CA1268461A - 2-(2-picolylsulfur)-trienoimidazole derivatives - Google Patents

2-(2-picolylsulfur)-trienoimidazole derivatives

Info

Publication number
CA1268461A
CA1268461A CA000574551A CA574551A CA1268461A CA 1268461 A CA1268461 A CA 1268461A CA 000574551 A CA000574551 A CA 000574551A CA 574551 A CA574551 A CA 574551A CA 1268461 A CA1268461 A CA 1268461A
Authority
CA
Canada
Prior art keywords
alkyl
denotes
compound
formula
alkoxy
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Expired - Fee Related
Application number
CA000574551A
Other languages
French (fr)
Inventor
Hans-Jochen Lang
Klaus Weidmann
Robert Rippel
Karl-Heinz Scheunemann
Andreas W. Herling
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Hoechst AG
Original Assignee
Hoechst AG
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Hoechst AG filed Critical Hoechst AG
Application granted granted Critical
Publication of CA1268461A publication Critical patent/CA1268461A/en
Anticipated expiration legal-status Critical
Expired - Fee Related legal-status Critical Current

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D495/00Heterocyclic compounds containing in the condensed system at least one hetero ring having sulfur atoms as the only ring hetero atoms
    • C07D495/02Heterocyclic compounds containing in the condensed system at least one hetero ring having sulfur atoms as the only ring hetero atoms in which the condensed system contains two hetero rings
    • C07D495/04Ortho-condensed systems
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P1/00Drugs for disorders of the alimentary tract or the digestive system
    • A61P1/04Drugs for disorders of the alimentary tract or the digestive system for ulcers, gastritis or reflux esophagitis, e.g. antacids, inhibitors of acid secretion, mucosal protectants
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P1/00Drugs for disorders of the alimentary tract or the digestive system
    • A61P1/12Antidiarrhoeals
    • YGENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
    • Y02TECHNOLOGIES OR APPLICATIONS FOR MITIGATION OR ADAPTATION AGAINST CLIMATE CHANGE
    • Y02PCLIMATE CHANGE MITIGATION TECHNOLOGIES IN THE PRODUCTION OR PROCESSING OF GOODS
    • Y02P20/00Technologies relating to chemical industry
    • Y02P20/50Improvements relating to the production of bulk chemicals
    • Y02P20/55Design of synthesis routes, e.g. reducing the use of auxiliary or protecting groups

Landscapes

  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Health & Medical Sciences (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • General Chemical & Material Sciences (AREA)
  • Medicinal Chemistry (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Engineering & Computer Science (AREA)
  • Animal Behavior & Ethology (AREA)
  • General Health & Medical Sciences (AREA)
  • Public Health (AREA)
  • Veterinary Medicine (AREA)
  • Heterocyclic Carbon Compounds Containing A Hetero Ring Having Oxygen Or Sulfur (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Plural Heterocyclic Compounds (AREA)

Abstract

Abstract of the disclosure:
Substituted thienoimidazole derivatives, processes for their preparation,pharmaceutical formulations containing them and their use as gastric acid secretion inhibitors.

The invention relates to compounds of the formula I
(I) in which A stands for (a) , (b) or (c)

Description

~268~i HOECHST AKTIENGESELLSCHAFT HOE 87/F 242 K Dr.~I/je aescription Substituted th;eno;midazole derivatives, processes for their preparat;on, pharmaceutical formulations contain;ng them and the;r use as gastric acid secretion inhibitors.

Thienoimidazole derivatives ~ith a gastric acid secre-tion-inhibit;ng action are kno~n from EP-A1-234,485, EP-A2-201,094 and EP-A-237,248.

The present invention r~lates to novel thienoimidazole derivatives of the for~ula I

R4 R ~ R~
C l~

in ~hich R2 R~
T denotes -S-, -SO- or -S02-, R1 and RZ are identical or different and denote hydrogen, halogen, cyano, nitro, trifluoromethyl~ tC1-C6)-alkyl, tC1-e6)-hydroxyalkyl, (C1-C~)-alkoxy, ~~[CH~O~cpHt2p~1-4)Halq~ preferabLy tC1-C8)-fluoroalkoxy~ tC1-Cg)-fluoroalk~nyloxy, tC1-Cg)-fluoroalkynyloxy, -OCFzCl or -0-CF2-CHFClr tC1-C6)-alkylmercapto, tC1-C~)-alkylsulfinyl, tt1 C6)-alkylsulfonyl, (C~-C6)-alkylcarbonyl, tC1-C6)-alkoxycDrbonyl, carbamoyl, N-tC1-C4)-alkylcarba~oyl, N,N-di-tC1-1:4~-alkylcarb3moyl, tC1-C6)-alkylcarbonyl-oxy, tC3-Cg)-cycloalkyl, phenyl~ benzyl, phenoxy, , ~

:
, . ;: ..

-- ~26~346 benzyloxy, anil;no, N-methylaniLino, phenylmercapto, phenylsulfonyl, phenylsulf;nyl, sulfamoyl, N-(C1-C4)-alkylsulfamoyl or N,N-di-~C1-C4)-alkylsulfamoyl, or, ;f A is as def;ned above under (a) or (c), can also together denote -[CH2]n- or -CH-CH-CH=CH-, ~here;n one CHz group ;s optionally replaced by NR', 0, S, S0 or S02, or denote a substituted (C6-C12)-aryloxy, (C7-C~ aralkyloxy, (C6-C~2)-aryL or (C7-C11)-aralkyl radical, ~hich carr;es in the aryl part 1, 2, 3, 4 or 5 ident;cal or d;fferent substituents from the ser;es compr;s;ng halogen, cyano, n;tro, tr;-fluoromethyl, (C1-C6~-alkyl, tC1-C6)-alkoxy, CCH2]o CpH(2p+1-q)Halq~ -OCF2Cl, -O-CF2-CHFCl, (C1-C6)-alkylmercapto, (C1-C~)-alkylsulfinyl, (C1-C6)-alkylsulfonyl, (C1-C6)-alkylcarbonyl, (C1-C6)-alkoxycarbonyl, carbamoyL, N-(C1-C~)-alkyl-carbamoyl, N,N-d;-(C1-C4)-alkylcarbamoyl, (C1-C6)-alkylcarbonyloxy, (C3-Cg)-cycloalkyl, NR'R"~ sulfamoyl, N-(C~-C4)-alkylsulfamoyl or N~rl-di-(c1-c4)-alkyl sulfamoyl, R3denotes hydrDgen, (C1-C6)-alkanoyl, (C1-C~-alkyl-carbamoyl, (C1-C6)-aLkoxycarbonyl, ben~yloxycarbonyl or ~nother phys;olog;cally tolerated Nim-protective group, uhich can preferably be spl;t off in an acid ~ed;um and/or under physiolog;cal conditions, such as, for example, (C1-C1o)-acyloxy-(C1-C6)-alkyl, preferably tC1-C10)-alkanoyloxy-tC1-C6)-alkyl, benzoyloxy-(C1-CO)-alkyl, benzyloxycarbonyloxy-(C1-C6)-alkyl or tC1-C6)-alkoxycarbonyloxy-(C1-C6) alkyl~

R4 and R5 are identical or different and denote hydrogen or (C1-C3)-alkyl, a) R6 denotes hydrogen and R8 denotes f~uorine, chlorine or bromine, or b) R6 denotes (C1-C3)-alkyl and " ~ .

:.,,: , -R denotes fluorine, or c) R6 denotes fluorine or bromine and R8 denotes hydrogen, or d) R6 denotes fluorine and R8 denotes tC1-C3)-alkyl, or e) one of the substituents R6 ancl RB denotes the radical -0-CCH2~O-CpHt2p+1_q)Halq and the other denotes hydrogen, halogen, (C1-C3)-alkyl or ~he radical -0-lCH2~O-CpH(2p~1_q)Halq, or f) one of the substituents R6 and R8 denotes a substitu-ted (CS-C12)-aryloxy radical or ~C7-C11~-aralkyloxy radical, Yhich carries in the aryl part 1, 2~ 3, 4 or S identical or different substituents from the ~eries co~prising halogen, cyano, nitro, trifluoromethyl, (C1-C6)-alkyl, (C1-C6)-alkoxy, -O-CCH2]0-CpH(2p+1_q)Halq, -OCF2Cl, -O-CF2-CHFCl, (C1-C6~-alkylmercapto, (C1-C6)-alkylsulfinyl, (C1-C6)-alkylsulfonyl, (Cl-C6)-alkylcarbonyl, (C1-C6)-alkoxycarbonyl, carbamoyl, N-(C1-C4)-alkyl-carbamoyl, N,N-di-(C1-C4)-alkylcarbamoyl, (C1-C6)-alkylcarbonyloxy, (C3-Cg)-cycloalkyl~ sulfamoyl, N-tC1-C4)-alkylsulfamoyl or N,N-di-(C1-C4)-alkyl-sulfamoyl, and the other denotes hydrogen, halogen, (C1-C3)-alkyl, the radical -0-tCH2]O-CpH(2p~ )Halq or a substituted (C6-C12)-aryloxy radical or (C7-C11)-aralkyloxy radical~

Hal denotes halogen, for example fluorine, chlorine or bromine, preferably fluorine, 30 R7 denotes hydrogen, halogen, (C1-C12)-alkYl~ (C1-C12)-alkoxy, -0-~SH~]o-cpH(~ +1-q)Halq~ -NR'R", (cl-c12)-alk9xy-~c1-cl2)-a~kyl~ (c1-c12)-alk .. .. . ,. ..

~26~3461 tCl-C12)-alkoxy, (C7-C11)-aralkyloxy, (C1-C12)-alkylmercapto, (C1-C12)-alkylsulfinyl or (C1-C12)-alkylsulfonyl, or ;f at Least one o~ the substituents R6 and ~8 denotes a substitu~ed (C6-C12)-aryloxy radical or (C7-C11)-aralkyloxy radical, R7 can lilte~ise denote a (C6-C1~)-aryloxy radical or (C7-C11)-3ralkyloxy radical sub-stituted as defined above under f), R5 and R6 together stand for -~CHi~]j-, R' and R" are ;dentical or different and denote hydrogen, (C6-C12)-arYl or (C1-C12)-alkylf or R' and R" together stand for -~CH2]h-, in ~hich one CH2 group can be replaced by 0, S, N-(C1-C4)-alkanoylimino or N-(C1-C4)-alkoxylcarbonylimino~
h is 3, 4, 5 or 6, preferably 4 to 6, i is 1, 2, 3 or 4, preferably 1 to 3, n is 3 or 4, o is 0, 1, 2 or 3, preferably 0 or 1, p is 1, 2, 3, 4, S~ 6, 7 or 8, preferably 1 to 5, and q is 0 or 1 to (2pl1), and physiologicalLy tolerated salts thereof, vith the proviso that the compounds 5-methyl-2-(2-pyridylmethylthio)-3H-thienot2,3-d~imida-zole, S-methyl-2-((4-methoxy-2-pyridyl)methyl~hio)-3H-th;eno-t2,3-d~imidazole,
2-(pyridyl)methylthio-3H-thieno~2,3-dJimidazole, 2-t~4-methoxy-2--pyridyl)methylth;o)-3H-~hieno~2,3-d]-. -!; :.

1.26~3~6~

imida~ole, 5-acetyl-2-(t4-methoxy-3,5-dimethyl-2-pyr;dyl)methylthio)-3H-th;eno-t2,3-d~;m;dazole, methyl 2-((4-~ethoxy-3,5-d;methyl-2-pyr;dyl)methylth;o)-5 3H-th;enol2,3-d~imidazole-5-carboxylate, 5-acetyl-2-((4-~ethoxy-2-pyr;dy~)methylth;o)-3H-thieno-t2,3-d]im;dazole, 5-acetyl-2-(2-pyr;dyl)methylthio-3H-thieno~2,3-d~i0;da-zole, and the correspond;ng sulfinyl compounds are excluded.

