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FI114395B - Process for Preparation of Esters and Intermediate Pharmacologically Efficient Thienyl Carboxylic Acids and Amino Alcohols - Google Patents

Process for Preparation of Esters and Intermediate Pharmacologically Efficient Thienyl Carboxylic Acids and Amino Alcohols Download PDF

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FI114395B
FI114395B FI921087A FI921087A FI114395B FI 114395 B FI114395 B FI 114395B FI 921087 A FI921087 A FI 921087A FI 921087 A FI921087 A FI 921087A FI 114395 B FI114395 B FI 114395B
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thienyl
tropanyl
formula
epoxy
methyl
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FI921087A0 (en
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Rolf Banholzer
Richard Reichl
Rudolf Bauer
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Boehringer Ingelheim Pharma
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D451/00Heterocyclic compounds containing 8-azabicyclo [3.2.1] octane, 9-azabicyclo [3.3.1] nonane, or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane or granatane alkaloids, scopolamine; Cyclic acetals thereof
    • C07D451/14Heterocyclic compounds containing 8-azabicyclo [3.2.1] octane, 9-azabicyclo [3.3.1] nonane, or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane or granatane alkaloids, scopolamine; Cyclic acetals thereof containing 9-azabicyclo [3.3.1] nonane ring systems, e.g. granatane, 2-aza-adamantane; Cyclic acetals thereof
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P11/00Drugs for disorders of the respiratory system
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
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    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D451/00Heterocyclic compounds containing 8-azabicyclo [3.2.1] octane, 9-azabicyclo [3.3.1] nonane, or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane or granatane alkaloids, scopolamine; Cyclic acetals thereof
    • C07D451/02Heterocyclic compounds containing 8-azabicyclo [3.2.1] octane, 9-azabicyclo [3.3.1] nonane, or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane or granatane alkaloids, scopolamine; Cyclic acetals thereof containing not further condensed 8-azabicyclo [3.2.1] octane or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane; Cyclic acetals thereof
    • C07D451/04Heterocyclic compounds containing 8-azabicyclo [3.2.1] octane, 9-azabicyclo [3.3.1] nonane, or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane or granatane alkaloids, scopolamine; Cyclic acetals thereof containing not further condensed 8-azabicyclo [3.2.1] octane or 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring systems, e.g. tropane; Cyclic acetals thereof with hetero atoms directly attached in position 3 of the 8-azabicyclo [3.2.1] octane or in position 7 of the 3-oxa-9-azatricyclo [3.3.1.0<2,4>] nonane ring system
    • C07D451/06Oxygen atoms
    • C07D451/10Oxygen atoms acylated by aliphatic or araliphatic carboxylic acids, e.g. atropine, scopolamine

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Abstract

The new compounds of formula (I) (where A, R1, Ra and R2 are defined in the description) can be manufactured by processes known per se and used as the active ingredients of drugs.

Description

1 114395114395

Menetelmä farmakologisesti vaikuttavien tienyylikarboksyylihappojen ja aminoalko-holien estereiden valmistamiseksi ja välituote - Förfarande för framställning av far-makologiskt verksamma tienylkarboxylsyrors och aminoalkoholers estrar och mel-lanprodukt 5A process for the preparation of pharmacologically active esters of thienylcarboxylic acids and aminoalcohols and an intermediate - Förfarande för framställning av pharma- logologic verksamma thienylcarboxylsyrors and aminoalkoholers estrar och mel-lanprodukt

Keksintö koskee menetelmää valmistaa farmakologisesti vaikuttavia tienyylikarboksyylihappojen ja aminoalkoholien estereitä, joilla on kaava IThe present invention relates to a process for the preparation of pharmacologically active esters of thienylcarboxylic acids and amino alcohols of formula I

[=\ 10 aΊΞ(=/ m[= \ 10 aΊΞ (= / m

R^C-CO-OAR ^ C-CO-OA

jossa 15 A on ryhmäwherein 15 A is a group

ru-CHru CH

/ l®\ -CH R-N-R' Q (m/ l® \ -CH R-N-R 'Q {m

\ IXIX

20 CH2-CH20 CH 2 -CH

• ‘ · jossa :; Q on yksi seuraavista kaksiarvoisista ryhmistä \ ’1 i 25 -CH2-CH2-, -CH2-CH2-CH2-, -CH=CH-, 0': -CH-CH- \ / o • * • %» 30 ja R on mahdollisesti halogeenisubstituoitu tai hydroksisubstituoitu Ci-C^-alkyyliradi- * · · *:, kaali, R' on Ci-C4-alkyyliradikaali ja R ja R' voivat myös yhdessä muodostaa CrC6- " ”: alkyleeniradikaalin, ja jossa positiivisen varauksen ekvivalentiksi vastapainoksi aset- • · tuu anioni (XB), 2 114395• '· where:; Q is one of the following bivalent radicals '-CH 2 -CH 2 -, -CH 2 -CH 2 -CH 2 -, -CH = CH-, O': -CH-CH-? is an optionally halogen-substituted or hydroxy-substituted C 1 -C 4 -alkyl radical, R 'is a C 1 -C 4 -alkyl radical and R and R' may also be taken together to form a C 1 -C 6 alkylene radical, and wherein sets anion (XB), 2 114395

Ri on tienyyli-, fenyyli-, furyyli-, syklopentyyli- tai sykloheksyyliradikaali, jolloin nämä radikaalit voivat myös olla metyylisubstituoituja, tienyyli ja fenyyli voivat myös olla fluorisubstituoituja tai kloorisubstituoituja, 5 R2 on vety, OH, CrQ-alkoksi tai Ci-C4-alkyyli,R1 is a thienyl, phenyl, furyl, cyclopentyl or cyclohexyl radical, whereby these radicals may also be methyl-substituted, thienyl and phenyl may also be fluoro-substituted or chloro-substituted, R2 is hydrogen, OH, C1-C4-alkoxy or C1-C4-alkyl ,

Ra on H, F, Cl tai CH3.Ra is H, F, Cl or CH3.

Keksinnön menetelmällä saaduissa kaavan I mukaisissa yhdisteissä Ri on edullisesti 10 tienyyli, R2 on edullisesti OH. Ryhmällä -OA on edullisesti α-konfiguraatio ja on johdettu esimerkiksi skopiinista, tropiinista, granatoliinista tai 6,7-dehydrotropiinista tai vastaavista nor-yhdisteistä; -OA:lla voi kuitenkin olla myös β-konfiguraatio, kuten pseudotropiinissa, pseudoskopiinissa.In the compounds of formula I obtained by the process of the invention, R 1 is preferably thienyl, R 2 is preferably OH. The -OA group preferably has the α configuration and is derived, for example, from scopine, tropine, granatoline or 6,7-dehydrotropin or similar nor compounds; However, -OA may also have the β-configuration as in pseudotropin, pseudoscopin.

15 Vastaavia radikaaleja ovat esimerkiksi / Π /“Tl .15 Corresponding radicals are, for example, / Π / “Tl.

\_1_ λ_!_ / I |\ / Γ, |\ .\ _1_ λ _! _ / I | \ / Γ, | \.

·;· λ . I / '·—l—1/ "· / n /-1—il·; · Λ. I / '· —l — 1 / "· / n / -1 — il

\---1 - XlL\ --- 1 - XlL

: -o-^ R-N ^ , -ο<; κ|-Γ> x® *::: -o^ ®n x® \ Is— • * · *·:·’ 20 * * · 114395: -o- ^ R-N ^, -ο <; κ | -Γ> x® * ::: -o ^ ®n x® \ Is— • * · * ·: · '20 * * · 114395

Substituentti R on edullisesti alempi alkyyliradikaali, kuten CH2, C2H5, n-C3H7, i-C3H7, R' on edullisesti CH3. R ja R' ovat yhdessä esimerkiksi -(ChWs'· R:n halogeenisubsti-tuentteina on sopiva F, tai toisella sijalla Cl.The substituent R is preferably a lower alkyl radical such as CH 2, C 2 H 5, n-C 3 H 7, i-C 3 H 7, R 'is preferably CH 3. For example, R and R 'together are - (ChWs' · R as halogen substituents is a suitable F, or Cl is in the second position).

5 Jos R on halogeenisubstituoitu tai hydroksisubstituoitu alkyyliradikaali, se on edullisesti -CH2-CH2F tai -CH2-CH2OH. Niinpä ryhmä A on esimerkiksi radikaali yhdisteistä skopiini, N-etyylinorskopiini, N-isopropyylinorskopiini, tropiini, N-isopropyylinortro-piini, 6,7-dehydrotropiini, Ν-β-fluorietyylinortropiini, N-isopropyyli-6,7-dehydronor-tropiini, N-metyyligranatoliini tai vastaavista kvaternäärisistä yhdisteistä, jolloin 10 anioni on edullisesti Br' tai CH3S03‘·When R is a halogen substituted or hydroxy substituted alkyl radical, it is preferably -CH 2 -CH 2 F or -CH 2 -CH 2 OH. Thus, for example, Group A is a radical of the compounds scopine, N-ethylnorscopine, N-isopropylnorcopine, tropine, N-isopropylnortropine, 6,7-dehydrotropine, Ν-β-fluoroethylnortropine, N-isopropyl-6,7-dehydronorthropine, -methylgranatoline or the like quaternary compounds, wherein the anion is preferably Br 'or CH 3 SO 3' ·

Kaavan III mukaisena happamana radikaalina 1C R —- — 15 R1-C-CO- ^111^ R2 20 v-j 25 30 • I · 4 114395 erityisen sopivia ovat seuraavat: F=\ F=\ \=/ LL/ L/ 5 HO-C-CO- to3-co- HO—i-CO-As the acidic radical of formula III, the following compounds are particularly suitable: F = \ F = \ \ = / LL / L / 5 HO -C-CO- to3-co- HO-i-CO-

D O DD O D

P b p HO-C-CO- HC-CO- H-C-C-CO-P b p HO-C-CO-HC-CO-H-C-C-CO-

, 1 / 3 I, 1/3 I

ö 6- O6- 6- O

15 p> r^s ΠΡ =/ kb HO-C-CO- HO-C-CO- HO—C—CO—15 p> r ^ s ΠΡ = / kb HO-C-CO-HO-C-CO-HO-C-CO-

, " <P b <P, '<P b <P

: Keksinnön mukaisella menetelmällä saadut kvaternääriset yhdisteet ovat erityisen : sopivia terapeuttiseen käyttöön, kun tertiääriset yhdisteet puolestaan ovat tärkeitä ·· 25 välituotteina.The quaternary compounds obtained by the process of the invention are particularly suitable for therapeutic use, while the tertiary compounds are important as intermediates.

