GB2146023A - Aminocyclopentanes and their preparation and pharmaceutical formulation - Google Patents
Aminocyclopentanes and their preparation and pharmaceutical formulation Download PDFInfo
- Publication number
- GB2146023A GB2146023A GB08422453A GB8422453A GB2146023A GB 2146023 A GB2146023 A GB 2146023A GB 08422453 A GB08422453 A GB 08422453A GB 8422453 A GB8422453 A GB 8422453A GB 2146023 A GB2146023 A GB 2146023A
- Authority
- GB
- United Kingdom
- Prior art keywords
- compounds
- compound
- formula
- phenyl
- alkyl
- 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.)
- Granted
Links
- 238000002360 preparation method Methods 0.000 title claims description 19
- 239000008194 pharmaceutical composition Substances 0.000 title claims description 5
- NISGSNTVMOOSJQ-UHFFFAOYSA-N cyclopentanamine Chemical class NC1CCCC1 NISGSNTVMOOSJQ-UHFFFAOYSA-N 0.000 title description 6
- 150000001875 compounds Chemical class 0.000 claims description 196
- -1 pyrrolidino, piperidino, hexamethyleneimino Chemical group 0.000 claims description 56
- 125000001997 phenyl group Chemical group [H]C1=C([H])C([H])=C(*)C([H])=C1[H] 0.000 claims description 42
- ZUOUZKKEUPVFJK-UHFFFAOYSA-N phenylbenzene Natural products C1=CC=CC=C1C1=CC=CC=C1 ZUOUZKKEUPVFJK-UHFFFAOYSA-N 0.000 claims description 41
- 238000000034 method Methods 0.000 claims description 40
- 235000010290 biphenyl Nutrition 0.000 claims description 39
- 125000002496 methyl group Chemical group [H]C([H])([H])* 0.000 claims description 34
- LFQSCWFLJHTTHZ-UHFFFAOYSA-N Ethanol Chemical compound CCO LFQSCWFLJHTTHZ-UHFFFAOYSA-N 0.000 claims description 31
- 125000000217 alkyl group Chemical group 0.000 claims description 26
- 150000003839 salts Chemical class 0.000 claims description 26
- 239000002253 acid Substances 0.000 claims description 23
- 125000004435 hydrogen atom Chemical group [H]* 0.000 claims description 21
- 125000001495 ethyl group Chemical group [H]C([H])([H])C([H])([H])* 0.000 claims description 17
- 229910052757 nitrogen Inorganic materials 0.000 claims description 13
- 125000001544 thienyl group Chemical group 0.000 claims description 12
- 125000000956 methoxy group Chemical group [H]C([H])([H])O* 0.000 claims description 9
- 230000008569 process Effects 0.000 claims description 8
- 239000012453 solvate Substances 0.000 claims description 8
- 125000003545 alkoxy group Chemical group 0.000 claims description 7
- 150000002148 esters Chemical class 0.000 claims description 7
- 125000001511 cyclopentyl group Chemical group [H]C1([H])C([H])([H])C([H])([H])C([H])(*)C1([H])[H] 0.000 claims description 6
- 125000001624 naphthyl group Chemical group 0.000 claims description 6
- 125000004169 (C1-C6) alkyl group Chemical group 0.000 claims description 5
- 125000005677 ethinylene group Chemical group [*:2]C#C[*:1] 0.000 claims description 5
- 229910052736 halogen Inorganic materials 0.000 claims description 5
- 150000002367 halogens Chemical class 0.000 claims description 5
- 125000000623 heterocyclic group Chemical group 0.000 claims description 5
- 125000000587 piperidin-1-yl group Chemical group [H]C1([H])N(*)C([H])([H])C([H])([H])C([H])([H])C1([H])[H] 0.000 claims description 5
- 125000003944 tolyl group Chemical group 0.000 claims description 5
- 125000006705 (C5-C7) cycloalkyl group Chemical group 0.000 claims description 3
- 125000002947 alkylene group Chemical group 0.000 claims description 3
- 150000001408 amides Chemical class 0.000 claims description 3
- 125000003277 amino group Chemical group 0.000 claims description 3
- 125000000490 cinnamyl group Chemical group C(C=CC1=CC=CC=C1)* 0.000 claims description 3
- 150000003840 hydrochlorides Chemical class 0.000 claims description 3
- 125000004433 nitrogen atom Chemical group N* 0.000 claims description 3
- 125000001436 propyl group Chemical group [H]C([*])([H])C([H])([H])C([H])([H])[H] 0.000 claims description 3
- 150000007970 thio esters Chemical class 0.000 claims description 3
- XYFCBTPGUUZFHI-UHFFFAOYSA-N Phosphine Chemical compound P XYFCBTPGUUZFHI-UHFFFAOYSA-N 0.000 claims description 2
- 125000005036 alkoxyphenyl group Chemical group 0.000 claims description 2
- 125000005037 alkyl phenyl group Chemical group 0.000 claims description 2
- 239000003937 drug carrier Substances 0.000 claims description 2
- 125000001301 ethoxy group Chemical group [H]C([H])([H])C([H])([H])O* 0.000 claims description 2
- 230000003301 hydrolyzing effect Effects 0.000 claims description 2
- 150000002825 nitriles Chemical class 0.000 claims description 2
- 125000003884 phenylalkyl group Chemical group 0.000 claims description 2
- 208000016057 CHAND syndrome Diseases 0.000 claims 1
- 230000002862 amidating effect Effects 0.000 claims 1