1H-Th;eno~3,4-d~imidazole derivatives of the formula I
in ~hich A is as defined ~bove under (b) are preferred.
T is preferabLy an -S0- group.

Particularly preferred co~pounds of the formula I are those in ~hich A is preferably as def;ned above under tb), T preferably denotes an -S0- group, R1 and R2 are identical or different and denote hydrogen, (C1-C3)-alkyl, halogen, (C1-C4)-alkoxy or (C1~C4)-alkoxycarbDnyl, R3 is as defined above, R4 and R5 each denote hydrogen, R6 and R8 are identical or different and are as defined above under a) - e) and R7 denotes hydrogen, (C1-C3)-alkyl or a halogenated alkoxy, alkenyloxy or alkynyloxy radical of the formula ~o-~cH2~o-cpH~2p~l-q)Halqo ~C1-C7)-alkoxy, benzyloxy or (C1-C7~-alkoxy-(C~-C3)-alkyl, and in ~hich halogen preferably denotes fluorine, ~684~,~

chlorine or brom;ne, o is 0 or 1, p is 1 to 8 and q is 0 or 1 to ~2p+1), and but in part;cular those compounds of the formula I in ~hich A js preferably as defined abovl- under (b~, T preferably denotes an -S0- group, R1 and R2 are identical or different and denote hydrogen or (C1-C3)-aLkyl, R3 is as defined above, R4 and R5 each denote hydrogen, R~ and R8 are ;dentical or different and are as defined above under a) - e) and R7 denotes hydrogen, (C1-C4)-alkoxy, a fluorinated n-alkoxy radical of the formula ~o-tcH2]o-cpHt2p+1-q)Halq or (C1-C3)-aLkyl, in ~hich halogen denotes fluorine, o is 1, p is 1 to 5 and q is 0 or 1 tD t2p~1).

Compounds ~hich are of particular importance are 2-t3-methoxy-4-(2,2,2-trifluoroethoxy)-2-picolylsulfinyl~-1~-thienoC3,4-d~imidazole, 2-[3-methoxy-4-t2,2,3,3~tetrafluoropropoxy)-2-picolyl-suLfinyl]-1H-th;eno~3,4-d]imidazols, 2-C3-methoxy-4-t2,2,3,3,3-pentafluoropropoxy)-2-picolyl-sulfinyl]-1H-th;enoC3,4-d3îmidazole, 2-C3-methoxy-4-t2,2r3,3,4,4,4-heptafluorobutoxy)-2-picolylsulfinyl:l-lH-thieno~3,4-d~imidazole, 2-~3-bromo-4-mel:ho~y-2-picolylsulfinyl)-1H-thienoC3,4-d~-imidazole, 2-(4-methoxy-5-bromo-2-picolylsulfinyl)-1H-thienoC3,4-d~-imidazole, ~nd - ~ `, '` .,~'.: :, . ............... .
: : , : ::

~: :::. - . .

126~

2-t4-methoxy-5-chloro-2~picolylsulfinyl)-1H-thieno[3,4-d~-i~idazole.

Alkyl and rad;cals derived therefrom, such as, for example, alkoxy, alkylmercapto, alkylsulf;nyl, alkyl-sulfony~, aralkyl or alkanoyl, can be straight-chain or branched.

(C6-C12)-Aryl is, for example, phenyl, naphthyl or biphenylyl, and phenyl is preferred.

(C7-C~ Aralkyl is, for example, benzyl or phenethyl, preferably benzyl. This correspondingly applies to radicals derived therefrom, such as aralkyloxy.

Halogen stands for fluorine, chlorine, bromine or iodine.

Suitable Nim-protective groups R3 are described, for example, in connection ~ith substituted picolylsulfinyl-benzimidazoles in EP-A-176,308 and EP-A2-221,041, and for ~hienoimidazole compounds in EP-A-234,485.

Preferred Nim-protective groups are those ~hich can be split off in the presence of acid, preferably in a pH
range of about 1 - ~ and/or under physiological eondi-tions.

Any ch;ral C and S ato~s present can occur both in theR- and in the S-configuration. In such cases, the com-pounds of the formula I are in the form of the pure enantiomers or as a stereoisomer mixture tsuch as an enantiomer mixture and diastereomer m;xture).

Possible salts ~re, in particular, alkali metal and alkaline eareh ~etal salts and salts ~ith physiologically tolerated amines.

The invention turthermore relates to a process for the :

.: : . .

i268461 preparation of compounds of the formula I, which com-prises a) reacting compounds of the formula II

~ ~ x~ tII) in ~hich A, R1, R2 and R3 are as defined above and x1 ;. denotes a Leaving group or ii. denotes -SH, -S M or -SOz-M , with compounds of the formula III

~ a X 2 C~
RS

10 in ~hich R4, R5, R6, R7 and R8 are as defined above and x2 in the abovementioned case i. denotes -SH, -S M or -SO~-Mt and in the above~entioned case ii. preferably denotes a leaving group or OH, or b) reacting eompounds of the for~ula IV

tIV) ~ NH-R3 in which A~ R1, R2 and R3 are as defined above, with compounds of ~he formula V

~C ~ ~ tV) i h h R4 R5 R6 R7 and R8 are as defined above and R stands for an ester;fying group, :

,. . ..

1;~6~34~1 i. if desired oxidizing any -S- groupts) present in compounds of the formula I to ~the) -S0- or -S02-group(s), ;i. if desired oxidi2;ng any -S0- groupts) present in compounds of the formula I to (the) -S02- group(s), ;;;. if desired acylating, alkylat;ng or aralkylating compounds of the formula I in ~hich R3 stands for hydrogen, iv. if desired hydrolysing compounds of the for~ula I in ~hich R3 does not denote hydrogen, and v. if desired converting compounds of the formula I
into their physiologically tolerated salts, it also being possible for t~o or ~ore of the ~easures i.-iv. to be carried out in a se~uence other than that sho~n.

M stands for cstions, such as, for example, aLkali netal, alkaline earth ~etal, ammonium or alkyla~monium ions, in particular sodium or potassium ions.

If in accordance ~ith the process variant (a) preferred here compounds of the formula II are reacted ~ith com-pounds of the formula III, X1 or x2 stands ~or a leaving group ~hich can be detached nucleoph;lically, such as Cl, 9r, I, -0-S02-CH3, -0-S02-CF3 or -0-S02-tC6H4-pCH3).

The reaction of a compound of the formula ~1 ~ith a com-pcund of the for~ula lII or salts thereof is carried outin an inert solvent, such as, frr example, ~ater, methyl-ene chloride, methanol, ethanol, acetone, ethyl acetate, toluene, tetrahydrofuran, acetonitrile, dimethylfor~-am;de, dimethyl~cetamide, dimethyl sulfoxide or mixtures of these solvents, advantageously in the presence of an : : ,.:, . ~ . - , ., . :, , ~268~

inorganic or organic base, such as, for example, sodium or potassium hydrox;de, carbonate, aLkoxide, hydride or amide, ammonia, triethylamine, tributylamine or pyridine, at -20 to ~150C, preferably at 0 - 80C.

The compounds of the formula lI are known compounds (see, for example, Gronowitz, "The Chemistry of Heterocyclic Compounds", Volume 44, "Th;ophene and its Derivatives", Parts 1-3, NeY York 1985-6) or they can be prepared analo-gously to kno~n processes, for example by cyclization of correspondingly substituted 2,3-, 3,4- or 4,5-diamino-thiophenes of the formula IV defined above ~ith corre-sponding sulfur compounds, such as carbon disulfide (for example DE-A-3,132,167).

The 2,3-, 3,4- or 4,5-diaminothiophenes required for this are either kno~n from the literature or can be prepared analogously to kno~n processes. They are obta;ned, for example, by reduction o~ correspondingly substituted aminonitrothiophenes.

In the esters of the formula V used in process variant ~b), R9 stands for an esterifying group, preferably lC1-C6)-alkyl or benzyl.

The reaction o~ a compound of the formula IY ~;th a com-pound of the formula V in 3ccordance ~ith process variant ~b) is carried out analogously to the procedures de-scribed in Preston et al., Benzimidazoles and CongenericTricyclic Compounds, Part 1, New York, pages 10-13.

If R3 denotes hydrogen, the compounds of the for~ula I
thus obtained can be converted into physiologically tolerated salts.

Compounds of the formula I where T = -S- can furthermore be converted inlto those uhere T - -S0- or -S02- ~ith suitable oxidizing agents. -S- groups in the substituents - : :;: , , ' :, ~ 26~3~6~

R1, R2 and R7 can also be oxidized in the same ~ay.

This reaction is carried out in a suitable inert solvent, such as, for example, ~ethylene chloride, chloroform, carbon tetrachloride, 1~2-dich~oroethane, toluene, ethyl acetate, acetic acid, trifluoroacetic acid, water~
0ethanol, ethanol or mixtures thereof, at -~0C to +150C, preferably at -1ûC to t40C.

Possible oxidizing agents are, fol example: hydrogen persxide, peracids and peresters, such as peracetic acid, trifluoroperacetic acid, monoperphthalic acid, m-chloro-perben~oic acid and esters thereof, ozone, d;nitrogen tetroxide, iodosobenzene, N-chlorosuccinimide, 1-chloro-ben~otriazole, sodium hypochlorite, sodium bromite, potassium peroxodisulfate, t-buty~ hypochlorite, tetra-butylammonium periodate or permanganate, sodium ~eta-periodate, selenium dioxide or ~anganese dioxide, cerium ammonium nitrate, chromic acid, chlorine, bro~ine, diaza-bicycloC2,~,2~octane-bromine complex, d;oxane dibromide, pyridinium perbromide, sulfur~l chloride, 2-arylsulfonyl-
3-aryloxaziridines and titanium teeraisopropylate/tert~
butyl hydroperoxide (if appropriate Yith the addition of dialkyl esters of (D)- or (L)-tartaric acid and a defined amount of ~ater).

Isolated and if appropriate immobili~ed oxid; ing enzymes or microorganisms can also be used as the oxid;zing agent.

The oxidizing agents are used in equimolar amounts, and also if appropriate in a slight excess of 5 - 10 mol X
in the case of oxidation to T - -S0- or in a larger excess and/or at a higher reaction temperature it oxida-tion to T = -S02- is required.

The invention ~urthermore relates to novel intermediates of the formula III. They can be prepared by methods . .: ..,' :' , ' :

, ~26~3~61 ~hich are kno~n to the expert, such as ar~e descr;bed, for exa~ple, in "The Chemistry of Heterocyclic Compounds -Pyridine and its Derivatives", pts. 2 and 3, E. Klings-berg Ed. Interscience Publishers, 1962.

In addition to the synthesis of the compounds of the for-~ula III, in which x2 denotes a leaving group, from com-pounds of ehe formula III, in ~hich x2 denotes a hydroxyl group, the compounds of the formula III, in ~hich x2 deno~es chlorine or bromine, can be prepared, for example, by haLogenation of the corresponding 2-picolines ~ith N-bro~osucc;nimide, trichloroisocyanuric acid (Chem. ~er.
120, 649-651 (1987)) or o~her N-halogenoamides, ~uch as N-chlorophtha~i~ide.

~ithout limiting the invent;on to the follow;ng examples, ssme preparat;on processes for $he compounds of the ~ormula III ;n wh;ch x2 denotes hydrDxyl are described belo~. They are converted ;nto compounds of the formula III, ;n wh;ch x2 denotes a leaving group, by standard methods.

Co~pounds of the formula III in ~hich x2 denotes a hydroxyl group, one of the substituents R6 and R8 denotes ~romine and the other denotes hydrogen can be obtained in accordance ~ith equation 1.

A mixture of the conpounds of the formula VII/VIII ;s obta;ned by brominat;on of 2-picol;ne by known processes (cf., for example, ~ull. Soc. Ch;m. France 2466, 1972).

After N-ox;dat;on, for example w;th m-chloroperbenzoic ac;d, and nitration, the compounds IX and X 3re separated by crystall;~ation or chromatography and prepared ;n a pure form.

