LT3231B - Methylpiperazinoazepine derivatives, preparation and use tereof - Google Patents

Methylpiperazinoazepine derivatives, preparation and use tereof Download PDF

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LT3231B
LT3231B LTIP378A LTIP378A LT3231B LT 3231 B LT3231 B LT 3231B LT IP378 A LTIP378 A LT IP378A LT IP378 A LTIP378 A LT IP378A LT 3231 B LT3231 B LT 3231B
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methylpiperazin
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diazepine
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Jean-Francois Fernand Liegeois
Jacques Elie Delarge
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Therabel Research Sa
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Abstract

Methylpiperazinoazepine derivatives of general formula (I), wherein X, R1, R2, N1 and N2 have various meanings, pharmaceutically acceptable salts thereof, and their preparation and use, are described.

Description

Išradimas susijęs su naujais metilpiperazinazepino dariniais ir jų netoksinėmis druskomis, taip pat su šių naujų junginių sinteze ir jų terapiniu panaudojimu.The present invention relates to novel methylpiperazinazepine derivatives and their non-toxic salts, as well as to the synthesis and therapeutic use of these novel compounds.

Nauji metilpiperazinazepino dariniai atvaizduoti bendra I formule:The novel methylpiperazinazepine derivatives are represented by the general formula I:

kuriojein which

X reiškia deguonies atomą, atomą sieros atomą, seleno arba NH arba NR3 grupę, kurioje R3 yra “G^ grupė, arba šakota arba nešakota nuo 1 anglies atomų alkilo grupė;X represents an oxygen atom, a sulfur atom, a selenium or a group NH or NR 3 wherein R 3 is a "G 6 " group or a branched or unbranched alkyl group of 1 carbon atom;

iki 4up to 4

Rx reiškia vandenilio atomą, halogeno atomą arba šakotą arba nešakotą nuo 1 iki 4 anglies atomų alkilo grupę;R x represents a hydrogen atom, a halogen atom or a branched or unbranched alkyl group of 1 to 4 carbon atoms;

Nx reiškia benzeno žiedą ir N2 piridino žiedą arba atvirkščiai, su sąlyga, kad tai Rx ir R2 yraN x represents a benzene ring and N 2 a pyridine ring, or vice versa, provided that R x and R 2 are

R2 reiškia vandenilio atomą, halogeno atomą arba šakotą arba nešakotą nuo 1 iki 4 anglies atomų alkilo grupę; ir vandenilis, o X yra siera, deguonis arba NHgrupė, Nx yra piridinas ir N2 benzenas, o piridino azoto atomas nėra padėtyje d', ir abu, Nx ir N2 gali būti benzenas, kai X yra seleno atomas.R 2 represents a hydrogen atom, a halogen atom or a branched or unbranched alkyl group of 1 to 4 carbon atoms; and hydrogen while X is sulfur, oxygen or NH, N x is pyridine and N 2 benzene, and the pyridine nitrogen atom is not in position d ', and both, N x and N 2 may be benzene when X is a selenium atom.

Kai kurie metilpiperazinazepino dariniai jau buvo paskelbti literatūroje (žr. Dupont ir kt., Actą cryst., C43, 716-718 (1987) deguonies dariniams; Hoffmann ir kt., U.S. Patentas Nr. 4163785 (1979) sieros junginiui; Chakrabarti ir kt., Journal of Medicinai Chemistry, t. 32, Nr. 10, 2375-2381 (1989) azoto dariniui). Tačiau priešingai šio išradimo dariniams, iki šiol paskelbti metilpiperazino azepinai nerodo įdomaus farmakologinio aktyvumo.Some derivatives of methylpiperazinazepine have already been reported in the literature (see Dupont et al., Act. Crystal., C43, 716-718 (1987) for oxygen derivatives; Hoffmann et al., U.S. Patent No. 4,363,785 (1979) for a sulfur compound; Chakrabarti et al. ., Journal of Medicinal Chemistry, Vol. 32, No. 10, 2375-2381 (1989) for a nitrogen derivative). However, in contrast to the derivatives of the present invention, the methylpiperazine azepines disclosed so far do not show interesting pharmacological activity.

Kaip jau buvo pažymėta aukščiau, metilpiperazinazepino dariniai šiame išradime yra atvaizduoti bendra I formule. Šakota arba nešakota alkilo grupė nuo 1 iki 4 anglies atomų yra suprantama anksčiau pateiktoje bendroje formulėje, kaip metilo, etilo, n-propilo, izopropilo, n-butilo, izobutilo ir tret-butilo grupės. Terminas halogenas reiškia chlorą, fluorą, jodą arba bromą.As noted above, the methylpiperazinazepine derivatives of the present invention are represented by the general Formula I. A branched or unbranched alkyl group of 1 to 4 carbon atoms is understood in the above general formula as methyl, ethyl, n-propyl, isopropyl, n-butyl, isobutyl and tert-butyl. The term halogen means chlorine, fluorine, iodine or bromine.

Reikšmingiausios junginių su bendra I formule klasės yra būtent klasė, kai R4 yra vandenilio atomas, chloro atomas, fluoro atomas arba metilo grupė, ir klasė, kur R2 yra vandenilio atomas arba chloro atomas. Ypač reikšminga šių junginių klasė yra ta, kur Rx yra vandenilis, chloras, fluoras arba metilas ir tuo pačiu metu R2 yra vandenilis arba chloras.The most significant classes of compounds of general formula I are, in particular, the class wherein R 4 is hydrogen, chlorine, fluorine or methyl, and the class wherein R 2 is hydrogen or chlorine. A particularly important class of these compounds is where R x is hydrogen, chlorine, fluorine or methyl and at the same time R 2 is hydrogen or chlorine.

I formulės dariniai, kurie gali būti netoksinių druskų pavidale, yra būtent neorganinių rūgščių druskos, tokios kaip hidrochloridai, hidrobromidai, fosfatai, sulfatai arba organinių rūgščių druskos, tokios kaip acetatai, citratai, maleatai, fumaratai ir metilsulfonatai.The derivatives of formula I which may be in the form of non-toxic salts are in particular salts of inorganic acids such as hydrochlorides, hydrobromides, phosphates, sulfates or salts of organic acids such as acetates, citrates, maleates, fumarates and methyl sulfonates.

Darinių pagal šį išradimą pavyzdžiai yra:Examples of derivatives of the present invention are:

11-(4-metilpiperazin-l-il)-5H-pirido(4,3-b)benzo1,5-diazepinas;11- (4-methylpiperazin-1-yl) -5H-pyrido (4,3-b) benzo-1,5-diazepine;

6-(4-metilpiperazin-l-il)pirido(2,3-b)benzo-1,4tiazepinas;6- (4-methylpiperazin-1-yl) pyrido (2,3-b) benzo-1,4-thiazepine;

8-chloro-6-(4-metilpiperazin-l-il)pirido(2,3b)benzo-1,4-tiazepino fumaratas;8-Chloro-6- (4-methylpiperazin-1-yl) pyrido (2,3b) benzo-1,4-thiazepine fumarate;

5-(4-metilpiperazin-l-il)pirido(2,3-b)benzo-1,5oksazepino maleatas;5- (4-methylpiperazin-1-yl) pyrido (2,3-b) benzo-1,5-oxazepine maleate;

8-chloro-5-(4-metilpiperazin-l-il)pirido(2,3b)benzo-l,5-oksazepino fumaratas;8-chloro-5- (4-methylpiperazin-1-yl) pyrido (2,3b) benzo-1,5-oxazepine fumarate;

5- (4-metilpiperazin-l-il)-8-metilpirido(2,3b)benzo-1,5-oksazepino fumaratas;5- (4-methylpiperazin-1-yl) -8-methylpyrido (2,3b) benzo-1,5-oxazepine fumarate;

6- (4-metilpiperazin-l-il)pirido(2,3-b)benzo-l,4oksazepino fumaratas;6- (4-methylpiperazin-1-yl) pyrido (2,3-b) benzo-1,4-oxazepine fumarate;

8-chloro-6-(4-metilpiperazin-l-il)pirido(2,3b)benzo-l,4-oksazepino fumaratas;8-chloro-6- (4-methylpiperazin-1-yl) pyrido (2,3b) benzo-1,4-oxazepine fumarate;

6- (4-metilpiperazin-l-il) -HH-pirido (2, 3-b) benzo1,4-diazepinas;6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3-b) benzo [1,4-diazepine];

8-chloro-6-(4-metilpiperazin-l-il)-HH-pirido(2,3b)benzo-1,4-diazepinas;8-chloro-6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3b) benzo-1,4-diazepine;

6-(4-metilpiperazin-l-il)-8-metil-llH-pirido(2,3b)benzo-1,4-diazepinas;6- (4-methylpiperazin-1-yl) -8-methyl-11H-pyrido (2,3b) benzo-1,4-diazepine;

9- chloro-6- (4-metilpiperazin-l-il) -HH-pirido (2,3b)benzo-1,4-diazepinas;9-chloro-6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3b) benzo-1,4-diazepine;

8-fluoro-6- (4-metilpiperazin-l-il) -HH-pirido (2,3b)benzo-l,4 diazepinas;8-fluoro-6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3b) benzo-1,4 diazepine;

5-formil-ll-(4-metilpiperazin-l-il)-5H-pirido(4,3b)benzo-1,5 diazepinas;5-formyl-11- (4-methylpiperazin-1-yl) -5H-pyrido (4,3b) benzo-1,5 diazepine;

ll-formil-5-(4-metilpiperazin-l-il)-HH-pirido (2,3-b)benzo-1,5 diazepinas;11-formyl-5- (4-methylpiperazin-1-yl) -H-pyrido (2,3-b) benzo-1,5 diazepine;

11-trifluorometilkarbonil-5-(4-metilpiperazin-lil) -HH-pirido (2,3-b) benzo-1,5-diazepinas ;11-trifluoromethylcarbonyl-5- (4-methylpiperazin-1-yl) -HH-pyrido (2,3-b) benzo-1,5-diazepine;

ll-formil-6- (4-metilpiperazin-l-il) -HH-pirido (2,3-b)benzo-l,4-diazepinas;11-formyl-6- (4-methylpiperazin-1-yl) -H-pyrido (2,3-b) benzo-1,4-diazepine;

10- (4-metilpiperazin-l-il)-pirido(4,3-b)benzo-l,4tiazepinas;10- (4-methylpiperazin-1-yl) -pyrido (4,3-b) benzo-1,4-thiazepine;

5- (4-metilpiperazin-l-il)dibenzo(b,f)1,4selenazepinas;5- (4-methylpiperazin-1-yl) dibenzo (b, f) 1,4-selenazepine;

6- (4-metilpiperazin-l-il)dipirido(2,3-b:3', 2'f)1,4-tiazepinas;6- (4-methylpiperazin-1-yl) dipyrido (2,3-b: 3 ', 2'f) 1,4-thiazepine;

6-(4-metilpiperazin-l-il)11-metil-llH-pirido(2,3b)benzo-1,4-diazepinas.6- (4-methylpiperazin-1-yl) 11-methyl-11H-pyrido (2,3b) benzo-1,4-diazepine.

Nauji junginiai pagal šį išradimą gali būti sintetinami pagal bendrą būdą iš žinomų arba lengvai sintetinamų azepinonų, atitinkančių II formulę:The novel compounds of the present invention may be synthesized according to the general procedure from known or readily synthesized azepinones of formula II:

kurioje X, R! ir R2 yra tokie, kaip apibrėžta čia aukščiau, ir kur Nx ir N2 yra benzeno arba piridino žiedas.where X, R! and R 2 is as defined herein above, and wherein N x and N 2 are a benzene or pyridine ring.

