dehydrohalogenating agent such as potassium carbonate, sodium acetate, pyridine or a tertiary amine implemented. The reaction can be carried out without a solvent or in the presence of a solvent, for example in an organic solvent such as acetone, chloroform, benzene, toluene and the like. are executed.

In step (2) the 2- (B-hydroxyethyl) -2-azaquinolizidine obtained is used or using 2- (γ-hydroxypropyl) -2-azaquinol-7-zidine in a conventional manner a halogenating agent such as thionyl chloride and the like. This reaction can also be carried out without use or with the use of solvents Are used as solvents chloroform, dichloromethane or the like. Used can be.

In the step (3) the halogenated compound obtained, e.g. 2-haloalkyl-2-azaquinolizidine with a phenothiazine derivative or 5H-dibenzo (b , f) -azepine derivative of the general formula (V) in an organic solvent such as benzene, toluene, xylene and the like. In the presence of a condensing agent such as sodium amide, sodium hydride, metallic sodium or the like. Condensed.

The condensation reaction is suitably carried out at rrt temperature or carried out at the boiling point of the solvent used.

Compounds of the above general formula (VI) can according to converted to their salts by a conventional process. As suitable acids Inorganic and organic acids can be named for the formation of salts result in pharmaceutically acceptable salts, e.g. such as hydrochloric acid, hydrobromic acid, Phosphoric acid, sulfuric acid, acetic acid, lactic acid, salicylic acid, benzoic acid, Tartaric acid, maleic acid, gallic acid, methane sulfonic acid and the like.

The invention is further illustrated by the following examples: Example 1 2 (γ-Hydro: γpropyl) -2-azaquinolizidine and its hydrochloride 20.8 g of 1- (β-chloroethyl) -2-chloromethylpiperidine and 21.5 g of triethylamine are dissolved in 100 ml of chloroform. To the received Solution becomes a solution of 8.7 g of 3-amino-1-propanol in 60 ml of chloroform dropwise added. The mixture is refluxed for 18 hours and then under reduced pressure Pressure restricted. The residue obtained is washed with an aqueous sodium hydroxide solution adjusted to alkaline and the deposited base is extracted with chloroform. The chloroform extract is dried over anhydrous sodium sulfate and distilled off The chloroform is distilled in vacuo to a basic compound with a boiling point from 125 - 1280C / 2 mm Hg.

The base is dissolved in anhydrous ethanol and acidic with ethanolic Hydrochloric acid adjusted. The deposited crystals are used for filtration separated and recrystallized from anhydrous ethanol, leaving pure crystals with a melting point of 232-2360C.

Analysis for C11H24N20C12 calculated: C%: 48.71; H: 8.93; N%: 10.33 found : Cm: 48.69; H%: 9.07) N%: 10.12 Example 2 2- (B-Hydroxyethyl) -2-azaquinolizidine To the resulting solution, which is obtained by dissolving 12.8 g of l- (8-chloroethyl) -2-chloromethylpiperidine and 13.2 g of triethylamine is obtained in 80 ml of chloroform, one is added dropwise Solution of 4.4 g of monoethanolamine in 40 ml of chloroform was added. The mixture will Refluxed for 18 hours and then in the same manner as in the example 1 described, further treated, whereby 2- (B-hydroxyethyl) -2-azaquinolizidine with a boiling point of 100-103 ° C / 2 mm Hg is obtained.

Example 3 2- (γ-chloropropyl) -2-azaquinolizidine 8 g 2- (γ-hydroxypropyl) -2-azaquinolizidine, obtained according to Example 1, is dissolved in 100 ml of dichloromethane. To the received Solution becomes a solution consisting of 17 g of thionyl chloride in 80 ml of dichloromethane, added drop by drop. The mixture is refluxed for 3 hours and then concentrated under reduced pressure. The residue is dissolved in ice water and Made alkaline with aqueous sodium hydroxide solution. The precipitated base is taken up in ether, the ether extract is dried and the ether is distilled off, It is then redistilled in vacuo, and 2- (ß-chloropropyl) -2-azaquinolizidine is obtained with a boiling point of 129-133 0cm 5 mm Hg. The hydrochloride has a melting point from 235 - 2370C.

Analysis calculated as C11 H23 N2 C13: C%: 45v609 H%: 8.00; N: 9.67 found: C%: 44.89, H: 8.12; N: 9.60 Example 4 2- (B-chloroethyl) -2-azaquinolizidine 4 g 2- (ß-hydroxyethyl) -2-azaehinolizidine, obtained according to Example 2, are dissolved in 50 ml of dichloromethane. To the received Solution becomes a solution of 9 g of thionyl chloride in 40 ml of dichloromethane dropwise added. The mixture is refluxed for 3 hours and then becomes a small amount of water dripping; travel added.

