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SK21698A3 - Novel 1-ar(alk)yl-imidazolin-2-ones containing a disubstituted amine radical in the 4th position, having an anti-convulsive effect, and process for their production - Google Patents

Novel 1-ar(alk)yl-imidazolin-2-ones containing a disubstituted amine radical in the 4th position, having an anti-convulsive effect, and process for their production Download PDF

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SK21698A3
SK21698A3 SK216-98A SK21698A SK21698A3 SK 21698 A3 SK21698 A3 SK 21698A3 SK 21698 A SK21698 A SK 21698A SK 21698 A3 SK21698 A3 SK 21698A3
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morpholinoimidazolin
chlorophenyl
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SK284868B6 (en
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Hans-Joachim Lankau
Manfred Menzer
Klaus Unverferth
Karl Gewald
Harry Schafer
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Dresden Arzneimittel
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D233/00Heterocyclic compounds containing 1,3-diazole or hydrogenated 1,3-diazole rings, not condensed with other rings
    • C07D233/54Heterocyclic compounds containing 1,3-diazole or hydrogenated 1,3-diazole rings, not condensed with other rings having two double bonds between ring members or between ring members and non-ring members
    • C07D233/66Heterocyclic compounds containing 1,3-diazole or hydrogenated 1,3-diazole rings, not condensed with other rings having two double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
    • C07D233/88Nitrogen atoms, e.g. allantoin
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    • A61P21/00Drugs for disorders of the muscular or neuromuscular system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P21/00Drugs for disorders of the muscular or neuromuscular system
    • A61P21/02Muscle relaxants, e.g. for tetanus or cramps
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/08Antiepileptics; Anticonvulsants

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Abstract

Compounds with an anti-convulsive effect of general formula (1) in which X = hydrogen, C1-C4 alkyl, C1-C4 alkoxy, trifluoromethyl, halogen and R<1> or R<2> = C1-C4 alkyl, cycloalkyl or heteroalkyl.

Description

- AR (ALK) YLIMIDAZOLÍN - 2 - ÓNY OBAHUJÚCE V POLOHE 4 DISUBSTITUOVANÝ AMÍNOVÝ ZVYŠOK A SPÔSOB ICH PRÍPRAVY- AR (ALK) YLIMIDAZOLINE - 2 - OONS CONTAINING IN POSITION 4 DISUBSTITUTED AMINE RESIDUE AND METHOD OF PREPARATION

Oblasť technikyTechnical field

Vynález sa týka 1 - ar (alk) ylimidazolín - 2 - ónov, ktoré obsahujú dis'ubstituovaný amínový zvyšok v polohe 4, spôsobov ich prípravy a ich použitia ako farmaceutických prostriedkov na ošetrovanie porúch centrálneho nervového systému, najmä rôznych foriem epilepsií.The invention relates to 1-ar (alk) ylimidazolin-2-ones containing a disubstituted amine residue at the 4-position, to processes for their preparation and to their use as pharmaceutical compositions for the treatment of central nervous system disorders, in particular various forms of epilepsy.

Doterajší stav technikyBACKGROUND OF THE INVENTION

- ar (alk) ylimidazolín - 2 - óny s nesubstituovaným amínovým alebo metylamínovým zvyškom v polohe 4 sa pripravujú podľa doterajšieho stavu techniky reakciou 1 - ar (alk) yliminoacetamidov s brómkyánom. N-alkyláciou 4-amino 1ar(alk)ylimidazolín-2-ónov, pripravovaných týmto spôsobom, sa získajú 3-alkyl-, alebo 1-iminoalkyl-3-alkyl-1-ar(alk)ylimidazolín-2-óny pri tautomerizácii aminoskupiny na iminoskupinu v polohe 4. Ďalšia N - alkylácia vedúca ku zlúčeninám so všeobecným vzorcom 1 teda nie je možná, takže zlúčeniny podľa tohto vynálezu sa nemôžu týmto spôsobom pripravovať [USP 4 044 021, DE 2 251 354],The ar (alk) ylimidazolin-2-ones with an unsubstituted amine or methylamine residue at the 4-position are prepared according to the prior art by reacting 1-ar (alk) yliminoacetamides with cyanogen bromide. N-alkylation of the 4-amino-1 &apos; (alk) ylimidazolin-2-ones prepared in this way gives 3-alkyl- or 1-iminoalkyl-3-alkyl-1-ar (alk) ylimidazolin-2-ones by tautomerization of the amino group Thus, further N-alkylation leading to the compounds of formula 1 is not possible, so that the compounds of the present invention cannot be prepared in this way [US 4 044 021, DE 2 251 354],

- ar (alk) ylimidazolín - 2 - óny s disubstituovaným amínovým zvyškom v polohe 4 doposiaľ neboli opísané.ar (alk) ylimidazolin-2-ones with a disubstituted amine residue at the 4-position have not been described.