Šiuo požiūriu tam tikras skaičius azepinonų, kurie jau yra paskelbti literatūroje, pateikiami žemiau:In this regard, a number of azepinones already published in the literature are listed below:

5,11-dihidro-6H-pirido(2,3-b)benzo-1,4-diazepin-6onas;5,11-Dihydro-6H-pyrido (2,3-b) benzo-1,4-diazepin-6one;

6,ll-dihidro-5H-pirido(2,3-b)benzo-l,5-diazepin-5onas;6,11-dihydro-5 H -pyrido (2,3-b) benzo-1,5-diazepin-5 one;

5.10- dihidro-llH-pirido(4,3-b)benzo-l,5-diazepin11-onas;5.10-dihydro-11 H -pyrido (4,3-b) benzo-1,5-diazepin-11-one;

5.11- dihidro-ll-metil-6H-pirido(2,3-b)benzo-1,4diazepin-6-onas;5.11-dihydro-11-methyl-6H-pyrido (2,3-b) benzo-1,4-diazepin-6-one;

5H,6H-pirido(2,3-b)benzo-1,5-oksazepin-5-onas;5H, 6H-pyrido (2,3-b) benzo-1,5-oxazepin-5-one;

5H,6H-pirido(2,3-b)benzo-l,4-oksazepin-6-onas;5H, 6H-pyrido (2,3-b) benzo-1,4-oxazepin-6-one;

5.11- dihidro-8-metil-6H-pirido(2,3-b)benzo-1,4diazepin-6-onas;5.11-dihydro-8-methyl-6H-pyrido (2,3-b) benzo-1,4-diazepin-6-one;

9-chloro-5,ll-dihidro-6H-pirido(2,3-b)benzo-l,4diazepin-6-onas;9-chloro-5,11-dihydro-6H-pyrido (2,3-b) benzo-1,4-diazepin-6-one;

10H, HH-dibenzo (b, f) 1,4-selenazepin-l 1-onas .10H, HH-dibenzo (b, f) 1,4-selenazepin-11-one.

Paskutinis paminėtas azepinonas, t.y. 10H, HH-dibenzo(b, f)-1,4-selenazepin-ll-onas galėtų būti sintetinamas iš 2,2'-dibromobenzanilido. Sintetinama taip: 150 ml sauso dimetilformamido, 0,015 molio seleno, 0,06 molio natrio patalpinama apvaliadugnėj e kolboje. Mišinys šildomas maišant keturias valandas 100 C temperatūroje. Kai viskas ištirpsta, pridedama 0,025 moliai 2,2'-dibromobenzanilido ir maišoma 20 vai. 100110°C temperatūroje. Tirpalas išpilamas į ledo ir druskos rūgšties mišinį. Nuosėdos filtruojamos. Gautas produktas paveikiamas verdančiu alkoholiu ir filtruojamas. Darinys perkristalinamas iš dimetilformamido ir vandens mišinio. Lyd.t. 275°C.The last mention of azepinone, i.e. 10H, HH-dibenzo (b, f) -1,4-selenazepin-11-one could be synthesized from 2,2'-dibromobenzanilide. Synthesize as follows: Place 150 ml of dry dimethylformamide, 0.015 mol of selenium and 0.06 mol of sodium in a round-bottomed flask. The mixture is heated with stirring at 100 ° C for four hours. When all is dissolved, 0.025 mol of 2,2'-dibromobenzanilide is added and stirred for 20 hours. At 100110 ° C. The solution is poured into a mixture of glacial and hydrochloric acid. The precipitate is filtered off. The resulting product is treated with boiling alcohol and filtered. The derivative is recrystallized from a mixture of dimethylformamide and water. Melting point 275 ° C.

Tam tikro skaičiaus originalių azepinonų, kurie nėra aprašyti literatūroje, sintezė aprašyta žemiau.Synthesis of a number of original azepinones not described in the literature is described below.

sintezėsynthesis

8-Chloro-5H,6H-pirido(2,3-b)benzo-l,5-oksazepin-5-onas (II formulė: X=0, RX=C1 padėtyje b, R2=H, N^piridinas su N padėtyje d', N2=benzenas).8-Chloro-5H, 6H-pyrido (2,3-b) benzo-1,5-oxazepin-5-one (Formula II: X = O, R X = C 1 at position b, R 2 = H, N with N at position d ', N 2 = benzene).

2-Chloropiridin-3-karboninės rūgšties chloranhidrido (0,1 mol) tirpalas po truputį pilamas į 2-amino-4chlorofenolio (0,2 mol) tirpalą tetrahidrofurane (150 ml) . Mišinys virinamas maišant vieną valandą. Praskiedžiamas vienu litru vandens. Susidarę nuosėdos filtruojamos, plaunamos ir džiovinamos. Negrynas produktas naudojamas kitoje stadijoje. Oksazepinas sintetinamas, veikiant amidą teoriniu natrio etilato absoliučiame etanolyje kiekiu. Natrio druska išskiriama išgarinant tirpiklį. Norima ciklizacija atliekama virinant 3-4 vai. dimetilformamide. Mišinys koncentruojamas, vakuume nudistiliuojant DMF, ir kristalinamas 0°C temperaLT 3231 B tūroje. Išskirtas produktas perplaunamas šaltu metanoliu ir perkristalinamas iš DMF/metanolio mišinio. Lyd.t. 300°C.A solution of 2-chloropyridine-3-carboxylic acid chloro-anhydride (0.1 mol) was added slowly to a solution of 2-amino-4-chlorophenol (0.2 mol) in tetrahydrofuran (150 ml). The mixture is refluxed for one hour. Dilute with one liter of water. The precipitate formed is filtered, washed and dried. The impure product is used at another stage. Oxazepine is synthesized by treating the amide with a theoretical amount of sodium ethylate in absolute ethanol. The sodium salt is isolated by evaporation of the solvent. The desired cyclization is carried out by boiling for 3-4 h. dimethylformamide. The mixture was concentrated by vacuum distillation of DMF and crystallized at 0 ° C in a 3231 B volume. The isolated product is washed with cold methanol and recrystallized from DMF / methanol. Melting point 300 ° C.

sintezėsynthesis

5H,6H-8-metilpirido(2,3-b)benzo-1,5-oksazepin-5-onas (II formulė: X=0, R1=CH3 padėtyje b, R2=H, N1=piridinas su N padėtyje d', N2=benzenas)5H, 6H-8-methylpyrido (2,3-b) benzo-1,5-oxazepin-5-one (Formula II: X = O, R 1 = CH 3 at position b, R 2 = H, N 1 = pyridine with N at position d ', N 2 = benzene)

Ši medžiaga sintetinama pagal 1 sintezės metodiką, panaudojant pradinėmis medžiagomis 2-chloropiridin-3karboninę rūgštį ir 2-amino-4-metilfenolį. Lyd.t. 203°C.This material is synthesized according to Synthesis Method 1 using 2-chloropyridine-3-carboxylic acid and 2-amino-4-methylphenol as starting materials. Melting point 203 ° C.

sintezėsynthesis

8-chloro-5H,6H-pirido(2,3-b)benzo-1,4-oksazepin-6-onas (II formulė: X=0, R^H, R2=C1 padėtyje b', Nr=benzenas, N2=piridinas su N padėtyje d)8-Chloro-5H, 6H-pyrido (2,3-b) benzo-1,4-oxazepin-6-one (Formula II: X = O, R 1 H, R 2 = C 1 at position b ', N r = benzene, N 2 = pyridine with N in position d)

5-Chlorosalicilo rūgšties fenilo esteris sintetinamas virinant 0,1 molį fenolio ir 0,1 molį 5-chlorosalicilo rūgšties, esant POC13, 2 vai. Reagentas nudistiliuo j amas vakuume. Gauta tešlos pavidalo masė veikiama vandeniu. Susidarę nuosėdos filtruojamos ir plaunamos vandeniu. Lyd.t. 8 9°C.The phenyl ester of 5-chlorosalicylic acid is synthesized by boiling 0.1 mol of phenol and 0.1 mol of 5-chlorosalicylic acid in POCl for 3 , 2 hours. The reagent was distilled off under vacuum. The resulting dough mass is treated with water. The precipitate formed is filtered off and washed with water. Melting point Mp 9 ° C.

Norimas junginys yra gaunamas, kaitinant iki lydymosi 0,05 molio aukščiau pagaminto esterio su 0,1 molio 3amino-2-chlorpiridino tol, kol baigiasi reakcija. Masė apdorojama 30 ml etanolio ir trinama, kol gaunamos filtravimui tinkamos nuosėdos. Po išskyrimo produktas plaunamas etanoliu ir perkristalinamas iš dioksano arba DMF/metanolio mišinio. Lyd.t. 280°C.The title compound is obtained by heating to 0.05 mol of the above ester with 0.1 mol of 3 amino-2-chloropyridine until the reaction is complete. The mass is treated with 30 ml of ethanol and triturated until a precipitate suitable for filtration is obtained. After isolation, the product is washed with ethanol and recrystallized from dioxane or DMF / methanol. Melting point 280 ° C.

sintezėsynthesis

5H,6H-Pirido(2,3-b)benzo-l,4-tiazepin-6-onas (II formulė: X=S, R1=R2=H, Nx=benzenas, N2=piridinas su N padėtyje d) metodas:5H, 6H-Pyrido (2,3-b) benzo-1,4-thiazepin-6-one (Formula II: X = S, R 1 = R 2 = H, N x = Benzene, N 2 = Pyridine with N in position d) method:

a) 2-(Feniltio)piridin-3-karboninės rūgšties sintezė 0,2 moliai tiofenolio ir 0,2 moliai 50% NaH disperguojama 50 ml propileno glikolio. Į šį mišinį pridedama 0,1 molio 2-chloropiridin-3karboninės rūgšties, ir mišinys pašildomas iki virimo. Po reakcijos tirpiklis nugarinamas. Liekana apdorojama vandeniu ir terpė padaroma lygi pH=7. Tiofenolio perteklius ekstrahuojamas chloroformu. Vandeninė fazė gryninama aktyvuota anglimi ir parūgštinama. Produktas išsikiria baltų miltelių pavidalu. Lyd.t. 164°C.a) Synthesis of 2- (Phenylthio) pyridine-3-carbonic acid 0.2 mol of thiophenol and 0.2 mol of 50% NaH are dispersed in 50 ml of propylene glycol. To this mixture is added 0.1 mol of 2-chloropyridine-3-carboxylic acid and the mixture is brought to boiling. After the reaction, the solvent is evaporated. The residue is treated with water and the medium is adjusted to pH = 7. The excess thiophenol is extracted with chloroform. The aqueous phase is purified with activated carbon and acidified. The product is a white powder. Melting point 164 ° C.

b) Ankstesnis junginys paverčiamas į azidą aukščiau gautos rūgšties chloranhidrido reakcijos pagalba. Rūgšties chloranhidridas supilamas į atšaldyto natrio azido tirpalo perteklių. Supylus, mišinys maišomas 1/4 vai. ir praskiedžiamas vandeniu. Produktas išskiriamas ir išdžiovinus toks ir naudojamas kitai reakcijai. Šio junginio ciklizacija atliekama pagal tokią metodiką. 1 g negryninto azido po truputį dedamas maišant į AlCl3 tirpalą orto-dichlorbenzene 120°C temperatūroje. Temperatūra palaikoma 1/2 vai. laikotarpyje. Mišinys apdorojamas chloroformu ir ekstrahuojamas 0,1 N druskos rūgštimi. Rūgštinė fazė yra reekstrahuojama keletą kartų CHC13. Chloroforminės fazės sujungiamos, džiovinamos ir koncentruojamos vakuume. Liekana užpilama acetonu ir paliekama 2 vai. šaldytuve. Nuosėdos filtruojamos. Lyd.t. 206-208ūC.b) The above compound is converted to the azide by reaction of the above acid with the acid anhydride. Add the acid anhydride to an excess of the cooled sodium azide solution. After stirring, the mixture is stirred for 1/4 hour. and diluted with water. The product is isolated and then dried and used for another reaction. The cyclization of this compound is carried out according to the following procedure. 1 g of crude azide is added slowly with stirring to a solution of AlCl 3 in ortho-dichlorobenzene at 120 ° C. The temperature is maintained for 1/2 hour. period. The mixture is treated with chloroform and extracted with 0.1 N hydrochloric acid. The acidic phase is reextracted several times with CHC1 3 . The chloroform phases are combined, dried and concentrated in vacuo. The residue is taken up in acetone and left for 2 hours. in the fridge. The precipitate is filtered off. Melting point 206-208 ū C.

metodas:method:

0,01 molio 3-amino-2chloropiridino su 0,01 molio 2-tiosalicilo rūgšties kaitinama iki lydymosi temperatūros kol baigiasi reakcija. Atšaldžius liekana užpilama 30 ml etanolio. Keletą minučių virinama ir po to leidžiama atvėsti. Nuosėdos filtruojamos, plaunamos etanoliu ir džiovinamos. Lyd.t. 205-208°C.0.01 mol of 3-amino-2-chloropyridine with 0.01 mol of 2-thiosalicylic acid are heated to the melting point until the reaction is complete. After cooling, add 30 ml of ethanol to the residue. Boil for a few minutes and then allow to cool. The precipitate is filtered off, washed with ethanol and dried. Melting point 205-208 ° C.