Keksinnön menetelmän mukaiset uudet yhdisteet ovat vahvoja antikolinergisiä ainei- .,,; ’ ta, ja niillä on pidentynyt vaikutus. Ainakin 24 tuntia kestävä vaikutus saavutetaan :,,, · inhaloiduilla annoksilla, jotka ovat pg-alueella. Lisäksi toksisuus on samaa luokkaa : \ # 30 kuin kaupallisella tuotteella ipratropiumbromidi, samalla kun terapeuttinen vaikutus ; 1 “; on voimakkaampi. Keksinnön menetelmällä saadut uudet yhdisteet soveltuvat anti- |. kolinergisen luonteensa mukaisesti esimerkiksi kroonisen umpeuttavan keuhkoput- ‘ ” ’. kentulehduksen ja (lievän - kohtuullisen vakavan) astman hoitoon, myös vagaalisesti » » indusoidun sinusbradykardian hoitamiseksi.The novel compounds of the process of the invention are potent anticholinergic agents. And have a longer lasting effect. The effect is maintained for at least 24 hours with:,,, inhaled doses in the pg range. In addition, the toxicity is of the same class: \ # 30 as the commercial product ipratropium bromide, while having a therapeutic effect; 1 "; is stronger. The novel compounds obtained by the process of the invention are suitable for anti-. according to its cholinergic nature, for example, chronic obstructive bronchodilation. for the treatment of inflammation of the field and asthma (mild to moderate), including for the treatment of vagal induced sinus bradycardia.

5 1143955, 114395

Kun uusien aktiivisten valmistusaineiden käyttöä (erityisesti kvaternääristen yhdisteiden) käyttöä inhalaatiolla suositellaan hengitysteiden sairauksiin, jonka tuloksena sivuvaikutukset vältetään suurelta osin, suoritetaan anto sinusbradykardiaan edullisesti laskimonsisäisesti tai oraalisesti. Siten on osoittautunut edulliseksi, että uudet 5 yhdisteet jättävät suuressa määrin vaikuttamatta ruoansulatuskanavaan.Where the use of new active ingredients (particularly quaternary compounds) by inhalation is recommended for respiratory diseases, which results in the avoidance of side effects to a large extent, administration to the sinus bradycardia is preferably performed intravenously or orally. Thus, it has proven to be advantageous that the new compounds do not largely affect the gastrointestinal tract.

Keksinnön mukaisella menetelmällä saadut yhdisteet käsitellään antoa varten tavanomaisia apu- ja/tai täyteaineita käyttämällä antamaan tavanomaisia galeenisia valmisteita, esimerkiksi inhalaatioliuoksia, suspensioita nesteytetyissä ponneaineissa, 10 valmisteita, jotka sisältävät liposomeja tai proliposomeja, injektioliuoksia, tabletteja, päällystettyjä tabletteja, kapseleita, inhalaatiojauheita tavanomaisessa inhalaatiolait-teessa käytettäväksi.The compounds of the invention are processed for administration using conventional excipients and / or excipients to provide conventional galenical formulations, for example, inhalation solutions, suspensions in liquefied propellants, formulations containing liposomes or proliposomes, injection solutions, tablets, inhaled capsules, for use in tea.

Formulaatioesimerkit (mitat ovat yksikössä paino-%): 15 1. Kontrolloitu annosaerosoli keksinnön mukainen aktiivinen valmistusaine 0,005 sorbitaanitrioleaatti 0,1 20 monofluoritrikloorimetaani ja ’· difluoridikloorimetaanl 2:3 100:aan :,,, ·' Suspensio kaadetaan tavanomaiseen aerosolisäiliöön, jossa on annosteluventtiili.EXAMPLES OF FORMULATION (DIMENSIONS UNIT BY WEIGHT BY WEIGHT): 15 1. Controlled Dose Aerosol Active Ingredient of the Invention 0.005 Sorbitan Trioleate 0.1 20 Monofluorotrichloromethane and '· Difluorochlorochloromethane 2: 3 to 100: ,,, ·' The suspension is poured into a conventional aerosol container .

1 “ ‘ Edullisesti jaetaan 50 pl suspensiota/käynnistys. Aktiivista valmistusainetta voidaan ;‘ : 25 tarvittaessa mitata myös suurempi määrä (esimerkiksi 0,02 paino-%).1 "'Preferably 50 µl of suspension / start is dispensed. The active ingredient can also be: ': if necessary, a larger amount (e.g., 0.02% by weight) may also be measured.

2. Tabletit2. Tablets

Keksinnön mukainen aktiivinen valmistusaine 0,05 30 kolloidinen piihappo 0,95 laktoosi 65,00 perunatärkkelys 28,00 ·*·:, polyvinyylipyrrolidoni 3,00Active ingredient according to the invention 0.05 30 colloidal silica 0.95 lactose 65.00 potato starch 28.00 · * ·:, polyvinylpyrrolidone 3.00

Na-selluloosaglykolaatti 2,00 35 magnesiumstearaatti 1,00 6 114395Na-Cellulose Glycolate 2.00 35 Magnesium Stearate 1.00 6 114395

Ainesosat käsitellään tavanomaisella tavalla, jolloin saadaan 200-mg tabletteja.The ingredients are processed in a conventional manner to give 200 mg tablets.

Uusien yhdisteiden edulliset ominaisuudet osoitetaan esimerkiksi keuhkoputkien laajenemisen estolla kanissa (asetyylikoliinikouristukset laskimonsisäisesti). Uusien 5 aktiivisten valmistusaineiden laskimonsisäisen annon jälkeen (annos 3 pg/kg laskimonsisäisesti) maksimaalinen vaikutus oli 10 - 40 min kuluttua. 5 tunnin jälkeen estovaikutus ei vielä ollut laskenut puoleen, ts., puoliintumisaika on yli, joissain tapauksissa huomattavasti yli 5 tuntia, kuten selvitetään alla luettelomaisesti esitetyllä jäännösvaikutuksilla 5 tunnin kuluttua: 10 yhdiste jäännösvaikutus yksikössä % A 76 B 76 15 C 81 D 61 E 68 F 73 G 69 I I t > · I · » I » » tThe beneficial properties of the novel compounds are demonstrated, for example, by the inhibition of bronchodilation in the rabbit (intravenous acetylcholine seizures). Following intravenous administration of the new 5 active ingredients (3 pg / kg i.v.), the maximal effect was obtained after 10-40 min. After 5 hours, the inhibitory effect had not yet halved, i.e., the half-life is greater than, in some cases, significantly more than 5 hours, as explained by the residual effects listed below after 5 hours: 10 compound residual activity% A 76 B 76 15 C 81 D 61 E 68 F 73 G 69 II t> · I · »I» »t

Yhdisteet, joilla on kaava 7 114395 F=\ L> iCompounds of Formula 7 114395 F = \ L> i

HO-C-CO-AHO-C-CO-A

R1 yhdiste A Ri 5 - -,-K Br& A / L \ 2-tienyyli -o—ch3-iP-ch3 10 ._- Bi© B -o—^CHa-sS-cHa \ ^"W11 ,_j.. Br© 15 D -o—/ ch3-^-ch3 2-tienyyli :V: E / j Br° -o—/ CH3-]p-CH3 3-tienyyli ; 20 \_I__ *· : __. Br© F -o_V ch3-i0-ch(ch3)2 syklopentyyli C> 25 ,-,-, ΒΛ G / cR 1 Compound A R 5 - -, - K Br &lt; + &gt; L-2-thienyl-o-ch 3-iP-ch 3 10. Br © 15 D-o - / ch 3 - ^ - ch 3 2-thienyl: V: E / j Br ° -o - / CH 3 -? - CH 3 3-thienyl; o_V ch3 -10-ch (ch3) 2 cyclopentyl C> 25, -, -, ΒΛ G / c

· -O—/ CH2-I©-CH2-CH2F· -O— / CH2-I © -CH2-CH2F

'' \ syklopentyyli > 1'' \ cyclopentyl> 1

Yhdiste CCompound C

8 114395 [=Ν8 114395 [= Ν

SS

— / t_ Br® HO-C-CO-O-<^ CH3-|1-CH3 'y- / t_ Br® HO-C-CO-O - <^ CH3- | 1-CH3 'y

Huomautukset: 5 1. Yhdisteet, joissa Ri ei ole 2-tienyyli, ovat rasemaatteja.Notes: 1. Compounds where R 1 is not 2-thienyl are racemates.

2. Yhdisteet ovat kaikissa tapauksissa 3a-yhdisteitä.2. In each case, the compounds are 3a compounds.

10 Keksinnön menetelmän mukaisten yhdisteiden valmistuksessa voidaan käyttää sinänsä tunnettuja menetelmiä.Methods known per se can be used in the preparation of the compounds of the process of the invention.