- 150000001735 carboxylic acids Chemical class 0.000 claims 1
- 229940067003 orabase Drugs 0.000 claims 1
- DIKBFYAXUHHXCS-UHFFFAOYSA-N bromoform Chemical compound BrC(Br)Br DIKBFYAXUHHXCS-UHFFFAOYSA-N 0.000 description 114
- 239000000543 intermediate Substances 0.000 description 114
- ZMANZCXQSJIPKH-UHFFFAOYSA-N Triethylamine Chemical compound CCN(CC)CC ZMANZCXQSJIPKH-UHFFFAOYSA-N 0.000 description 94
- 239000000243 solution Substances 0.000 description 75
- 238000004587 chromatography analysis Methods 0.000 description 63
- OKKJLVBELUTLKV-UHFFFAOYSA-N Methanol Chemical compound OC OKKJLVBELUTLKV-UHFFFAOYSA-N 0.000 description 57
- 239000000203 mixture Substances 0.000 description 55
- 238000000746 purification Methods 0.000 description 48
- 238000004458 analytical method Methods 0.000 description 45
- YXFVVABEGXRONW-UHFFFAOYSA-N Toluene Chemical compound CC1=CC=CC=C1 YXFVVABEGXRONW-UHFFFAOYSA-N 0.000 description 40
- 239000002904 solvent Substances 0.000 description 35
- CSCPPACGZOOCGX-UHFFFAOYSA-N Acetone Chemical compound CC(C)=O CSCPPACGZOOCGX-UHFFFAOYSA-N 0.000 description 33
- WYURNTSHIVDZCO-UHFFFAOYSA-N Tetrahydrofuran Chemical compound C1CCOC1 WYURNTSHIVDZCO-UHFFFAOYSA-N 0.000 description 33
- VEXZGXHMUGYJMC-UHFFFAOYSA-N Hydrochloric acid Chemical compound Cl VEXZGXHMUGYJMC-UHFFFAOYSA-N 0.000 description 31
- HEMHJVSKTPXQMS-UHFFFAOYSA-M Sodium hydroxide Chemical compound [OH-].[Na+] HEMHJVSKTPXQMS-UHFFFAOYSA-M 0.000 description 31
- 239000000284 extract Substances 0.000 description 30
- 239000004305 biphenyl Substances 0.000 description 28
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- 239000007787 solid Substances 0.000 description 22
- IJGRMHOSHXDMSA-UHFFFAOYSA-N Atomic nitrogen Chemical compound N#N IJGRMHOSHXDMSA-UHFFFAOYSA-N 0.000 description 20
- 239000008363 phosphate buffer Substances 0.000 description 20
- 239000004480 active ingredient Substances 0.000 description 18
- XLYOFNOQVPJJNP-UHFFFAOYSA-N water Substances O XLYOFNOQVPJJNP-UHFFFAOYSA-N 0.000 description 18
- IAZDPXIOMUYVGZ-UHFFFAOYSA-N Dimethylsulphoxide Chemical compound CS(C)=O IAZDPXIOMUYVGZ-UHFFFAOYSA-N 0.000 description 16
- 239000000047 product Substances 0.000 description 15
- WEVYAHXRMPXWCK-UHFFFAOYSA-N Acetonitrile Chemical compound CC#N WEVYAHXRMPXWCK-UHFFFAOYSA-N 0.000 description 14
- UWAOHFMOWBQIJH-UHFFFAOYSA-N 3-cyclopentylpropanal Chemical compound O=CCCC1CCCC1 UWAOHFMOWBQIJH-UHFFFAOYSA-N 0.000 description 12
- UHOVQNZJYSORNB-UHFFFAOYSA-N Benzene Chemical compound C1=CC=CC=C1 UHOVQNZJYSORNB-UHFFFAOYSA-N 0.000 description 12
- RTZKZFJDLAIYFH-UHFFFAOYSA-N Diethyl ether Chemical compound CCOCC RTZKZFJDLAIYFH-UHFFFAOYSA-N 0.000 description 12
- 239000002585 base Substances 0.000 description 11
- ZMXDDKWLCZADIW-UHFFFAOYSA-N N,N-Dimethylformamide Chemical compound CN(C)C=O ZMXDDKWLCZADIW-UHFFFAOYSA-N 0.000 description 10
- 238000006243 chemical reaction Methods 0.000 description 10
- 239000000725 suspension Substances 0.000 description 10
- YMWUJEATGCHHMB-UHFFFAOYSA-N Dichloromethane Chemical compound ClCCl YMWUJEATGCHHMB-UHFFFAOYSA-N 0.000 description 9
- XEKOWRVHYACXOJ-UHFFFAOYSA-N Ethyl acetate Chemical compound CCOC(C)=O XEKOWRVHYACXOJ-UHFFFAOYSA-N 0.000 description 9
- VYPSYNLAJGMNEJ-UHFFFAOYSA-N Silicium dioxide Chemical compound O=[Si]=O VYPSYNLAJGMNEJ-UHFFFAOYSA-N 0.000 description 9
- 238000002425 crystallisation Methods 0.000 description 9
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- 239000010410 layer Substances 0.000 description 9
- 238000010992 reflux Methods 0.000 description 9
- QYKIQEUNHZKYBP-UHFFFAOYSA-N Vinyl ether Chemical compound C=COC=C QYKIQEUNHZKYBP-UHFFFAOYSA-N 0.000 description 8
- 230000000694 effects Effects 0.000 description 8
- OZAIFHULBGXAKX-UHFFFAOYSA-N 2-(2-cyanopropan-2-yldiazenyl)-2-methylpropanenitrile Chemical compound N#CC(C)(C)N=NC(C)(C)C#N OZAIFHULBGXAKX-UHFFFAOYSA-N 0.000 description 7
- QTBSBXVTEAMEQO-UHFFFAOYSA-N Acetic acid Chemical compound CC(O)=O QTBSBXVTEAMEQO-UHFFFAOYSA-N 0.000 description 7
- CPELXLSAUQHCOX-UHFFFAOYSA-N Hydrogen bromide Chemical class Br CPELXLSAUQHCOX-UHFFFAOYSA-N 0.000 description 7
- 229910017974 NH40H Inorganic materials 0.000 description 7
- LYCAIKOWRPUZTN-UHFFFAOYSA-N Ethylene glycol Chemical compound OCCO LYCAIKOWRPUZTN-UHFFFAOYSA-N 0.000 description 6
- NQRYJNQNLNOLGT-UHFFFAOYSA-N Piperidine Chemical compound C1CCNCC1 NQRYJNQNLNOLGT-UHFFFAOYSA-N 0.000 description 6
- JUJWROOIHBZHMG-UHFFFAOYSA-N Pyridine Chemical compound C1=CC=NC=C1 JUJWROOIHBZHMG-UHFFFAOYSA-N 0.000 description 6
- 239000003153 chemical reaction reagent Substances 0.000 description 6