The compounds of the formuLae XI and XlII in ~hich R7 denotes alkoxy are ;n each case obta;ned from the .

' .

: . .
..
: . , . .:

;84 compounds of the formulae IX and X and the corresponding alcoholates MR7, in ~hich M is as defined on page 9, S and are reacted, for example, ~ith acetic anhydride or (CF3CO)20 ~ith subsequent hydrolysis of the aceta~es to give the compounds of the for~ulae XII and XIV.

Equation 1:
R6,R3-r 1-1250-1i503 )~R8 R6 E3,.

(VI) tVII) ~VIII) 1 . m~C~35 er~R8 R6 ~E3 Z. HNO3 /H2504 C~3 ~J CH3)~
O O
~IX) (X) 5;7 R7 > ~ C2 / ~ ~c O~ ) ar ~Ra CH3 1 2. NoOH HOCH2 ( lX) (Xl ) tXI ) MR7 ~ c20/~cO>) ~8 ~XIII) (XIV) The synthesis of compounds of the formula III in which x2 denotes a hydroxyl group, R6 denotes hydrogen and R8 denotes chlorine is shown in equation 2. The 5-amino-2-picoline XV obtainable by known processes via degradation reactions of carboxylic acid der;vat;ves of S-~ethyl-nicotinic acid (cf. J. Prakt. Chem. 133 t1932] 19) is reacted by reactions fam;liar to the expert (5andmeyer . . , ~.. , . ,, , ' . . . .

6~4~1 reaction, N-oxidation, nitrat;on, reaction with alcohol-a~es, rearrangement with acetic anhydride, acetate hydroly-sis) to give compounds of the formula XX.

Equation 2:
R ~ NoNO2/HCI R ~ Cl R ~ C
H3C ~ CuCI ~ll ~ m~ CPEIS> ,,~!~

S (XV) tXVI) (XVII) HNO3/H25O4 R ~ Cl M~ R ~ 1. ~c~ cOH~ ~ C

C 1 H3C ~ HOH2C
O o tXVIII) (XIX) tXX) Compounds of the formuLa lII in ~hich x2 denotes a hydroxyL group, R6 denotes hydrogen or ~ethyl and R8 denotes fluorine can be obtained as sho~n in equation 3.

The compounds of the formula VIII can be converted into 5-amino-2-picolines XY under the conditions of the Ullmann reaction tcf. Rec. Trav. Chim. 84 t7), 951-64 11965)).

The compounds XV are ~ike~ise accessible via degradation reactions of carboxylic acid derivatives of 6-~ethyl-nicotinic acid of the formula XXI. The synthesis of the fluorine derivatives XXII is advantageously carried out under the conditions of the Schiemann reaction, as is known for XXII tR6 = ~) tcf. J. Med. Chem. 13, 1124 ~1970)).

The 4-nitro 5-fluoro-2-picolines of the for~ula XXIII
are reduced, as is kno~n for the analogous 3-fluorine isomers, to the a~ino derivatives XXIV (cf. Rocz. Chem.
41 t2), 279-87 t1967)) and these are converted into .. . .
::, .

. ,,,, : ~ . ~ ..

the dihalides XXV.

Equation 3: R6 = H, CH3 R~ V 1 1 1 ) H3C~/ / X ~ N3 ~ NH2 od-r NHNH2 ) CUSO~

R~ ~ ~ 1 m~CPE3~i> ~ F- /~cO~I
2 HNO~ / d >
C N- H3C H250~ H3C
~XV) ~XXlI) ~XXI11) R~ NoN02/HCI ~ R~ 1 . m~CPE15) R~
od. NN02~HElr4 ~ 2. MR H3C)`lN

~XX1V) ~XXV~ Y ~ F~ Cl) ~XXVI ) F
l ~C2 R~
2 . N o O
HQH2C N~
~XXV~ I ) , ' After N-oxidation, replacement of the 4-halogen by alco-S holate R7 and rearrangement, preferably with acetic anhydride or trifluoroacetic anhydride, and acetate hydrolysis, the picolyl alcohols of the formula XX~II are obta;ned.

The corresponding compounds ~here R6 = fluorine and R8 = H or ~C1-C3)-alkyl can be prepared in an analogous manner.

Compounds of the formula III in ~hich X denotes a hydroxyl group and both R6 and R8 denote fluorine or ~L26~

chlorine can be obtained, for e~ample, ;n accordance ~ith equat;on 4:

quation 4:

R~R8 ~ R6 7 RB R ~.
od . R ~ ~ . E3 . Li~:l I H4 ,~H

Y ~ F~ Cl) (XXIX) / (XXX) R6 R7 RE1 R6 R R9 2 ~-CPE15 R6 R7 R8 3 . NoOH > ~f RO2C ) 2HC H H3C~H HOH2C~H
~XXXI) ~XXXII) ~XXXIII) Replacement react;ons Yith nucleoph;les, such as, for example, amines and alcoholates, on the halogen der;va-tives XXVIII lead to compounds of the formula XXIX, reduction of ~hich gives XXX, cf. J. Chem. Soc. 1965, 10 575. Esters of the formula XXXI can be obtained by reaction of tompounds of the formula XXX ~ith salts of malonic acid diesters, and these decarboxylate following acid or alkaline hydrolysis in an acid medium to give the substituted 3,5-dihalogeno-2-picolines of the formula 15 XXXII.

The compounds of the formula XXX can also be reacted directly ~ith organometallic reagents, such as, for example, methylmagnesium halides or methyllith;um, to give XXXII.

20 Useful substances can also be obtained from compounds of the formula XXX by nucleophil;c replacement ~ith C1-synthones, such as, for example, salts of dithianes or cyanides, and these lead to co~pounds of the formula XXXIII via further reactions.

., ~ , . . .
- , ~ -: - . .: , ,~
- ~ .: : ., : :

. ............. . :
:.. - ; , ~26~4i~

Compounds of the formula III ;n which x2 denotes a hydroxyl group, R6 denotes an alkoxy radical and R8 denotes hydrogen can be prepared in accordance with equation 5:

Equation 5:
HO~ 20/R' X R 0~ _ 3 H3CJ~ 2 . NH3 o~ JJ 2 . m~CPE~S

(XXX~V) ~XXXV) ~)X
xxxvlo; X - O) 1.~2.: ~XXXVI~; X - 1) R 0~ 1 ~c20 R 0 O O
~XXXVlI) ~XXXVII1) Maltol XXXIV is alkylated Yith an alkyl halide R'X in the presence of silver oxide to give 3-alkoxy-pyran-4-ones, 1û uhich are reacted ~ith aqueous ammonia to give 2-methyl-3-alkoxy-4-pyridones of the formula XXXV (J. Org~ Chem.
29, 776 (1~64)).

Substituted 3-benzyloxy derivativçs can be obtain~d in an analogous manner by alkylation of ~al~ol ~ith the corresponding benzyL halides.

The compounds isomeric to the compounds of the formula XXXVIII ~here R6 = hydrogen and R8 = alkoxy are obtained by analogous react;ons ~ith 5-hydroxy-2-methyl-4-pyranone, prepared from Kojic acid.

The compounds of the formula XXXV are converted into 2-methyl-3-alkoxy-4-chloropyridines ~ith a halo~enating agent, for example POCl3, and 4-alkoxy derivatives are obtained from these ~ith an alcohol R7H in the presence of a base.

. ,~, , ' . : ,.,~ :' -. . : .

- ., ., - . . -.. ~.. - ,, .,. , ~

, 1268~61 The reaction of the analogous N-oxides XXXVIb with alco-holates to give compounds of the formula XXXVII is advan-tageous.

Co~pounds of the formula XXXV can also be alkylated directly in the presence of silver ox;de to give com-pounds of the formula XXXIX.

R3CO ~ H3C

xxxv~ ~xxxlx R7 - ~c~^c7)-~lkoxY) Processes for the preparation of 3,4-dialkoxy-2-picolines and 4,5-dialkoxy-2-picolines are described in EP-A-166,287 and EP-A-208,452.

Co~pounds of the for~ula III in ~hich x2 denotes a hydroxyl group, one of the substituents R6 and R8 denotes an alkoxy substituent nr a halogenated, preferably fluorinated, alkoxy radical R~ and the other can be -hydrogen, halogen, alkyl, alkoxy or a halogenated, preferably f~uorinated alkoxy radical Rf, can be prepared in accordance ~ith equation 6:

:: ~ . ~.- . . ......... . :
: .:.. ....

... .....

~Z~46~

Equation 6:

HO R0 RrO~R9 ~ . m~CPeS
~ 1 2. nitrat;on H3C ~ ~3C ~ ~N03/~25 ~xxxx) txxxx1) R F~ ~, R B R ~ 0~ R9 H~C ~ H3C ~, 2. NoOH oq, O O
(XXXXlI) (XXXX~I1) R~O ~ R8 ~ ~ R~- ~CH2)O CpH( 2P~ 1 ~q ) -lCH2c o 'O, 1 J
~XXXXIV) S Compounds of the formula XXXXI are obtained by adding 3-hydroxy-2-picolines of the formuLa XXXX onto correspond-ingly halogenated olefins (for example CF2=CF2 or rFz=cClF).

Halogenated carbenes can furthermore be produced from aLkyl halides and a base, for example CF~ from CHCLF2, and these likewise lead to compounds of the formula XXXXI
by insertion into the OH bond of the 3-hydroxy-2-pico-lines (cf. J. Org. Chem. 25~ Z009 (1960)). S-Tr;-fluoromethoxy-2-picollne is obtained as is described, for example, in J. Org. Chem. 29, 1 (1964) and J. Med. Chem.
13, 1124 (1970).

The isomeric 5-hydroxy-2-picolines can be reacted in an analogous manner.

In the preparation processes shown in the above equations, - , . .
.

~2~ 4~jl the substituents and variables have the definitions given above, unless defined otherw;se ;n an ;ndividual case.

In add;t;on to the th;enoim;dazole der;vat;ves descr;bed ;n the ;~lustrat;ve ~xampLes, the compounds of the general formula I ~hich are summar;zed ;n the foll~ing Table 1 and salts thereof, for example, are also obtained accord-ing to th~ invention.

Abbreviations used:
methyl (Me), ethyl (Et), propyl (F'r), butyl (Bu), hexyl (Hex), acetyl (Ac), phenyl (Ph), cyclo (c), iso (;).

Table R
~ '~( >~ , T = SO

Rl R2 R3 R4 R5 R6 R7 ~~~ R3 H H H H H H OEt Cl H H H H H H OPr Cl H H H H H H OiPr Cl H H H H H H OCH~Ph C:l H H H H H H 1)(~H2)20Me t:l H H H H H H OC:H2CF3 Cl H H H H H H OcH2cF2cF3 Cl H H H H H H OEt Br H H H H H H OPr E~r . H H H H H H OCH2Ph Br H H H H H H I:S(CH2)20Me Br H H H H H H OCH2CF3 Br H H H H H H OcH2cF2cF3 13r H H H H H H OCH2Ph F
H H H H H H O(CH2)20~e ,. : .,, . . ~ : .

~2~8~3~

Table, Continuati~n Rl '5 ( , T c SO

Rl R2 R3 R4 ~ 5 R16 R7-- -- R8 ff H H H H F OMe H
H H H H H F OEt H H H M H F OPr H
H H H H H F OCH2Ph H H H H H F O(cH2)2~)Me H
H H H H H F OM~ Me H H H H H F OEt Me H H H }I H F OPr Me H H H H H F OiPr Me H H H H H F OCH2Ph Me H H H H H F O(CH2)2oMe Me H H H H H F OCH2~F3 Me H H H H H Me OEt F
H H H H H Me OPr F
H H H H H Me OCH2Ph F
H H H H H Me O ( CH2 ) 20Me H 3I H H H Me OCH2CF3 F
H H ~ H H H OMe F
H H H H H H O t F
H H H ~I H H O~r F
H H H H ~I N O~Pr F

; , ~: ' " ' ~ ~ ' - . - , ..