Keksinnön menetelmälle on tunnusomaista se, että vaihtoesteröidään kaavan IV mukainen esteri ; · 15 [=\ vv Ra L-^-vS (iv) : ·' Rj-C-CO-OR" ;: r2 i 1 I > 1 1 20The process of the invention is characterized in that the ester of formula IV is esterified by transesterification; · 15 [= \ vv Ra L - ^ - vS (iv): · 'Rj-C-CO-OR ";: r2 i 1 I> 1 1 20

* 1 I* 1 I

jossa R" on Ci-C4-alkyyliradikaali ja Ri, R2 ja Ra ovat edellä määritellyt, käyttämällä ,:. kaavan V mukaista aminoalkoholiawherein R "is a C 1 -C 4 alkyl radical and R 1, R 2 and R a are as defined above, using: - an amino alcohol of formula V

I II I

·;· f-u-CH·; · F-u-CH

/ 2 1 \ 25 ho-ch q" q (v) \h2—ch > » 9 114595 jossa Q on edellä määritelty ja Q" on =NR tai =NH, inertissä orgaanisessa liuotti-messa tai sulatteessa, vaihtoesteröintikatalysaattorin läsnä ollessa, ja saatu yhdiste, jolla on kaava (VI) 5/ 2 1 \ 25 ho-ch q "q (v) \ h2-ch> 9114595 wherein Q is as defined above and Q" is = NR or = NH, in an inert organic solvent or melt, in the presence of a transesterification catalyst, and the compound of formula (VI) 5 obtained

R--S CH-,-CHR - S CH -, - CH

Τ' / i\ R^C-CO-O-CH Q" Q (VI)Τ '/ i \ R ^ C-CO-O-CH Q "Q (VI)

R> \ IXR> \ IX

10 CH2--CH10 CH 2 - CH

jossa Q" on =NR, kvaternisoidaan käyttämällä alkaanin reaktiivista monofunktio-nalisoitua johdannaista Z-(CrCralkyyli), jossa Z on poistuva ryhmä.wherein Q "is = NR, is quaternized using an alkane reactive monofunctionalized derivative Z- (C 1 -C 4 alkyl) where Z is a leaving group.

15 Keksinnön menetelmän mukaisesti vaihtoesteröinti suoritetaan kuumentaen orgaanisessa liuottimessa, esimerkiksi tolueeni, ksyleeni, heptaani, tai sulatteessa, käyttämällä katalysaattorina vahvoja emäksiä, kuten natriummetylaatti, natriumetylaatti, natriumhydridi, metallinen natrium. Vapautuneen alemman alkoholin poistamiseksi tasapainosta käytetään alennettua painetta, alkoholi tislataan mahdollisesti pois 20 atseotrooppisesti. Vaihtoesteröinti tapahtuu lämpötiloissa, jotka eivät yleensä ole yli 95 °C. Usein vaihtoesteröinti etenee suositummin sulassa. Vaadittaessa vapaat : emäkset voidaan saada sinänsä tunnetulla tavalla tertiääristen amiinien happoaddi- tiosuoloista sopivia emäksisiä yhdisteitä käyttämällä. Kvaternisointi suoritetaan sopi-i vissa liuottimissa, esimerkiksi asetonitriili tai asetonitriili/metyleenikloridi, edullisesti * 25 huoneenlämpötilassa; menetelmässä käytetään edullisesti kvaternisointireagenssina ; ; : vastaavaa alkyylihalogenidia, esimerkiksi alkyylibromidia. Vaihtoesteröintituotteet, joissa Q’ on NH, käytetään lähtöaineina niille yhdisteille, joissa R ja R' yhdessä ovat C4-C6-alkyleeniryhmä.According to the process of the invention, the transesterification is carried out by heating in an organic solvent, for example toluene, xylene, heptane, or in a melt, using strong bases such as sodium methylate, sodium ethylate, sodium hydride, metallic sodium as catalyst. To reduce the released lower alcohol from equilibrium, a reduced pressure is used, possibly distilling off the alcohol azeotropically. The transesterification takes place at temperatures not generally above 95 ° C. Often, transesterification proceeds more favorably in the melt. When required, the free: bases may be obtained in a manner known per se from the acid addition salts of the tertiary amines using appropriate basic compounds. The quaternization is carried out in suitable solvents, for example acetonitrile or acetonitrile / methylene chloride, preferably at room temperature; the method is preferably used as a quaternization reagent; ; : a corresponding alkyl halide, for example alkyl bromide. Exchange esterification products wherein Q 'is NH are used as starting materials for those compounds wherein R and R' together are a C 4 -C 6 alkylene group.

I t » · ; - | 30 Muuttaminen tertiääriseksi ja sitten kvaternääriseksi yhdisteeksi tapahtuu sopivien I I · ’,···, 1,4-dihalogeenialkaanien, 1,5-dihalogeenialkaanien tai 1,6-dihalogeenialkaanien » · ’ ·' avulla välituotteita eristämättä.I t »·; - | Conversion to a tertiary and then quaternary compound is accomplished by the use of appropriate I · ', ···, 1,4-dihaloalkanes, 1,5-dihaloalkanes or 1,6-dihaloalkanes, without isolation of intermediates.

J I ♦ » I I tl 1 » « · » » t · ίο 114395 Lähtöaineet voidaan saada tunnetuille yhdisteille analogisesti sikäli kuin niitä ei jo ole kuvattu.114395 Starting materials may be obtained analogously to known compounds insofar as they have not already been described.

Esimerkkejä: 5 metyylidi-(2-tienyyli)glykolaatti dimetyylioksalaatista ja 2-tienyylimagnesiumbromi-dista; etyylidi-(2-tienyyli)glykolaatti(2-tienyyli)glyoksaalihaposta ja 2-tienyylilitiumista; etyylihydroksifenyyli-(2-tienyyli)asetaatti metyylifenyyliglyoksylaatista ja 2-tienyyli-magnesiumbromidista tai metyyli-(2-tienyyli)glyoksylaatista ja fenyylimagnesium-10 bromidista.Examples: 5 methyl di- (2-thienyl) glycolate of dimethyl oxalate and 2-thienyl magnesium bromide; ethyl di (2-thienyl) glycolate (2-thienyl) glyoxalic acid and 2-thienyl lithium; ethyl hydroxyphenyl (2-thienyl) acetate from methyl phenylglyoxylate and 2-thienylmagnesium bromide or methyl (2-thienyl) glyoxylate and phenylmagnesium 10 bromide.

Metyyli-2-tienyyliglyoksylaatti ja sykloheksyyli- tai syklopentyylimagnesiumbromidi voidaan saattaa reagoimaan samalla lailla.Methyl 2-thienylglyoxylate and cyclohexyl or cyclopentylmagnesium bromide can be reacted similarly.

Myös aminoalkoholien valmistukseen on käytettävissä useita menetelmiä.Several methods are also available for the preparation of amino alcohols.

1515

Pseudoskopiini voidaan saada tavalla, joka kuvataan julkaisussa: M.Polonovski et ai.; Buli. soc. chim. 43 (1928) 79. Pseudotropenoli voidaan poistaa saadusta seoksesta (fraktiokiteytys tai tislaus), esimerkiksi tavalla, joka kuvataan julkaisuissa: V. Hayakawa et ai., J. Amer. Chem. Soc. 100(6) (1978) 1786; tai R. Noyori et ai., J.Pseudoscopin can be obtained in the manner described by M.Polonovski et al .; Buli. soc. chim. 43 (1928) 79. The pseudotropenol may be removed from the resulting mixture (fractional crystallization or distillation), for example, as described in V. Hayakawa et al., J. Amer. Chem. Soc. 100 (6): 1786 (1978); or R. Noyori et al., J.

20 Amer. Chem. Soc. 96(10) (1974) 3336.20 Amer. Chem. Soc. 96 (10) 3336 (1974).

» · • · · • · v.: Vastaavat metyyliesterit voidaan valmistaa tavanomaisella tavalla lähtien 2-furyyli- •«· :: glyoksyylinitriilistä tai 3-furyyliglyoksyylinitriilistä 2-furyyliglyoksaalihapon tai 3-furyy- *: : liglyoksaalihapon kautta, jotka voidaan saada niistä. Vastaavat glykolaatit saadaan : 25 näistä kuvatulla tavalla käyttämällä 2-bromitiofeenin tai 3-bromitiofeenin organome- v : tallisia johdannaisia. Organometalliset yhdisteet, jotka voidaan saada 2-, 3- tai 4- halogeenipyridiinistä, voidaan saattaa reagoimaan metyyli-2-tienyyliglyoksylaatin tai .. !: metyyli-3-tienyyliglyoksylaatin kanssa, jolloin saadaan vastaavat glykolaatit.The corresponding methyl esters may be prepared in a conventional manner starting from 2-furyl-glycyl nitrile or 3-furylglyoxylnitrile via 2-furylglyoxalic acid or 3-furyl-*: liglyoxalic acid which can be obtained therefrom. The corresponding glycolates are obtained: 25 of these as described using organometallic derivatives of 2-bromothiophene or 3-bromothiophene. Organometallic compounds which may be obtained from 2-, 3- or 4-halo-pyridine may be reacted with methyl 2-thienylglyoxylate or n-methyl 3-thienylglyoxylate to give the corresponding glycolates.

: * . 30 Tienyyliglykolaatit, joissa tiofeenirengas sisältää fluoria 2- tai 3-asemassa, valmiste- taan esimerkiksi lähtemällä 2-fluoritiofeenistä tai 3-fluoritiofeenistä (brominointi, jolloin saadaan 2-bromi-3-fluoritiofeeni tai 2-bromi-5-fluoritiofeeni), ja vastaaviksi ....: organometallisiksi yhdisteiksi muuttamisen jälkeen reaktio sopivien glyoksylaattien • · kanssa, jolloin saadaan glykolaatteja.: *. Thienylglycolates in which the thiophene ring contains fluorine in the 2- or 3-position are prepared, for example, by starting from 2-fluorothiophene or 3-fluorothiophene (bromination to give 2-bromo-3-fluorothiophene or 2-bromo-5-fluorothiophene) and the like. ....: After conversion to organometallic compounds, reaction with appropriate glyoxylates to yield glycolates.