- XCIXKGXIYUWCLL-UHFFFAOYSA-N cyclopentanol Chemical compound OC1CCCC1 XCIXKGXIYUWCLL-UHFFFAOYSA-N 0.000 description 6
- 229910052739 hydrogen Inorganic materials 0.000 description 6
- 230000007062 hydrolysis Effects 0.000 description 6
- 238000006460 hydrolysis reaction Methods 0.000 description 6
- 150000002440 hydroxy compounds Chemical class 0.000 description 6
- HQKMJHAJHXVSDF-UHFFFAOYSA-L magnesium stearate Chemical compound [Mg+2].CCCCCCCCCCCCCCCCCC([O-])=O.CCCCCCCCCCCCCCCCCC([O-])=O HQKMJHAJHXVSDF-UHFFFAOYSA-L 0.000 description 6
- 239000012044 organic layer Substances 0.000 description 6
- SQGYOTSLMSWVJD-UHFFFAOYSA-N silver(1+) nitrate Chemical compound [Ag+].[O-]N(=O)=O SQGYOTSLMSWVJD-UHFFFAOYSA-N 0.000 description 6
- 239000007858 starting material Substances 0.000 description 6
- YLQBMQCUIZJEEH-UHFFFAOYSA-N tetrahydrofuran Natural products C=1C=COC=1 YLQBMQCUIZJEEH-UHFFFAOYSA-N 0.000 description 6
- 125000004178 (C1-C4) alkyl group Chemical group 0.000 description 5
- RYHBNJHYFVUHQT-UHFFFAOYSA-N 1,4-Dioxane Chemical compound C1COCCO1 RYHBNJHYFVUHQT-UHFFFAOYSA-N 0.000 description 5
- UFHFLCQGNIYNRP-UHFFFAOYSA-N Hydrogen Chemical compound [H][H] UFHFLCQGNIYNRP-UHFFFAOYSA-N 0.000 description 5
- 210000001772 blood platelet Anatomy 0.000 description 5
- 150000001732 carboxylic acid derivatives Chemical class 0.000 description 5
- 239000003054 catalyst Substances 0.000 description 5
- 238000007796 conventional method Methods 0.000 description 5
- UREBWPXBXRYXRJ-UHFFFAOYSA-N ethyl acetate;methanol Chemical compound OC.CCOC(C)=O UREBWPXBXRYXRJ-UHFFFAOYSA-N 0.000 description 5
- 239000000706 filtrate Substances 0.000 description 5
- 238000001914 filtration Methods 0.000 description 5
- 239000001257 hydrogen Substances 0.000 description 5
- LPNYRYFBWFDTMA-UHFFFAOYSA-N potassium tert-butoxide Chemical compound [K+].CC(C)(C)[O-] LPNYRYFBWFDTMA-UHFFFAOYSA-N 0.000 description 5
- 230000009467 reduction Effects 0.000 description 5
- 229920006395 saturated elastomer Polymers 0.000 description 5
- 208000010110 spontaneous platelet aggregation Diseases 0.000 description 5
- 206010006482 Bronchospasm Diseases 0.000 description 4
- ROSDSFDQCJNGOL-UHFFFAOYSA-N Dimethylamine Chemical compound CNC ROSDSFDQCJNGOL-UHFFFAOYSA-N 0.000 description 4
- KFZMGEQAYNKOFK-UHFFFAOYSA-N Isopropanol Chemical compound CC(C)O KFZMGEQAYNKOFK-UHFFFAOYSA-N 0.000 description 4
- GUBGYTABKSRVRQ-QKKXKWKRSA-N Lactose Natural products OC[C@H]1O[C@@H](O[C@H]2[C@H](O)[C@@H](O)C(O)O[C@@H]2CO)[C@H](O)[C@@H](O)[C@H]1O GUBGYTABKSRVRQ-QKKXKWKRSA-N 0.000 description 4
- JGFZNNIVVJXRND-UHFFFAOYSA-N N,N-Diisopropylethylamine (DIPEA) Chemical compound CCN(C(C)C)C(C)C JGFZNNIVVJXRND-UHFFFAOYSA-N 0.000 description 4
- 239000000443 aerosol Substances 0.000 description 4
- 125000003710 aryl alkyl group Chemical group 0.000 description 4
- 230000007885 bronchoconstriction Effects 0.000 description 4
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- 235000003599 food sweetener Nutrition 0.000 description 4
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- 150000002430 hydrocarbons Chemical class 0.000 description 4
- 239000008101 lactose Substances 0.000 description 4
- RPNNPZHFJPXFQS-UHFFFAOYSA-N methane;rhodium Chemical compound C.[Rh] RPNNPZHFJPXFQS-UHFFFAOYSA-N 0.000 description 4
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- 229910000030 sodium bicarbonate Inorganic materials 0.000 description 4
- 238000003756 stirring Methods 0.000 description 4
- 239000003765 sweetening agent Substances 0.000 description 4
- DBGVGMSCBYYSLD-UHFFFAOYSA-N tributylstannane Chemical compound CCCC[SnH](CCCC)CCCC DBGVGMSCBYYSLD-UHFFFAOYSA-N 0.000 description 4
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- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
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- C07C405/0008—Analogues having the carboxyl group in the side-chains replaced by other functional groups
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- C07D231/12—Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members with only hydrogen atoms, hydrocarbon or substituted hydrocarbon radicals, directly attached to ring carbon atoms
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Description
1 GB 2 146 023 A 1
SPECIFICATION
Aminocyclopentanes and their preparation and pharmaceutical formulation The encloperoxides prostaglandins G2 and H2 and thromboxane A2 are naturally occurring reactive metabolites of arachidonic acid in human platelets. They are not only potent aggregatory agents but are also constrictors of vascular and bronchial smooth muscle, and therefore substances which antagonise their effects are of considerable interest in human medicine.