Je známy veľký počet zlúčenín s antikonvulzívnou aktivitou. V podstate ani dnes nemôžu byť všetky formy epilepsie uspokojivo liečené.A large number of compounds with anticonvulsant activity are known. In fact, even today, all forms of epilepsy cannot be treated satisfactorily.

Podstata vynálezuSUMMARY OF THE INVENTION

Vynález sa teda zakladá na predmete tvorby dostupných nových zlúčenín s výhodnými farmakologickými vlastnosťami, ktoré môžu byť využité napríklad ako látky s antiepileptickou aktivitou.Accordingly, the invention is based on the object of making available novel compounds with advantageous pharmacological properties, which can be used, for example, as substances with antiepileptic activity.

30894/H30894 / H

Podľa tohto vynálezu tieto nové zlúčeniny sú 1 - ar (alk) ylimidazolín - 2 - óny so všeobecným vzorcom 1According to the present invention, these novel compounds are 1-ar (alk) ylimidazolin-2-ones of formula 1

kde n je 0 alebo 1, m je 0,1, 2, 3, 4 alebo 5, x znamená atóm vodíka, C-i- C4- alkyl, C1- C4- alkoxyskupinu, trifluórmetyl alebo atóm halogénu,where n is 0 or 1, m is 0, 1, 2, 3, 4 or 5, x is hydrogen, C 1 -C 4 -alkyl, C 1 -C 4 -alkoxy, trifluoromethyl or halogen,

R1 a R2 predstavujú Cr C4- alkyl, cykloalkyl alebo heteroalkyl, pričom alkylová skupina obsahuje vždy 5 až 7 atómov uhlíka, aleboR 1 and R 2 represent C 1 -C 4 -alkyl, cycloalkyl or heteroalkyl, each alkyl group having 5 to 7 carbon atoms, or

R1 a R2 tvoria dohromady alkylénovú skupinu s 2 až 6 atómami uhlíka, kde -CH2skupina môže byť nahradená kyslíkom, dusíkom, alebo sírou.R 1 and R 2 together form an alkylene group having 2 to 6 carbon atoms, wherein the -CH 2 group may be replaced by oxygen, nitrogen, or sulfur.

Počet CH2 skupín je buď 0 (1 - arylimidazolín - 2 - óny) alebo 1 (1 aralkylimidazolín - 2 - óny).The number of CH 2 groups is either 0 (1-aryllimidazolin-2-one) or 1 (1-aralkylimidazolin-2-one).

Príklady zlúčenín so všeobecným vzorcom 1, ktoré je možné uviesť, sú:Examples of compounds of formula 1 that may be mentioned are:

- fenyl - 4 - morfolinoimidazolín - 2 - ón,- phenyl-4-morpholinoimidazolin-2-one,

- (4 - metoxy) - 4 - piperidínoimidazolín - 2 - ón,- (4-Methoxy) -4-piperidinoimidazolin-2-one,

- (4 - chlórfenyl) - 4 - morfolinoimidazolín - 2 - ón,- (4-chlorophenyl) -4-morpholinoimidazolin-2-one,

- (4 - chlórfenyl) - 4 - piperidínoimidazolín - 2 - ón,- (4-chlorophenyl) -4-piperidinoimidazolin-2-one,

- (4 - chlórfenyl) - 4 - dimetylaminoimidazolín - 2 - ón,- (4-chlorophenyl) -4-dimethylaminoimidazolin-2-one,

- (4 - brómfenyl) - 4 - morfolinoimidazolín - 2 - ón,- (4-bromophenyl) -4-morpholinoimidazolin-2-one,

- (3 - chlórfenyl) - 4 - morfolinoimidazolín - 2 - ón,- (3-chlorophenyl) -4-morpholinoimidazolin-2-one,