11 114395 2-fluoritiofeeni ja 3-fluoritiofeeni voidaan saattaa reagoimaan analogisesti, jolloin saadaan vastaavia glyoksylaatteja, Unterhalt, Arch. Pharm. 322, 839 (1989), jotka puolestaan, kuten jo kuvattiin, voidaan saattaa reagoimaan esimerkiksi 2-tienyyli-tai 3-tienyylijohdannaisten kanssa, jolloin saadaan glykolaatteja. Symmetrisesti sub-5 stituoituja ditienyyliglykolaatteja voidaan valmistaa analogisesti valitsemalla sopivat komponentit.11434395 2-Fluorothiophene and 3-Fluorothiophene can be reacted analogously to afford the corresponding glyoxylates, Unterhalt, Arch. Pharm. 322, 839 (1989), which in turn, as already described, may be reacted with, for example, 2-thienyl or 3-thienyl derivatives to yield glycolates. Symmetrically, sub-5-substituted dithienyl glycolates can be prepared analogously by selecting appropriate components.

Lisäreitti on käytettävissä menetelmällä, joka on analoginen bentsoiinikondensoinnin ja bentsiilihappotoisiintumisen kautta.An additional route is available by a process analogous to benzoic condensation and benzylic acid rearrangement.

1010

Seuraavat esimerkit kuvaavat keksintöä sitä rajoittamatta.The following examples illustrate the invention without limiting it.

Esimerkki 1 15 Skopiinidi-(2-tienyyli)glykolaatti 50,87 g (0,2 moi) metyylidi-(2-tienyyli)glykolaattia ja 31,04 g (0,2 mol) skopiinia liuotetaan 100 ml:aan absoluuttista tolueenia ja saatetaan reagoimaan haudelämpö-tilassa 90 °C lisäämällä 1,65 g (0,071 gramma-atomia) natriumia useissa erissä.Example 1 Scopine di (2-thienyl) glycolate 50.87 g (0.2 mol) of methyl di (2-thienyl) glycolate and 31.04 g (0.2 mol) of scopine are dissolved in 100 ml of absolute toluene and reaction at a bath temperature of 90 ° C by adding 1.65 g (0.071 grams) of sodium in several portions.

20 Tuloksena muodostunut metanoli tislataan reaktioseoksen lämpötilassa 78 - 90 °C i · paineessa 50 kPa. Noin 5 tunnin reaktioajan jälkeen reaktioseos sekoitetaan jään ja \ v suolahapon seokseen. Happofaasi erotetaan pois, säädetään alkaliseen pH-arvoon '...; natriumkarbonaattia käyttämällä, ja vapaa emäs uutetaan metyleenikloridia käyttä- • · mällä. Natriumsulfaatilla kuivaamisen jälkeen metyleenikloridi tislataan pois aienne- ’. ’1: 25 tussa paineessa, ja jäännös uudelleenkiteytettiin asetonitriiIistä; beigenvärisiä kiteitä v : (asetonitriiIistä), sp. 149-50 °C, saanto: 33,79 g (44,7 % teoreettisesta).The resulting methanol is distilled at a temperature of the reaction mixture between 78 ° C and 90 ° C under a pressure of 50 kPa. After a reaction time of about 5 hours, the reaction mixture is stirred into a mixture of ice and hydrochloric acid. The acid phase is separated off, adjusted to an alkaline pH '...; sodium carbonate, and the free base is extracted with methylene chloride. After drying over sodium sulfate, methylene chloride is distilled off. 1: 25 under pressure and the residue was recrystallized from acetonitrile; beige crystals v: (from acetonitrile), m.p. 149-50 ° C, yield: 33.79 g (44.7% of theory).

t » · · :...: Esimerkki 2 30 :' ’ ]: Skopiinidi-(2-tienyyli)glykolaatti 1:. 12,72 g (0,05 mol) metyylidi(2-tienyyli)glykolaattia ja 7,76 g (0,05 mol) skopiiniat: · ·: ...: Example 2 30: '']: Scopinide (2-thienyl) glycolate 1 :. 12.72 g (0.05 mol) of methyl di (2-thienyl) glycolate and 7.76 g (0.05 mol) of scopine

Ml· sulatetaan lämpöhauteessa 70 °C:ssa vesisuihkupumpun tyhjössä. Tähän sulattee- • · seen lisätään 2,70 g (0,05 mol) natriummetylaattia, ja kuumennetaan 1 tunnin ajan 12 114395 lämpöhauteessa 70 °C:ssa vesisuihkupumpun tyhjössä, ja seuraavaksi vielä 1 tunnin ajan lämpöhauteessa 90 °C:ssa. Kiinteytynyt sulate otetaan seokseen, jossa on 100 ml vettä ja 100 ml metyleenikloridia tarkkaillen lämpötilaa, ja metyleenikloridifaasi uutetaan useita kertoja vettä käyttäen. Metyleenikloridifaasi uutetaan käyttämällä 5 vastaavaa määrää laimeaa suolahappoa. Skopiinidi-(2-tie-nyyli)glykolaatti uutetaan yhdistetyistä vesifaaseista käyttämällä metyleenikloridia sen jälkeen kun on lisätty vastaava määrä natriumkarbonaattia, ja kuivataan natrium-sulfaatilla. Kuivatusta metyleenikloridiliuoksesta valmistetaan hydrokloridi tavalliseen tapaan. Kiteet suodatetaan pois imupullolla, pestiin asetonia käyttämällä ja kuivattiin alennetussa pai-10 neessa 35 °C:ssa. Vaaleankeltaisia kiteitä (metanolista), sp. 238-41 °C (hajoaa); saanto: 10,99 g (53,1 % teoreettisesta).Ml · is thawed in a heat bath at 70 ° C under vacuum of a water jet pump. To this melt is added 2.70 g (0.05 mol) of sodium methylate and heated for 12 hours in a 12114395 heat bath at 70 ° C under a vacuum of a water jet pump and then for an additional 1 hour in a heat bath at 90 ° C. The solidified melt is taken up in a mixture of 100 ml of water and 100 ml of methylene chloride, monitoring the temperature, and the methylene chloride phase is extracted several times with water. The methylene chloride phase is extracted using 5 equal volumes of dilute hydrochloric acid. The scopinide (2-thienyl) glycolate is extracted from the combined aqueous phases using methylene chloride after addition of the corresponding amount of sodium carbonate, and dried over sodium sulfate. From the dried methylene chloride solution, the hydrochloride is prepared in the usual manner. The crystals are suction filtered, washed with acetone and dried under reduced pressure at 35 ° C. Light yellow crystals (from methanol), m.p. 238-41 ° C (dec.); yield: 10.99 g (53.1% of theory).

Hydrokloridi voidaan muuttaa tavanomaisella tavalla emäkseksi.The hydrochloride can be converted to the base in a conventional manner.

Esimerkki 3 15Example 3 15

Skopiinidi(2-tienyyli)glykolaattiSkopiinidi (2-thienyl) glycolate

Sekoitetaan 38,15 g (0,15 mol) metyylidi(2-tienyyli)glyko-laattia ja 23,28 g (0,15 mol) skopiinia, lisätään 0,34 g (0,015 gramma-atomia) natriumia, ja seos sula-20 tetaan lämpöhauteessa 90 °C vesisuihkupumpun tyhjössä. Reaktio kestää 2,5 tuntia.38.15 g (0.15 mol) of methyl di (2-thienyl) glycolate and 23.28 g (0.15 mol) of scopine are mixed, 0.34 g (0.015 gram atom) of sodium are added and the mixture is melted. 20 is heated in a heat bath at 90 ° C under vacuum of a water jet pump. The reaction takes 2.5 hours.

• ’· Sitten lisätään 100 ml absoluuttista tolueenia, ja seosta sekoitetaan lämpöhauteessa :.v lämpötilassa 90 °C, kunnes muodostuu liuos. Reaktioliuos jäähdytetään huoneen- :... · lämpötilaan ja sekoitetaan jään ja jäällä jäähdytetyn suolahapon seokseen. Ulos '"': saostuva emäksisen esterin hydrokloridi suodatetaan pois imupullolla ja pestään *·.’*: 25 pienellä määrällä vettä ja suurella määrällä dietyylieetteriä. Suodosfaasit erotetaan v ·’ pois, ja vesifaasi uutetaan dietyylieetteriä käyttämällä. Imupullolla pois suodatettu hydrokloridi suspendoidaan (happamaan) vesifaasiin ja muutetaan emäkseksi tark-kaillen lämpötilaa ja lisäämällä vastaavan määrän natriumkarbonaattia; emäs uute-taan metyleenikloridia käyttämällä. Yhdistetyt metyleenikloridifaasit kuivataan natri-: \, 30 umsulfaatilla. Metyleenikloridin pois tislaamisen jälkeen jää jäljelle kiteitä, jotka .* * *: puhdistetaan aktiivihiilellä ja uudelleenkiteytetään asetonitriilistä. Vaaleankeltaisia kiteitä (asetonitriilistä), sp. 148-49 °C; **”. saanto: 39,71 g (70,1 % teoreettisesta).100 ml of absolute toluene are then added and the mixture is stirred in a heat bath at 90 ° C until a solution is formed. The reaction solution is cooled to room temperature and stirred in an ice / ice-cooled hydrochloric acid mixture. Exit '' ': the precipitating basic ester hydrochloride is filtered off with suction and washed with a small amount of water and a large amount of diethyl ether. The filtrate phases are separated off and the aqueous phase is extracted using diethyl ether. The hydrochloride is filtered off with suction. aqueous phase and basified with monitoring of temperature and addition of an appropriate amount of sodium carbonate, the base is extracted using methylene chloride. Light yellow crystals (from acetonitrile), mp 148-49 ° C; ** ". Yield: 39.71 g (70.1% of theory).