Our U.K. Patent Specification 2028805A describes a novel class of aminocyclopentane derivatives, 10 represented here bythe partial formula:
a 4 5 1,- CH22 3 2 ANR b R, c The compounds of Specification 2028805A inhibit blood platelet aggregation and bronchoconstriction. A 20 very broad range of compounds is described, one of the principal characteristics of which is an amino substituent -NIR b Watthe 2-position. This may be an acyclic or heterocyclic group of manytypes. The substituent -CH2XRa atthe 1-position can bevaried, and includes both saturated and unsaturated structures in which X is either -CH2CH2- or -CH=CH- and R' is an alkyl chain of variable length, terminally substituted by a carboxylic acid or esterfunction. As well as the possible variation in -NR b Rc and -CH2XR a, the compounds can have any one of eight different basic ring structures depending on the presence of an oxa function at the 3- andlor 5-positions and the presence or absence of a double bond at the 4,5- or 3,4 positions. The oxa function on the ring may be chosen from a wide range of possibilities, for example hydroxy, oxo, ether and ester groups.
Specification 2028805A thus embraces many different general possibilites and a large number of 30 inidividual compounds is exemplified. Nearly all of these have a ring structure which has oxa functions at both the 3- and 5-positions, the remainder being concerned with the other ring structures described. In general however a preference clearly emerges for compounds with 3- and 5- oxa functions. The usefulness of ring structures of this type is further emphasised in U.K. Patent Specifications 2070591A, 2075503A,
2079281A, 2097397A and 2108116A which also describe novel classes of aminocyclopentane derivatives.
These compounds also inhibit blood platelet aggregation and bronchoconstriction, but this activity is only associated with compounds which have a cyclopentane ring structure which has oxa functions at both the 3 and 5-positions.
We have now found a new group of aminocyclopentane derivatives which do not have an oxa function at the 3-position, but which surprisingly still have very good endoperoxide and thromboxane antagonist activity. The new compounds have a particularly advantageous profile of action, and are of special interest in the treatment of cardiovascular diseases, asthma and adult respiratory distress syndrome and for use in renal transplant and dialysis and in the prevention of relapse of healed peptic ulcers. The synthesis of the new compounds is generally also simpler and less expensive than the syntheses of many 3-oxa substituted aminocyclopentane derivatives previously proposed.
The invention thus provides compounds of the general formulae (1 a) and (1 b) OR2 01R 2 50,'(H2) 2 XWOOR1 JH2)2XW2 50 a) (1 b) 55 wherein R1 is a hydrogen atom, or a C1-6 alkyl or C7-jo aralkyl (e.g. phenalkyl) group; w is straight or branched C1-7 alkylene; 60 X is cis or trans -CH=CH-; Y is a saturated heterocyclic amino group (attached to the cyclopentane ring via the nitrogen atom) which has 5-8 ring members and (a) optionally contains in the ring -0-, -S-, -S02-, or -NR' (where R' is a hydrogen atom, C1-7 alkyl or aralkyl having a C1-4 alkyl portion); and/or (b) is optionally substituted by one or more C1-4 alkyl groups; 65 R 2 is 0) straight or branched C1.5 alkyl substituted by (a) phenyl [optionally substituted by C1-6 alkyl, C5-7 65 2 GB 2 146 023 A 2 cycloalky], phenylalkyl having a Cl-3 alkyl portion, thieny], phenyl (optionally substituted by Cl-4 alkyl, Cl-4 alkoxy, or phenyl)], (b) thienyl [optionally substituted by C5-7 cycloalkyl or phenyl (optionally substituted by Cl-3 alkyl, Cl-3 alkoxy or halogen], or (c) naphthyl (optionally substituted by Cl-4 alkyl or Cl-4 alkoxy) or (H) cinnamyi; and Z is -CH20H, -CHO or -CONHR 4 where R 4 is a hydrogen atom or a methyl group; 5 and the physiologically acceptable salts and solvates thereof.
In addition to having a desirable selectivity of action, compounds according to the invention also have the advantage of offering an attractive combination of high potency and good chemical stability. Additionally, compounds according to the invention have a solubility in water which is especially convenientfor their formulation for parenteral administration.
The structural formulae herein are to be understood to include the enantiomers of each of the compounds 10 concerned as well as mixtures of the enantiomers including racemates, even though the precise structure as set out only relates to one enantiomer.
The compounds of formula (1a) are generally preferred.
Suitable physiologically acceptable salts of the compounds of general formula (1) include acid addition salts derived from inorganic and organic acids, such as hydrochlorides, hydrobromides, sulphates, phosphates, maleates, tartrates, citrates, 2- chlorobenzoates, p-toluenesu 1 phonates, methanesul phonates, salicylates, fumarates, lactates, hydroxy-naphathalene-carboxylates (e.g. 1-hydroxy- or 3-hydroxy-2naphthalenecarboxylates) or furoates. The compounds may also form salts with suitable bases. Examples of such salts are alkali metal (e.g. sodium and potassium), alkaline earth metal (e.g. calcium or magnesium), ammonium and substituted ammonium (e.g. dimethylammonium,triethylammonium, 2-hydroxyethyI dimethylammonium, piperazine, N, N-d im ethyl pi perazine, piperidine, ethylenediamine and choline).
The heterocyclic amino group Y may for example have a 5, 6 or 7-membered ring, e.g. pyrrolidino, piperidino, morpholino, piperazino, thiomorpholino, 1,1 -dioxothiomorpholino, homomorpholino and hexamethyleneimino. Examples of the optional substituents (R 3) which may be present on a second nitrogen atom in the ring are methyl, ethyl, butyl, hexyl, benzy], and phenethyl. The carbon atoms of the heterocyclic rings may for example be substituted by methyl, ethyl or butyl.