.~

12~84~

Table, Continuation Rl T = SO

2 R3 ~4 ~5 R6 R7 R8 H H H ~ H Br OEt H H H H H Br OPr H
H H H H H Br OCH2Ph H
H H H H H Br O(CH2)20Me H
H H H H H 8r ocH2cF3 H
H H H H H OC~3 OMe H
H H H H H OCF3 OEt H
H H H H H OCF3 OPr H
H H H H H ~CF3 OCH2Ph H
H H H H H OCF3 OtCH2)20Me H

H H H H H OCF2H OMe H
H H H H H OCF2H OEt H
H H H H H OCF2R OPr H
H H H H H OCF2H O ( CH2 ) 20Me H
H H H H H OCF2CFzH OMe H H H H H OCF2CF2H i:Me Me H H H H H OCF2CF2H OEt ~e CH3 CH3 H H H OCF2CF2N OMe CH3 CH3 H H H OCF2CF2H OMe Me OCH2CF3 H H H ~I OCF2CF2H OMe H
OCH2~::F3 H H ~l H OCF2CF2H OMe Me 126~a~61 TabLe, Cont inuat ion Rl ~( , T = SQ
R

Rl R2 R3 R4 R5 R~; R7 R8 OCH2CF3 H H H H OCF2CF2H OCH2Ph H
OCH2CF3 H H H H H OMe OCF2CF2H
OCH2CF3 H H H H M~ . t)Me OCF2CF~H
OCH2CF3CF3 H H H H OCF2CF2H OMe H
OCH2CF2CF3 ~ H H H O ::F2CF2H OPr H
OCF2CF2X H H H H OCF2CF2H OMe 9CF2CF2H X H H H OCF~CF2H OEt H
OCF2CF2H H H H E~ OCF2cF2H OCH2Ph H
OCF2CF~H H H H H OMe OMe OCF2CF2H
H H H H H H OMe OCHF2 H H H H H H OEt OCHF2 ::
}I H H H H H OCH2Ph OCHF2 H H H H H H 0 ~ t:H2 ) 20Me OCF3 H H H H H H OMe OC:F3 H H H H H H OEt OCF3 H H H H H F OMe F
H H H H H F OEt F H
H H H H H F OCH2Ph F
H H H H H F O(CH2)2C~Me F
H H H H H Cl N~Me H
H H H H H Cl N~'hMe Me - :.
:. :....... .
~ '' ',':, ~ '~- ,' -126846:1 TableO Cont inuat ion ~ ~ ( , T = SG
R2>~

___ R2 R3 R4 R5 R6 R7 - - R8 H H H H H H NPhMe Cl H H H H H Me NPhMe Cl H H H H H F --NMe2 F

H H H H H F - ~ F

H H H H H F -N~-~O F

H H X H H Cl -NMe2 Cl ~_, H H H H H Cl - V . Cl H H H -H H Cl -N ~ 'Cl CH3 CH3 ~ H H OCH3OCH2CF3 CH3 C~3 H H H OCH3OcH2cF2cF2H
CH3 CH3 H H H OCH3O~H2CF2CF3 H
CH3 CH3 ~ H H OCH3 OCH?CF2CF2CF3 H
CH3 CH3 H H H O~H3 OCH2cF2~F2~F2cF2H H
H H H H H H OC~2~F3 OCH3 H H H H H H ocH2cF2GF2H OCH3 H H H H H H OCH2CF2CF3 O~H3 H H H H H H oCH2CF2CF2~F3 O~H3 H H H H H H OcH~cF2eF2~F2c~2H OCH3 CH3 CH3 H H X H OCH2CF3OC~3 CH3 . CH3 H ~ H H . OCH2CF2C~2~ ~CH3 - . :. - .

:: , : ,., . : .~ :. ,, - , ~, .- , , : .. ., :

12~84f~L

TabLe, Continuation >~
T = SO

Rl R2 R3 R4 R5 R6 _ R7 ~ 8 CH3 CH3 ~ H H HOCH2CF2CF3 oc~3 CH3 CH3 H H H XOCH2CF;~CF2CF3 OCH3 CH3 CH3 H H H HOCtl2CF2CF2CF2CF2H OCH3 OCH2CF3 ~ ~ H H OCH3 Ol:H2CF2CF3 H H H H H 4-chloroben- CX:H3 H
zyLoxy H H H H H - 4-fluoroben- OCH3 H
zyloxy H H H H 2,4-difluoro- OCH3 H
benzyloxy H H H H H 3,5-difluoro- OCH3 H
benzyloxy H H H H H 4,6-dichloro- OCH3 benzyloxy H H H H H 4,5-dichloro- OCH3 H
benzyloxy H H H H H 4-trifLuoro- OCH3 methylben-zyloxy , H H H H H 3,5-bis-tri- OCH3 H
flunromethyL-benzyloxy H H H H H 4-fluoroben- OCH2CF3 H
, zyloxy H H H H H 4-chloroben- OCH2CF3 H
ZylOXy H H H H H 4-trifluoro- OCH2CF3 benzyloxy ..
, . .:; .

: - : ~,:
. ::
; ~` : : ;' . ~
:

Table, Continuation R2 ' T = SO

Rl R2 R3 R4 R5 R6 R7 R8 _ _ H H H H ~ 3,5-bis-tri- OCH2CF3 H
fluoromethyl-benzyloxy CH3 CH3 ~ H H 4-tr;fluoro- OC~2CF3 H
methyl-benzyloxy H H H H H ~ O~H3 4-fluoro-benzyl-oxy H H H H H H Q~H3 4-tr;-fluoro-methyl-benzyl-oxy H H H H H H OCH2CF3 4-fluoro-benzyl-oxy H H H H H H OCH2CF3 ~-tr;-fluoro-methyl-benzyl-oxy The novel compounds of the formula I and their salts have useful pharmacological propert;es.

S They clearly inhibit gastric acid secretion and moreover have an excellent effect of protection of the stom3ch and intestine.

"Protection of ~he stomach and in~estine" in this connec-tion is understood as the prevention and treatment of gastrointestinaL diseases, in particular gastrointestinal inflammatory dis;eases and Lesions (such as, for examPle, ~;~68461 Ulcus ventriculi, Ulcus duodeni, gastritis, irriSated stomach of hyperacid or medicamentous or;gin~, ~hich can be caused, for example, by microorganisms, bacterial toxins, ~edicaments (for example antiinflammatories and antirheumatics), chemicals ~for example ethanol), gastric acid or stress situations.

On the basis of their excellent properties, the substitu-ted thienoimidazoles of the formula I and their pharma-cologically tolerated salts are outstandingly suitable for use in human and veterinary medicineO and they are used in particular for the treatment and prophylaxis of diseases of the stomach and intestine and those diseases based on excessive gastric acid secretion.

It has been found that colon H~/K~-ATPase (cf. ~ustin, Goodman, J. ~iol. Chem. 256 C1981~ 10651-10656~ is also greatly inhibited in vitro by compounds ~hich are formed ~hen the compounds of the formula I according to the invention are treated ~ith acid (for sxample ~ith sodium acetate/HCl buffer ~ith a pH of about 4-5.5). Such con-version products can also be formed in vivo during pas-sage of the co~pounds o~ the formula I through the gastro-intestinal tract. The extent to ~hich they are formed depends on the substitution pattern and on the pH.

Colon H+lK~-ATPase is attributed a decisive influence on the electrolyte equilibrium on the intestinal ~ucosa.
Colon H /K~-ATPase inhibitors, such as those mentioned above, can therefore intervene in this equilibrium and be used for the treatment of diseases ~i~h disturbed electrolyte equilibrium.

The inven~ion thus also relates to the ~se of compounds of the formula I or acid conversion products thereof in the treatment of diarrhea diseases. Examples of such diseases are inflammatory intestinal diseases, such as cholera, paratyphoid, travellers` diarrhea or other forms .~ .
. .

.
' ~ .: ' ' ' .

~268461 of secretory diarrhea, and also other ;ntestinal d;seases, such as Morbus Crohn, CoLit;s ulcerosa and regional enteritis.

The invent;on further~ore relates to conversion products ~hich are formed ~hen compounds o1 the formula I are treated ~ith acid.

The invention thus also relates to the compounds of the formula I according to the invent;on for use in the treat-~ent and prophylaxis of the abovementioned d;seases.

The invention like~ise relates to ehe use of the com-pounds according to the invention in the preparation of ~edicaments ~hich are used for ehe treatment and prophyl-axis of the abovementioned diseases.

The invention furthermore relates to medicaments contain-ing one or more compounds of the general formuia I and/or pharma~ologically tolerated salts thereof.

The med;caments are prepared by processes which are known per se and vith ~hich the expert is familiar~ The pharmacologic3lly active compounds ~= active compounds) according to the invention are used as medicaments either as such or, preferably, in comb;nation with suitable pharmaceutical auxiliaries in the form of tablets, coated tablets, capsules, suppositories, emulsions, suspensions or solutions, the active compound content advantageously being bet~een 0.1 and 96X.

The expert is familiar, on the basis of his kno~ledge, ~ith the auxiliaries vhich are suieable for the desired medicament fornulations7 In ~ddition to solvents, gel-forming agents, suppository bases~ tablet auxiliaries and other active compound excipients, it i5 also possible to use, for ex~Mple, antioxidants, dispersing agents, emulsifiers, foilm suppressants, flavor correctants, ~Z6~4~i1 preservatives, solubilizing agents or dyestuffs.

The active compounds can be administered orally or paren-terally, oral administration being preferred.

In general, it has proved advantageous in human ~edicine to administer the active compound or compounds, in the case of oral administration, in a daily dose of about 0.01 to about 20 mg/kg of body ~e;ght, if appropriate in the form of several, preferably 1 to 4, individual doses, in order to achieve the desired result. In the case of parenteral administration, similar or tespecially in the case of intravenous administratiorl of the active com-pounds) as a rule lower dosages can be used. The parti-cular optimum dosage required and the mode of adm;nistra-tion of the active soMpounds can easily be specified by any expert on the basis of his ~echnical kno~ledge.

If the compounds according to the invention and/or their salts are to be used for the treatment ot the abovemen-tioned diseases, the pharmaceutical formulat;ons can also contain one or more phar~acologically artive constituents from other groups of medicaments, such as antibiotics, for example ofloxacin, ~ntacids, for example aluminum hydroxide, magnesium aluminate, sucralfate and Bi salts, tranquillizers, such as benzodiazepines, for example diazepam; spasmolytics, such as, for examPle, bietamiver-;ne and camylofin; anticholinergics, such as, forexample, pirenzepine, telenzepine, oxyphencyclimine and phencarbam;de; local anesthetics, such as~ for example, tetracaine and procaine; and if appropriate also gastr;n antagonists, enzymes, vitamins or amino acids.

For the oral use form, the active compounds are mixed with the additives customary for this, such as exçipients, stabi-lizers or inert diluents, and are brought into suitabLe presentation fotms, such as tablets, coated tablets~ push-fit capsules, a~ueous, alcoholic or oily suspensions or . : ' :': :: ``

.

',: ': ::' ` `. `' 126~4~

aqueous, alcoholic or oily solutions, by customary methods.

lnert excipients which can be used are, for example, gum arabic, ~agnesia, Magnesium carbonate, lactose, ~ucose or starch, in particular ~aize starch. The Nixtures can there-by be formulated either as dry or as moist granules. Pos-sible oily excipients or solvents are, for ex~mple, vegetable and an;~al oils, such as sunflo~er oil or cod-liver oil.

For subcutaneous or intravenous administration, the active coopounds or phys;ologically tolerated salts thereof are dissolved, suspended or emulsified, if appropriate ~ith the substances customary for this, such as solubilizing agents, emulsifiers or other auxiliaries. Possible soLvents for the novel active compounds and the corresponding physiolog;cally tolerated salts are, for example: water, physiological saLine solutions or alcohols, for example ethanol, propanol or glycerol, and in add;tion also sugar solutions, such as glucose solutions or ~annitol solutions, or also a mixture of the various solvents nentioned.