sintezėsynthesis

5H,6H-Pirido(4,3-b)benzo-l,4-tiazepin-6-onas (II formulė: X=S, R1=R2=H, N^benzenas, N2=piridinas su N padėtyje b)5H, 6H-Pyrido (4,3-b) benzo-1,4-thiazepin-6-one (Formula II: X = S, R 1 = R 2 = H, N 2 - Benzene, N 2 = Pyridine with N b)

0,01 molio tiosalicilo rūgšties ir 0,01 molio 3-amino4-chloro-piridino, esant orto-dichlorobenzenui, virinama su grįžtamu šaldytuvu keletą valandų. Pasibaigus reakcijai, tirpiklis pašalinamas. Liekana užpilama nedideliu kiekiu vandens ir terpė padaroma iki pH=5-6. Junginys ekstrahuojamas chloroformu. Chl-orof orminiai ekstraktai išgarinami. Liekana užpilama vandeniniu bikarbonato tirpalu ir maišoma 1/2 vai. Suspenduotas junginys filtruojamas ir praplaunamas vandeniu. Lyd.t. 244°C.0.01 mol of thiosalicylic acid and 0.01 mol of 3-amino-4-chloro-pyridine in the presence of ortho-dichlorobenzene are refluxed for several hours. At the end of the reaction, the solvent is removed. The residue is poured into a small amount of water and the medium is made up to pH = 5-6. The compound is extracted with chloroform. Chl-orof ormic extracts were evaporated. The residue is taken up in aqueous bicarbonate solution and stirred for 1/2 hour. The suspended compound is filtered and rinsed with water. Melting point 244 ° C.

sintezėsynthesis

8-Chloro-5H,6H-pirido(2,3-b)benzo-1,4-tiazepin-6-onas (II formulė: X=S, Ri=H, R2=C1 padėtyje b', N^benzenas, N2=piridinas su N padėtyje d)8-Chloro-5H, 6H-pyrido (2,3-b) benzo-1,4-thiazepin-6-one (Formula II: X = S, R 1 = H, R 2 = C , N 2 = pyridine with N in position d)

Junginys sintetinamas pagal 4 sintezės 1 metodą. Lyd.t. 314°C.The compound is synthesized according to Synthesis 4 Method 1. Melting point 314 ° C.

sintezėsynthesis

5H,6H-Dipirido (2,3-b:3' ,2'-f)1,4-tiazepin-5-onas (formulė II: X=S, R1=R2=H, N1=N2=piridinas su N padėtyse d ir d')5H, 6H-Dipyrido (2,3-b: 3 ', 2'-f) 1,4-thiazepin-5-one (Formula II: X = S, R 1 = R 2 = H, N 1 = N 2 = pyridine with N at positions d and d ')

1,575 g 2-chloropiridin-3-karboninės rūgšties reaguojant su tionilo chloridu, gaunamas rūgšties chloranhidridas. Nugarinus reagento perteklių, liekana užpilama 20 ml dioksano ir po truputį pilama į 3,12 g 3-amino-2-merkaptopiridino tirpalą 50 ml dioksano, intensyviai maišant. Mišinys purtomas 1/4 vai. ir po to praskiedžiamas penkiskart didesniu vandens tūriu. Viskas ištirpsta ir terpė yra silpnai rūgštinė. Esančios nuosėdos pasirinktinai pašalinamos. Bikarbonato pagalba pH padaromas lygus 7 ir tirpalui leidžiama kristalintis. Gautas produktas džiovinamas ventiliuojamoje džiovinimo krosnyje ir perkristalinamas, jeigu reikalinga, iš tolueno. Lyd.t. 183°C.The reaction of 1.575 g of 2-chloropyridine-3-carboxylic acid with thionyl chloride gives the acid anhydride. After evaporation of the excess reagent, add the residue to 20 ml of dioxane and add gradually to a solution of 3.12 g of 3-amino-2-mercaptopyridine in 50 ml of dioxane with vigorous stirring. Shake the mixture for 1/4 hour. and then diluted five times with water. Everything dissolves and the medium is slightly acidic. Optional precipitate is removed. The pH is adjusted to 7 with the aid of bicarbonate and the solution is allowed to crystallize. The product obtained is dried in a ventilated oven and recrystallized from toluene if necessary. Melting point 183 ° C.

0,01 molio amido darinio pridedama į 0,012 molio Na tret-butilato suspensiją 50 ml DMF. Mišinys virinamas su grįžtamu šaldytuvu 10-20 vai., DMF nugarinamas vakuume ir liekana užpilama vandeniu (50 ml) . Nuosėdos filtruojamos, plaunamos vandeniu ir džiovinamos. Išdžiovinus, nuosėdos užpilamos eteriu ir ištrinamos. Nufiltravus ir išdžiovinus, produktas gali būti, jeigu reikalinga, perkristalinamas iš DMF. Lyd.t. 305°C.0.01 molar amide derivative is added to 0.012 mol Na tert-butylate suspension in 50 ml DMF. The mixture was refluxed for 10-20 h, the DMF was evaporated in vacuo and the residue was taken up in water (50 mL). The precipitate is filtered off, washed with water and dried. After drying, the precipitate is taken up in ether and removed. After filtration and drying, the product can, if necessary, be recrystallized from DMF. Melting point 305 ° C.

sintezėsynthesis

8-Chloro-5H,6H-pirido(2,3-b)benzo-1,4-diazepin-6-onas (II formulė: X=NH, R1=C1 padėtyje b', R2=H, N1=benzenas, N2=piridinas su N padėtyje d)8-Chloro-5H, 6H-pyrido (2,3-b) benzo-1,4-diazepin-6-one (Formula II: X = NH, R 1 = C 1 at position b ', R 2 = H, N 1 = benzene, N 2 = pyridine with N in position d)

1) 0,01 molio 5-chloro-2-nitrobenzoinės rūgšties, 20 ml SOC12 ir keletas lašų DMF virinama vieną valandą. SOC12 perteklius pašalinamas, liekana užpilama 20 ml' dioksano. Šis tirpalas po truputį sumaišomas su 0,015 molio 3-amino-2-chloropiridino tirpalu 20 ml dioksano. Po vienos valandos maišymo, mišinys praskiedžiamas penkiskart didesniu vandens tūriu. Nuosėdos filtruojamos ir plaunamos šaltu vandeniu. Jeigu reikalinga, produktas perkristalinamas iš izopropanolio. Lyd.t. 190°C.1) 0.01 mol of 5-chloro-2-nitrobenzoic acid, 20 ml of SOCl 2 and several drops of DMF are boiled for one hour. Excess SOC1 2 is removed and the residue is taken up in 20 mL of dioxane. This solution is gradually added to a solution of 0.015 mol of 3-amino-2-chloropyridine in 20 ml of dioxane. After stirring for one hour, the mixture is diluted five times with water. The precipitate is filtered off and washed with cold water. If necessary, the product is recrystallized from isopropanol. Melting point 190 ° C.

2) 0,01 molio nitro darinio ištirpinama 25 ml koncentruotos HCl. į šį tirpalą po truputį pridedama 11 g SnCl2.2H2O, ištirpinto 20 ml koncentruotos HCl. Po to tirpalas paliekamas vienai valandai vandens vonioje. Atšaldžius, nuosėdos filtruojamos, paveikiamos 10% NaOH ir ekstrahuojamos chloroformu. Chloroformo fazė džiovinama ir koncentruojama iki mažo tūrio, esant petrolio eteriui 100-140. Išsikristalinęs produktas po to filtruojamas ir praplaunamas petrolio eteriu 40-60. Lyd.t. 173°C.2) Dissolve 0.01 mol of nitro derivative in 25 ml of concentrated HCl. 11 g of SnCl 2 .2H 2 O dissolved in 20 ml of concentrated HCl are added gradually to this solution. The solution is then left for one hour in a water bath. After cooling, the precipitate is filtered, treated with 10% NaOH and extracted with chloroform. The chloroform phase is dried and concentrated to low volume in the presence of petroleum ether 100-140. The crystallized product is then filtered off and washed with petroleum ether 40-60. Melting point 173 ° C.

3) 0,01 molio amino darinio, gauto pagal 2), ištirpinama 18 ml dietilenglikolio monometilo eterio. Pridedama 0,2 ml 5% HCl. Mišinys maišant šildomas iki 130°C. Po 2-3 vai. kaitinimo gaunama suspensija. Kai tik reakcija baigiasi, mišinys atšaldomas ir filtruojamas. Išskirtas produktas plaunamas šaltu metanoliu ir perkristalinamas, jeigu reikalinga, iš dioksano. Lyd.t. 296°C.3) Dissolve 0.01 mol of the amino derivative obtained in 2) in 18 ml of diethylene glycol monomethyl ether. 0.2 ml of 5% HCl are added. The mixture is heated to 130 ° C with stirring. After 2-3 hours. heating the resulting suspension. Once the reaction is complete, the mixture is cooled and filtered. The isolated product is washed with cold methanol and recrystallized from dioxane if necessary. Melting point 296 ° C.

sintezėsynthesis

5,ll-Dihidro-8-fluoro-6H-pirido(2,3-b)benzo-l,45 diazepin-6-onas (II formulė: X=NH, R1=F padėtyje d', R2=H, Nx=benzenas, N2=piridinas su N padėtyje d)5,11-Dihydro-8-fluoro-6 H -pyrido (2,3-b) benzo-1,45 diazepin-6-one (Formula II: X = NH, R 1 = F at position d ', R 2 = H , N x = benzene, N 2 = pyridine with N in position d)

Šis junginys gaunamas pagal 8 sintezės metodiką, tačiau pradedant iš 5-fluoro-2-nitrobenzoinės rūgšties ir 3amino-2-chlorpiridino. Lyd.t. 270°C.This compound is prepared according to synthesis procedure 8, but starting from 5-fluoro-2-nitrobenzoic acid and 3 amino-2-chloropyridine. Melting point 270 ° C.

Šio išradimo metilpiperazinazepinų, atvaizduotų I formule bendras gavimo būdas, iš azepinonų, atvaizduotų II formule, gali būti atliktas trimis būdais, kurių schemos yra pateiktos ir komentuojamos žemiau.The general method of preparing the methylpiperazinazepines represented by Formula I of the present invention from the azepinones represented by Formula II can be accomplished in three ways, the schemes of which are set forth and commented below.

Schema A:Scheme A:

piridinas (II)pyridine (II)

Veikiant azepinoną (II) P2S5 piridine, sintezuojamas tionas (III) . Išskiriamas negrynas produktas, kurisThionium (III) is synthesized by the action of azepinone (II) on P 2 S 5 pyridine. A pure product is isolated which

R'=paranitrobenziltioR '= paranitrobenzylation

R=N-metilpiperazinil toks ir naudojamas ir is kurio, pridėjus kalio tret.butilato ir paranitrobenzilchlorido gaunamas tioeteris (IV). Sureagavus tioeteriui su N-metilpiperazinu, esant ledinės acto rūgšties, gaunamas junginys, atvaizduotas (I) formule (žr. Hunzicker 1588 (1967)).R = N-methylpiperazinyl is also used to give the thioether (IV) when potassium tert-butylate and paranitrobenzyl chloride are added. Reaction of the thioether with N-methylpiperazine in glacial acetic acid affords the compound represented by formula (I) (see Hunzicker 1588 (1967)).

Schema B:Scheme B:

ir kt., Helv.Chim.Actą, 50,and others, Helv.Chim.Actą, 50,

R=N-metilpiperazinilR = N-methylpiperazinyl

Azepinonai (II) sumaišomi su N-metilpiperazinu, esant TiCl4 tirpalo anizole. Šis mišinys leidžia gauti, maišant ir šildant, junginį (I) (žr. Chakrabarti J.K. ir kt., J.Med.Chem., 23, 878 (1980) ir Press J. ir kt., J. Med.Chem., 22, 725 (1979)).Azepinones (II) are mixed with N-methylpiperazine in the presence of TiCl 4 solution in anisole. This mixture allows compound (I) to be obtained by stirring and heating (see Chakrabarti JK et al., J.Med.Chem., 23, 878 (1980) and Press J. et al., J. Med.Chem. 22, 725 (1979).