Aqueous sodium hydroxide solution is added dropwise to the batch adjusted to alkaline, and then the base is taken up in dichloromethane. Of the Dichloromethane extract is dried, dichloromethane is distilled off and the residue distilled over in vacuo to give chloroethyl) -2-azaquinolizidine with a boiling point from 99 - 101 ° C / 3 mm Hg.

Example 5 10-E- {2- (2-Azaquinolizidyl)} -propyl3-phenothiazine To 0.6 g of sodium amide is added to a suspension of 2.8 g of phenothiazine in 25 ml of xylene, and the mixture is refluxed for 3 hours. After adding a solution of 3.4 g of 2- (γ-chloropropyl) -2-azaquinolizidine, obtained according to Example 3, in 15 ml of xylene the whole is refluxed for a further 5 hours and then with 1.5N hydrochloric acid extracted. The aqueous layer is washed with ether and with sodium hydroxide adjusted to alkaline. The precipitated base is taken up in Xther. The Xther solution is dried, ether is distilled off and the residue is redistilled in vacuo, around 10- 5- {2- (2-azaquinolizidyl)} - propatg -phenothiazine with a boiling point of 230 - 235 ° / 1.5 mm.

The hydrochloride has a melting point of 195 - 196 ° C.

Analysis calculated as 023 H31 N3S C12: C%: 61.02; H%: 6.85; N%: 9.31 Found: C%: 60.83; H%: 7s12; N%: 9.26 Example 6 10- [β- {2- (2-azaquinolizidyl)} - ethyl-phenothiazine 0.6Li.g of sodium amide becomes a suspension of 2.9 g of phenothiazine in 25 ml of xylene and the mixture is refluxed for 3 hours. Then one will Solution of 3.3 g of 2- (ß-chloroethyl) -2-azaquinolizidine, obtained according to Example 4, in 15 ml of xylene are added dropwise, and the whole thing is continued for 5 hours under Maintained reflux, washed with water and extracted with 1.5N hydrochloric acid. The acidic extract is made alkaline with sodium hydroxide. The so unusual Base is taken up in ether, and the ethereal solution is dried, ether is distilled off and the residue is redistilled in vacuo to give 10 -iss-i2- (2-azaquinolizidyl)) - ethyl4-phenothiazine with a boiling point of 225-227 ° C / 1t3 mrm Hg. The hydrobromide has a melting point of 189 - 191.50C and the picrate a melting point of 236 - 2390C.

Analysis as C22 H27 N3 S * 2 (N ° 2) 3 C6 H2 OH calculated: 0%: 49.57; H%: 4.04; Nu: 15.90 found: 0%: 49.21; H%: 4.15; N%: 15.04 Example 7 10- Fy- (2- (2-azaquinolizidyl) } -propy-2-chlorphenothiaZin 1.35 g of sodium amide become a suspension of 7.3 g of 2-chlorophenothiazine in 60 ml of xylene is added and the mixture is left for 3 hours held under reflux. A solution of 7.5 g of 2- (γ-chloropropyl) -2-azaquinolizidine is then used in 30 ml of xylene, obtained according to Example 3, added dropwise. The whole will continue 5 hours below Maintained reflux and then washed with water and extracted with 1.5N hydrochloric acid. The acidic extract is made with sodium hydroxide adjusted to alkaline, and the precipitated base is taken up in ether.

The ether solution is dried, ether is distilled off and the residue redistilled in vacuo to give 10- [γ-2- (2-azaquinolizidyl)) - propyl -2-chlorophenothiazine with a boiling point of 234-2360 "/ 1.5 mm Hg. The hydrochloride has a melting point of 195-19,700.

Analysis calculated as C23 H30 N3 S C13: 0%: 56.73; H%: 6.21; N%: 8.63 found: 0%: 56.41; H%: 6.50; N%: 8.35 Example 8 10-β- (2- (2-azaquinolizidyl) g -2-chlorophenothiazine 0.44 g of sodium amide are made into a suspension in 30 ml of toluene and 2.38 g of 2-chlorophenothiazine are added, and the mixture is taken for 3 hours Held at reflux. After a solution of 20 ml of toluene and 2.3 g of 2- (βB-chloroethyl) -2-azaquinolizidine, obtained according to Example 4, was added dropwise, the whole is continued for 5 hours refluxed, then washed with water and with 1.5N hydrochloric acid extracted.

The acidic extract is made alkaline with sodium hydroxide solution, and the precipitated base is taken up in ether. The ethereal solution is dried, Ether distilled off and the residue redistilled in vacuo to give 10-5β- {2- (2-azaquinolizidyl)} - ethyi - 2-chlorophenothiazine with a boiling point of 225-2280C / 1.4 mm Hg. The Picrat has one Melting point of 235-236.20C.