In general Y is preferably pyrrolidino, piperidino or hexamethyleneimino, optionally substituted by one or tWO Cl-4 alkyl (particularly methyl) groups, e.g. 4-methylpiperidino. Compounds of formula (1 a) in which Y is piperidino are particularly preferred on account of their potency, stability and solubility characteristics, particularly their potency.
Examples of the group R' are benzy] and Cl-3 alkyl groups, e.g. methyl or ethyl. In general, R' is preferably a hydrogen atom or a methyl group, particularly a hydrogen atom.
Where R 2 is a substituted alkyl group, the alkylene portion is preferably a methylene, ethylene or propylene group and in particular is a methylene group.
InR 2 groups of the type (i) (a), the phenyl group may be substituted by, for example, methyl, ethyl, t-butyl, 35 cyclohexyl, thienyl, benzyi, phenethy], or phenyl (optionally substituted by methyl, ethyl, methoxy or butoxy) groups.
In R 2 groups of the type (i) (b), the thienyl group may be substituted by, for example, cyclohexyl or phenyl (optionally substituted by methyl, ethyl, methoxy, ethoxy, chloro or bromo) groups.
In general R 2 is preferably (i) Cl-5 alkyl (particularly methyl, ethyl or propyl) substituted by (a) phenyl or 40 phenyl substituted by phenyl (Cl -3) alkyl, thieny], phenyl, Cl-4 alkylphenyl or Cl-4 alkoxyphenyl, (b) thienyl or phenylthienyl or (c) naphthyl, or (H) cinnamyl.
Particularly preferred R 2 groups are (i) methyl, ethyl or propyl (particularly methyl) substituted by naphthyl, thienyl substituted by phenyl and phenyl substituted (preferably in the para-position) by thienyl, benzy], phenyl, or phenyl substituted (preferably in the para-position) by methyl or methoxy, or (H) cinnamyl. 45 Especially preferred R 2 groups are benzyl substituted by phenyl, methylphenyl or methoxyphenyl, for example [(1,1'-biphenyi)-4-yil methyl, [4'-methoxy(l, V-bi phenyl)-4- yl]methyl or [4'-m ethyl (1,1'-biphenyl)-4 yllmethyl, particularly [(1,1'-biphenyi)-4-yil methyl.
Xis preferably cis -CH=CH-.
W may contain for example 1-5 carbon atoms in a straight or branched chain, and may be for example 50 -(CH2)2- or -(CH2)4-, particularly the former.
In general, the compounds of formula (1) in which the carbon atom carrying the -(C1-12)2XWCOOR1 group is in the R configuration (and mixtures containing this isomer) are preferred.
The preferences indicated above apply both separately and in combination with one or more of the other stated preferences. Thus a preferred group of compounds of the invention has the formula (1a) in which:
R' is a hydrogen atom or a methyl group, W is -(CH2)2-, X is cis -CH=CH-, R 2 is as defined above with reference to the general definition of the compounds of the invention or is a 60 preferred R 2 group as described above, and Y is piperidino, including their physiologically acceptable salts and solvates.
The 1 R-isomers of this latter group of compounds are generally preferred, as are compounds in which R' is a hydrogen atom or methyl (particularly a hydrogen atom) and R 2 is Cl-3 alkyl substituted by phenyl or 65 phenyl substituted by phenyl, Cl -4 a 1 kyl phenyl (e.g. methyl phenyl), 3 GB 2 146 023 A Cl -4 a Ikoxyphenyl (e.g. methoxyphenyl),thienyl or phenyl (Cl -3) alkyl (e.g. benzyi); naphthalenyl methyl; thienyimethyi; or cinnamyi. Compounds of this group in which R 2 is benzyl substituted by phenyl, methylphenyl or methoxyphenyl are particularly preferred. Especially important compounds of this group are those in which R 2 is [(1,1'-bi phenyl)-4-yll methyl, [4'-m ethyl (1, V-bi phenyl)-4-yl]m ethyl or [4,5 methoxy(l, 1'- biphenyi)-4-yl 1 methyl, particularly [(1,1'-biphenyi)-4-yil methyl. Particularly important compounds of the invention are:
[ 1 [2-[[(1, V-15 i p henyi)-4-yi lm ethoxy]-5-(1 -pipe ridinyl)cyclo pentyl 1 -4-h epten oi c acid; 11 R-[lot(Z),2Q,5p]]-(+)-7-[2-[[(1,1'-biphenyl)-4-yllmethoxy]-5-(1piperidinyi) cyclopentyll-4-heptenoic acid; [1(Y.,(Z),2ot,5p]-( )-7-[2-[[4'-methoxy(1,1'-biphenyi)-4-yilmethoxy]-5-(lpi peridinyi)cyclopentyll-4-heptenoic acid, and its 1 R isomer; [1 a(Z),2ot,5p]-( )-7-[2-[4-(phenyI methyl) phenyl methoxy]-5-(1 -pi peridi nyi)cyclopentyll-4-heptenoic acid, and its 1 R isomer; [ 1 et(Z),2ot,5p]-( )-7- [2-([4'-methyl (1, V-bi ph enyi)-4-yi 1 meth oxy]-5-(1 -pipe rid i nyOcycl o pentyl 1 -4-h epteno ic acid, and its 1 R isomer; [1a-(Z),2p,5(x]-( )-7-[2-(1-piperidinyi)-5-[4-(2thienyi)phenyimethoxylcyclop entyll-4-heptenoic acid, and its 15 1 R isomer; [lot(Z)2(x,5p]-(- )-7-[2-[3-[(1,1'-biphenyi)-4-yllpropoxy]-5-(1piperidinyi) cyelopentyi]-4-heptenoic acid, and its 1 R isomer; and their physiologically acceptable salts (particularly hydrochlorides) and solvates.
Compounds of formulae (1 a) and (1 b) inhibit blood platelet aggregation, bronchoconstriction and 20 vasoconstriction. A test to determine inhibition of blood platelet aggregation is as described by G.V. Born (Nature 194, 927-929, (1962)) except in that collagen is used instead of ADP as the pro-aggregatory agent.
Alternatively, starved guinea pigs are dosed orally with the compound to be tested in a suitable vehicle.