Schema C:Scheme C:

R=N-metilpiperazinilR = N-methylpiperazinyl

Ši schema pradedama azepinonu (II), kuris veikiamas POC13 ir DMF, ir gaunamas atitinkamas iminochloridas (V), kuris be tolesnio išskyrimo reakcijoje su Nmetilpiperazinu toluene sudaro jungini (I) · (Šiuo klausimu žr. Hunzicker F. ir kt., Helv.Chim.Acta, 49 (5), 1933 (1966)).This scheme begins with azepinone (II), which is treated with POCl 3 and DMF, and yields the corresponding iminochloride (V) which, without further isolation, reacts with N-methylpiperazine in toluene to form compound (I). .Chim.Acta, 49 (5), 1933 (1966)).

Žinoma, šio išradimo junginius galima sintetinti, nenaudojant azepinonu (II), kaip pradinių medžiagų ar tarpinių junginių, kaip bus parodyta žemiau, nurodant i 21 pavyzdžio metilpiperazinazepino sintezę, pradedant ortohalogennitropiridinu, atvaizduotu V formule:Of course, the compounds of the present invention can be synthesized without the use of azepinone (II) as starting materials or intermediates, as will be shown below, referring to the synthesis of Example 21 methylpiperazinazepine starting from orthohalogenitritropyridine represented by Formula V:

kurioje Hal reiškia halogeno atomą, kaip antai Cl, F, J arba Br, ir benzenkarboninės rūgšties, atvaizduotos formule (VI), reakcijos produktu.wherein Hal represents a reaction product of a halogen atom, such as Cl, F, J or Br, and benzenecarboxylic acid represented by formula (VI).

(VI), kur X yra toks, kaip apibrėžta anksčiau.(VI) wherein X is as previously defined.

Metilpiperazinazepinų, atvaizduotų (I) formule, druskos gali būti gaunamos metodais, kurie yra gerai žinomi praktikoje. Bendru būdu, šios druskos gali būti gaunamos, reaguojant metilpiperazinazepinui su ekvimolekuliniu rūgšties kiekiu adekvačiame tirpiklyje, tokiame kaip, pavyzdžiui, alkoholis, po to sekančiu druskos išsodinimu, pridedant kito tirpiklio, kuris maišosi su pirmuoju ir kuriame druska yra netirpi, pavyzdžiui, eterio, arba toliau neutralizuojant eterinį rūgšties ar rūgštis, fosforo Organinės rūgštys bazės tirpalą baze ar rūgštimi. Tinkamiausios iš neorganinių rūgščių yra vandenilio chlorido rūgštis, vandenilio bromo rūgštis, sieros rūgštis, perchloro rūgštis ir t.t.The salts of the methylpiperazinazepines represented by the formula (I) may be prepared by methods well known in the art. In general, these salts may be prepared by reacting methylpiperazinazepine with an equimolecular acid in an appropriate solvent such as alcohol, followed by precipitating the salt by adding another solvent which is miscible with the former and in which the salt is insoluble, such as ether, or further neutralizing the ethereal solution of the acid or acids, phosphorus Organic acids with a base or acid. Preferred inorganic acids are hydrochloric acid, hydrobromic acid, sulfuric acid, perchloric acid and the like.

yra arba karboksirūgštys arba sulforūgštys, tokios kaip acto, citrinos, maleino, fumaro, propano, glikolio, pieno, askorbininė, pamoinė, gintaro, vyno, fenilacto, benzoinė, p-aminobenzoinė, antranilo, p-hidroksibenzoinė, salicilo, metansulfoninė, etandisulfoninė, gliukurono rūgštys ir t.t.are either carboxylic or sulfuric acids such as acetic, citric, maleic, fumaric, propane, glycolic, lactic, ascorbic, pamoic, amber, tartaric, phenylacetic, benzoic, p-aminobenzoic, anthranilic, p-hydroxybenzoic, salicylic, methanesulfonic, glucuronic acids and so on

Kai kurių šio išradimo metilpiperazinazepinų sintezių detalūs pavyzdžiai yra pateikiami žemiau.Detailed examples of some syntheses of the methylpiperazinazepines of the present invention are provided below.

pavyzdysexample

11-(4-metilpiperazin-l-il)-5H-pirido(4,3-b)benzo-l,5diazepinas (I formulė: X=NH, R1=R2=H, N1=piridinas su N padėtyje b', N2=benzenas).11- (4-Methylpiperazin-1-yl) -5 H -pyrido (4,3-b) benzo-1,5-diazepine (Formula I: X = NH, R 1 = R 2 = H, N 1 = Pyridine with N) b ', N 2 = benzene).

A metodas:Method A:

1) 0,01 molio 5,10-dihidro-llH-pirido(4,3)benzo-l,5diazepin-ll-ono veikiama P2S5 pertekliumi verdančiame piridine. Po kelių valandų kaitinimo, tirpiklio ir reagento perteklius pašalinamas. Liekana rūpestingai apdorojama ledu. Susidarę nuosėdos išskiriamos ir tokios naudojamos sekančioje stadijoje.1) 0.01 mol of 5,10-dihydro-11 H -pyrido (4,3) benzo-1,5-diazepin-11-one is treated with an excess of P 2 S 5 in boiling pyridine. After heating for several hours, remove excess solvent and reagent. The residue is carefully treated with ice. The resulting precipitate is isolated and used in the next step.

2) 5,2 g tiolaktamo pridedama į kalio tret-butilato suspensiją 80 ml dioksano (gautą tokiu būdu: 1,64 g kalio ištirpinama 40 ml tret-butanolio, pasibaigus dujų išsiskyrimui, tirpiklis pašalinamas ir liekana užpilama 80 ml dioksano). Mišinys virinamas vieną valandą. Po to, pridedama 4,1 g paranitrobenzilchlorido. Viskas virinama keturias valandas. Tirpiklis pašalinamas. Liekana užpilama chloroformu ir praplaunama šarminiu tirpalu. Chloroforminė fazė džiovinama ir išgarinama iki sausumo. Liekana perkristalinama iš petrolio eterio/acetono mišinio. Lyd.t. 127°C.2) 5.2 g of thiolactam are added to a suspension of potassium tert-butylate in 80 ml of dioxane (obtained as follows: 1.64 g of potassium is dissolved in 40 ml of tert-butanol, the solvent is removed at the end of gas evolution and 80 ml of dioxane is added). The mixture is boiled for one hour. Thereafter, 4.1 g of paranitrobenzyl chloride were added. All boil for four hours. The solvent is removed. The residue is taken up in chloroform and washed with an alkaline solution. The chloroform phase is dried and evaporated to dryness. The residue is recrystallized from petroleum ether / acetone. Melting point 127 ° C.

3) 4,3 g tioeterio, gauto 2)-ame, virinama su grįžtamu šaldytuvu, esant N-metilpiperazino (10 ml) ir 0,1 ml ledinės acto rūgšties, 24 valandų laikotarpyje. Išgarinus iki sausumo, liekana užpilama praskiesta acto rūgštimi. Atsiradę galimos nuosėdos nufiltruojamos.3) 4.3 g of the thioether obtained in 2) is refluxed in the presence of N-methylpiperazine (10 ml) and 0.1 ml of glacial acetic acid for 24 hours. After evaporation to dryness, the residue is taken up in dilute acetic acid. The resulting precipitate is filtered off.

spalva panaikinama, veikiant aktyvuota Bazė išsodinama pridedant koncentruoto filtruojama, praplaunama vandeniu ir Produktas gali būti perkristalinamas išdecolorization, activated by treatment, the base is precipitated by the addition of concentrated filtrate, rinsed with water and the product can be recrystallized from

Filtrato anglimi. amoniako, džiovinama.Filtrate carbon. of ammonia, dried.

dichlormetano/heksano mišinio. Lyd.t. 216°C,dichloromethane / hexane mixture. Melting point 216 ° C,

B metodas:Method B:

0,01 molio 5,10-dihidro-llH-pirido(4,3-b)benzo-l,5diazepin-11-ono sumaišoma su 10 ml N-metilpiperazino. Maišant, atsargiai pridedama į diazepinono suspensiją 1,2 ml TiCl4 tirpalas 5 ml anizolo. Reakcija vykdoma maišant 2-3 valandas 120°C temperatūroje. Mišinys atšaldomas ir paveikiamas lediniu vandeniu. Tirpalo pH turi būti šarminis. Po to produktas ekstrahuojamas dichlormetanu. Išgarinus tirpiklį, liekana gryninama silikagelio kolonėlėje (eliuavimo fazė: acetonas/petrolio eteris 40-60:9/1). Pašalinus eliuentą, produktas perkristalinamas iš heksano. Lyd.t. 216°C.0.01 mol of 5,10-dihydro-11 H -pyrido (4,3-b) benzo-1,5-diazepin-11-one is mixed with 10 ml of N-methylpiperazine. With stirring, 1.2 ml of TiCl 4 solution in 5 ml of anisole are carefully added to the diazepinone suspension. The reaction was carried out with stirring at 120 ° C for 2-3 hours. The mixture is cooled and treated with ice water. The pH of the solution should be alkaline. The product is then extracted with dichloromethane. After evaporation of the solvent, the residue is purified on a silica gel column (elution phase: acetone / petroleum ether 40-60: 9/1). After removal of the eluent, the product is recrystallized from hexane. Melting point 216 ° C.

pavyzdysexample

6-(4-metilpiperazin-l-il)pirido(2,3-b)benzo-1,4tiazepinas (I formulė: X=S, R1=R2=H, N1=benzenas, N2=piridinas su N padėtyje d) g 5H,6H-pirido(2, 3-b)benzo-1,4-tiazepin-6-ono viri5 narna 20 valandų su fosforo oksichlorido pertekliumi ir lašais N,N-dimetilanilino. Į tirpalą pripilama bevandenio tolueno ir išgarinama iki sausumo. Liekana užpilama 5 ml bevandenio tolueno ir pridedamas Nmetilpiperazino perteklius. Po to mišinys virinamas 2-4 valandas. Kai tik reakcija baigiasi, tirpiklis pašalinamas. Spalvota masė užpilama chloroformu ir praplaunama du kartus vandeniu. Chloroforminės fazės spalva panaikinama anglimi ir džiovinama. Sukoncentravus iki mažo tūrio, mišinys praleidžiamas per silikagelio kolo15 nėlę (Woelm akt. III). Eliuentas acetonas. Atskyrus, skirtingos fazės, turinčios aukščiau paminėtą produktą išgarinamos iki sausumo. Liekana perkristalinama iš petrolio eterio 100/140. Lyd.t. 134°C.6- (4-Methylpiperazin-1-yl) pyrido (2,3-b) benzo-1,4-thiazepine (Formula I: X = S, R 1 = R 2 = H, N 1 = Benzene, N 2 = Pyridine At N (d) g of 5H, 6H-pyrido (2,3-b) benzo-1,4-thiazepin-6-one was boiled for 20 hours with excess phosphorus oxychloride and drops of N, N-dimethylaniline. Add anhydrous toluene to the solution and evaporate to dryness. The residue is taken up in 5 ml of anhydrous toluene and an excess of N-methylpiperazine is added. The mixture is then refluxed for 2-4 hours. As soon as the reaction is complete, the solvent is removed. The colored mass is filled with chloroform and washed twice with water. The chloroform phase is decolorized with carbon and dried. When concentrated to a low volume, the mixture is passed through a silica gel column (Woelm Act. III). Elution with acetone. After separation, the different phases containing the above product are evaporated to dryness. The residue is recrystallized from petroleum ether 100/140. Melting point 134 ° C.

3 pavyzdysExample 3

8-Chloro-6-(4-metilpiperazin-l-il)pirido(2,3-b)benzo1,4-tiazepino fumaratas (I formulė: X=S, R]=H, R2=C1 padėtyje b'8-Chloro-6- (4-methylpiperazin-1-yl) pyrido (2,3-b) benzo1,4-thiazepine fumarate (Formula I: X = S, R 1 = H, R 2 = C 1 at position b '

N2=piridinas su N padėtyje d').N 2 = pyridine with N at position d ').