- (4 - chlórfenyl) - 4 - hexametyléniminoimidazolín - 2 - ón,- (4-chlorophenyl) -4-hexamethyleniminoimidazolin-2-one,

- (4 - chlórfenyl) - 4 - (metylpiperazíno) imidazolín - 2 - ón,- (4-chlorophenyl) -4- (methylpiperazino) imidazolin-2-one,

- (4 - metylfenyl) - 4 - morfolinoimidazolín - 2 - ón,- (4-methylphenyl) -4-morpholinoimidazolin-2-one,

- (4 - chlórfenyl) -4 - (cyklohexylmetylamíno) imidazoiín - 2 - ón,- (4-chlorophenyl) -4- (cyclohexylmethylamino) imidazolin-2-one,

- (4 - fluórfenyI) - 4 - morfolinoimidazolín - 2 - ón a- (4 - fluorophenyl) -4 - morpholinoimidazolin - 2 - one a

- benzyl - 4 - morfolinoimidazolín -- 2 - ón.- benzyl - 4 - morpholinoimidazolin - 2 - one.

30894/H30894 / H

Podľa tohto vynálezu sa môžu zlúčeniny so všeobecným vzorcom 1 pripravovať novým spôsobom prípravy, reakciou zlúčenín so všeobecným vzorcom 2According to the present invention, compounds of formula 1 can be prepared by a novel method of preparation, by reacting compounds of formula 2

H kde n je 0 alebo 1, m je 0, 1, 2, 3, 4, alebo 5, x znamená atóm vodíka, Ci- C4- alkyl, Cr C4- alkoxyskupinu, trifluórmetyl alebo atóm halogénu, so sekundárnym amínom.H wherein n is 0 or 1, m is 0, 1, 2, 3, 4, or 5, x is H, C C 4 - alkyl, C r C 4 - alkoxy, trifluoromethyl or halogen, with a secondary amine .

Príprava zlúčenín so vzorcom 1 sa môže inak uskutočniť v rozpúšťadle alebo v nadbytku sekundárneho amínu pri teplotách medzi 50 °C a 160 °C. Vhodné rozpúšťadlá sú predovšetkým aromatické uhľovodíky, napríklad benzén, toluén, chlórbenzén alebo dichlórbenzén.Alternatively, the preparation of the compounds of formula 1 can be carried out in a solvent or in an excess of the secondary amine at temperatures between 50 ° C and 160 ° C. Suitable solvents are, in particular, aromatic hydrocarbons, for example benzene, toluene, chlorobenzene or dichlorobenzene.

Reakcia sa predovšetkým uskutočňuje v prítomnosti látok viažucich vodu, ako zeolitov alebo síranu sodného. Reakcia môže byť urýchlená pridaním všeobecne užívaného katalyzátora kondenzácie, ako je 4 -toluénsulfónová kyselina.In particular, the reaction is carried out in the presence of water binders, such as zeolites or sodium sulfate. The reaction may be accelerated by the addition of a commonly used condensation catalyst such as 4-toluenesulfonic acid.

Zlúčeniny podľa vynálezu sú vhodné na prípravu farmaceutických prostriedkov. Farmaceutické prostriedky môžu obsahovať jednu alebo viacero zlúčenín podľa vynálezu. Na prípravu farmaceutických prostriedkov sa môžu použiť zvyčajné farmaceutické expicienty a pomocné látky.The compounds of the invention are suitable for the preparation of pharmaceutical compositions. The pharmaceutical compositions may contain one or more compounds of the invention. Conventional pharmaceutical excipients and excipients may be used to prepare the pharmaceutical compositions.

Lieky vhodné na podávanie sa môžu pripravovať spôsobmi, ktoré sú všeobecne známe a zvyčajné vo farmaceutickej praxi.Medicaments suitable for administration may be prepared by methods well known and customary in pharmaceutical practice.

Zlúčeniny podľa vynálezu majú výrazný antikonvulzívny účinok.The compounds of the invention have a pronounced anticonvulsant effect.