Yhdisteet, joilla on kaava 13 114395Compounds of formula 13114395

Taulukko ITable I

5 (^s ho-c-co-oa R1 10 sp. [°c]5 (^ s ho-c-co-oa R1 10 sp [° c]

No. A Ri emäs hydro- kloridi 15 1 3a-(6B,7B-epoksi)-tropanyyli 2-tienyyli 149-50 238-41 2 3oc-tropanyyli 2-tienyyli 167-8 253 3 3a-(6,7-dehydro)-tropanyyli 2-tienyyli 164-5 4 3a-(N-8-fluorietyyli)- 2-tienyyli nortropanyyli 236 20 5 3a-(N-isopropyyli)- granatanyyli 2-tienyyli 232 : : 6 3a-(N-isopropyyli)- ’ : nortropanyyli 2-tienyyli 256 7 3a-(6B,76-epoksi)-N- 25 isopropyylinortropanyyli 2-tienyyli 206 : 8 3a-(66,76-epoksi)-N-etyyli- 2-tienyyli nortropanyyli 212-3 9 3oc-(N-etyyli)-nortropanyyli 2-tienyyli 256-7 10 3a-(N-N-metyyli)granatanyyli 2-tienyyli 241 30 11 3a-(66,76-epoksi)-N-8- 2-tienyyli ;‘: fluorietyylinortropanyyli 188-90 12 3a-(6B,7B-epoksi)-N-n- 2-tienyyli 104-6 ’ . propyylinortropanyyliWell. A 1 Base Hydrochloride 15 1 3a- (6B, 7B-Epoxy) -tropanyl 2-thienyl 149-50 238-41 2 3oc-tropanyl 2-thienyl 167-8 253 3 3a- (6,7-dehydro) - tropanyl 2-thienyl 164-5,43a- (N-8-fluoroethyl) -2-thienyl nortropanyl 236 20 5 3a- (N-isopropyl) -granatanyl 2-thienyl 232: 6 3α- (N-isopropyl) - ' : nortropanyl 2-thienyl 256 7 3α- (6β, 76-epoxy) -N-25 isopropylnortropanyl 2-thienyl 206: 8 3α- (66.76-epoxy) -N-ethyl-2-thienyl nortropanyl 212-3 9 3oc - (N-ethyl) -nortropanyl 2-thienyl 256-7103a- (NN-methyl) granatanyl 2-thienyl 241 30 11 3a- (66.76-epoxy) -N-8- 2-thienyl; 188-9012 3a- (6B, 7B-Epoxy) -Nn-2-thienyl 104-6 '. propyylinortropanyyli

Sp. [°C] 14 114395Sp. [° C] 14114395

No. A Ri emäs hydro- kloridi 5 13 3a-(66,76-epoksi)-N-n- 2-tienyyli butyylinortropanyyli 225-7 14 3a-(66,76-epoksi)-tropanyyli fenyyli 246-7 15 3a-tropanyyli fenyyli 243-4 16 3a-(N-6-fluorietyyli)- fenyyli 10 nortropanyyli 219-20 17 3a-(6,7-dehydro)tropanyyli fenyyli 181-3 18 3a-(N-etyyli)-nortropanyyli fenyyli 231-2 19 3a-(N-isopropyyli)- nortropanyyli fenyyli 246-7 15 20 3a-tropanyyli sykloheksyyli 260 21 3a-(N-6-fluorietyyli)- sykloheksyyli nortropanyyli 203-4 22 3a-(68,78-epoksi)-tropanyyli syklopentyyli 237 23 3a-tropanyyli syklopentyyli 260 20 24 3a-(N-8-fluorietyyli)- syklopentyyli ; nortropanyyli 182-3 25 3a-(N-etyyli)-nortropanyyli syklopentyyli 227-8 :...: 26 3a-(N-isopropyyli)- nortropanyyli syklopentyyli 174-5 25 27 38-(66,78-epoksi)-tropanyyli 2-tienyyli 240-2 v *’ 28 36-tropanyyli 2-tienyyli 217-9 29 36-(6,7-dehydro)tropanyyli 2-tienyyli 233-5 ..1: 30 3a-(6,7-dehydro)-tropanyyli 3-tienyyli 247-8 31 3a-(66,76-epoksi)-tropanyyli 3-tienyyli 242-3 : 30 32 3a-(66,76-epoksi)-tropanyyli 2-furyyli 33 3a-(6,7-dehydro)-tropanyyli 2-furyyli 34 3a-tropanyyli 2-furyyli ....: 35 3a-tropanyyli 2-pyridyyli 36 3a-(66,76-epoksi)-tropanyyli 2-pyridyyliWell. A 1 Basic Hydrochloride 5 13 3α- (66.76-epoxy) -Nn-2-thienyl butylnortropanyl 225-7 14 3α- (66.76-epoxy) -tropanyl phenyl 246-7 15 3α-tropanyl phenyl 243- 4 16 3a- (N-6-fluoroethyl) phenyl 10 nortropanyl 219-20 17 3a- (6,7-dehydro) tropanyl phenyl 181-3 18 3a- (N-ethyl) -nortropanyl phenyl 231-2 19 3a (N-Isopropyl) -Nortropanyl Phenyl 246-7 15 20 3a-Tropanyl Cyclohexyl 260 213a- (N-6-Fluoroethyl) Cyclohexyl Nortropanyl 203-4 22 3a- (68,78-Epoxy) Tropanyl Cyclopentyl 237 23 3a -tropanyl cyclopentyl 260 20 24 3- (N-8-fluoroethyl) cyclopentyl; nortropanyl 182-3 25 3a- (N-ethyl) -nortropanyl cyclopentyl 227-8: ...: 26 3a- (N-isopropyl) nortropanyl cyclopentyl 174-5 25 27 38- (66,78-epoxy) -tropanyl 2-thienyl 240-2 v ′ 28 36-tropanyl 2-thienyl 217-9 29 36- (6,7-dehydro) tropanyl 2-thienyl 233-5.1: 30 3α- (6,7-dehydro) -tropanyl 3-thienyl 247-8 31 3a- (66.76-epoxy) -tropanyl 3-thienyl 242-3: 30 32 3a- (66.76-epoxy) -tropanyl 2-furyl 33 3a- (6.7 -dehydro) -tropanyl 2-furyl 34 3a-tropanyl 2-furyl ....: 35 3a-tropanyl 2-pyridyl 36 3- (66.76-epoxy) -tropanyl 2-pyridyl

Sp. [°C] 15 114395Sp. [° C] 15114395

No. A Ri emäs hydro- kloridi 5 37 3a-(6,7-dehydro)-tropanyyli 2-pyridyyli 38 3a-tropanyyli 3-tienyyli 39 3a-(6,7-dehydro)-tropanyyli syklopentyyli 40 3a-(66,78-epoksi)-tropanyyli sykloheksyyli 41 3a-(6,7-dehydro)-tropanyyli sykloheksyyli 10Well. A 1 Basic Hydrochloride 5 37 3α- (6,7-Dehydro) Tropanyl 2-Pyridyl 38 3α-Tropanyl 3-Thienyl 39 3α- (6,7-Dehydro) Tropanyl Cyclopentyl 40 3α- (66.78- epoxy) -tropanyl cyclohexyl 41 3- (6,7-dehydro) -tropanyl cyclohexyl 10

Huomautus: kaikki hydrokloridit sulavat hajoten.Note: All hydrochlorides will melt with decomposition.

Esimerkki 4 15 Skopiinidi-(2-tienyyli)glykolaattimetobromidi 10,0 g (0,0265 mol) skopiinidi-(2-tienyyli)glykolaattia liuotetaan seokseen, jossa on 20 ml vedetöntä metyleenikloridia ja 30 ml vedetöntä asetonitriiliä, ja käsitellään 12,8 g:Ha (0,1325 mol) metyylibromidia (50-% liuoksena vedettömässä asetonitrii-20 Iissä), ja reaktioseos saa seistä 24 tuntia huoneenlämpötilassa tiiviisti suljetussa • * astiassa. Tämän aikana saostuu kiteitä. Ne suodatetaan imupullolla, pestään mety- ; :; leenikloridia käyttämällä, ja kuivataan 35 °C:ssa alennetussa paineessa. Valkoisia kiteitä (metanoli/asetonista), sp. 217-8 °C (hajoaa) kuivaamisen jälkeen 111 °C:ssa alennetussa paineessa.Example 4 Scopinide (2-thienyl) glycolate metobromide 10.0 g (0.0265 mol) of scopine di (2-thienyl) glycolate are dissolved in a mixture of 20 ml of anhydrous methylene chloride and 30 ml of anhydrous acetonitrile and treated with 12.8 g : Ha (0.1255 mol) methyl bromide (50% solution in anhydrous acetonitrile-20) and the reaction mixture is allowed to stand for 24 hours at room temperature in an airtight container. During this time crystals precipitate. They are suction filtered, washed with methylene chloride; :; lene chloride and dried at 35 ° C under reduced pressure. White crystals (from methanol / acetone), m.p. 217-8 ° C (decomposes) after drying at 111 ° C under reduced pressure.