Ni=benzenas,Ni = benzene,

Pradedant 5H, 6H-pirido(2,3-b)benzo-l,4-tiazepin-6-onu, aukščiau paminėta metilpiperazinazepino bazė gaunama 30 pagal pavyzdžio 2 metodą. Išgarinus chloroforminės ištirpinama minimaliame verdančio Pridedamas ekvimolekulinis fumaro rūgšties kiekis, anksčiau ištirpintas karštame alkoholyje. Tirpalas atšaldomas. Jeigu produktas nesikris35 talina bestovint, pridedama eterio, kurio pagalba sukeliama kristalizacija. Paliekama stovėti, o gautos frakcijas, liekana alkoholio kiekyje.Starting with 5H, 6H-pyrido (2,3-b) benzo-1,4-thiazepin-6-one, the above methylpiperazinazepine base is obtained according to Method 2 of Example 2. After evaporation, chloroform dissolves in a minimum boiling Add equimolecular amount of fumaric acid previously dissolved in hot alcohol. Cool the solution. If the product does not crystallize, the ether is added to aid in crystallization. It is left standing and the fractions obtained are left in the alcohol content.

baltos nuosėdos išskiriamos ir praplaunamos eteriu. Lyd.t. 198ŪC.the white precipitate is isolated and washed with ether. Melting point 198 U C.

pavyzdysexample

5-(4-metilpiperazin-l-il)pirido(2,3-b)benzo-1,5oksazepino maleatas (I formulė: X=0, R1=R2=H, N1=piridinas su N padėtyje d’, N2=benzenas)5- (4-Methylpiperazin-1-yl) pyrido (2,3-b) benzo-1,5-oxazepine maleate (Formula I: X = O, R 1 = R 2 = H, N 1 = Pyridine with N at position d ' , N 2 = benzene)

Produktas, gautas iš 5H,6H-pirido(2,3-b)benzo-1,5oksazepin-2-ono pagal 2 pavyzdžio metodiką. Po to chloroforminės frakcijos išgarinamos iki sausumo. Liekana užpilama metiletilketonu. Pridedamas ekvimolekulinis maleino rūgšties, ištirpintos metiletilketone, kiekis, ir po to bevandenis eteris. Produktas išsikristalina. Jis išskiriamas ir praplaunamas eteriu. Lyd.t. 206°C.Product obtained from 5H, 6H-pyrido (2,3-b) benzo-1,5-oxazepin-2-one according to the procedure of Example 2. The chloroform fractions are then evaporated to dryness. The residue is taken up in methyl ethyl ketone. An equimolar amount of maleic acid dissolved in methylethylketone was added followed by anhydrous ether. The product crystallizes. It is isolated and rinsed with ether. Melting point 206 ° C.

pavyzdysexample

8-Chloro-5-(4-metilpiperazin-l-il)pirido(2,3-b)benzo1,5-oksazepino fumaratas (I formulė: X=0, R1=C1 padėtyje b, R2=H, N1=piridinas su padėtyje d', N2=benzenas)8-Chloro-5- (4-methylpiperazin-l-yl) pyrido (2,3-b) benzo1,5-oxazepine fumarate (Formula I: X = 0, R @ 1 = C1 in position b, R 2 = H, N 1 = pyridine with position d ', N 2 = benzene)

Pradedant oksazepinu, aprašytu 1 sintezėje, ir panaudojant 2 pavyzdžio metodą, junginys išskiriamas fumarato pavidale taip pat, kaip 3 pavyzdyje. Lyd.t. 260°C.Starting with the oxazepine described in Synthesis 1 and using the method of Example 2, the compound is isolated in the form of fumarate in the same manner as in Example 3. Melting point 260 ° C.

pavyzdysexample

5-(4-metilpiperazin-l-il)8-metilpirido(2,3-b)benzo-1,5oksazepino fumaratas (I formulė: X=0, Rg=CH3 padėtyje b, R2=H, N^piridinas su N padėtyje d', N2=benzenas)5- (4-Methylpiperazin-1-yl) 8-methylpyrido (2,3-b) benzo-1,5-oxazepine Fumarate (Formula I: X = O, R g = CH 3 at position b, R 2 = H, N 2 -Pyridine with N at position d ', N 2 = benzene)

Pradedant oksazepinu, aprašytu 2 sintezėje, ir panaudojant 2 pavyzdžio metodą, junginys išskiriamas fumarato pavidale taip pat, kaip 3 pavyzdyje. Lyd.t. 235°C.Starting with the oxazepine described in Synthesis 2 and using the method of Example 2, the compound is isolated in the form of fumarate in the same manner as in Example 3. Melting point 235 ° C.

pavyzdysexample

6-(4-metilpiperazin-l-il)pirido(2, 3-b)benzo-l,4oksazepino fumaratas (I formulė: X=0, R1=R2=H, Ng=benzenas, N2=piridinas su N padėtyje d)6- (4-Methylpiperazin-1-yl) pyrido (2,3-b) benzo-1,4-oxazepine fumarate (Formula I: X = O, R 1 = R 2 = H, Ng = Benzene, N 2 = Pyridine with N in position d)

Pradedant 5H, 6H-pirido (2,3-b)benzo-l,4-oksazepin-6-onu ir panaudojant 2 pavyzdžio metodiką, junginys išskiriamas fumarato pavidale. Lyd.t. 183°C.Starting with 5H, 6H-pyrido (2,3-b) benzo-1,4-oxazepin-6-one and following the procedure of Example 2, the compound is isolated in the form of fumarate. Melting point 183 ° C.

pavyzdysexample

8-Chloro-6-(4-metilpiperazin-l-il)pirido(2,3-b)benzo1,4-oksazepino fumaratas (I formulė: X=0, R=H, R=C1 padėtyje b', N=benzenas, N=piridinas su N padėtyje d)8-Chloro-6- (4-methylpiperazin-1-yl) pyrido (2,3-b) benzo1,4-oxazepine fumarate (Formula I: X = 0, R = H, R = C1 at position b ', N = benzene, N = pyridine with N in position d)

Pradedant 8-chloro-5H,6H-pirido(2,3-b)benzo-l,4-oksazepin-6-onu iš 3 sintezės, junginys gaunamas pagal metodiką, aprašytą 2 pavyzdyje. Junginys išskiriamas fumarato pavidale taip pat, kaip 3 pavyzdyje. Lyd.t. 250°C.Starting from the synthesis of 8-chloro-5H, 6H-pyrido (2,3-b) benzo-1,4-oxazepin-6-one, the compound is obtained according to the procedure described in Example 2. The compound is isolated in the form of fumarate in the same manner as in Example 3. Melting point 250 ° C.

pavyzdysexample

6-(4-metilpiperazin-l-il)-llH-pirido(2,3-b)benzo-1,4diazepinas (I formulė: X=NH, R,=R2=H, Nx=benzenas, N2=piridinas su N padėtyje d)6- (4-Methylpiperazin-1-yl) -IIH-pyrido (2,3-b) benzo-1,4-diazepine (Formula I: X = NH, R 1 = R 2 = H, N x = Benzene, N 2 = pyridine with N in position d)

Pradedant 5,ll-dihidro-6H-pirido(2,3-b)benzo-l,4-diazepin-6-onu, atliekama kondensacija pagal 1 pavyzdžio B procesą. Lyd.t. 141UC.Starting with 5,11-dihydro-6H-pyrido (2,3-b) benzo-1,4-diazepin-6-one, condensation is carried out according to Example 1, Process B. Melting point 141 U C.

pavyzdysexample

8-Chloro-6-(4-metilpiperazin-l-il)-llH-pirido(2,3b)benzo-1,4-diazepinas (I formulė: X=NH, R1=C1 padėtyje b', R2=H, N1=benzenas, N2=piridinas su N padėtyje d)8-Chloro-6- (4-methylpiperazin-1-yl) -1H-pyrido (2,3b) benzo-1,4-diazepine (Formula I: X = NH, R 1 = C 1 at position b ', R 2 = H, N 1 = benzene, N 2 = pyridine with N in position d)

Pradedant 8 sintezės diazepinonu, aukščiau paminėtas produktas gaunamas pagal metodiką, aprašytą 1 pavyzdyje, metodas B. Lyd.t. 180°C.Starting with diazepinone 8 synthesis, the above product is obtained according to the procedure described in Example 1, Method B. Lyd.t. 180 ° C.

pavyzdysexample

6-(4-metilpiperazin-l-il)-8-metil-llH-pirido(2,3b)benzo-1,4-diazepinas (I formulė: X=NH, R1=CH3 padėtyje b', R2=H, Nx=benzenas, N2=piridinas su N padėtyje d)6- (4-methylpiperazin-1-yl) -8-methyl-11 H -pyrido (2,3b) benzo-1,4-diazepine (Formula I: X = NH, R 1 = CH 3 at position b ', R 2 = H, N x = benzene, N 2 = pyridine with N in position d)

Pradedant 5,ll-dihidro-8-metil-6H-pirido(2,3-b)benzo1,4-diazepin-6-onu, aukščiau paminėtas junginys gaunamas pagal 1 pavyzdžio metodą B. Lyd.t. 157°C.Starting with 5,11-dihydro-8-methyl-6H-pyrido (2,3-b) benzo [1,4-diazepin-6-one], the above compound is obtained according to the method of Example 1, B. Lyd.t. 157 ° C.

pavyzdysexample

9-Chloro-6-(4-metilpiperazin-l-il)-HH-pirido(2,3b)benzo-1,4-diazepinas (I formulė: X=NH, R1=C1, padėtyje c', R2=H, N1=benzenas, N2=piridinas su N padėtyje d)9-Chloro-6- (4-methylpiperazin-1-yl) -H-pyrido (2,3b) benzo-1,4-diazepine (Formula I: X = NH, R 1 = Cl, in position c ', R 2 = H, N 1 = benzene, N 2 = pyridine with N in position d)

Pradedant 9-chloro-5,ll-dihidro-6H-pirido(2,3-b)benzo1,4-diazepin-6-onu, aukščiau paminėtas produktas gaunamas pagal 1 pavyzdžio metodą B. Lyd.t. 186°C.Starting with 9-chloro-5,11-dihydro-6H-pyrido (2,3-b) benzo-1,4-diazepin-6-one, the above product is obtained according to the method of Example 1, B. Melting point. 186 ° C.

pavyzdysexample

8-Fluoro-6-(4-metilpiperazin-l-il)-HH-pirido(2,3b)benzo-1,4-diazepinas (I formulė: X=NH, R4=F padėtyje b', R2=H, N1=benzenas,8-Fluoro-6- (4-methylpiperazin-1-yl) -H-pyrido (2,3b) benzo-1,4-diazepine (Formula I: X = NH, R 4 = F at position b ', R 2 = H, N 1 = benzene,

N2=piridinas su N padėtyje d)N 2 = pyridine with N in position d)

Pradedant 9 sintezės diazepinonu, aukščiau paminėtas junginys gaunamas pagal 1 pavyzdžio metodą B. Lyd.t. 188°C.Starting with diazepinone 9 synthesis, the above compound is obtained according to the method of Example 1, B. Lyd.t. 188 ° C.

pavyzdysexample

5-Formil-ll-(4-metilpiperazin-l-il)-5H-pirido(4,3b)benzo-1,5-diazepinas5-Formyl-11- (4-methylpiperazin-1-yl) -5H-pyrido (4,3b) benzo-1,5-diazepine

O // (I formulė: X=N-C , R1=R2=H, N1=piridinas su N padėtyje H b', N2=benzenas)O // (Formula I: X = NC, R 1 = R 2 = H, N 1 = Pyridine with N at H b ', N 2 = Benzene)

Šis pavyzdys pradedamas 1 pavyzdžio junginiu. 15 cm3 acto rūgšties anhidrido atšaldoma ir maišant po truputi pridedama 7 cm3 99% skruzdžių rūgšties. Mišinys laikomas 15 min. 50°C temperatūroje ir po to atšaldomas ledo vonioje. Pridedama 0,01 molio 1 pavyzdžio junginio ir mišinys maišomas visą naktį. Mišinys apdorojamas ledu, šarminamas ir ekstrahuojamas dichlormetanu. Džiovinama ir koncentruojama vakuume, ir perkristaiinama iš heksano. Lyd.t. 19βυϋ.This example begins with the compound of Example 1. 15 cm 3 of acetic anhydride are cooled and 7 cm 3 of 99% formic acid is added slowly with stirring. The mixture is kept for 15 minutes. 50 ° C and then cooled in an ice bath. 0.01 mol of the compound of Example 1 is added and the mixture is stirred overnight. The mixture is treated with ice, basified and extracted with dichloromethane. Dry and concentrate in vacuo and recrystallize from hexane. Melting point 19β υ ϋ.

pavyzdys ll-Formil-5-(4-metilpiperazin-l-il)-llH-pirido(2,3b)benzo-1,5-diazepinasExample 1111-Formyl-5- (4-methylpiperazin-1-yl) -IIH-pyrido (2,3b) benzo-1,5-diazepine