Pre svoj antikonvulzívny účinok boli testované in vivo po i.p. (interperitoneálnom) podaní myšiam alebo krysám (p.o. - perorálne podanie), podľaBecause of their anticonvulsant effect, they were tested in vivo after i.p. (interperitoneal) administration to mice or rats (p.o. - oral administration), according to

30894/H medzinárodne zvyčajného štandardu (Pharmac. Weekblad, Sc. Ed. 14, 132 (1992) a Antiepileptic Drugs, 3. Vyd., Raven Press, New York (1989) (Tabuľka 1)).30894 / H of the International Standard (Pharmac. Weekblad, Sc. Ed. 14, 132 (1992) and Antiepileptic Drugs, 3rd Ed., Raven Press, New York (1989) (Table 1)).

Napríklad pre zlúčeninu 2, (1-(4- chlórfenyl) - 4 - morfolinoimidazolín - 2 on) u krysy bola stanovená dávka ED50 (p.o) pre maximálny elektrošok 21 mg/kg, ED50 v s.c. penterazolovom teste bola stanovená 16 mg/kg a NT50 pre neurotoxicitu bola stanovená > 400 mg/kg. V porovnaní s tým sú známe antiepileptiká účinné v maximálnom elektrošokovom modeli alebo v pentetrazolovom teste, alebo, v prípade relatívne vysokej aktivity, sú silne neurotoxické v PTZ teste.For example, for compound 2, (1- (4-chlorophenyl) -4-morpholinoimidazolin-2-one) in the rat, the ED50 (p.o) dose for the maximum electroshock 21 mg / kg, ED50 in s.c. the penterazole assay was determined to be 16 mg / kg and the NT50 for neurotoxicity was> 400 mg / kg. In contrast, known antiepileptic drugs are effective in a maximum electroshock model or in a pentetrazole assay, or, in the case of relatively high activity, are highly neurotoxic in a PTZ assay.

30894/H30894 / H

Tabuľka 1Table 1

zlúčenina podlá pr. the compound according to Ex. Log p2Log p 2 ' Test31 Test 31 Dávka4Batch 4 ' Účinnosť5Efficiency 5 ' 1 1 MES MES 100 100 30 30 0, 64 0, 64 PTZ PTZ 100 100 30 30 2 2 MES MES 300 300 30 30 1, 48 1, 48 PTZ PTZ 30 30 70 70 3 3 MES MES 100 100 100 100 2, 29 2, 29 PTZ PTZ 100 100 100 100 4 4 MES MES 300 300 30 30 0, 48 0, 48 PTZ PTZ 300 300 30 30 5 5 MES MES 300 300 100 100 2, 17 2, 17 PTZ PTZ 300 300 100 100 6 6 MES MES 300 300 100 100 1, 61 1, 61 PTZ PTZ 100 100 20 20 7 7 MES MES 300 300 100 100 1,53 1.53 PTZ PTZ 100 100 100 100 8 8 MES MES 300 300 30 30 1, 45 1, 45 PTZ PTZ 100 100 100 100 9 9 MES MES 100 100 30 30 0, 97 0, 97 PTZ PTZ 100 100 100 100 10 10 MES MES 300 300 10 10 1,28 1.28 PTZ PTZ 300 300 70 70 11 11 MES MES 300 300 100 100 2, 56 2, 56 PTZ PTZ 300 300 40 40

Porovnávacia látka Reference substance Test3Test 3 ' Dávka4Batch 4 ' Účinnosť5Efficiency 5 ' Karbamazepín carbamazepine MES MES 100 100 100 100 PTZ PTZ 100 100 0 0 Valproát valproate MES MES 100 100 0 0 PTZ PTZ 100 100 30 30

30894/H30894 / H

Poznámky k tabuľke 1:Notes to Table 1:

1) Očíslovanie zlúčenín viď. pracovné príklady1) For compound numbering, see p. working examples

2) Rozdeľovači koeficient oktanol / voda2) Octanol / water partition coefficient

3) MES = maximálny elektrošok, PTZ = pentetrazol podaný s.c.3) MES = maximum electroshock, PTZ = pentetrazole administered s.c.

4) v mg/kg4) in mg / kg

5) v % ochránených zvierat5) in% of protected animals

Príklady uskutočnenia vynálezuDETAILED DESCRIPTION OF THE INVENTION

Príprava nových zlúčenín so všeobecným vzorcom 1 bude bližšie vysvetlená prostredníctvom pracovných príkladov.The preparation of the novel compounds of formula 1 will be explained in more detail by way of working examples.

Pracovné príkladyWorking examples

Všeobecný postup prípravy zlúčenín so všeobecným vzorcom 1 podľa tabuľky 1, príklady 1 až 11.General Procedure for the Preparation of Compounds of Formula 1 according to Table 1, Examples 1 to 11.