Platelet rich plasma is prepared from each animal and aggregation to a range of collagen concentrations is measured after the method of Born. Collagen concentration effect curves for each sample of plasma are calculated and results are expressed as the shift of the curves following treatment with the compound.
The ability of the compounds of the invention to inhibit vasoconstriction or bronchoconstriction is determined using the relevant isolated tissue (e.g. spirally cut rat aortic strip or guinea-pig lung parenchymal strip) by measuring the effect of the compound to be tested on the contraction of the tissue to [1R-[1(x,4u-,5p(Z),6a(1E,3S)11-7-[6-(3-hydroxy-l-octenyi)-2-oxabicylo[2,2, 1]hept-5-yll-5-heptenoic acid (U 46619).
The compounds are thus of interest in the treatment of asthma, and as inhibitors of platelet aggregation and thrombosis for use in renal transplant and dialysis and the treatment or prevention of occlusive vascular diseases such as atherosclerosis, peripheral vascular disease, cerebral vascular disease including transient ischaemic attacks, stroke, pulmonary embolism, diabetic retinopathy, post operative thrombosis, angina and 35 myocardial infarction.
The compounds are also of potential use in the treatment of adult respiratory distress syndrome and the prevention of relapse of healed peptic ulcers.
The compounds may be formulated in a conventional mannerfor use with one or more pharmaceutical carriers.
For oral administration, the pharmaceutical composition may take the form of, for example, tablets, capsules, powders, solutions, syrups, or suspensions prepared by conventional means with acceptable excipients.
The compounds may be formulated for parenteral administration by continuous infusion. Formulations for injections may be presented in unit dosage form in ampoules, or in multi-dose containers, with an added 45 preservative. The compositions may take such forms as suspensions, solutions or emulsions in oil or aqueous vehicles, and may contain formulatory agents such as suspending, stabilising and/or dispersing agents. Alternatively, the active ingredient may be in powder form for reconstitution before use with a suitable vehicle, e.g. sterile pyrogen-free water.
For administration by inhalation the compounds are conveniently delivered in the form of an aerosol spray 50 presentation from pressurised packs or a nebuliser, or as a cartridge from which the powdered composition may be inhaled with the aid of a suitable device. In the case of a pressurised aerosol the dosage unit may be determined by providing a valve to deliver a metered amount.
For use as antithrombotic agents, the compounds are preferably administered orally, for example in amounts of 0.05 to 1 Orng/kg body weight, 1 to 4 times daily, or intravenously, for example in amounts of 0.01 55 to 25 mg/kg body weight, 1 to 4 times daily.
For use in the treatment of asthma, the compounds may also be administered orally in amounts of 0.05 to 10mg/kg body weight, 1 to 4 times daily; preferably however they are administered by inhalation at doses varying from 0.02 to 30mg, preferably 0.02 to 3mg, 1 to 4times daily. The compounds may be used in combination with other antiasthmatic agents.
The precise dose administered will of course depend on the age and condition of the patient.
Suitable methods for preparing compounds of formula (1) are described below, the groups R' -R 4, W, X and Y being as defined above except where otherwise indicated.
4 GB 2 146 023 A (a) Compounds of formula (1a) maybe prepared by reacting a compound of formula (2) 4 0 (2) 10 with an appropriate Wittig reagent, e.g. a phosphorane of formula R5P=CHWC02R' (where R'is C1-6 alkyl or 3 aryl, e.g. monocyclic aryl such as phenyl) or a salt thereof, e.g. the potassium salt. Suitable reaction solvents include hydrocarbons (e.g. benzene and toluene), ethers (e.g. tetrahydrofuran) and dial kyisu lphoxides (e.g. 15 dimethylsulphoxide). The reaction may be carried out at any suitable temperature from -70'to 50'C, preferably at room temperature. The reaction is particularly suitable for the preparation of compounds in which R' is a hydrogen atom. The intermediate aldehydes of formula (2) may be prepared bythe following sequence:
0 0710 OH 20 25 OH OR 2 30 6 OR OR 6 1 71 35 (7) A lactone of formula (4) is prepared from the corresponding lactone (3) by catalytic hydrogenation, using for example a catalyst such as rhodium on charcoal in a solvent such as ethyl acetate. The lactone (4) is then reduced to the corresponding lactols (5), for example with diisobutylaluminium hydride in a solvent such as dichloromethane at a low temperature, e.g. -780C. These are then treated with an appropriate Wittig reagent40 (e.g. R5P=CHOR 6, 5 6 3 whereR isasdefinedaboveandR is C1-4 alkyl), as described for process (a) above, to give the hydroxy compound (6). The group R 2 is then introduced by etherification of the hydroxy compound (6) with an appropriate reagent R 2 L (where L is a leaving group, e.g. halogen or tosyiate), for example by reaction at room temperature in the presence of a suitable base (e.g. sodium hydride) in a suitable solvent (e.g. dimethylformamide). The resulting vinyl ether (7) is then hydrolysed to give the desired aldehyde (2), 45 for example using a dilute acid such as hydrochloric acid in a suitable solvent (e.g. acetone).
Lactones of formula (3) may be prepared by the method described in UK Patent Specification 2028805A using the appropriate amine YH.
In another process, the vinyl ethers of formula (7) may be prepared by a sequence of reactions involving dehydroxylation and subsequent modification of an intermediate cyclopentanol as described in the 50 experimental section at the end of this specification.
(b) Compounds of forrinula (1a) in which R' is a hydrogen atom maybe prepared by hydrolysing a corresponding ester, amide or nitrile.
The hydrolysis of the above starting materials can in general be effected by conventional methods under acidic or basic conditions, for example in an organic or aqueous organic solvent at any suitable temperature 55 up to and including reflux. Suitable bases include inorganic bases such as alkali metal hydroxides (e.g.