The following examples are intended to illustrate the procedures according to the invention ~ithout limiting the invent;on to the substances Rentioned here as repres-entatives.

The melting points and decomposition points stated are not corrected or standardi2ed.
,~
5-Chloro~2~p;coli-ns ~a~/e a) 5-Chloro-2-picoline N-oxide 21.3 9 of m-chloroPerbenzoic acid (m-CP8A) are added in portions to 13.0 9 of 5-chloro-2-picoline in 250 ml of methylene chloride at room temperatureO ~ith stirring. After 2 hours, the m;xture ;s extracted twice by shaking with 20D m~ of saturated aqueous NaHC03 solution each time and then three times by ,, - , . .., : . ' .`' ~' :, . . ~ ' : ' . :: . ' . -'' ',.. ;'"' ;-~684~,~

shaking ~ith 200 mL of saturated aqueous NaHS03 solution each time. The bicarbonate solution is extracted three times ~ith 100 ml of methylene chLor-ide each time and the combined organic phases are dried and freed from the solvent. After trituration ~ith petroleum ether, the crystalline eitle comp~und is obtained, melting point 73-76C.

b) 4-Nitro-5-chloro-2-picoline H-oxide 12 9 of 5-chloro-2-picoline ~-oxide are introduced in portions into a mixture of 40 nll of concentrated sul-furic acid and 40 ml of fuming nitric acid, with cooling. The mixture is then heated at 35 to 40C
for 1 hour and at 65 to 70C for 2 houre. After cooling, it is stirred ~ith 250 9 of ice, brought to pH 10 to 11 with 10 N sodium hydroxide solution and extracted ~ith ethyl acetate. After being freed from ~he solvent, the residue is treated ~i~h diisopropyl ether, melting point 115-117C.

c) 4-~ethoxy-5-chloro-2-picoline N-oxide 2D 3.5 9 of 4-nitro-5-chloro-~-picoline N-oxide in 50 ml of anhydrous nethanol are added at -10C to a sodium methylate solution prepared ~rom 1.5 9 of sodium and 150 ~l of ~ethanol. The mixture is allo~ed to ~arm slo~ly to room temperature and is then heated under reflux for 1 hour. The solvent is no~ distilled off under reduced pressure, water is added to the residue, the mixture is extracted ~ith ~ethylene chloride and the solvent is stripped off. Colorless crystals from -diisopropyl e~her, melting point 137-139C.

d) 5-ChLoro-2-hydroxy~ethyL-4--ethoxypyridine 8.5 g of 3-chloro-4-~ethoxy-Z-picoline N-oxide are dissolved in 16 ml of glacial acetic acid, and 24 ml of acetic anhydride are added at 80C, with stirring.
The ~ixture is heated at 110 to 120C for 1.5 hours and then allowed to cool to 80C and 40 ml of . . - . .- . .

.:

~268461 - ~2 -methanol are added drop~ise. The mixture is then concentrated under reduced pressure, 35 ml of ~ater, 13.6 9 of eaust;c soda, in smalL poreions~ and 15 ml of dioxane are then added to the residue and this mix-ture is heated under reflux for 2 hours. After cool-ing, it is extracted with methylene chloride, the soL-vent is driven off and the res;ldue is made to crystal-lize ~ith diisopropyl ether. S~lid, ~elting point 78-e) 5-ChLoro-2-chloro~ethyl-4-oethoxypyridine hydroehloride A solueion of 8.0 ml of thionyl chloride in 20 ml of ~ethylene chloride is added drop~ise to a ~ixture of
4.5 9 of 5-chloro-2-hydroxymethyl-4-methoxypyridine and 100 ml of methylene chloride at 0C and the mix-ture is then stirred at room temperature for 2 hours.The sol~ent is driven off and the residue is ~ade to crystallize ~ith diethyl ether. Colorless crystals, melting point 136-137C.

f) 2-14-~ethoxy-5-chloro-2-picolyl~ercapto)-1H-thieno-~3,~-d]i-idazole dih~droehloride 1.56 9 of 2-çercapto-thienol3,4-d~imidazole and 2.3 9 of 4-methoxy 5-chloro-2-picolyl chloride hydrochloride are heated at 60C ;n 100 ml of ethanol for about 1 hour and then hea~ed under reflux for 1.5 hours. After filtration, the crystalline substance is suspended in acetone, the suspension ;s stirred at room temperature for 1 hour and the crystals are filtered off ~ith suct;on and dried in air, melting point ~ 260C.

The filtrate is treated ~ith animal charcoal and con-centrated in vacuo and the residue is ~ade to trystal-lize ~ith acetone, ~elting point > 260C~

9) 2-(4-~lethoxy-5-rhloro-2-picolyloerc~pto~-1H-thieno-C3,4-d~i-idazole 1.4 9 of the title compound from Example 1 f) are . :~ ., "

~L~68461 suspended in 70 ml of ethanol and 2 ml of triethyl-amine are added at room temperature, ~ith stirring~
The solution thus obtained is stirred at room tempera-ture for about 1 hour, a suspension is formed ~ith S active charcoal, the ~ixture is filtered and ths fil-trate is concentrated in vacuo. ~ater is added to the residue and the mixture is extracted with methylene chloride. After evaporation of the solven~, the residue is made to crystallize ~ith diisopropyl ether, melting point 135-137C.

h) 2-(4-~ethoxy-5-chLoro-2-picolylsulfinyL)-1H-~hieno-C3,4-d~i0idazole 0.308 g of n-chloroperbenzoic acid (85~ pure) in 10 ml of methylene chloride is added drop~ise to 0.44 9 of the title compound of Example 1 9) in a t~o-phase mixture of 70 ml of methylene chloride and 4Q ~l of aquPous KH2P04/Na2HP04 buffer solution (pH = 7.5) at 0 to 5C, ~ith stirring. After about 3D minutes, the organ;c phase is concentrated and the residue ;s chromatographed on silica gel using methyLene chLor-ide/ethyl acetate~ The product is ~ade to crystallize from the corresponding fractions with ethyl acetate, melt;ng po;nt 159C tdecompos;t;on~, or is recrys-tall;zed from ethanol.
Exa-ple 2 a) 3-8rooo-2-piGoline N-oxide and 5-bro~o-2-picoline N-oxide The title compounds are obta;ned analogously to Example 1 a) from 43 9 of a mixture cons;st;ng of 3-bromo-2-picoline and 5-bromo-2-p;coline ~ith 60 g o~
m-chloroperbenzoic acid ~85X pure). The mixture of the title compounds is made to crystallize ~ith diiso-propyl ether, ~elting point 65-80C tnot sharp)~

.
: . - - .

~68~6~

b) 3-~roao-4-nitro-2-picoline N-oxide and 5-bro~o-~-nitro-2-picoline N-oxide 26.3 9 of the t;tle compounds from Example 2 a) are :
stirred in 50 ml of H2504 / Sû ml of HN03 at 60 to 65C for 7 hours, analogously to Example 1 b).

The 5-;somer, mslting point 133-135C, is preferen-tially crystaLli.ed from the evaporation residue with a mixture of ethyL acetate and di;sopropyl ether t1 :
1). On chromatographic separation of the ~other liquor uith toluene / ethyl acetate (1 : 1) on s;lica gel, further 5-bro~o-4-nitro-2-picoline N-oxide is first eluted, follo~ed by 3-bromo-4-nitro-2-picoline N-oxide, melting point 111-113C (from petroleum ether).
Exa~ple 3 a~ e~hoxy-S-bro~o-2-picoline N-oxide The title compound is obtained from 8.2 g of 4-nitro-
5-bromo-2-picoline N-oxide and 0.87 9 of Na in nethanol analogously to Example 1 c). After evapora-tion of the methylene chloride, the residue is ~ade tocrystallize ~ith diisopropyl ether, melting point 146-148C.

b) ~-Wethoxy-5-bro~o-2-hydroxy~ethylpyridine
6.6 9 of 4-methoxy-5-bromo-2-picoline N-oxide are reacted with 7 ml of glacial acetic atid, 15 ml of acetic anhydride, 20 ml of me~hanol, 20 ml of ~ater, 8 9 of NaOH and 20 ml of dioxane analogously to Example 1 d). The crude product is made to crystal-lize ~ith diisopropyl ether, melting point 80-~2C.

c) 4-~ethoxy-5-bro~o-2-chloro~ethylpyridine h~drochloride The title compound is obtained fro~ 4.3 9 of the title compound from Example 3 b) and 5.0 ml of thionyl chloride analogously to Example 1 e), melting point .

. ~ -, . . ~ .
. ' - . ' ''i':
., . . ~ .
. .. ~ ~ .
, .,. ..... :~ :; ; :

.,, . ,.... .. :

~L268461 > 300C (from d;isopropyl ether~.

d) 2-(4-Methoxy-5-brooo-2-picolyloercapto)-1H-thieno[3,4-d]ioidazole dihydrochloride 1.2 9 of 2-mercapto-thienor3,4-d]imidazole are suspen-ded in 50 ml of ethanolO 2.0 g of 4-methoxy-5-bromo-2-chloromethylpyridine hydrochloride are added and the mixture is stirred at 60C for 1 hour. It is freed from the solvent and the res;due is Made to crystal-li~e ~ith diethyl ether, melting po;nt ~ 300C.

10 ~) 2-(4-~ethoxy-5-brooo-2-pitoLyl~ercapto)-1H-thienor3~4-d~i-idazole
7 nl of triethylamine are added to 2.15 9 of the title compound from Example 3 d) in 50 ml of Methanol.
Analogously to Example 1 9), ~he product crystallizes on addition of water, melt;ng po;nt 165C ~decomposi-tion].

f) 2-t4-~ethoxy-5-bro~o-2-picol~lsulfinyl)-1H-thieno~3,4-d~i~idazole The title co~pound is obtained analogously to ExampLe 1 h) from 1.1 9 of the title compound from Example ~ ~ Orv ~ e ~ ~Of ~
' 3 e) and 0.725 9 of ~r~t~P~ ~e~-acid. On tr~at-~ent of the residue, the tiele compound crystallizes frDm a Little diethyl ether/ethyl acetate t1 ~ 1), melting point 140C ldecomposit;on].

Further product is obtained from the mother liquor, ~hich becomes dark in color, by evaporation and immediate treatment ~ith ~ little ethyl acetate.
Exa-pLe 4 a) 3-~romo-4--ethoxy-2-picoline N-oxide The title compound is obtained analogously ~o Examples 1 c) and 3 a) fro~ 4.6 9 of 3-bromo-4-nitro-2-picoline N-ox;de in 40 ml of methanol with a sodium methylate . :. ::, :' ~ .. i'; : ' .

- - - :
.- .~
.. ~. ~ , :
- . . :

~2~846 so~ution prepared from 0.5 9 of sodium and 20 ml of ~ethanol, melting point 80-82C (from diisopropyl ether).

b) 3-8ro-o-4-~ethoxy-~-hydroxy~ethylpyridine 3.8 9 of the title compound from Example 4a) are stirred ~ith 30 ml of acetic anhydride at 80-85C for 1 hour. 25 ml of methanoL and, after concentration, 30 ~l of 5 N sodium hydroxide solution and 10 mL of dioxane are added, analogously to Examples t d)/3 b).
The product crystallizes from diisopropyl ether, melt-ing point 109-111C.

c) 3-Bro~o-~-~e~hoxy-2-chloro-ethy~prridine hydrochloride 1.9 9 of the ~itle compound of Example 4 b~ are reac-ted ~ith 2.5 ml of thionyl chloride analogously to Examples 1 e) and 3 c). The product is made to crystallize vith diisopropyl ether, ~elting point 142-d) 2-(3-Bro-o-4-~ethoxy-2-picolyl-ercapto)-1H-thienoC3,4-d3i-idazole dihydrochloride 2.3 9 of 3-bromo-4-methoxy-2-chloromethyl-pyridine hydrochloride are added to 1.3 9 of 2-mercapto-thieno-C3,4-d]imidazole in 50 ~l of ethanol, with stirring, and the ~ixture is kept at 60C for 30 minutes. The product is filtered off with suct;on and dr;ed in vacuo, melting po;nt > 300C.

e) 2-(3-Bro~o-~ ~ethoxy-2-pieolyl~ercaPto)-1H-thienoC3,4-d~i-;dazole 2.9 ml of triethylamine are added to 2~4 9 of the di-hydrochloride from Example 4 d) in 50 ml of methanol analogously to Example 1 9). Af~er concentration and additicn of a litt~e ~ater, the residue crystallizes, melting point 168C Zdecoeposition~.