Variant AVariant A

0,05 mol 1 - arylimidazolín - 2,4 - dión so všeobecným vzorcom 2 (n = 0), 200 mg 4 - toluénsulfónovej kyseliny sa pridá k 100 ml príslušného sekundárneho amínu. Zmes sa potom zahrieva pod spätným chladičom v Soxhletovom extraktore za predchádzajúceho naplnenia exrakčného nadstavca 25 g vodou - viažúcou pevné látky (vhodné sú síran sódno - vápenatý, síran horečnatý, NaOH, KOH, zeolity). Po reakčnom čase od 8 do 30 hodín sa roztok sfiltruje za tepla a destiluje do približne polovičného objemu v rotačnej odparovačke. Číry roztok sa ochladí ľadovým kúpeľom a získaná kryštalická zmes sa oddelí od amínu. Východisková látka obsiahnutá v surovom produkte sa extrahuje 50 ml horúceho acetónu. Produkt sa rekryštalizuje z n - propanolu.0.05 mol of 1-arylimidazoline-2,4-dione of formula 2 (n = 0), 200 mg of 4-toluenesulfonic acid are added to 100 ml of the corresponding secondary amine. The mixture is then heated to reflux in a Soxhlet extractor with a pre-charge of 25 g of water-binding solids with an extraction tube (sodium-calcium sulfate, magnesium sulfate, NaOH, KOH, zeolites). After a reaction time of 8 to 30 hours, the solution is filtered hot and distilled to approximately half the volume in a rotary evaporator. The clear solution was cooled with an ice bath and the resulting crystalline mixture was separated from the amine. The starting material contained in the crude product is extracted with 50 ml of hot acetone. The product is recrystallized from n-propanol.

Z neoddeleného amínu sa môže znovu získať okolo 0,02 mol nezreagovaného 1 - arylimidazolín - 2,4 - diónu.From the non-separated amine, about 0.02 mol of unreacted 1-arylimidazoline-2,4-dione can be recovered.

Variant BVariant B

0,05 mol 1 - aralkylimidazolín - 2,4 - dión so všeobecným vzorcom 2 (n = 1) sa nechá reagovať so sekundárnym amínom, ako je opísané pod A. Po reakčnom čase od 8 do 30 hodín sa roztok za tepla sfiltruje, a potom sa odparí do sucha0.05 mol of 1-aralkylimidazoline-2,4-dione of formula 2 (n = 1) is reacted with a secondary amine as described under A. After a reaction time of 8 to 30 hours, the solution is filtered hot, and then evaporated to dryness

30894/H v rotačnej odparovačke. K odparku látke sa pridá 50 ml dichlórmetánu a 50 ml 2N (mol/l) HCI. Organická fáza sa oddelí a vodná fáza ešte dvakrát extrahuje dichlórmetánom. Izolovaná vodná fáza sa alkalizuje 50 ml 10 % NaOH a 1 - 4 amino - 1 - aralkylimidazolín - 2 - ón sa extrahuje 100 ml dichlórmetánu. Esterové extrakty sa sušia síranom sodným. Po oddestilovaní dichlórmetánu sa surový produkt rekryštalizuje z etanolu alebo acetónu.30894 / H in rotary evaporator. To the residue was added 50 mL of dichloromethane and 50 mL of 2N (mol / L) HCl. The organic phase is separated and the aqueous phase is extracted twice more with dichloromethane. The isolated aqueous phase was basified with 50 ml of 10% NaOH and the 1-4 amino-1-aralkylimidazolin-2-one was extracted with 100 ml of dichloromethane. The ester extracts were dried over sodium sulfate. After distilling off the dichloromethane, the crude product is recrystallized from ethanol or acetone.

Variant CVariant C

0,05 mol 1 - ar (alk) ylimidazolín - 2,4 - diónu so všeobecným vzorcom 2 sa nechá reagovať so 100 ml dimetylamónium dimetylkarbamátu, ako je opísané pod A a B. Po reakčnom čase 40 hodín sa zmes spracuje podľa varianty A alebo B.0.05 mol of 1-ar (alk) ylimidazoline-2,4-dione of formula 2 is reacted with 100 ml of dimethylammonium dimethylcarbamate as described under A and B. After a reaction time of 40 hours, the mixture is worked up according to variant A or B.