O // (I formulė: X=N-C , R1=R2 :=H, Nn=piridinas su N padėtyje \O // (Formula I: X = NC, R 1 = R 2 : = H, Nn = Pyridine with N in position \

H d' , N2=benzenas)H d ', N 2 = benzene)

Šis junginys pradedamas junginiu, aprašytu straipsnyje Chekrabarti ir kt., J.Med.Chem., t. 32, No 10, 23752381 (1989), kuris formilinamas pagal 14 pavyzdžio metodiką. Lyd.t. 194°C.This compound starts with the compound described in Chekrabarti et al., J.Med.Chem. 32, No 10, 23752381 (1989), which is formylated according to the procedure of Example 14. Melting point 194 ° C.

pavyzdys ll-Trifluormetilkarbonil-5-(4-metilpiperazin-l-il)-11Hpirido(2,3-b)benzo-1,5-diazepinas (I formulė: X=N-CO-CF3, R,=R2=H, N^piridinas su N padėtyje d', N2=benzenas)Example 11 11-Trifluoromethylcarbonyl-5- (4-methylpiperazin-1-yl) -11H-pyrido (2,3-b) benzo-1,5-diazepine (Formula I: X = N-CO-CF 3 , R 1 = R 2 = H, N ^ pyridine with N at position d ', N 2 = benzene)

Šis pavyzdys pradedamas junginiu, aprašytu straipsnyje, paminėtame 15 pavyzdyje. 0,02 molio šio junginio sumaišoma su 15 ml trifluoracto rūgšties anhidrido ir keletu lašų N, N-dimetilanilino gerai šaldant, po to mišinys virinamas 5 minutes ir maišomas vieną naktį. Mišinys išpilamas ant ledo, pašarminamas ir ekstrahuojamas chloroformu. Gryninamas silikagelio kolonėlėje ir koncentruojamas. Perkristalinamas iš heksano. Lyd.t. 183°C.This example begins with the compound described in the article mentioned in Example 15. 0.02 mol of this compound is mixed with 15 ml of trifluoroacetic anhydride and a few drops of N, N-dimethylaniline under reflux, followed by boiling for 5 minutes and stirring overnight. The mixture is poured onto ice, basified and extracted with chloroform. Purify on a silica gel column and concentrate. Recrystallization from hexane. Melting point 183 ° C.

pavyzdys ll-Formil-6-(4-metilpiperazin-l-il)-HH-pirido (2,3b)benzo-1,4-diazepinasExample 11 11-Formyl-6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3b) benzo-1,4-diazepine

O // (I formulė: X=N-C , R1=R2=H, N,=benzenas, N2=piridinas H su N padėtyje d)O // (Formula I: X = NC, R 1 = R 2 = H, N, = Benzene, N 2 = Pyridine H with N in D)

Šis pavyzdys pradedamas 9 pavyzdžio junginiu, kuris formilinamas pagal 14 pavyzdžio metodiką. Lyd.t. 202°C.This example begins with the compound of Example 9, which is formylated according to the procedure of Example 14. Melting point Mp 202 ° C.

pavyzdysexample

10-(4-metilpiperazin-l-il)pirido(4,3-b)benzo-1,4tiazepinas (I formulė: X=S, R1=R2=H, N^benzenas, N2=piridinas su N padėtyje b)10- (4-Methylpiperazin-1-yl) pyrido (4,3-b) benzo-1,4-thiazepine (Formula I: X = S, R 1 = R 2 = H, N 2 - Benzene, N 2 = Pyridine with N in position b)

Pradedant tiazepinonu, aprašytu 5 sintezėje, aukščiau minėtas junginys gaunamas panaudojant 2 pavyzdžio metodiką. Lyd.t. 143-144°C.Starting with the thiazepinone described in Synthesis 5, the above compound is obtained using the procedure of Example 2. Melting point 143-144 ° C.

pavyzdysexample

5- (4-metilpiperazin-l-il)dibenzo(b,f)1,4-selenazepinas (I formulė: X=Se, R1=R2=H, N1=N2=benzenas)5- (4-Methylpiperazin-1-yl) dibenzo (b, f) 1,4-selenazepine (Formula I: X = Se, R 1 = R 2 = H, N 1 = N 2 = Benzene)

Pradedant 10H, HH-dibenzo(b,f)1,4-selenazepin-ll-onu, aukščiau paminėtas junginys gaunamas panaudojant 2 pavyzdžio metodiką. Lyd.t. 107°C.Starting with 10H, HH-dibenzo (b, f) 1,4-selenazepin-11-one, the above compound is obtained using the procedure of Example 2. Melting point Mp 107 ° C.

pavyzdysexample

6- (4-Metilpiperazin-l-il)dipirido(2,3-b:3',2'-f)1,4tiazepinas (I formulė: X=S, R1=R2=H, N1=N2=piridinas su N padėtyse d ir d')6- (4-Methylpiperazin-1-yl) dipyrido (2,3-b: 3 ', 2'-f) 1,4-thiazepine (Formula I: X = S, R 1 = R 2 = H, N 1 = N 2 = pyridine with N at positions d and d ')

Šis produktas gaminamas, pradedant junginiu, aprašytu 7 sintezėje ir panaudojant 2 pavyzdžio metodiką. Lyd.t. 170°C.This product is prepared starting from the compound described in Synthesis 7 and using the procedure of Example 2. Melting point 170 ° C.

pavyzdysexample

6-(4-Metilpiperazin-l-il)-11-metil-llH-pirido(2,3b)benzo-1,4-diazepinas (I formulė: X=N-CH3, R1=R2=H, N^benzenas, N2=piridinas su N padėtyje d)6- (4-Methylpiperazin-1-yl) -11-methyl-11 H -pyrido (2,3b) benzo-1,4-diazepine (Formula I: X = N-CH 3 , R 1 = R 2 = H, N ^ benzene, N 2 = pyridine with N in position d)

0,02 moliai 2-chloro-3-nitropiridino, 0,01 molio Nmetilantranilo rūgšties, 5 g bevandenio K2CO3 ir 50 ml sauso izopropanolio virinama su grįžtamu šaldytuvu 24 valandas. Išgarinus tirpiklį, liekana užpilama vandeniu ir virinama esant aktyvuotos anglies. Atšaldžius, tirpalas parūgštinamas iki pH apie 3. Produktas išsėda geltonų miltelių pavidale, ir jis yra filtruojamas, plaunamas vandeniu ir džiovinamas. Lyd.t. 174°C.0.02 mol of 2-chloro-3-nitropyridine, 0.01 mol of N-methylanthranilic acid, 5 g of anhydrous K 2 CO 3 and 50 ml of dry isopropanol are refluxed for 24 hours. After evaporation of the solvent, the residue is taken up in water and boiled in the presence of activated carbon. After cooling, the solution is acidified to pH about 3. The product settles as a yellow powder and is filtered, washed with water and dried. Melting point 174 ° C.

0,005 moliai gautos rūgšties suspenduojama bevandeniame eteryje. Junginys esterifikuojamas diazometanu, kuris gaminamas pradedant 4 g nitrozometilurėjos, pastarąją skaidant soda, esant eterio. Eterinis diazometano tirpalas po truputį pilamas ant nitratinės rūgšties eterinio tirpalo. Kai tik reakcija baigiasi, tirpiklis nugarinamas. Liekana apdorojama NaHCO3 tirpalu ir ekstrahuojama du kartus su CHC13. Chloroforminis tirpalas džiovinamas ir koncentruojamas, esant petrolio eterio 100-140. Išsikristalinęs produktas po to filtruojamas ir praplaunamas petrolio eteriu 40-60. Lyd.t. 71°C.0.005 mol of the resulting acid is suspended in anhydrous ether. The compound is esterified with diazomethane, which is prepared starting with 4 g of nitrosomethylurea, the latter being decomposed by soda in ether. The diazomethane ethereal solution is gradually added to the ethereal solution of nitric acid. As soon as the reaction is complete, the solvent is evaporated. The residue is treated with NaHCO 3 solution and extracted twice with CHCl 3 . The chloroform solution was dried and concentrated in the presence of 100-140 petroleum ether. The crystallized product is then filtered off and washed with petroleum ether 40-60. Melting point 71 ° C.

0,01 molio nitroesterio darinio (ištirpinto 150 ml etanolio) yra katalitiškai hidrinamas su paladžiu ant anglies (Pd/C 10%; 1 g) žemo slėgio hidrogeneratoriuje. Po 2 vai. reakcija baigiasi ir tirpiklis išgarinamas. Liekana (amino esteris) užpilama 50 ml anizolo ir supilama į apvaliadugnę kolbą. Pridedama 20 ml Nmetilpiperazino. Mišinys šildomas maišant prie 120°C. Ant mišinio atsargiai užpilamas 5 ml TiCl4 tirpalas 10 ml anizolo. Reakcijos turinys virinamas su grįžtamu šaldytuvu 12 valandų. Po to mišinys atšaldomas ir apdorojamas 10 ml izopropanolio, 10 ml koncentruoto amoniako ir 2 g silikagelio. Mišinys filtruojamas, ir surinktos nuosėdos rūpestingai praplaunamos chloroformu. Filtratas praplaunamas vieną kartą vandeniu ir po to ekstrahuojamas 2N HCl. Šis tirpalas dekolorizuojamas aktyvuota anglimi ir pašarminamas amoniaku. Susidarę nuosėdos ekstrahuojamos chloroformu. Chloroforminės frakcijos surenkamos ir koncentruojamos iki mažo tūrio. Gauta liekana gryninama silikagelio kolonėlėje, eliuentu naudojant acetono ir petrolio eterio 40-60 mišinį 9/1. Išskyrus, produktas perkristalinamas dichlormetano ir heksano mišinyje. Lyd.t. 146°C.0.01 mol of a nitroester derivative (dissolved in 150 ml of ethanol) is catalytically hydrogenated with palladium on carbon (Pd / C 10%; 1 g) in a low pressure hydrogen generator. After 2 or. the reaction is complete and the solvent is evaporated. Transfer the residue (amino ester) into 50 ml of anisole and transfer to a round-bottomed flask. 20 ml of N-methylpiperazine are added. The mixture is heated with stirring at 120 ° C. Carefully pour 5 ml of TiCl 4 solution into 10 ml of anisole. The reaction contents were refluxed for 12 hours. The mixture is then cooled and treated with 10 ml of isopropanol, 10 ml of concentrated ammonia and 2 g of silica gel. The mixture is filtered and the collected precipitate is carefully washed with chloroform. The filtrate is washed once with water and then extracted with 2N HCl. This solution is decolorized with activated carbon and basified with ammonia. The resulting precipitate is extracted with chloroform. Chloroform fractions were collected and concentrated to low volume. The resulting residue was purified on a silica gel column using acetone / petroleum ether 40-60 9/1 as eluent. Except, the product is recrystallized from a mixture of dichloromethane and hexane. Melting point 146 ° C.

Šio išradimo junginiai buvo tiriami farmakologiniais testais naudojamais nustatyti poveikiui į centrinę ir periferinę nervų sistemą. Sekantys rezultatai gauti iš 1, 10, 11, 17, 18 ir 19 pavyzdžių medžiagoms, patvirtina šias hipotezes ir tuo pačiu antidepresinį, antipsichotinį, anksiolitinį, neuroleptinį ir sedatyvinį šio išradimo junginių aktyvumą.The compounds of the present invention were tested by pharmacological tests used to determine effects on the central and peripheral nervous system. The following results from Examples 1, 10, 11, 17, 18 and 19 confirm the hypotheses and thus the antidepressant, antipsychotic, anxiolytic, neuroleptic and sedative activity of the compounds of this invention.