~- '- . .~ ,, :~

'. :. : ' '' 1;~6~'~6~L

f) 2-(3-Bro-o-4-~ethoxy-2-picolylsulfinyl)-1H-thieno~3,4-d]i~idazole 0.44 9 of m-chloroperbenzoic acid (85X pure) in 15 ml of methylene chloride are added drop~ise to 0.72 g of the title compound from Example 4 e) in 120 rl of methylene chloride and 50 ml of aqueous KH2P04/Na2HP04 buffer solution (pH = 7.5) analogously to Example 1 h).
After concentration of the organic phase, the residue is made to crystallize with ethyl acetate, melting point 160C (polymerization?).
xa-ple 5 a) 2-~ethy~-3-~ethox~-4-ch~oro-pyridine N-oxide 11.2 9 of 3-methoxy 2-methyl-4(1H)-pyridone are heated under reflux in 100 ~l of phosphorus oxychloride for 10 hours. The ~ixture is then concentrated, 2 por-tions of 30 ml each of toluene are added and the 0ix-ture is concentrated each time, the residue is taken up in 150 ml of ~ater, the mixture is brought to pH 11 ~ith K2C03 and extracted ~ith methylene thloride and the organic phase is ~ashed ~ith water, dried and freed from the sol~ent.

The ti~le conpound is obtained from the pale bro~n oil (9 9) ~ith m-chloroperben~oic ac;d in methylene chlor-ide under standard condit;ons, melting point 88-89C
(from petroleum ether).

b~ 2-~ethyL-3,4-di~ethoxy-pyridine N-o~ide A sodium methylate solution prepared from 1.14 9 of sodium and 50 ml of methanol is added dropwise to 8 9 of the title compound from Example 5 a) in 100 ml of anhydrous methanol, the mixture is heated at the boil-ing point for 20 hours and concentrated, ~ater is added, the mixture is extracted with methylene chlor-ide ~nd the extract is concentrated to give the title compound, melt;ng point 111-113C.

: -,:
:. ~ ;: ..
' . '' :.~ . . . .:.
:,,~ :

1~6~3461 c) 3,4-Di~lethoxy-2-hydroxy~ethrl-pyridine 5.8 9 of the product described above are reacted in 10 ml of glac;al acetic acid, 15 ml of acetic anhyd-ride, 20 ml of ~ethanol, 20 ~l of ~ater, 8 9 of NaOH
and 20 ml of dioxane analogously ~o Example 1 d), melting point 86-88C (from diisopropyl ether).

d) 3,4-Di~ethoxy-2-chloro~ethy~-pyridine hydrochloride 3.4 9 of the above product are reacted w;th 5 ml of thionyl chloride analogously to Example 1 e). Melting point 150-151C ldecomposition~ (from diethyl ether).

e) Z-(3,~-Di-ethoxy-2-picolyl-ercDpto~-1H-thieno~3,4-d~-i~idazole 1.56 9 of 2-~ercaptsthieno~3,4^d~im;dazole in 70 ml of ethanol are reacted ~ith 2.3 9 of 3,4-dimethoxy-2-chloromethy~-pyridine hydrochloride analogously to Example 1 f).
Melting point 148-150C Cdecomposition].
The product is then treated ~ith 2.5 ml of triethyl-amine in 60 ml of ~ethanol analogously to Example 1 9).
Melting point 141-142C ~decomposit;on~.

f) 2-(3,~-Di-ethoxy-2-pico~ylsulfinyl)-1H-thienoC3,~]-i~idazole - 0.75 9 of the titLe compound from Example 5 e) is oxidized ~;th 0.55 9 of m-chloroperbenzoic arid in 100 ml of ~ethylene chloride and 50 ml of Na2HP04/KH2P04 buffer solut;on (pH = 7.5) analogously to Example 1 h)r After the mixture has been concentrated, the residue is ~ade to crystaLlize uith diethyl ether, ~elting point 13g-140C.
Exa-p~e 6 a) 2-~rovo~ethyl-3-fluoropyri~ine 1.11 9 of 3-fluoro-2-p;coline are dissolved in 50 ml of CCl4, 3.6 9 of ~-bromosuccinim;de and 0.1 g of -: ~ . . - ...

.
....

" ,.~ -1268~61 - - 39 - ;
~20bisisobuSyronitrile ~re sdded ~nd the ~ixture ix l~
stirred for 2 hours ~hile boiling under reflux. After cooling and tiltr~tion, the solvent is removed in v~cuo. The crude product shous the expected ~ol~cular pe3k of 189 ~/e in the ~ass spectrum.

b) 2-(3-Fluoro-2-picolyl~ercapto-1H-thienoC3,~-dJi-id~role ~ of 2--crc~pto-thienot3,4-d~iMidJzol~ 2nd 1.9 9 of 2-bro~o~ethyl-3-fluoropyridin~e are stirred w;th 2.8 g of po~dered anhydrous K2C03 in 3bout 100 ~l of ~cetone for ~ hours, uithouS cooling. Aft~r filtration and re~ov~l of the solvent in vacuo, the crude product is purified by colu~n chromatography on silica gel with a ~obile phase oixture of cyclohexane/ethyl acetate.
The product fraction h~s ~n Rf of about 0.95.

e) 2-~3-Fluoro-2 picolylsulfinyl-1N-thieno~3,4-~]i~id3~ole 530 ~9 of the coopound from the precedin~ st~ge are dissolved in S0 ~l of CH2Cl2 and the solution is stirred ~ith ~44 mg of ~-chloroperbenzoic ~cid at room temperatur~ for 4 hours. The solution is ~ashed 2D successively ~ith NaHS03 solution, NaHC03 solut;on ~nd H20 and dried ~ith Na2S04. The crude product obtained ~fter re~oval of the solvent is subjected to colu~n chrooatogr3phy ~SiO2: CH2Cl2: ~cetone = 7/3).
The product fractions are concentrated ~nd the residue is stirred ~ith diisoprop~l ether and filtered off.
~eltin~ point 145C; MS gives a ~olecu~ar peak of 282 m/e; (M~H)~.

The compounds of the formula I(A as defined ab~ve under (b)) in the following Examples 7 to 22 are obtained by procedures analogous to those described in Examples 1 to 6:

:

i :': ' ,:

126~34~.1 Ex. T R3 ~6 _ R7 X8 Melti,n~ D~int 7 S H CH3 OCH3 F . 170-173 C
8 SO H CH3 O~H3 F ab 145~C tdecomp.
9 S H H H OCHF2 (MS: M~=313 SO H H H OCHF2 116C rdecomp.~
MS(Dl~ M~41=329 11 S H H H Cl 160C ~decomp.
1~ SO H H H Cl 15'7~C tdecomP-~
13 S H OCH3 H H 180C rdecomp.
14 SO H OCH3 H ~1 85- 90C rdecomp.

16 SO H H H OCH3 152-154CIdecomp.]
17 S ~1 9CHF2 ~ H 103C ldeco~p~];M+=313 18 SO H OCHF2 H H 78C ~decomp.~;M+H+-330 19 S H OCH2CF3 0CH2CF3 H 145C tdecomP.~;M~=443 SO H OCH2CF3 OCH2CF3 H 154l: rdecomp.~;M+H~=460 21 S H OCF2CF2H OCH3 H Ol ;M~H~=394 22 SO H OCF2CF2H OCH3 H ~38C [deco;:p.~ ;M~H~C410 Rl, R2, R4 and R5 are in each case hydrogen Exa-ple 23 a~ 2-~ethyl-3--ethoxy-4-(2,2,2-trifluoroethoxy~pyridine N-oxide 6.7 9 of potassium tert.-butylate are added in por-tions to 20 ml of tr;fluoroethanol at -20C, w;th stirring and under a nitrogen atmosphere~ After the mixture has been ~armed ~o 0C, 5.2 9 of 2-methyl-3-methoxy-4-chloro-pyridine N-oxide (~itle compound from Example 5 a) are added in port;ons. The mixture is heated under reflux for 3 hours and allo~ed to cool to room temperature, a further 3.45 9 of potassium tert.-butylate are added and the mixture is heated under reflux for 2 hours. After cooLing, 40 ml of ~ater are added to the reaction mixture, the mixture . ~

~Z6~34~

is extracted ~ith methylene chlor;de and the extract is dried over MgS04 3nd freed from the solvent in vacuo. The oily crude product obtained is reacted further.

b) 3-~ethoxy-4-(2,2,2-trif~uoroethoxy)-2-hydroxy-~ethyl-pyridine 8 9 of the title compound from Example 23 a) are dis-solved in 16 ml of glacial acetic acid, and 24 ml of acetic anhydride are added at ~0C, with stirring.
The mixture is heated at 110C for 2 hours and then cooled to 80C, and 40 ml of methanol are added drop~ise to the reaction mixture. The mi~ture is then concentrated in vacuo, the oily residue is ~dded to 75 ~l of 2 N methanolic NaOH and the ~ixture is stirred for 30 minutes. After treatment ~ith active charcoal and fil~ration, the filtrate is concentrated in vacuo, 50 ml of ~ater are added to the residue, ~he mixture is extracted ~ith methylene chloride, the extract is dried tMgS04) and concentrated and the residue is treated ~ith diisopropyl ether. Colorless crystals, meleing point 107-108C.

c) 3-~ethoxy-4-t2,2,2-~rifluoroethoxy)-2-chloro~ethyl-Prridine hydrochloride A solution of 6.0 ml vf thionyl ehloride in 15 ml of methylene chloride tS added drop~ise to a mixture of 3.9 g of the above product and 1~0 ml of methylene chloride at 0C and the mixture is then stirred at roon temperature for 2 hours. The solvent is driven o~f and the residue is made to crystallize ~ith d;iso-propyl ether. Colorless crystals, melting point 166-168C.

d) 2-t3-~ethoxy-4-t2,2~2-trifluoroethoxy)-2-pico~yl-er-capto)-1H-thienoC3,~-d~i~idazole dihydrochloride 1.0 9 of 2-~ercapto-thienoC3,4-d~im;dazole and 1.9 9 of the above product are heated at 60C in 60 ~l of .. ,...... - ; ,.

~2~8 ethanol for about 1 hour, and the m;xture is then heated under reflux for 1.5 hours. After treatment with active charcoal, f;ltra~ion and concentration, the res;due is made to ~rystall;~e with acetone~
Melting point from 188C (decompos;tion).

e~ 2-(3-~ethoxy-4-~2,2,2-trifluoroethoxy)-2-pico~ylmer-capto)-1H-thieno~3,4-d~i-ida~ole 2.1 9 of the title compound from Example 23 d) are suspended in 80 ml of methanol, and 4 ml of triethyl-amine are added at room te~perature, ~;th stirring.The solution thus obtained is stirred at room tempera-ture for about 1 hour, a suspension is formed vith active charcoal, the suspension ;s filtered and the filtrate is contentrated in vacuo. On adding ~ater~
the colorless product crystallizes. Melting point 147-148C.

f) 2-t3-~ethoxy-~-~2,2,2-trifluoroethoxy)-2-picoly~sulf-inyl)-1H-thienoC3,$-d3i~idazole 0.42 9 of ~-chloroperben oic aciJ t85% pure) in 10 ml of ~ethylene chloride is added dropwise to 0.75 9 of the title compound from Example 23 e) in a t~o-phase mixture of 80 ~l of ~ethyLene ~hloride and ~0 ml of aqueous KHzPO4/Ha2HPO4 buffer solution (pH = 7.5) at O to 5C, ~ith stirring. Af~er about 30 minutes, the organic phase is separa~ed off, dried and concen-trated and the residue is ~ade to crystalli~e ~ith diethyl ether. Melting point 135-137C.