NaOH), alkali metal carbonates (e,gX2C03) and alkaline earth metal hydroxides (e.g. Ba(0]-IM. Suitable organic bases include tetra alkylammonium hydroxides [e.g. ("Bu)4N'OH-1. Suitable acids include inorganic acids such as hydrochloric acid and organic acids such as trifluoroacetic acid and acetic acid. Suitable solvents include ethers (e.g. diethyl ether, dioxan and tetra hyd rofu ran), halogenated hydrocarbons (e.g. 60 CH2C12), hydrocarbons (e.g. toluene), dipolar aprotic solvents (e.g. acetone, acetonitrile, dimethyIsulphoxide and dimethylformamide) and alcohols (e.g. methanol, ethanol and ethylene glycol). Where desired the solvents may be used in combination with water.
The specific hydrolysis method will of course depend on the particular nature of the starting material.
The acid of formula (1a) produced maybe isolated in the form of a salt, for example a salt with an inorganic 65 GB 2 146 023 A 5 acid, such as hydrochloric acid. This is particularly convenient and advantageous when the hydrolysis is effected with the same acid; salt formation and hydrolysis then take place in the same reaction step.
The starting materials for this process may for example be corresponding compounds of formula (8) OR2 5 .-(CH2)2XW 10 Y (8) where Z1 is (a) -COOR1a where R 1 a is di- or tri-aryimethyl (e,g. di- or tri phenyl methyl), trihydrocarbylsilyl (e.g. diphenyl-t-butylsilyl), -CH2M3, - CH2CH=CH2, C1-6 alkyl (optionally substituted atthe n-position by Cl-C, alkoxy or C1-6 alky[thio) or a 5- or 6- membered cycloalkyl group containing -0- in the ring (e.g. 20 tetrahydrofuran-2-yl ortetrahydropyran-2-y1) (b) -CON137. where R' is -H or C1-4 alkyl, or (c) -CN.
Suitable examples of W' groups are:
(1) -CH8R9R10 in which R' and R9 are each phenyl (optionally substituted by C1-4 alkyl, C1-4 alkoxy, 25 di-(C1-4) alkylamino, nitro or halogen) and W' is a hydrogen atom or a substituted or unsubstituted phenyl group as defined for R' and R9; (2) -SIR11R 12 W' where R' 1, R 12 and R 13 are aryl (e.g. phenyl) or Cl - 6 alkyl; (3) -CH2M3; (4) -CH2CH=CH2; 30 (5) -CH(R 14)BCH2R15 where B is -0- or -S-, and where R 14 and R15 are -H or Cl-4 alkyl (e.g. -CH20CH3, -CH(C1-13)0CH2CH3 or -CH2SCH3) or where R 14 and R 15 together represent - (CHA2- or -(CH2)3- and B is -0-; and (6) Cl-6alkyl.
35 Specific examples of the groups of the type (1), include triphenyimethyl (in which the phenyl groups are optionally substituted by methyl, methoxy or nitro) or diphenyimethyl (in which the phenyl groups are optionally substituted by halogen, methyl, methoxy or dimethylamino).
The latter group of esters (and other esters in which Z1 is a group of the type (a)) may be hydrolysed by the methods described above. The process is particularly useful in preparing a salt of a compound of formula 40 (1 a) by treating a compound of formula (8) (e.g. a compound in which Z1 is a group (a), particularly where Ria is a group (1), e.g. tri phenyl methyl) with an acid or a base. Thus for example a hydrochloride of a compound of formula (1 a) may be prepared by treating a solution of the compound of formula (8) as just mentioned with hydrogen chloride or hydrochloric acid. This method is particularly suitable in the preparation of the preferred compounds of formula (1a) described above.
Esters in which R1a is a group (2) may also be removed using a fluoride (e.g. tetra-n-butylammonium fluoride, KF or HF), for example using tetrahydrofuran or aqueous CH3CN as the reaction solvent.
Esters in which R1a is -CH2M3 may also be removed by reduction e.g. with a metal such as zinc under mildly acidic conditions for example using an aqueous phosphate buffer. Tetrahydrofuran, dioxan and dimethoxyethane are suitable solvents.
When R is a group of type (5) and B is S, hydrolysis may also be effected in the presence of Hgll salts e.g.
mercuric trifluoroacetate for example using aqueous CH3CN as solvent. These esters may also be hydrolysed in the presence of Ag11 salts (e.g. AgNO3), for example using aqueous tetrahydrofuran, dioxan, dimethoxyethane or CH3M as solvent.
The hydrolysis of the derivatives of formula (8) in which Z1 is a group of the type (b) or (c) can in general be 55 effected using an inorganic base (e.g. KOH) in a suitable solvent such as aqueous ethanol or ethylene glycol at a temperature up to and including reflux.
The starting materials for process (b) may be prepared from the corresponding carboxylic acid (i.e. the compound of formula (1 a) in which R' is -H) by conventional methods, for example as described in UK Patent Specification 2129796A. Alternatively, the Z1 group may be introduced by use of a Wittig reagent of 60 the formula R5P=CHM1 in process (a) above.
3 (c) Compounds of formula (1a) in which R' is Cl-6alkyl orC7-1o aralkyl maybe prepared byesterification of the corresponding carboxylic acid. Conventional esterification techniques maybe used, for example by reaction with an appropriate alcohol in the presence of a mineral acid such as hydrochloric acid or sulphuric acid.
6 GB 2 146 023 A 6 Alternatively the acid may be converted into an activated derivative (e.g. a corresponding mixed anhydride) e.g. by reaction with an alkyl chloroformate (e.g. isobutyl chloroformate) in the presence of a suitable base, e.g. triethylamine or pyridine. The activated derivative can then be reacted with an appropriate alcohol, for example using a solvent such as acetone and a temperature of -1 O'C to room temperature.
(d) Compounds of formula (1a) maybe prepared by dehydroxylation (homolytic cleavage of the carbon-oxygen bond) of a corresponding alcohol of formula (9) 1,,(CH2)2XWCOOR1 HO A Y (9) 15 20 for example via tri-n-butyltin hydride reduction of a thioester derivative such as the thiocarbonyl imidazolide. The reaction is particularly suitable for the preparation of compounds in which R' is alkyl or aralkyl.