30894/H30894 / H

Tabuľka 2Table 2

Pr. Pr. R1 R 1 R2 R 2 Var boiling Reakčný čas(hod) Response time (hours) Tepl. top.fC) Temp. top.fC) Výťažok (%) yield (%) 1 1 -o -about —\ /° - \ / ° A A 15 15 248 248 42 1)42 1 ) 2 2 /“X — N 0 / "X - N 0 A A 15 15 266 266 75 n 75 n 3 3 -O“ -ABOUT" -3 -3 A A 20 20 246 246 60 1)60 1 ) 4 4 -ch4Ž)- ch 4F) N\ z°- N \ z ° B B 15 15 158 158 48 48 5 5 C α C α /—\ — N N-CM, \t / - \ - N N-CM \ t A A 12 12 254 254 68 1)68 1 ) 6 6 ~Ό^α ~ Ό ^ α CH., z J — N CH,CH., From J - N CH, C C ' 40 '40 292 292 13 13 7 7 -o -about A A 30 30 190 190 52U 52U 8 8 — Nl\__ Q - Nl \ __ Q A A 15 15 268 268 65 1)65 1 ) 9 9 — \ /° - \ / ° A A 18 18 255 255 54 O 54 O 10 10 Cl -ó Cl -about — t/ \> - t / \> B B 30 30 237 237 27 27 11 11 -O -ABOUT A A 8 8 216 216 88 1)88 1 )

1) pri počítaní výťažku sa započítali opätovne získané východiskové materiály 1) The recovered starting materials were included in the yield calculation

30894/H30894 / H

Claims (7)