The following inter~ediates of the formulae XXXXVI-XXXXYIII can be prepared, for example, analogously to Equation 5:

, . . . .

.:
. .

C~130 Xxxxv~
Exalple _Meltir~3 point 24 0cH2cF2cF2H 40- 42 C

26 oCH2CF2CF2~F3 128-130 C
27 ocH2cF2cF2cF2cF2H 0 i l CH30~,~

Exalple No. R7 PRlting point .
28 0cH2cF2c F2H 45-47 C
29 0cH2cF2cF3 Oi l 31 OCH2CF2CE'2CF2CF2H Oi l .
~as reacted directly - : ::: .: ~ : ,:

~2~84 l-IC
XXXXVl~I
i~xanple ting point 32 O~H2CF2CF2H 133 C decomposition 33 OC~2cF2cF3 155 C
34 OCH2CF2CF21::F~ 161-163 C

The following compounds of the for~ul3 1 are obt~ined anaLogously to Examples 5 and 23:

~ \)- T - C ~ R El R2 i H

Exalple N~. . T Rl R2 R6 R7 R8 Melting i int(C) 36 S H H OCH3 OCH2CF2CF2H ~ 127-129 37 S H H OCH3 0~2cF2~F3 ~ 142 38 S ~ H OCH3 OcH2cF2~F2cF3 H 133-135 39 S H H ~ ~r}~3 OcH2cF2cF2cF2~F2~ ~ 110 SO H H ~CH3 O~H2~ F2CF2H ~ 133-135 41 SO ~1 H OCH3 0C~2CF2~F3 ~ 137 decomposi~;on 42 SO H H OCH3 Ot ~2CE~2~ F2c~3 H 113-115 ~ :
43 SO H H OCH3 OCH2CF2CF2CF2CF2H H 103 decomposit;on 44 S HPhenyl H ~I ~ 153-157 ~henyl ~ OCH3 H 1~2-185 .,.

.: , : . ,, ~ -. ~ - ..
:. .
- . ,. ~ : .,; :

~;~68~

Exaple T ~1 R2 R6 R7 R8 (C) No. _ _ _ _ 46 S H Phenyl CH3 OCH3 CH3 192-195 47 S H 4-Methoxy- H H ~ 141-143 phenyl 48 S H " H OC~3 H 170-173 49 S H " CH3 OCH~ CH3 151-154 S H Phenyl H OCH2CF2CF2CF3 H 216 51 S H 4-Methoxy- H OCH2CF2CF2CF3 H 203 phenyl 52 S OCH3 C~2CH3 H H H 106-110 53 S H CON(C2Hs)2 H H ~ 102-104 ~Cl 54 SO H Phenyl H H H 137-141 SO H n H OCH3 H 130-135 56 SO H n CH3 OCH3 CH3 160-165 57 SO ~ 4-Methoxy- H ~ H 164^167 phenyl decompos;t;on 58 SO H ~ H OCH3 H 162-165 59 S0 H n CH3 OCH3 CH3 162-165 decompos;tion SO X Phenyl ~ ocH2cF2cF2cF3 ~ 80 61 SO H 4-Methoxy- H OCH~CF2CF2CF3 H 79 phenyl R2~ ~ C~

Exalple T Rl ~2 R6 R7 ~8 ~ CC:) No. _ __ ~__ __ __ 62 S -CH2SCH2- H H H lB6-188 63 S C2~H3 CO2CH3 H OCH3 H 156-159 64 SO CO2CH3 CO2CH3 H OCH3 H ~40 decompos;t;on .,.. - . : . . , . :

...: .
, ,.. ,~ ~,. . , `~ ; . . ~, : .:
.... .. .

:` : . ~ :- : .. ~

Claims (16)

THE EMBODIMENTS OF THE INVENTION IN WHICH AN EXCLUSIVE
PROPERTY OR PRIVILEGE IS CLAIMED ARE DEFINED AS FOLLOWS:
1. A compound of the formula I
(I) in which A stands for a) , b) of c) T denotes -S-, -SO- or -SO2-, R1 and R2 are identical or different and denote hydrogen, halogen, cyano, nitro, trifluoromethyl, (C1-C6)-alkyl, (C1-C6)-hydroxyalkyl, (C1-C6)-alkoxy, -O-[CH2]o-CpH(2p+1-q)Halq, (C1-C6)-alkyl-mercapto, (C1-C6)-alkylsulfinyl, (C1-C6)-alkyl-sulfonyl, (C1-C6)-alkylcarbonyl, (C1-C6)-alkoxy-carbonyl, carbamoyl, N-(C1-C4)-alkylcarbamoyl, N,H-di-(C1-C4)-alkylcarbamoyl, (C1-C6)-alkylcarbonyl-oxy, (C3-C8)-cycloalkyl, phenyl, benzyl, phenoxy, benzyloxy, anilino, N-methylanlino, phenylmercapto, phenylsulfonyl, phenylsulfinyl, sulfamoyl, N-(C1-C4)-alkylsulfamoyl or N,N-di-(C1-C4)-alkylsulfamoyl, or, if A is as defined above under (a) or (c), can also together denote -[CH2]n- or -CH=CH-CH=CH-, wherein one CH2 group is optionally replaced by NR', O, S, SO or SO2, or denote a substituted (C6-C12)-aryloxy, (C7-C11)-aralkyloxy, (C6-C12)-aryl or (C7-C11)-aralkyl radical, which carries in the aryl part 1, 2, 3, 4 or 5 identical or different substituents from the series comprising halogen, cyano, nitro, tri-fluoromethyl, (C1-C6)-alkyl, (C1-C6)-alkoxy, -O-[CH2]o-CpH(2p+1-q)Halq, -OCF2Cl, -O-CF2-CHFCL, (C1-C6)-alkylmercapto, (C1-C6)-alkylsulfinyl, (C1-C6)-alkylsulfonyl, (C1-C6)-alkylcarbonyl, (C1-C6)-alkoxycarbonyl, carbamoyl, N-(C1-C4)-alkyl-carbamoyl, N,N-di-(C1-C4)-alkylcarbamoyl, (C1-C6)-alkylcarbonyloxy, (C3-C8)-cycloalkyl, NR'R", sulfamoyl, N-(C1-C4)-alkylsulfamoyl or N,N-di-(C1-C4)-alkyl-sulfamoyl, R3 denotes hydrogen, (C1-C6)-alkanoyl, (C1-C6)-alkyl-carbamoyl, (C1-C6)-alkoxycarbonyl, benzyloxycarbonyl or another physiologically tolerated Nim-protective group, R4 and R5 are identical or different and denote hydrogen or (C1-C3)-alkyl, a) R6 denotes hydrogen and R8 denotes fluorine, chlorine or bromine, or b) R6 denotes (C1-C3)-alkyl and R8 denotes fluorine, or c) R6 denotes fluorine or bromine and R8 denotes hydrogen, or d) R6 denotes fluorine and R8 denotes (C1-C3)-alkyl, or e) one of the substituents R6 and R8 denotes the radical -O-[CH2]o-CpH(2p+1-q)Halq and the other denotes hydrogen, halogen, (C1-C3)-alkyl or the radical -O-[CH2]o-CpH(2p+1-q)Halq, or f) one of the substituents R6 and R8 denotes a substitu-ted (C6-C12)-aryloxy radical or (C7-C11)-aralkyloxy radical, which carries in the aryl part 1, 2, 3, 4 or 5 identical or different substituents from the series comprising halogen, cyano, nitro, trifluoromethyl, (C1-C6)-alkyl, (C1-C6)-alkoxy, -O-[CH2]o-CpH(2p+1-q)Halq, -OCF2Cl, -O-CF2-CHFCl, (C1-C6)-alkylmercapto, (C1-C6)-alkylsulfinyl, (C1-C6)-alkylsulfonyl, (C1-C6)-alkylcarbonyl, (C1-C6)-alkoxycarbonyl, carbamoyl, N-(C1-C4)-alkyl-carbamoyl, N,N-di-(C1-C4)-alkylcarbamoyl, (C1-C6)-alkylcarbonyloxy, (C3-C8)-cycloalkyl, sulfamoyl, N-(C1-C4)-alkylsulfamoyl or N,N-di-(C1-C4)-alkyl-sulfamoyl, and the other denotes hydrogen, halogen, (C1-C3)-alkyl, the radical-O-[CH2]o-CpH(2p+1-q)Halq or a substituted (C6-C12)-aryloxy radical or (C7-C11)-aralkyloxy radical, Hal denotes halogen, R7 denotes hydrogen, halogen, (C1-C12)-alkyl, (C1-C12)-alkoxy, -O-[CH2]o-CpH(2p+1-q)Halq, -NR'R", (C1-C12)-alkoxy-(C1-C12)-alkyl, (C1-C12)-alkoxy-(C1-C12)-alkoxy, (C7-C11)-aralkyloxy, (C1-C12)-alkylmercapto, (C1-C12)-alkylsulfinyl or (C1-C12)-alkylsulfonyl, or if at least one of the substituents R6 and R8 denotes a substituted (C6-C12)-aryloxy radical or (C7-C11)-aralkyloxy radical, R7 can likewise denote a (C6-C12)-aryloxy radical or (C7-C11)-aralkyloxy radical sub-stituted as defined above under f), R5 and R6 together stand for -[CH2]i-, R' and R" are identital or different and denote hydrogen, (C6-C12)-aryl or (C1-C12)-alkyl, or R' and R" together stand for -[CH2]h-, in which one CH2 group can be replaced by O, S, N-(C1-C4)-alkanoylimino or N-(C1-C4)-alkoxylcarbonylimino, h is 3, 4, 5 or 6, i is 1, 2, 3 or 4, n is 3 or 4, o is 0, 1, 2 or 3, p is 1, 2, 3, 4, 5, 6, 7 or 8, and q is 0 or 1 to (2p+1), and physiologically tolerated salts thereof, with the proviso that the compounds 5-methyl-2-(2-pyridylmethylthio)-3H-thieno[2,3-d]imida-zole, 5-methyl-2-((4-methoxy-2-pyridyl)methylthio)-3H-thieno-[2,3-d]imidazole, 2-(pyridyl)methylthio-3H-thieno[2,3-d]imidazole, 2-((4-methoxy-2-pyridyl)methylthio)-3H-thieno[2,3-d]-imidazole, 5-acetyl-2-((4-methoxy-3,5-dimethyl-2-prridyl)methylthio)-3H-thieno-C2,3-d]imidazoLe, methyl 2-((4-methoxy-3,5-dimethyl-2-pyridyl)methylthio)-3H-thieno[2,3-d]imidazole-5-carboxylate, 5-acetyl-2-((4-methoxy-2-pyridyl)methylthio)-3H-thieno-[2,3-d]imidazole, 5-acetyl-2-(2-pyridyl)methylthio-3H-thieno[2,3-d]imida-zole, and the corresponding sulfinyl compounds are excluded.
2. A compound of the formula I as claimed in claim 1, in which A is as defined under (b) in claim 1, or a physio-logically tolerated salt thereof.
3. A compound of the formula I as claimed in claim 1, in which T stands for -SO-, or a physio-logically tolerated salt thereof.
4. A compound of the formula I as claimed in claim 1, in which R1 and R2 are identical or different and denote hydrogen, (C1-C3)-alkyl, halogen, (C1-C4)-alkoxy or (C1-C4)-alkoxycarbonyl, R3 is as defined in claim 1, R4 and R5 each denote hydrogen, R6 and R8 are identical or diffelent and are as defined in claim 1 under a) - e) and R7 denotes hydrogen, halogen, (C1-C3)-alkyl or a halogenated alkoxy, alkenyloxy or alkynyloxy radical of the formula -O-[CH2]o-CpH(2p+1-q)Halq, (C1-C7)-alkoxy, benzyloxy or (C1-C7)-alkoxy-(C1-C3)-alkyl, and o is 0 or 1, p is 1 to 8 and q is 0 or 1 to (2p+1), or a physiologically tolerated salt thereof.
5. A compound as claimed in claim 4 in which the halogen in R7 denotes fluorine, chlorine or bromine.
6. A compound of the formula I as claimed in claim l, in which R1 and R2 are identical or different and denote hydrogen or (C1-C3)-alkyl, R3 is as defined in claim 1, R4 and R5 each denote hydrogen, R6 and R8 are identical or different and are as defined in claim 1 under a) - e) and R7 denotes hydrogen, (C1-C4)-alkoxy, a fluorinated n-alkoxy radical of the formula -O-[CH2]o-CpH(2p+1-q)Halq or (C1-C3)-alkyl, in which halogen denotes fluorine, o is 1, p is 1 to 5 and q is 0 or 1 to (2p+1), or a physiologically tolerated salt thereof.
7. 2-[3-Methoxy-4-(2,2,2-trifluoroethoxy)-2-picolylsul-finyl]-1H-thieno[3,4-d]imidazole, 2-[3-Methoxy-4-(2,2,3,3-tetrafluoropropoxy)-2-picolyl-sulfinyl]-1H-thieno[3,4-d]imidazole, 2-[3-Methoxy-4-(2,2,3,3,3-pentafluoropropoxy)-2-picolyl-sulfinyl]-1H-thieno[3,4-d]imidazole, 2-[3-Methoxy-4-(2,2,3,3,4,4,4-heptafluorobutoxy)-2-picolyl-sulfinyl]-1H-thieno[3,4-d]imidazole, 2-(3-bromo-4-methoxy-2-picolylsulfinyl)-1H-thieno[3,4-d]-imidazole, 2-(4-Methoxy-5-bromo-2-picolylsulfinyl)-1H-thieno[3,4-d]-imidazole, 2-(4-Methoxy-5-chloro-2-picolylsulfinyl)-1H-thieno[3,4-d]-imidazole, or a physiologically tolerated salt thereof.
8. A process for the preparation of a compound of the formula I, which comprises a) reacting a compound of the formula II
(II) in which A, R1, R2 and R3 are as defined in claim 1 and X1 i. denotes a leaving group or ii. denotes -SH, -S-M+ or -SO2-M+, M+ standing for a cation, with a compound of the formula III
(III) in which R4, R5, R6, R7 and R8 are as defined in claim 1 and X2 in the abovementioned case i. denotes -SH, -S-M+ or -SO2-M+ and in the abovementioned case ii. denotes a leaving group or OH, or b) reacting a compound of the formula IV
(IV) in which A, R1, R2 and R3 are as defined in claim 1, with a compound of the formula V
(V) in which R4, R5, R6, R7 and R8 are as defined in claim 1 and R9 stands for an esterifying group, i. if desired oxidizing any -S- group(s) present in a compound of the formula I to (the) -SO- or -SO2-group(s), ii. if desired oxidizîng any -SO- group(s) present in a compound of the formula I to (the) -SO2- group(s), iii. if desired acylating, alkylating or aralkylating a compound of the formula I in which R3 stands for hydrogen, iv. if desired hydrolysing a compound of the formula I in which R3 does not denote hydrogen, and v. if desired converting a compound of the formula I
into its physiologically tolerated salts, it also being possible for two or more of the measures i.-iv. to be carried out in a sequence other than that shown.
9. The use of a compound as claimed in any one of claims 1 to 3 as medicine.
10. The use of a compound as claimed in any one of claims 1 to 3 as a gastric acid secretion inhibitor.
11. The use of a compound as claimed in any one of claims 1 to 3 as a medicine in the treatment of inflammatory intestinal diseases.
12. The use of a compound as claimed in one of claims 1 to 3 as medicine in the treatment of diarrhea.
13. An agent containing a compound as claimed in any one of claims 1, 2 or 3 and a pharmaceutically acceptable excipient and, if desired, one or more of other additives, auxiliaries and preservatives.
14. An agent containing a compound as claimed in any one of claims 4, 5,or 6, and a pharmaceutically acceptable excipient and, if desired, one or more of other additives, auxiliaries and preservatives.
15. An agent containing a compound as claimed in claim 7 and a pharmaceutically acceptable excipient and, if desired, one or more of other additives, auxiliaries and preservatives.
16. A process for the preparation of an agent containing a compound as claimed in any one of claims 1, 2 or 3, which comprises bringing a compound as claimed in any one of claims 1 to 3 into a suitable presentation form together with a physiologically acceptable excipient and if appropriate other additives, auxiliaries and/ox preservatives.
CA000574551A 1987-08-15 1988-08-12 2-(2-picolylsulfur)-trienoimidazole derivatives Expired - Fee Related CA1268461A (en)