Tn vitro: Giminingumo testai D2 dopaminerginiams ir muskarinerginiams receptoriamsTn in vitro: Affinity assays for D 2 dopaminergic and muscarinic receptors

Kodas The code Inhibicija, % ('Hspiperono surišimas) Inhibition,% ('Hspiperone Binding) Inhibicija, % (3H QNB surišimas)Inhibition,% ( 3 H QNB binding) Klozapinas Klotiapinas Haloperidolis I pavyzdys 10 pavyzdys II pavyzdys 17 pavyzdys 18 pavyzdys 19 pavyzdys Clozapine Clothiapine Haloperidol Example I Example 10 Example II Example 17 Example 18 Example 19 57,3 94, 6 100 56, 2 31,5 24, 8 22,8 50,2 26, 7 57.3 94, 6 100 56, 2 31.5 24, 8 22.8 50.2 26, 7 80,35 38,05 0 4,48 62, 08 67,3 43,38 57,61 78, 31 80.35 38.05 0 4.48 62, 08 67.3 43.38 57.61 78, 31

D2 Dopaminerginiai receptoriai:D 2 Dopaminergic receptors:

Charakterizavimas ( H) spiperono pakeitimo testuCharacterization by (H) spiperone replacement test

Membranų paruošimas:Preparation of membranes:

Iš Wistar žiurkių patinėlių (200-250 g) pašalinamos smegenys. Latakėlis greitai perpjaunamas ir homogenizuojamas į 20 ml buferio (50 nM Tris/HCl, pH=7,4, 25°C) Teflon homogenizatoriaus pagalba. Homogenatas centri10 du minučių kartusMale Wistar rats (200-250 g) are removed from the brain. The gutter is rapidly cut and homogenized in 20 ml buffer (50 nM Tris / HCl, pH = 7.4, 25 ° C) using a Teflon homogenizer. Homogenate centri10 for two minutes

Galutinis fuguojamas 4 C temperatūroje ir 10000 G laikotarpyje, koncentratas praplaunamas lediniu buferiu ir recentrifuguoj amas koncentratas suspenduojamas lediniame buferyje (50 nM Tris/HCl, pH=7,4), turinčiame 5 nM magnio sulfato, 0,5 nM EDTA. Po rehomogenizavimo suspensija privedama iki 1 mg baltymo mililitre. Baltymo kiekis nustatomas Lowry ir kt. metodu (J.Biol.Chem., 193, 265-275 (1951)), kur standartu naudojamas jaučio serumo albuminas.The final is centrifuged at 4 ° C for 10,000 G, the concentrate is washed with ice buffer and the recentrifugation concentrate is suspended in ice buffer (50 nM Tris / HCl, pH 7.4) containing 5 nM magnesium sulfate, 0.5 nM EDTA. After rehomogenization, the suspension is brought to 1 mg of protein per ml. Protein content was determined by Lowry et al. (J. Biol. Chem. 193, 265-275 (1951)) using bovine serum albumin as the standard.

Surišimo testas:Binding test:

Yra naudojamas Tecott ir kt. pasiūlytas metodas (Biol. Psvchiatry 21, 1114-1122 (1986). (3H)-Spiperono surišimas Įvertinamas tokio mišinio pagalba: 200μ1 membranos preparato (0,1-0,2 mg baltymo), 100 μΐ (10~6 M) tiriamos medžiagos ir 600 μΐ buferio iki galutinio tūrio 1 ml. Kontroliniai mėgintuvėliai, kurie imami kaip nespecifinio surišimo standartai, taip pat turiIs used by Tecott et al. proposed method (Biol. Psvchiatry 21, 1114-1122 (1986). ( 3 H) -Spiperone Binding Estimated with the following mixture: 200μ1 membrane preparation (0.1-0.2 mg protein), 100 μΐ (10 ~ 6 M) of test substance and 600 μΐ buffer to a final volume of 1 ml. Control tubes, which are taken as non-specific binding standards, also have

1 μΜ(ι) butaklamolio. Pavyzdžiai (trigubai) po to inkubuojami su 0,5 nM (3H) spiperonu 25°C temperatūroje 60 minučių. Si stadija yra sustabdoma greitu vakuuminiu suspensijos filtravimu per stiklo tekstūros filtrą GF/C. Filtras praplaunamas tris kartus 5 ml ledinio buferio. Radioaktyvumas matuojamas skysčių scintiliacijos spektrometru (LKB Rack Beta 1219) . Rezultatai pateikiami procentų skirtumu tarp kontrolės (1μΜ(1 ) butaklamolio) ir tiriamos medžiagos.1 μΜ (ι) butaclamol. The samples (triplicate) were then incubated with 0.5 nM ( 3 H) spiperone at 25 ° C for 60 minutes. This step is stopped by rapid vacuum filtration of the suspension through a glass texture filter GF / C. Wash the filter three times with 5 ml of ice-buffer. Radioactivity is measured on a liquid scintillation spectrometer (LKB Rack Beta 1219). Results are expressed as percentage difference between control (1µΜ (1) butaclamol) and test substance.

Muskarikinių receptorių charakterizavimasCharacterization of muscarinic receptors

Surišimas su receptoriais:Receptor binding:

Metodas inspiruotas technika, aprašytas Yamamura irThe method is inspired by the technique described by Yamamura and

Snyder (Proc.Natl.Sci.USA 71, 1725 (1974)). Greitai pašalinus CFY, žiurkių smegenys (130-180 g) perpjaunamos, siekiant pašalinti smegenėles. Kiti audiniai homogenizuojami su Potter 0,32 M sacharozės ir 50 nM mris/HCl buferio pH 7,5 tirpale. Baltymo koncentracija įstatoma pagal Peterson metodą iAnai.Biochem. 83, 346Snyder (Proc.Natl.Sci.USA 71, 1725 (1974)). Following rapid removal of CFY, the rat brain (130-180 g) is incised to remove the cerebellum. Other tissues were homogenized with Potter in 0.32 M sucrose and 50 nM m ris / HCl buffer pH 7.5. Protein concentration is determined by the Peterson method iAnai.Biochem. 83, 346

977)) .977)).

išimo testas atliekamas Iris kartus 25°C peratūroje. . Inkubacinė terpė (1 ml) susideda iš 60the passage test is performed Iris times at 25 ° C. . The incubation medium (1 ml) consisted of 60

3r NaCl, Tris/HCl buferio su pH 7,5 ir 1,5 riM (3H) QNB3 r NaCl, Tris / HCl buffer with pH 7.5 and 1.5 riM ( 3 H) QNB

•)w England Nuclear, specifinis akt.: 1,18 TBq/mol) . akcija su homogenatu, turinčiu 250-400 ųg baltymo palaikoma 60 minučių. Nespecifinis surišimas realizuojamas 10’5 M atropinu. Veikimas sustabdomas, greitai filtruojant ant Whatman stiklo filtro GF/C. Laisvas ligandas pašalinamas tokiu būdu. Kiekvienas pavyzdys praplaunamas su 2x10 ml šalto buferio. Filtrai džiovinami, sudedami i tolueno tirpalą scintiliacij ai ir patalpinami i scintiliacini skaičiuoklį (Packard Tricarb skysčių scintiliaciojos skaičiuoklis) vienai dienai. Receptoriaus surišimas yra tiesiogiai proporcingas proteino koncentracijai iki 700 ųg baltymo mililitre.•) w England Nuclear, specific act: 1.18 TBq / mol). the action with the homogenate containing 250-400 µg of protein is maintained for 60 minutes. Non-specific binding is accomplished by 10 ' 5 M atropine. The operation is stopped by rapid filtration on a Whatman glass filter GF / C. The free ligand is removed in this manner. Each sample is washed with 2x10 ml cold buffer. The filters are dried, placed in a toluene solution for scintillation and placed in a scintillation counter (Packard Tricarb liquid scintillation counter) for one day. Receptor binding is directly proportional to a protein concentration of up to 700 µg protein per milliliter.

In vivo: Apomorfino antagonizmo testas.In vivo: Apomorphine antagonism assay.

Daugelis junginių, esant 20 mg/kg, mažina gyvūnų judrumą ir pasižymi sedatyviniu efektu, daugeliu atvejų junginiai rodo aktyvumą, kurio intensyvumas yra tarp klozapino (20 mg/kg) aktyvumo(į) ir haloperidolio (0,63 mg/kg) aktyvumo (Į į į į į) . Pateikiami tokie pavyzdžių rezultatai.Many compounds at 20 mg / kg decrease the motility of animals and have a sedative effect, in most cases the compounds show activity between the activity of clozapine (20 mg / kg) and haloperidol (0.63 mg / kg). In to in). The following sample results are given.

Pavyzdys An example 1 1 Pavyzdys An example 5 5 Pavyzdys An example 7 7th Pavyzdys An example 8 8th Pavyzdys An example 10 10th Pavyzdys An example 11 11th Pavyzdys An example 12 12th Pavyzdys An example 13 13th Pavyzdys An example 19 19th

Katalepsijos testasThe Catalepsy Test

Žr. GRAY W.D. OSTARBERG A. C., RAUH C. E.,See also: GRAY W.D. OSTARBERG A.C., RAUH C.E.,

Arch.Int.Pharmacodyn. 134, 198, 1961 ir Costall B.,Arch.Int.Pharmacodyn. 134, 198, 1961 and Costall B.,

Olley J.E. Neuropharmacology 10, 297, 1971.Olley J.E. Neuropharmacology 10, 297, 1971.

Šis testas yra būdingas ekstrapiramidaliniams efektams, kuriuos turi daugelis neuroleptikų (nepageidautinas antrinis efektas). Šio išradimo junginiai iššaukia labai mažą katalepsiją ir todėl nepasižymi šiuo nepageidautinu antriniu efektu. Tačiau kai kurie produktai rodė nežymią katalepsiją.This test is characterized by the extrapyramidal effects that many neuroleptics have (undesirable secondary effect). The compounds of the present invention induce very low catalepsy and thus do not exhibit this undesirable secondary effect. However, some products showed slight catalepsy.

- Pavyzdys 1 ir 3: katalepsija, esant dozėms virš 40 mg/kg- Examples 1 and 3: catalepsy at doses above 40 mg / kg

- Pavyzdys 4: silpnas kataleptinis efektas, pradedant 20 mg/kg dozėmis- Example 4: weak cataleptic effect starting at 20 mg / kg

- Klozapinas: silpnas kataleptinis efektas, pradedant 20 mg/kg dozėmis.- Clozapine: weak cataleptic effect at doses of 20 mg / kg.

Šis išradimas taip pat susijęs su farmacinėmis kompozicijomis, kurios turi savyje, kaip aktyvias sudedamąsias dalis, vieną arba daugiau junginių, atvaizduotų (I) formule, arba viena, arba su kitomis aktyviomis medžiagomis, turinčiomis panašius arba skirtingus efektus, mišinyje su atitinkamu farmaciniu užpildu.The present invention also relates to pharmaceutical compositions comprising, as active ingredients, one or more compounds represented by the formula (I) or one or other active substances with similar or different effects in admixture with a suitable pharmaceutical excipient.

Šios farmacinės kompozicijos gali būti kietos, kaip antai vienasluoksnės ar daugiasluoksnės nepadengtos ar padengtos tabletės, kapsulės, plėvelės, dispersabilūs ar tirpūs milteliai, žvakutės arba skystos, kaip antai, tirpalai, koloidai, suspensijos, emulsijos, sirupai, preparatai, skirti pareteriniam naudojimui, pavyzdžiui, aerozolių formoje.These pharmaceutical compositions may be solid, such as monolayer or multilayer uncoated or coated tablets, capsules, films, dispersible or soluble powders, suppositories or liquids, such as solutions, colloids, suspensions, emulsions, syrups, formulations for parenteral use, e.g. , in the form of aerosols.

Kietos kompozicijos, naudojamos per burną, gali būti gaminamos sumaišius vieną arba daugiau medžiagų, atitinkamai pagal šį išradimą, pavyzdžiui, su pieno cukrumi, cukraus pudra, krakmolu, talku, su produktais, skirtais sulaikyti arba prailginti efektą, pavyzdžiui, celiulizoės acetoftalatu, glicerilstearatais, jonitais.Solid compositions for oral use may be prepared by mixing one or more substances according to the present invention, for example, with milk sugar, sugar powder, starch, talc, products for retention or prolonging effect, such as cellulose acetophthalate, glyceryl stearates, ionic.

Žvakutės gali būti gaminamos, įterpiant vieną arba daugiau medžiagų, atitinkamai pagal šį išradimą, pavyzdžiui, į kakavos sviestą arba į bet kokią kitą atitinkamą medžiagą, tokią kaip sočiųjų riebiųjų rūgščių mono-, di- ir trigliceridus.The suppositories may be prepared by the incorporation of one or more substances according to the present invention, for example, into cocoa butter or any other suitable material such as mono-, di- and triglycerides of saturated fatty acids.