.··; 25. ··; 25

Kvaternääriset yhdisteet, joilla on kaava ie 114395Quaternary compounds of the formula ie 114395

Taulukko IITable II

5 r^s *==<5 r ^ s * == <

HO-C-CO-OAHO-C-CO-OA

R1 10 No. A Rl Sp. [°C] 1 3a-(68,7B-epoksi)-tropanyyli- metobromidi 2-tienyyli 217-18 2 3a-tropanyylimetobromidi 2-tienyyli 263-64 15 3 3a-(6,7-dehydro)-tropanyyli- metobromidi 2-tienyyli 191-92 4 3a-(N-6-fluorietyyli)-nortro- panyylimetobromidi 2-tienyyli 242-43 5 3a-tropanyyli-6-fluorietobromidi 2-tienyyli 214-15 20 6 3a-(N-isopropyyli)- • granatanyylimetobromidi 2-tienyyli 229-30 7 3cc-(N-isopropyyli)- nortropanyylimetobromidi 2-tienyyli 245-46 i 8 3a-(66,76-epoksi)-N-isopropyyli- ,: 25 nortropanyyli-metobromidi 2-tienyyli 223-24 . 9 3a-(66,78-epoksi)-N-etyyli- nortropanyylimetobromidi 2-tienyyli 215-16 :' 10 3a-(N-etyyli)-nortropanyyli- ; metobromidi 2-tienyyli 260-61 :·. 30 11 3a-(N-metyyli)-granatanyyli- .··*. metobromidi 2-tienyyli 246-47 ’. _ 12 3a-(66,78-epoksi)-N-fluorietyy- linortropanyylimetobromidi 2-tienyyli 182-83 » ·R1 10 No. Rl Sp. [° C] 13a - (68.7B-epoxy) -tropanyl-methobromide 2-thienyl 217-18-23a-tropanyl-methyl-bromide 2-thienyl 263-64153- 3 - (6,7-dehydro) -tropanyl-methobromide 2 -thienyl 191-92 4- 3a- (N-6-fluoroethyl) -nortropanylmethobromide 2-thienyl 242-43,53a-tropanyl-6-fluoroethobromide 2-thienyl 214-1520 6 3a- (N-isopropyl) - • granatanylmetobromide 2-thienyl 229-30 7c- (N-isopropyl) -nortropanylmethobromide 2-thienyl 245-46-8 3a- (66.76-epoxy) -N-isopropyl-: 25-nortropanyl-methobromide 2-thienyl 223- 24th 9α- (6,6,78-epoxy) -N-ethylnortropanylmetobromide 2-thienyl 215-16: 10β- (N-ethyl) -nortropanyl; metobromide 2-thienyl 260-61: ·. 30 11 3a- (N-Methyl) -Granatanyl · · *. metobromide 2-thienyl 246-47 '. - 12 3a- (6,6,78-epoxy) -N-fluoroethyl orthropanylmethobromide 2-thienyl 182-83 »·

No. A Ri Sp. [°C] 17 114395 13 3a-(66,78-epoksi)-N-n-propyy- linortropanyylimetobromidi 2-tienyyli 209-10 5 14 3a-tropanyyli-6-hydroksietobromidi 2-tienyyli 231-32 15 3a-(66,76-epoksi)-tropanyyli- metobromidi fenyyli 217-18 16 3a-tropanyylimetobromidi fenyyli 273-74 17 3a-(N-8-fluorietyyli)-nortropanyyli- 10 metobromidi fenyyli 215 18 3a-(6,7-dehydro)-tropanyyli- metobromidi fenyyli 170-71 19 3a-(N-etyyli)-nortropanyyli- metobromidi fenyyli 249-50 15 20 3a-(N-isopropyyli)-nortro- panyylimetobromidi fenyyli 259-60 21 3a-tropanyylietobromidi fenyyli 248-49 22 3a-(N-etyyli)-nortropanyyli- etobromidi fenyyli 244-45 20 23 3a-(6B,76-epoksi)-tropanyyli- • etobromidi fenyyli 226 v,: 24 3a-tropanyyli-6-fluorietobromidi fenyyli 241 25 3a-tropanyylimetobromidi sykloheksyyli 278 : 26 3a-(N-6-fluorietyyli)nortro- 25 panyylimetobromidi sykloheksyyli 198 v : 27 3a-tropanyyli-6-fluorietobromidi sykloheksyyli 233-34 28 3a-tropanyylimetobromidi syklopentyyli 260 29 3a-tropanyylietobromidi syklopentyyli 235-36 ) » ( 30 3a-(N-etyyli)-nortropanyyli- 30 metobromidi syklopentyyli 251-52 31 3a-(N-isopropyyli)-nortropa- nyyli metobromidi syklopentyyli 244-45 ...,: 32 3a-tropanyyli-6-fluorietobromidi syklopentyyli 189-90 • *Well. Ri Sp. [° C] 17114395 13a- (66.78-epoxy) -Nn-propyl-orthropanyl-methobromide 2-thienyl 209-105143-a-tropanyl-6-hydroxy-ethobromide 2-thienyl 231-32153- (66.76 -epoxy) -tropanyl-methobromide phenyl 217-18 16 3a-tropanyl-methobromide phenyl 273-74 17 3α- (N-8-fluoroethyl) -nortropanyl-methobromide phenyl 215 18 3α- (6,7-dehydro) -tropanyl-methobromide phenyl 170-71 19 3a- (N-ethyl) -nortropanyl-methobromide phenyl 249-50 15 20 3a- (N-isopropyl) -nortropanyl-methobromide phenyl 259-60 21 3a-tropanyl-ethobromide phenyl 248-49 22 3a- (N -ethyl) -nortropanyl-ethobromide phenyl 244-45 20 23 3α- (6β, 76-epoxy) -tropanyl-ethobromide phenyl 226v ,: 24 3α-tropanyl-6-fluoro-ethobromide phenyl 241 25 3α-tropanyl-methobromide cyclohexyl 278: 26 3α- (N-6-fluoroethyl) nortropanylmethobromide cyclohexyl 198v: 27 3α-tropanyl-6-fluoroethobromide cyclohexyl 233-34 28 3α-tropanylmethobromide cyclopentyl 260 29 3a-tropanyl ethobromide cyclopentyl 235-36) »(30 3a- (N-ethyl) -nortropanyl-30-methobromide cyclopentyl 251-52 31 3a- (N-isopropyl) -nortropanyl methobromide cyclopentyl 244-45 ...,: 32 3a-tropanyl-6-fluoroethobromide cyclopentyl 189-90 • *

No. A Ri Sp. [°C] 18 114395 33 3cc-(N-8-fluorietyyli)nortro- panyylimetobromidi syklopentyyli 226-27 5 34 3a-(6,7-dehydro)tropanyyli- metometaanisulfonaatti 2-tienyyli 225-6 35 3a-(68,76-epoksi)-tropanyyli- metobromidi 2-tienyyli 218-20 36 3a-tropanyylimetobromidi 2-tienyyli 243-4 10 37 3a-(6,7-dehydro)-tropanyyli- metobromidi 2-tienyyli 211-4 38 3a-(6,7-dehydro)-tropanyyli- metobromidi 3-tienyyli 182-3* 39 3a-(6B,76-epoksi)-tropanyyli- 15 metobromidi 3-tienyyli 217-8 40 No. Γ.η (-t-)-enantiomeeri 41 No. l:n (-)-enantiomeeri 42 3a-(66,76-epoksi)-tropanyyli- metobromidi 2-furyyli 20 43 3a-(6,7-dehydro)-tropanyyli- • ’ · metobromidi 2-furyyli 44 3a-tropanyylimetobromidi 2-furyyli :,,,: 45 3oc-(68,78-epoksi)tropanyyli- ‘: : metobromidi 2-pyridyyli : 25 46 3a-(6,7-dehydro)-tropanyyli- :, : metobromidi 2-pyridyyli 47 3a-tropanyylimetobromidi 2-pyridyyli 48 3a-tropanyy!imetobromidi 3-tienyyli 49 3a-(6,7-dehydro)-tropanyyli- 30 metobromidi syklopentyyli 50 3a-(66,76-epoksi)-tropanyyli- ';, metobromidi sykloheksyyli 19 Π4395Well. Ri Sp. [° C] 18114395 33 3c- (N-8-Fluoroethyl) nortropanylmethobromide cyclopentyl 226-27-534 3a- (6,7-dehydro) tropanylmethane sulfonate 2-thienyl 225-6 35 3a- (68.76 -epoxy) -tropanyl-methobromide 2-thienyl 218-20 36 3a-tropanyl-methobromide 2-thienyl 243-4 10 37 3a- (6,7-dehydro) -tropanyl-methobromide 2-thienyl 211-4 38 3a- (6, 7-Dehydro) -tropanyl-methobromide 3-thienyl 182-3 * 39 3a- (6B, 76-epoxy) -tropanyl-methobromide 3-thienyl 217-8 Γ.η (-t -) - Enantiomer 41 1 - (-) - Enantiomer 42 3a- (6,6,76-epoxy) -tropanyl-methobromide 2-furyl 20 43 3a- (6,7-dehydro) -tropanyl-4'-metobromide 2-furyl 44 3a-tropanyl-methobromide 2-furyl:,,: 45 3c- (68.78-epoxy) tropanyl ':: methobromide 2-pyridyl: 25 46 3α- (6,7-dehydro) -tropanyl :,: metobromide 2-pyridyl 47 3a-Tropanylmethobromide 2-Pyridyl 48 3a-Tropanylmethobromide 3-Thienyl 49 3a- (6,7-Dehydro) -tropanyl-Metobromide Cyclopentyl 50 3a- (66.76-Epoxy) -tropanyl ', Metobromide Cyclohexyl 19 Π4395

No. A Ri Sp. [°C] 51 3a-(6,7-dehydro)-tropanyyli- metobromidi sykloheksyyli 5 52 3a-(66,76-epoksi)-tropanyyli- metobromidi syklopentyyli * sisältää kidemetanolia 10 Huomautus: Kaikki taulukossa olevat yhdisteet sulavat hajoten.Well. Ri Sp. [° C] 51 3a- (6,7-Dehydro) -tropanyl-methobromide cyclohexyl-5 52 3a- (66.76-epoxy) -tropanyl-methobromide cyclopentyl * contains crystal methanol 10 Note: All compounds in the table decompose.