1. Nová zlúčenina so všeobecným vzorcom 1 kde n je 0 alebo 1, m je 0,1, 2, 3, 4 alebo 5, x znamená atóm vodíka, Cp C4- alkyl, C1- C4- alkoxyskupinu, trifluórmetyl alebo atóm halogénu,A novel compound of formula 1 wherein n is 0 or 1, m is 0, 1, 2, 3, 4 or 5, x is hydrogen, C 1 -C 4 -alkyl, C 1 -C 4 -alkoxy, trifluoromethyl or halogen, R1 a R2 znamenajú C1- C4- alkyl, cykloalkyl alebo heteroalkyl pričom alkylová skupinaR 1 and R 2 are C 1 -C 4 -alkyl, cycloalkyl or heteroalkyl wherein the alkyl group I 1 obsahuje vždy 5 až 7 atómov uhlíka, aleboI 1 always contains 5 to 7 carbon atoms, or R1 a R2 tvoria spolu alkylénovú skupinu s 2 až 6 atómami uhlíka, kde -CH2- skupina môže byť nahradená kyslíkom, dusíkom, alebo sírou.R 1 and R 2 together form an alkylene group having 2 to 6 carbon atoms, wherein the -CH 2 - group may be replaced by oxygen, nitrogen, or sulfur. 2. Zlúčenina podľa nároku 1, ktorou jeA compound according to claim 1 which is 1 - fenyl - 4 - morfolinoimidazolín - 2 - ón,1-phenyl-4-morpholinoimidazolin-2-one, 1 - (4 - metoxy) - 4 - piperidínoimidazolín - 2 - ón,1- (4-methoxy) -4-piperidinoimidazolin-2-one, 1 - (4 - chlórfenyl) - 4 - morfolinoimidazolín - 2 - ón,1- (4-chlorophenyl) -4-morpholinoimidazolin-2-one, 1 - (4 - chlórfenyl) - 4 - piperidínoimidazolín - 2 - ón,1- (4-chlorophenyl) -4-piperidinoimidazolin-2-one, 1 - (4 - chlórfenyl) - 4 - dimetylamínoimidazolín - 2 - ón,1- (4-chlorophenyl) -4-dimethylaminoimidazolin-2-one, 1 - (4 - brómfenyl) - 4 - morfolinoimidazolín - 2 - ón,1- (4-bromophenyl) -4-morpholinoimidazolin-2-one, 1 - (3 - chlórfenyl) - 4 - morfolinoimidazolín - 2 - ón,1- (3-chlorophenyl) -4-morpholinoimidazolin-2-one, 1 - (4 - chlórfenyl) - 4 - hexametyléniminoimidazolín - 2 - ón,1- (4-chlorophenyl) -4-hexamethyleniminoimidazolin-2-one, 1 - (4 - chlórfenyl) - 4 - (metylpiperazíno) imidazolín - 2 - ón,1- (4-chlorophenyl) -4- (methylpiperazino) imidazolin-2-one, 1 - (4 - metylfenyl) - 4 - morfolinoimidazolín - 2 - ón,1- (4-Methylphenyl) -4-morpholinoimidazolin-2-one 1 - (4 - chlórfenyl) - 4 - (cyklohexylmetylamíno) imidazolín - 2 - ón,1- (4-chlorophenyl) -4- (cyclohexylmethylamino) imidazolin-2-one, -|_(4_ fluórfenyl) - 4 - morfolinoimidazolín - 2 - ón a- | - (4-fluorophenyl) -4-morpholinoimidazolin-2-one a 1 - benzyl - 4 - morfolinoimidazolín - 2 - ón.1-Benzyl-4-morpholinoimidazolin-2-one. 30894/H30894 / H 3. Spôsob prípravy zlúčenín so všeobecným vzorcom 1, vyznačujúci sa tým, že sa zlúčeniny so všeobecným vzorcom 2 (2) kde x znamená atóm vodíka, Cr C4- alkyl, Cr C4- alkoxyskupinu, trifluórmetyl alebo atóm halogénu, nechajú reagovať so sekundárnym amínom so všeobecným vzorcom HNR1R2 , kde R1 a R2 majú význam uvedený vyššie, pri teplote od 50 °C do 160 °C.3. A process for the preparation of compounds of general formula 1, characterized in that the compound of formula 2 (2) wherein X is hydrogen, Cr C 4 - alkyl, C r C 4 - alkoxy, trifluoromethyl or halogen, are reacted with a secondary amine of the formula HNR 1 R 2 , wherein R 1 and R 2 are as defined above, at a temperature of from 50 ° C to 160 ° C. 4. Farmaceutický prostriedok, vyznačujúci sa tým, že ako aktívnu látku obsahuje aspoň jednu zlúčeninu so všeobecným vzorcom 1, a prípadne farmaceutické expicienty a pomocné látky.Pharmaceutical composition, characterized in that it contains at least one compound of the general formula 1 as active substance and optionally pharmaceutical excipients and auxiliaries. 5. Farmaceutický prostriedok podľa nároku 4, vyznačujúci sa tým, že ako aktívne látky obsahuje aspoň jednu zo zlúčenín podľa nároku 2..Pharmaceutical composition according to claim 4, characterized in that it contains as active substances at least one of the compounds according to claim 2. 6. Použitie zlúčeniny so všeobecným vzorcom 1 na výrobu liekov na ošetrovanie epileptických porúch.Use of a compound of formula 1 for the manufacture of a medicament for the treatment of epileptic disorders. 7. Použitie zlúčeniny podľa nároku 2 na výrobu liekov na ošetrovanie epileptických porúch.Use of a compound according to claim 2 for the manufacture of a medicament for the treatment of epileptic disorders.
SK216-98A 1995-09-05 1996-07-26 1-Ar(alk)yl-imidazolin-2-ones, process for their production, use of them and pharmaceutical composition containing them SK284868B6 (en)

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DE19532668A DE19532668A1 (en) 1995-09-05 1995-09-05 Novel, anticonvulsant 1-ar (alk) yl-imidazolin-2-ones which contain a disubstituted amine radical in the 4-position, and process for their preparation
PCT/EP1996/003295 WO1997009314A1 (en) 1995-09-05 1996-07-26 Novel 1-ar(alk)yl-imidazolin-2-ones containing a disubstituted amine radical in the 4th position, having an anti-convulsive effect, and process for their production

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US20050070537A1 (en) * 2002-10-10 2005-03-31 Chris Rundfeldt Use of dihydroimidazolones for the treatment of dogs
RU2354377C2 (en) * 2003-07-11 2009-05-10 Берингер Ингельхайм Ветмедика Гмбх Method of treatment or prevention of central nervous system diseases by means of compounds possessing selectivity with respect to alpha-3-subunit of benzodiazepine receptor
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US9820988B2 (en) 2014-03-24 2017-11-21 Boehringer Ingelheim Vetmedica Gmbh Treatment of epileptic disorders in feline animals
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