Applications Claiming Priority (6)

Application Number Priority Date Filing Date Title
DEP3727244.6 1987-08-15
DE3727244 1987-08-15
DE3744022 1987-12-24
DEP3744022.5 1987-12-24
DE3816996 1988-05-19
DEP3816996.7 1988-05-19

Publications (1)

Publication Number Publication Date
CA1268461A true CA1268461A (en) 1990-05-01

Family

ID=27196347

Family Applications (1)

Application Number Title Priority Date Filing Date
CA000574551A Expired - Fee Related CA1268461A (en) 1987-08-15 1988-08-12 2-(2-picolylsulfur)-trienoimidazole derivatives

Country Status (15)

Country Link
EP (1) EP0304732A3 (en)
JP (1) JPS6470492A (en)
KR (1) KR890003772A (en)
CN (1) CN1029973C (en)
CA (1) CA1268461A (en)
DE (1) DE3827276A1 (en)
DK (1) DK454588A (en)
FI (1) FI89602C (en)
HU (1) HU208539B (en)
IL (1) IL87428A (en)
MA (1) MA21352A1 (en)
NO (1) NO167511C (en)
NZ (1) NZ225805A (en)
PT (1) PT88258B (en)
TN (1) TNSN88083A1 (en)

Families Citing this family (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
FI885878A (en) * 1987-12-22 1989-06-23 Hoechst Ag SUBSTITUTE TIENOIMIDAZOLDERIVAT, FOERFARANDE FOER DERAS FRAMSTAELLNING, DESSA INNEHAOLLANDE PHARMACEUTICAL COMPOSITION OCH DERAS ANVAENDNING SOM INHIBITORER VID AVSOENDRING AV MAGSYRA.
US5164407A (en) * 1989-07-03 1992-11-17 Merck & Co., Inc. Substituted imidazo-fused 5-membered ring heterocycles and their use as angiotensin ii antagonsists
CN108191745A (en) * 2018-01-08 2018-06-22 滁州学院 The preparation method of 2- methylol -3,4- dimethoxy-pyridines

Family Cites Families (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
GB8417171D0 (en) * 1984-07-05 1984-08-08 Beecham Group Plc Compounds
FI861772A (en) * 1985-05-07 1986-11-08 Chemie Linz Ag THEN THEN (2,3-D) IMIDED INSULATED FOR THE FRAME FRAMEWORK.
ES2032394T3 (en) * 1986-02-20 1993-02-16 Hoechst Aktiengesellschaft PROCEDURE FOR PREPARING SUBSTITUTED TENOIMIDAZOLE DERIVATIVES.
JP2662754B2 (en) * 1992-07-20 1997-10-15 新日本製鐵株式会社 Backing steel material for tank bottom plate welding and corrosion prevention method for tank bottom plate

Also Published As

Publication number Publication date
EP0304732A3 (en) 1990-06-13
DK454588D0 (en) 1988-08-12
HUT50480A (en) 1990-02-28
NO883610D0 (en) 1988-08-12
FI883738A0 (en) 1988-08-11
NZ225805A (en) 1991-01-29
NO883610L (en) 1989-02-16
DE3827276A1 (en) 1989-03-23
HU208539B (en) 1993-11-29
EP0304732A2 (en) 1989-03-01
NO167511B (en) 1991-08-05
MA21352A1 (en) 1989-04-01
IL87428A0 (en) 1989-01-31
NO167511C (en) 1991-11-13
CN1029973C (en) 1995-10-11
IL87428A (en) 1993-01-31
CN1032340A (en) 1989-04-12
FI89602C (en) 1993-10-25
FI883738A (en) 1989-02-16
FI89602B (en) 1993-07-15
PT88258B (en) 1995-05-04
TNSN88083A1 (en) 1990-07-10
KR890003772A (en) 1989-04-18
PT88258A (en) 1989-06-30
JPS6470492A (en) 1989-03-15
DK454588A (en) 1989-02-16

Similar Documents

Publication Publication Date Title
KR930010495B1 (en) Process for preparation of pyridine derivatives
DE69433353T2 (en) BICYCLIC, HETEROCYCLIC SULFONAMIDES AND SULFONIC ACID ESTERS
EP0652872B1 (en) Optically pure magnesium -salt of pyridinylmethyl sulfinyl-1h-benzimidazole compound
CA2083606C (en) Dialkoxy-pyridinyl-benzimidazole derivatives, process for their preparation and their pharmaceutical use
CA1337197C (en) Subtituted thienoimidazole derivatives, a process for their preparation, pharmaceutical compositions containing them, and their use as inhibitors of gastric acid secretion
EP0233284A1 (en) Pharmacological compounds.
KR100812586B1 (en) Quinazoline compounds useful as p38 kinase inhibitors
NO154883B (en) ANALOGY PROCEDURE FOR THE PREPARATION OF NEW THERAPEUTICALLY ACTIVE 2-ACYLAMINOMETHYL-1,4-BENZODIAZEPINES.
PT86186B (en) METHOD FOR PREPARING BENZIMIDAZOLE DERIVATIVES AND PHARMACEUTICAL COMPOSITIONS CONTAINING THEM
EP0387821A2 (en) 2-Alkyl-4-arylmethylaminoquinolines, their use and medicines containing them
CA1268461A (en) 2-(2-picolylsulfur)-trienoimidazole derivatives
SK14672001A3 (en) Novel synthesis and crystallization of piperazine ring-containing compounds
CA1287631C (en) 5-substituted-6-aminopyrimidine derivatives, composition and uses
WO1987005021A1 (en) Benzimidazoles and their pharmaceutical use
EP0336544A1 (en) Heteroaryl 4-amino-3-acylquinoline derivatives and their use as inhibitors of gastric secretion
AU618540B2 (en) Substituted thienoimidazole derivatives, a process for the preparation thereof, pharmaceutical compositions containing them, and the use thereof as inhibitors of gastric acid secretion, as gastroprotectives and as medicaments for intestinal inflammations
WO1992006979A1 (en) New diazines
CZ177892A3 (en) AMINOMETHYL SUBSTITUTED 2,3-DIHYDROPYRAN(2,3-b)PYRIDINES, PROCESS OF THEIR PREPARATION AND THEIR USE IN MEDICAMENTS
US4847287A (en) Pure enantiomers of 4,5-disubstituted gamma-butyrolactams, and their use as antiamnestic agents
JPH0749423B2 (en) 2-Alkylsulfinyl-4 (3H) -quinazolinone derivatives, method for producing the same and antiulcer drug containing the same
AU622866B2 (en) Substituted thienoimidazole derivatives, processes for their preparation, pharmaceutical formulations containing them and their use as gastric acid secretion inhibitors
US5114955A (en) Substituted thienoimidazole derivatives
EP0412529B1 (en) Imidazole derivatives, process for the preparation of the same and antiulcer agents containing the same
EP0319170A2 (en) Acyl derivatives of hydroxy pyrimidines
US4800200A (en) 4,8-dihydro-8-arylisoxazolo[4,3-e][1,4]-oxazepin-5(6H)-ones

Legal Events

Date Code Title Description
MKLA Lapsed