» »* » 114395 5»» * »114395 5

Yhdisteet, joilla on kaava 20Compounds of Formula 20

Taulukko IIITable III

HO-C-CO-OAHO-C-CO-OA

^R1 10 No. A Rl Sp. [°C] hydrokloridi 1 3a-(66,76-epoksi)-tropanyyli fenyyli 246-7 15 2 3a-(6,7-dehydro)-tropanyyli fenyyli 261-2 3 3a-(6B,76-epoksi)-tropanyyli 3-tienyyli 4 3a-(6,7-dehydro)-tropanyyii 3-tienyyii 5 3cc-tropanyyli 3-tienyyli 6 3a-(N-metyyli)-granatanyyli 3-tienyyli * · 1« »^ R1 10 No. Rl Sp. [° C] Hydrochloride 13α- (66.76-epoxy) -tropanyl phenyl 246-7 15α-3α- (6,7-dehydro) -tropanyl phenyl 261-23β- (6β, 76-epoxy) tropanyl 3-thienyl 4 -3a- (6,7-dehydro) -tropanyl 3-thienyl 5 3c-tropanyl 3-thienyl 6 3a- (N-methyl) -grananyl 3-thienyl * · 1 «»

Taulukko IVTable IV

21 11439521, 114395

Yhdisteet, joilla on kaava 5Compounds of Formula 5

Ur/ R.-c-co-o-aUr / R.-c-co-o-a

Hn 10Hn 10

No. A R2 Sp. [°C] hydrokloridi 15Well. R2 Sp. [° C] hydrochloride 15

1 3a-(6B,7B-epoksi)-tropanyyli H13? - (6B, 7B-Epoxy) -tropanyl H

2 3a-(6,7-dehydro)-tropanyyli H2 3a- (6,7-dehydro) -tropanyl H

3 3a-(6B,7B-epoksi)-tropanyyli metyyli 4 3a-(6,7-dehydro)-tropanyyli metyyli 210-2,5 20 5 3a-(6B,7B-epoksi)-tropanyyli metoksi 6 3a-(6,7-dehydro)-tropanyyli metoksi • · * • * * t * • > • · • · · • I * • * » I ‘ » * * · I · > » · t t * » ( » • » }3α- (6β, 7β-epoxy) -tropanylmethyl 4α- (6β, 7β-dehydro) -tropanylmethyl 210-2.5 20 5α- (6β, 7β-epoxy) -tropanyl methoxy 6α- , 7-Dehydro) -tropanyl Methoxy • · * • * * t * •> • • • • • I * • * »I '» * * · I ·> »· tt *» (»•»}

» I»I

Taulukko VTable V

Yhdisteet, joilla on kaava 22 1 14395Compounds of formula 22 1 14395

5 Ra-P5 Ra-P

HO-C-CO-OAHO-C-CO-OA

R1 10 No. A Ri Ra Sp. [°C] 1 3a-(66,76-epoksi)tropanyyli 2-tienyyli 5-metyyli 2 3a-(6,7-dehydro)-tropanyyli 2-tienyyli 5-metyyli 3 3a-tropanyyli 2-tienyyli 5-metyyli 15 4 3a-(68,78-epoksi)-tropanyyli 2-(5-metyyli)- tienyyli 5-metyyli 5 3a-(6,7-dehydro)-tropanyyli 2-(5-metyyli)- tienyyli 5-metyyli 6 3a-tropanyyli 2-(5-metyyli)- 20 tienyyli 5-metyyli I 7 3a-(68,76-epoksi)-tropanyyli 2-tienyyli 5-fluori 8 3a-(6,7-dehydro)-tropanyyli 2-tienyyli 5-fluori ; 9 3a-tropanyyli 2-tienyyli 5-fluori : 10 3a-(6B,76-epoksi)-tropanyyli 2-(5-fluori)- ; ' : 25 tienyyli 5-fluori ; ;11 3a-(6,7-dehydro)-tropanyyli 2-(5-fluori)- tienyyli 5-fluori . ’ 12 3a-tropanyyli 2-(5-fluori)- i ]: tienyyli 5-fluori tR1 10 No. A Ri Ra Sp. [° C] 13α- (66.76-epoxy) tropanyl 2-thienyl 5-methyl-2,3α- (6,7-dehydro) -tropanyl 2-thienyl 5-methyl-3α-tropanyl 2-thienyl 5-methyl 4α- (68.78-epoxy) -tropanyl 2- (5-methyl) -thienyl 5-methyl-5α- (6,7-dehydro) -tropanyl 2- (5-methyl) -thienyl 5-methyl-6α -tropanyl 2- (5-methyl) -20-thienyl 5-methyl-7α- (68.76-epoxy) -tropanyl 2-thienyl 5-fluoro-β- (6,7-dehydro) -tropanyl 2-thienyl -fluorine; 9α-tropanyl 2-thienyl 5-fluoro: 10α- (6β, 76-epoxy) -tropanyl 2- (5-fluoro) -; ': Thienyl 5-fluoro; 11a - (6,7-dehydro) -tropanyl 2- (5-fluoro) -thienyl 5-fluoro. '12 3a-Tropanyl 2- (5-fluoro) -1] thienyl 5-fluoro t

* I* I

! t » t * ϊ ί » S ! I »! t »t * ϊ ί» S! I »

Taulukko VITable VI

23 11439523 114395

Yhdisteet, joilla on kaava 5 f=\Compounds of Formula 5 f = \

HO-<p~CO-OAHO- <p ~ CO-OA

R1 10R1 10

No. A Ri Ra Sp. [°C] 1 3a-(66,76-epoksi)tropanyyli- 2-tienyyli 5-metyyli metobromidi 15 2 3a-(6,7-dehydro)tropanyyli- 2-tienyyli 5-metyyli metobromidi 3 3a-tropanyylimetobromidi 2-tienyyli 5-metyyli 4 3a-(66,76-epoksi)tropanyyli- 2-(5-metyyli)- metobromidi tienyyll 5-metyyli 20 5 3a-(6,7-dehydro)tropanyyli- 2-(5-metyyli)- , ·· metobromidi tienyyli 5-metyyli 6 3a-tropanyylimetobromidi 2-(5-metyyli)- : tienyyli 5-metyyli 7 3a-(66,70-epoksi)tropanyyli- 2-tienyyli 5-fluori :: 25 metobromidi 8 3a-(6,7-dehydro)tropanyyli- 2-tienyyli 5-fluori metobromidi 9 3a-tropanyylimetobromidi 2-tienyyli 5-fluori ·../ 10 3a-(66,76-epoksi)tropanyyli- 2-(5-fluori)- Γ’.. 30 metobromidi tienyyli 5-fluori ; 11 3cc-(6,7-dehydro)tropanyyli- 2-(5-fluori)- metobromidi tienyyli 5-fluori 12 3a-tropanyylimetobromidi 2-(5-fluori)- tienyyli 5-fluoriWell. A Ri Ra Sp. [° C] 13? - (66.76-epoxy) tropanyl-2-thienyl 5-methyl methobromide 15? 3? - (6,7-dehydro) tropanyl-2-thienyl 5-methyl methobromide 3? 5-methyl-4 - [(6,7,7-epoxy) tropanyl-2- (5-methyl) -metobromide thienyl] -5-methyl-5 - [(6,7-dehydro) tropanyl-2- (5-methyl) -, ·· Metobromide thienyl 5-methyl 6 3α-tropanylmethobromide 2- (5-methyl) -: thienyl 5-methyl 7β- (6,6,70-epoxy) tropanyl-2-thienyl 5-fluoro :: 25 methobromide 8 3α- ( 6,7-dehydro) tropanyl-2-thienyl 5-fluoro-methobromide 9a-tropanyl-methobromide 2-thienyl-5-fluoro · 10 3α- (66.76-epoxy) tropanyl-2- (5-fluoro)-- 30 Metobromide Thienyl 5-Fluoro; 11c- (6,7-Dehydro) tropanyl-2- (5-fluoro) -metobromide thienyl 5-fluoro 12 3a-tropanyl-methobromide 2- (5-fluoro) thienyl 5-fluoro

Yhdisteet, joilla on kaava 24 114395Compounds of formula 24 114395

Taulukko VIITable VII

5 ρ=\ *5 ρ = \ *

HO-C-CO-OAHO-C-CO-OA

1010

No. A Ri Sp. [°C] 1 3a-(6B,7B-epoksi)tropanyyli- fenyyli 211-2 metobromidi 15 2 3a-(6,7-dehydro)tropanyyli- fenyyli 158-60* metobromidi 3 3a-(6B,7B-epoksi)tropanyyli- 3-tienyyli metobromidi 4 3a-(6,7-dehydro)tropanyyli- 3-tienyyli 20 metobromidi • 5 3oc-tropanyylimetobromidi 3-tienyyli : 6 3a-(N-metyyli)granatanyyli- 3-tienyyli : metobromidi .' : 25 * (kidemetanolin kanssa) 25 114395Well. Ri Sp. [° C] 13a - (6B, 7B-epoxy) tropanyl-phenyl 211-2 methobromide 15-23a- (6,7-dehydro) tropanyl-phenyl 158-60 * metobromide 3a-3a (6B, 7B-epoxy) tropanyl-3-thienyl methobromide 4 3a- (6,7-dehydro) tropanyl-3-thienyl 20 methobromide • 5 3 C -tropanylmethobromide 3-thienyl:? : 25 * (with crystal methanol) 25 114395