Skystos kompozicijos gali būti gaminamos, pavyzdžiui, ištirpinant, suspenduojant arba emulguojant paruošimo laiku arba tiesiogiai prieš naudojimą vieną ar daugiau medžiagų, atitinkamai pagal šį išradimą, ir, be to, bet kokį produktą, kurio buvimas laikomas pageidautinu ar reikalingu, kaip pavyzdžiui, apsaugantys agentai tokie kaip metil arba propil p-hidroksibenzoatai, tirštintojai ir emulgatoriai, tokie kaip celiuliozės dariniai ir sorbito polioksietilenesteriai, saldinančios medžiagos ir aromatinės medžiagos, tokios kaip cukrus, sacharinas, sorbitolis, natūralūs ar sintetiniai alkoholiai, izotonizatoriai, kaip natrio chloridas, arba buferiai, tokie kaip natrio fosfatai distiliuotame vandenyje, kituose priimtinuose hidroksiliniuose skysčiuose, tokiuose kaip etanolis, glicerinas, kai kurie glikoliai, šių tirpiklių mišiniuose arba farmaciškai priimtinuose aliejuose.Liquid compositions may be prepared, for example, by reconstitution, suspension or emulsification at the time of preparation or immediately prior to use of one or more substances, respectively, of the present invention, and, in addition, any product considered to be desirable or necessary such as methyl or propyl p-hydroxybenzoates, thickeners and emulsifiers such as cellulose derivatives and polyoxyethylene esters of sorbitol, sweetening and flavoring agents such as sugar, saccharin, sorbitol, natural or synthetic alcohols, isotonic agents such as sodium chloride, or buffers such as such as sodium phosphates in distilled water, other acceptable hydroxylic liquids such as ethanol, glycerol, some glycols, mixtures of these solvents, or pharmaceutically acceptable oils.

Claims (9)

IŠRADIMO APIBRĖŽTISDEFINITION OF INVENTION 1. Metiipiperazinazepino darinys, kurio bendra formulė I:1. Methipiperazine azepine derivative of general formula I: CH5 iCH 5 i kurioje:where: X yra deguonies atomas, sieros atomas, seleno atomas arba NH ar NR3 grupė, kurioje R3 yra -C , -CX is an oxygen atom, a sulfur atom, a selenium atom or a group NH or NR 3 wherein R 3 is -C, -C Ή 'CK grupė, arba nešakota ar šakota nuo 1 iki 4 anglies atomų turinti alkilo grupė;Ή 'CK group, or a straight or branched alkyl group containing from 1 to 4 carbon atoms; Rx yra vandenilio atomas, halogeno atomas arba šakota ar nešakota nuo 1 iki 4 anglies atomų turinti alkilo grupė;R x is a hydrogen atom, a halogen atom, or a branched or unbranched alkyl group containing from 1 to 4 carbon atoms; R2 yra vandenilio atomas, halogeno atomas arba šakota ar nešakota nuo 1 iki 4 anglies atomų turinti alkilo grupė; ir Nx yra benzeno žiedas ir N2 piridino žiedas arba atvirkščiai, su sąlyga, kad kai Rx ir R2 yra vandenilis, o X yra siera, deguonis ar NH grupė, Nx yra piridinas ir N2 benzenas, o piridino azotas nėra padėtyje d', ir abu, Nx ir N2, gali būti benzenas, kai X yra seleno atomas;R 2 is a hydrogen atom, a halogen atom, or a branched or unbranched alkyl group containing from 1 to 4 carbon atoms; and N x is a benzene ring and N 2 is a pyridine ring, or vice versa, provided that when R x and R 2 are hydrogen and X is sulfur, oxygen or NH, N x is pyridine and N 2 is benzene and pyridine nitrogen is not at position d ', both of N x and N 2 may be benzene when X is a selenium atom; arba farmaciškai priimtinos druskos.or pharmaceutically acceptable salts. 2. Darinys pagal 1 punktą, besiskiriantis tuo, kad I formulėje Rx yra vandenilio atomas arba metilo grupė.2. A derivative according to claim 1, wherein in formula I, R x is a hydrogen atom or a methyl group. 3. Darinys pagal 1 arba 2 punktą, besiskiriantis tuo, kad I formulėje R2 yra vandenilio atomas arba chloro atomas.3. A derivative according to claim 1 or 2, wherein in formula I, R 2 is a hydrogen atom or a chlorine atom. 4. Darinys pagal bet kurį iš 1-3 punktų, besiskiriantis tuo, kad jį gauna druskos pavidale, pasirinktos iš grupės, apimančios hidrochloridus, hidrobromidus, sulfatus, fosfatus, acetatus, citratus, maleatus, fumaratus ir metansulfonatus.4. A derivative according to any one of claims 1 to 3 which is obtained in the form of a salt selected from the group consisting of hydrochlorides, hydrobromides, sulfates, phosphates, acetates, citrates, maleates, fumarates and methanesulfonates. 5. Darinys pagal bet kurą iš 1-4 punktų, besiskiriantis tuo, kad jį pasirenka iš grupės, apimančios:A derivative according to any one of claims 1 to 4, wherein it is selected from the group consisting of: 11-(4-metilpiperazin-l-il)-5H-pirido(4,3-b)benzo1,5-diazepinas;11- (4-methylpiperazin-1-yl) -5H-pyrido (4,3-b) benzo-1,5-diazepine; 6-(4-metilpiperazin-l-il)-pirido(2,3-b)benzo-l,4tiazepinas;6- (4-methylpiperazin-1-yl) -pyrido (2,3-b) benzo-1,4-thiazepine; 8-chloro-6-(4-metilpiperazin-l-il)pirido(2,3b)benzo-1,4-tiazepino fumaratas;8-Chloro-6- (4-methylpiperazin-1-yl) pyrido (2,3b) benzo-1,4-thiazepine fumarate; 5-(4-metilpiperazin-l-il)-pirido(2,3-b)benzo-l,5oksazepino maleatas;5- (4-methylpiperazin-1-yl) -pyrido (2,3-b) benzo-1,5-oxazepine maleate; 8-chloro-5-(4-metilpiperazin-l-il)pirido(2,3b)benzo-l,5-oksazepino fumaratas;8-chloro-5- (4-methylpiperazin-1-yl) pyrido (2,3b) benzo-1,5-oxazepine fumarate; 5-(4-metilpiperazin-l-il)-8-metilpirido(2,3b)benzo-1,5-oksazepino fumaratas;5- (4-methylpiperazin-1-yl) -8-methylpyrido (2,3b) benzo-1,5-oxazepine fumarate; 6-(4-metilpiperazin-l-il)-pirido(2,3-b)benzo-l,4oksazepino fumaratas;6- (4-methylpiperazin-1-yl) -pyrido (2,3-b) benzo-1,4-oxazepine fumarate; 8- (chloro-6-(4-metilpiperazin-l-il)pirido(2,3b)benzo-1,4-oksazepino fumaratas;8- (chloro-6- (4-methylpiperazin-1-yl) pyrido (2,3b) benzo-1,4-oxazepine fumarate; 6- (4-metilpiperazin-l-il) -HH-pirido (2,3-b) benzo1,4-diazepinas;6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3-b) benzo-1,4-diazepine; 8- chloro-6-(4-metilpiperazin-l-il)-HH-pirido(2, 3b)benzo-1,4-diazepinas;8-chloro-6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3b) benzo-1,4-diazepine; 6-(4-metilpiperazin-l-il)-8-metil-llH-pirido(2,3b)benzo-1,4-diazepinas;6- (4-methylpiperazin-1-yl) -8-methyl-11H-pyrido (2,3b) benzo-1,4-diazepine; 9- chloro-6-(4-metilpiperazin-l-il)-HH-pirido(2,3b)benzo-l,4-diazepinas;9-chloro-6- (4-methylpiperazin-1-yl) -HH-pyrido (2,3b) benzo-1,4-diazepine; 8-fluoro-6~(4-metilpiperazin-l-il)-HH-pirido(2,3b)benzo-l,4-diazepinas;8-fluoro-6- (4-methylpiperazin-1-yl) -H-pyrido (2,3b) benzo-1,4-diazepine; 5-formil-ll-(4-metilpiperazin-l-il)-5H-pirido(4,3b)benzo-l,5-diazepinas;5-formyl-11- (4-methylpiperazin-1-yl) -5H-pyrido (4,3b) benzo-1,5-diazepine; ll-formil-5-(4-metilpiperazin-l-il)-HH-pirido (2,3-b)benzo-l,5-diazepinas;11-formyl-5- (4-methylpiperazin-1-yl) -HH-pyrido (2,3-b) benzo-1,5-diazepine; 11-trifluormetiikarboni1-5-(4-metilpiperazin-lil) -llH-pirido(2,3-b)benzo-l,5-diazepinas;11-trifluoromethylcarbonyl-5- (4-methylpiperazin-1-yl) -1H-pyrido (2,3-b) benzo-1,5-diazepine; 11 :ormil-6-(4-metilpiperazin-l-il)-llH-pirido ( -b)benzo-1,4-diazepinas;11 : ormyl-6- (4-methylpiperazin-1-yl) -IIH-pyrido (-b) benzo-1,4-diazepine; 10- 4-metilpiperazin-l-il)pirido(4,3-b)benzo-1,4ti .'.epinas;10- (4-methylpiperazin-1-yl) pyrido (4,3-b) benzo-1,4-thiophene; 5-(4-metilpiperazin-l-il)dibenzo(b,f)-1,4-selenazepinas;5- (4-methylpiperazin-1-yl) dibenzo (b, f) -1,4-selenazepine; 6-(4-metilpiperazin-l-il)dipirido(2,3—b:3’, 2'-f)1,4-tiazepinas;6- (4-methylpiperazin-1-yl) dipyrido (2,3-b: 3 ', 2'-f) 1,4-thiazepine; 6-(4-metilpiperazin-l-il)-11-metil-llH-pirido(2,3b)benzo-1,4-diazepinas.6- (4-methylpiperazin-1-yl) -11-methyl-11H-pyrido (2,3b) benzo-1,4-diazepine. 6. Metilpiperazinazepino darinių, atitinkančių bendrą I formulę, kurioje X, Rlr R2, N4 ir N2, turi aukščiau nustatytas reikšmes, gavimo būdas, besiskiriantis tuo, kad šį darinį gauna iš junginio, atitinkančio II formulę:Metilpiperazinazepino sixth derivatives of general Formula I in which X, R lr R 2, N 4 and N 2 have the above-stated values, the method characterized in that the derivative obtained by a compound corresponding to formula II: kurioje X, Rx ir R2, yra tokie, kaip nustatyta aukščiau ir kur Nx ir N2 kiekvienas yra benzeno žiedas arba piridino žiedas.wherein X, R x and R 2 are as defined above and wherein N x and N 2 are each a benzene ring or a pyridine ring. 7. Metilpiperazinazepino darinių, atitinkančių bendrą I formulę, kurioje X, Rlz R2, Nx ir N2 turi aukščiau nustatytas reikšmes, gavimo būdas, besiskiriantis tuo, kad šiuos darinius gauna iš ortohalogennitropiridino, atitinkančio V formulę:7. Metilpiperazinazepino derivatives of general Formula I in which X, R 2 R o, N x and N 2 have the above-stated meaning, said method characterized in that these derivatives receives from ortohalogennitropiridino corresponding to formula V: v, kurioje Hal yra halogeno atomas, toks kaip Cl, F, J arba Br ir benzenkarboninės rūgšties, atitinkančios VI formulę:v wherein Hal is a halogen atom such as Cl, F, J or Br and benzoic acid of formula VI: kurioje X toks, kaip anksčiau nustatyta, reakcijos produkto.wherein X is as previously defined in the reaction product. 8. Farmacinė kompozicija, besiskirianti tuo, kad susideda iš darinio, apibrėžto bet kuriame iš 1-5 punktų, sumaišyto su farmaciškai priimtinu užpildu arba pasirinktinai kitu terapiniu agentu.8. A pharmaceutical composition comprising a derivative as defined in any one of claims 1 to 5 in admixture with a pharmaceutically acceptable excipient or optionally another therapeutic agent. 9. Darinio pagal bet kurį iš 1-5 punktų panaudojimas preparatų, veikiančių centrinę arba periferinę nervų sistemą ir turinčių tokį poveikį, kaip antidepresinį, antipsichotinį, anksiolitinį, neuroleptinį arba sedatyvinį, gamybai.Use of a derivative according to any one of claims 1 to 5 for the manufacture of a preparation having a central or peripheral nervous system action, such as antidepressant, antipsychotic, anxiolytic, neuroleptic or sedative.
LTIP378A 1990-09-26 1993-03-03 Methylpiperazinoazepine derivatives, preparation and use tereof LT3231B (en)

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