Analysis calculated as C22 H26 N3 SCl'2 <NO2) 3 C6 2 OH: C%: 47.58; H%: 3.76; N%: 14.69 Found: C%: 47.43; H%: 3.89; N%: 14.37 example 9 5- (2-azaquinolizidyl)} -ethy-lo, ll-dihydro-5H-dibenzo- (b, f) -azepine and its hydrochloride 0.25 g sodium amide and 1.25 g 10,11-dihydro-5H-dibenzo- (b, f) -azepine become 20 ml of anhydrous xylene is added and the mixture is refluxed for 3 hours.

A solution of 1.3 g of 2- (B-chloroethyl) -2-azaquinolizidine is then added in 10 ml of anhydrous xylene added dropwise, and the whole is another 7 Refluxed for hours. After cooling, it is diluted with 1.5 N hydrochloric acid extracted. The aqueous solution is made alkaline with sodium hydroxide and the base taken up in ether. The ether layer is washed with water and dried and ether distilled off.

The residue is redistilled in vacuo to obtain the end product.

The base obtained in this way is dissolved in anhydrous ether and washed with acidified with an ethereal hydrochloric acid solution. The precipitated crystals are separated by filtration and recrystallized with anhydrous ethanol, whereby pure hydrochloride with a melting point of 204.5-2060C is obtained.

Analysis calculated as C211 H31 N3 2 HC1 N O: C%: 63.71; H%: 7.80; N%: 9.29 Found: CX: 6.97; Ha: 7.87; N%: 8.93 Example 10 5- F-f 2- (2-azaquinolizidyl)) -propyl-10, II-dihydro-5H-dibenzo- (b, f) -azepine and its hydrochloride 0.26 g sodium amide and 1.3 g 10,11-dihydro-5H-dibenzo- (b, f) -azepine are added to 20 ml of anhydrous xylene and the mixture is left for 3 hours held under reflux. Then a solution in 10 ml of anhydrous xylene of 1.45 g of 2- (γ-chloropropyl) -2-azaquinolizidine dropwise added and refluxed for a further 7 hours. Through the same post-treatment, as described in Example 9, the desired base is obtained from the reaction mixture obtain. The base is dissolved in anhydrous ether and washed with ethereal hydrochloric acid acidified. The precipitated crystals are separated off by filtration and Recrystallized from anhydrous ethanol, leaving pure crystals with a melting point of 212-213.80C can be obtained.

Analysis calculated as C25 H33 N32HCl H20: C%: 64.37; H%:?, 99; Nu: 9.01 Found: C%: 64.12; N9: 8.16; N%: 9.07 Example 11 5- Eß-f2- (2-azaquinolizidyl)} -ethyl-5H-dibeno- (b, f> -azepine and its hydrobromide will be 0.59 g sodium amide and 2.9 g 5H-dibenzo- (b'f) -azepine added to 50 ml of anhydrous xylene and the mixture refluxed for 3 hours held. Then a solution in 25 ml of anhydrous xylene of 3 g of 2- (ß-chloroethyl) -2-azaquinolizidine is added dropwise, and the whole thing is continued for 7 hours held under reflux. After the same post-treatment as in the example 9, the base is obtained as the end product. The base is in anhydrous Ether dissolved and acidified with essential hydrobromic acid. The eliminated Crystals are separated by filtration and recrystallized from anhydrous ethanol, whereby pure crystals with a melting point of 221-2230C are obtained.

Analysis calculated as C24 H29 N3 2HBrzH20: C%: 53.45; H%: 6ffi17; Nu: 7.79 found: C%: 5S31; H%: 6.35; N%: 7.80

Claims (6)

Claims 1.) New 2-azaquinolizidine derivatives of the general formula wherein X is a hydrogen atom, halogen atom, a halomethyl group or a methoxy group) Z is a sulfur atom or a radical -CH = CH- or -CH9-CH2- and n is a number from 1 to 5, as well as their pharmaceutically acceptable acid addition salts. 2.) 2-azaquinolizidine derivatives according to claim 1, wherein n is the number 2 or 3 represents. 3.) Process for the preparation of 2-azaquinolizidine derivatives of the general formula wherein X is a hydrogen atom, a halogen atom, a halomethyl group or methoxy group and Z is a sulfur atom or a radical -CH2 = CH- or -CH2-CH- and n is a number from 1-5, characterized in that a compound of general formula where n has the meaning already mentioned and X 'represents a halogen atom, with a phenothiazine or 5H-dibenzo- (b, f) -azepine derivative of the general formula wherein X and Z have the meaning already mentioned, is converted. 4.) The method according to claim 3, characterized in that the compound having the general formula by halogenating a compound having the general formula is obtained, where n represents an integer from 1 to 5. 5.) Process according to claim 4, characterized in that the compound of the general formula by reacting 1- (ß-chloroethyl) -2-chloromethylpiperidine with a hydroxyalkylamine of the general formula NH2 (-CH) ñOH, in which n is an integer from 1 to 5. 6.) Use of the new 2-azaquinolizidine derivatives mentioned in claim 1 and their acid addition salts as an active ingredient for the production of medicaments with neurotropic and antihistamine effects.