Taulukko VIIITable VIII

Kvaternääriset yhdisteet, joilla on kaava 5 f==r\Quaternary compounds of formula 5 f == r \

SS

R--C-CO-OAR - C-CO-OA

r1-, io ------r1-, io ------

No. A R2 Sp. [°C]Well. R2 Sp. [° C]

1 3a-(66,76-epoksi)-tropanyyli- H13α- (66.76-epoxy) -tropanyl-H

15 metobromidi15 Metobromide

2 3a-(6,7-dehydro)-tropanyyli- H2 3a- (6,7-dehydro) -tropanyl-H

metobromidi 3 3a-(66,73-epoksi)-tropanyyli- metyyli metobromidi 20 4 3a-(6,7-dehydro)-tropanyyli- metyyli 206-8 ; · metobromidi v,: 5 3a-tropanyylimetobromidi metoksi *...· 6 3a-(N-metyyli)-tropanyyli- metobromidi metoksi 25methobromide 3α- (6,6,73-epoxy) -tropanylmethyl methobromide 20β-3- (6,7-dehydro) -tropanylmethyl 206-8; · Methobromide v: 5 3a-tropanylmethobromide methoxy * ... · 6 3a- (N-methyl) -tropanylmethobromide methoxy 25

Claims (5)

26 11439526 114395 1. Menetelmä valmistaa farmakologisesti vaikuttavia tienyylikarboksyylihappojen ja aminoalkoholien estereitä, joilla on kaava I 5 F=\ R--S a 1=^/ (i) RrC-CO-OA r2 10 jossa A on ryhmä CH2-CH / 0 \ -CH R-N-R' Q (n) 15 \ CH;,—-CH jossa Q on yksi seuraavista kaksiarvoisista ryhmistä 20 -ch2-ch2-, -ch2-ch2-ch2-, -ch=ch-, : -CH -CH- / \ / ' ä O \ i 25 : ja R on mahdollisesti halogeenisubstituoitu tai hydroksisubstituoitu Ci-C,-alkyyliradi-.,; i * kaali, R' on Ci-Q-alkyyliradikaali ja R ja R' voivat myös yhdessä muodostaa CrC6- :alkyleeniradikaalin, ja jossa positiivisen varauksen ekvivalentiksi vastapainoksi aset-30 tuu anioni (Χθ), R! on tienyyli-, fenyyli-, furyyli-, syklopentyyli- tai sykloheksyyliradikaali, jolloin nämä ’ ’ ‘ ; radikaalit voivat myös olla metyylisubstituoituja, tienyyli ja fenyyli voivat myös olla fluorisubstituoituja tai kloorisubstituoituja, 27 114395 R2 on vety, OH, Ci-Q-alkoksi tai CrQ-alkyyli, Ra on H, F, Cl tai CH3, tunnettu siitä, että kaavan IV mukainen esteri 5 F=\ R--S a (IV) R^C-CO-OR" r2 10 jossa R" on Ci-Q-alkyyliradikaaii ja Ri, R2 ja Ra ovat edellä määritellyt, vaihto-esteröidään käyttämällä kaavan V mukaista aminoalkoholia1. A process for preparing pharmacologically active esters of thienylcarboxylic acids and amino alcohols of the formula I 5 F = R - S a 1 = ^ / (i) R 1 -C-CO-OA 2 R 2 wherein A is CH 2 -CH / O RNR 'Q (n) 15 \ CH;, -CH where Q is one of the following bivalent groups 20 -ch2-ch2-, -ch2-ch2-ch2-, -ch = ch-, -CH-CH- / \ ???????? and R is optionally halogen substituted or hydroxy substituted C 1 -C 6 alkyl radical; i * calix, R 'is a C 1 -C 4 alkyl radical and R and R' may also be taken together to form a C 1 -C 6 alkylene radical, and in which the anion (Χθ), is a thienyl, phenyl, furyl, cyclopentyl or cyclohexyl radical, wherein these are ""; the radicals may also be methyl-substituted, thienyl and phenyl may also be fluoro-substituted or chloro-substituted; R 11 is hydrogen, OH, C 1 -C 4 -alkoxy or C 1 -C 4 -alkyl, R a is H, F, Cl or CH 3, characterized in that the ester 5 F = 1 R - S a (IV) R 1 -C-CO-OR "r 2 10 wherein R" is a C 1 -C 4 alkyl radical and R 1, R 2 and R a are as defined above, aminoalcohol 15 HO-CH Q” Q (V) ΧΧχ0Η2— jossa Q on edellä määritelty ja Q" on =NR tai =NH, inertissä orgaanisessa liuotti-20 messa tai sulatteessa, vaihtoesteröinti-katalysaattorin läsnä ollessa, ja saatu yhdiste, jolla on kaava (VI) I I * -\ ..· n--C ru-CH ! ΚΠΞ|ζ=ι/ ^Γ2 |X ;;i 25 RrC-C0-0-CH Q" Q (VI) \ 1/^ CH2---—CH :jossa Q" on =NR, kvaternisoidaan käyttämällä alkaanin reak-tiivista monofunktiona-:' ·.. 30 lisoitua johdannaista Z-(CrGt-alkyyli), jossa Z on poistuva ryhmä.HO-CH Q "Q (V) ΧΧχ0Η2— wherein Q is as defined above and Q" is = NR or = NH, in an inert organic solvent or melt, in the presence of a transesterification catalyst, and the compound of formula ( VI) II * - \ .. · n - C ru-CH! ΚΠΞ | ζ = ι / ^ Γ2 | X ;; i 25 RrC-C0-0-CH Q "Q (VI) \ 1 / ^ CH2-. - - CH: where Q "is = NR is quaternized using an alkane reactive monofunctional derivative Z- (C 1 -C 4 alkyl) where Z is a leaving group. 2. Patenttivaatimuksen 1 mukainen menetelmä valmistaa kaavan I mukainen yhdis- » ’.'te, jossa Ri on 2-tienyyli, tunnettu siitä, että käytetään vastaavia lähtöaineita. 28 114395A process according to claim 1 for the preparation of a compound of formula I wherein R 1 is 2-thienyl, characterized in that the corresponding starting materials are used. 28, 114395 3. Patenttivaatimuksen 1 tai 2 mukainen menetelmä kaavan I mukaisen yhdisteen valmistamiseksi, jossa Rx on 2-tienyyli ja A onA process for the preparation of a compound of formula I according to claim 1 or 2, wherein Rx is 2-thienyl and A is 5 CH3-®N-CH3 ^0 -p tai _^_ -^CH3®N-CH3 xG 10 sen 3a-muodossa, jossa X9 on anionin ekvivalentti, joka on Br9 tai CH3S039, tunnettu siitä, että käytetään vastaavia lähtöaineita.CH3-®N-CH3 ^ O -p or _ ^ _ - ^ CH3®N-CH3 xG10 in its 3a form, wherein X9 is the anion equivalent of Br9 or CH3SO39, characterized in that the corresponding starting materials are used. 4. Patenttivaatimuksen 1 mukainen menetelmä valmistaa yhdiste, jonka kaava on 15 [=Λ _ S H0-Cj-C0-0Br ° tai CH3Sof 20 [=^ S ——/ : ; tai -\ _ SA process according to claim 1 for the preparation of a compound of the formula 15 [= Λ -SH0-C3-C0-0Br ° or CH3Sof20 [= ^ S -— /:; it - \ _ S 25 H0-(^-CO-0 -<(CH3l|^H3 Br° tai CH3SC>f S 30 sen 3cx-muodossa, tunnettu siitä, että käytetään vastaavia lähtöaineita. .» · *11· t · 29 11439525 H0 - (^ - CO-0 - <(CH3l | ^ H3 Br ° or CH3SC> f S 30 in its 3cx form, characterized in that the corresponding starting materials are used.) »· * 11 · t · 29 114395 5. Lähtöaineena käytettävä kemiallinen yhdiste, tunnettu siitä, että sillä on kaava _ S 5 ( /~1 N H0-(j:-C0-0 fjjCH3 O S -/ tai 10 \ H /Ί- HO-(j>CO-C) lj!CH3 s -/ 15 t f · t 30 11439 55. Chemical compound used as starting material, characterized in that it has the formula _S5 (/ ~ 1N H0- (j: -C0-0 fjjCH3 OS - / or 10 \ H / Ί-HO- (j> CO-C ) lj! CH3 s - / 15 tf · t 30 11439 5
FI921087A 1989-09-16 1992-03-13 Process for Preparation of Esters and Intermediate Pharmacologically Efficient Thienyl Carboxylic Acids and Amino Alcohols FI114395B (en)

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DE3931041A DE3931041C2 (en) 1989-09-16 1989-09-16 Esters of thienyl carboxylic acids with amino alcohols, their quaternization products, processes for their preparation and medicaments containing them
DE3931041 1989-09-16
PCT/EP1990/001517 WO1991004252A1 (en) 1989-09-16 1990-09-08 New esters of thienyl carboxylic acids and amino alcohols, their quaternization products, and manufacture and use of said compounds
EP9001517 1990-09-08

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PT95312A (en) 1991-05-22
KR910006272A (en) 1991-04-29
NO921002L (en) 1992-03-13
CZ452390A3 (en) 1998-11-11
SI9011744A (en) 1997-10-31
PL168468B1 (en) 1996-02-29
DE10299026I1 (en) 2002-11-07
NO921002D0 (en) 1992-03-13
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ES2052125T3 (en) 1994-07-01
UA41272C2 (en) 2001-09-17
NO301478B1 (en) 1997-11-03
PH31617A (en) 1999-01-12
IL95691A (en) 1996-07-23
HU9200857D0 (en) 1992-05-28
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WO1991004252A1 (en) 1991-04-04
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