The reduction is preferably carried out in a hydrocarbon solvent (e.g. toluene) at a temperature up to and including reflux in the presence of a radical initiator e.g. azobisisobutyronitrile.
The thioester derivative may be conveniently prepared from the alcohol (9) using a suitable reagent (e.g. 1,1'-thiocarbonyidiimidazole) in a suitable solvent (e.g. tetrahydrofuran) at room temperature.
Alcohols of formula (9) may be prepared by the methods generally described in UK Patent Specifications 2075503A and 2097397A.
(e) Compounds of formula (1a) may also be prepared by reduction of a corresponding compound of formula (1a) in which Xis an acetylene group. Suitable methods of reduction including using hydrogen in the presence of a catalyst e.g. palladium on a support (e.g. CaC03 or BaS04) and poisoned for example by lead or quinoline. Suitable solvents include ethyl acetate and methanol. This reaction is particularly suitable for preparing compounds in which X is cis-CH=CH-.
Compounds of formula (1a) in which X is an acetylene group may be prepared from compounds of formula (9) in which X is an acetylene group using the method described in (d) above.
Compounds of formula (9) in which X is an acetylene group may be prepared bythe methods generally described in UK Patent Specifications 2075503A and 2097397A.
(f) Compounds of formula (1a) in which X istrans -CH=CH- maybe prepared by isomerising the corresponding cis compound. The isomerisation may for example be effected by treatment with p-toluene 40 sulphinic acid in dioxan (e.g. at reflux) or azobisisobutyronitrile and thiophenol, using for example a hydrocarbon solvent (e.g. benzene) and any suitable temperature up to reflux.
(g) Compounds of formula (1a) in which R' is a hydrogen atom may also be prepared by oxidising the corresponding aldehyde or primary alcohol (i.e. a compound of formula (1 b) in which Z is -CHO or CH20H.
Suitable methods of oxidation include using a Crv' oxidising agent in a suitable solvent, e.g. chromic acid 45 in acetone (e.g. Jones reagent, preferably used in the presence of a diatomaceous silica such as Celite) or Cr03 in pyridine. These reagents are for example used at temperatures of - 20'C to room temperature.
The oxidation may also be effected with oxygen in the presence of a catalyst such as platinum dioxide in a suitable solvent (e.g. acetone) at an elevated temperature (e.g. 50'C).
(h) Compounds of formula 0b) in which Z is -CH20H maybe prepared by reducing a corresponding 50 compound of formula (1 a) in which R' is a methyl group, for example with LiAll-14.
(i) Compounds of formula (1b) in which Z is -CHO maybe prepared by oxidising the corresponding compound of formula (1 b) in which Z is -CH20H, using for example an activated sulphur reagent, e.g. (i) N-chlorosuccinimide-dimethyisulphide complex in a suitable solvent (e.g. toluene or dichloromethane) at temperatures of from example -25 to 25'C, preferably at 0-5'C, or (ii) pyridine -S03 complex in dimethyl-sulphoxide, preferably at O'C to room temperature.
(j) Compounds of formula (1b) in which Zis -CONHR 4 may be prepared by amidation of the parent carboxylic acid i.e. the corresponding compound of formula (1 a) in which R' is a hydrogen atom.
Conventional methods for converting acids into amides may be used, for example by treating the acid with isobutylchloroformate in the presence of triethylamine and reacting the resulting reactive derivative of the 60 carboxylic acid with ammonia or an amine R 4 NH2.
(k) Where salts of compounds of the invention are desired such salts maybe formed by conventional methods, for example by treatment with an acid or with abase.
Treatment may for example be effected in a suitable solvent such as an ether (e.g. diethylether), acetonitrile, acetone, chloroform, dichloromethane, ethyl acetate, iso- propyl acetate or an alcohol, e.g. 65 7 GB 2 146 023 A 7 methanol, ethanol or iso-propanol.
Salts may also be formed by conversion of one salt of a compound of the invention into another, e.g. by ion exchange using conventional methods.
When a specific enantiomer of formula (1) is required, starting materials having the desired stereochernical configuration should be used in the above processes. Such starting materials may be 5 prepared for example from an enantiomeric bicyloheptenone as described in European Patent Specification
74856 using the methods generally described in UK Patent Specifications 2028805A. 2075503A and
2097397A.
The following examples illustrate the invention. Temperatures are in 'C. 'Dried' refers to drying with MgS04- Hyflo' is a
filtration acid. Chromatography and thin layer chromatography (t.l.c.) are using silica gel unless stated otherwise.
The following abbreviations are used:- THF DIVIF Dibal DIVISO EA 20 ER PE IPA A1BN tetrahydrofuran dimethylformamide diisobutylaluminium hydride (1 M in hexane) dimethyisulphoxide ethyl acetate diethyl ether petroleum ether (b. p. 40-60') isopropyl acetate azobisisobutyronitrile The preparations of the following intermediates are described in British Patent Specification 2097397A.
Intermediate 1 [1R-(endo,anti)]-(-)-6-[[(1,1'-Biphenyl)-4-yilmethoxy]-8-(1-piperidinyi)2-o xabicyclo[3.2.lloctan-3-one.
Intermediate 2 [1 R-[1 a-(Z),2p,3p,5a]l -(+)-Methyl 7-[5-[[1,1'-Biphenyi)-4-yilmethoxy1 3-hydroxy-2-(1piperidinyi)cyclopenty)1-4-heptenoate.
Intermediate 3 [1 R-[1 u.(Z),2p,3p,5(xll-(+)-7-[5-[[(1,1'-Biphenyl)-4-yilmethoxy]-3hydroxy-2-(4mo rpholinyi)cyclopentyll-435 heptenoic acid.
Intermediate 4 [1 R-[1 et(Z),2p,3p,5etll-(+)-7-[5-[[(1,1'-Biphenyl)-4-yilmethoxy]-3- hydroxy-2-(1 -piperidinyi)cyclopentyll-4heptenoic acid.
The preparation of the following intermediate is described in British Patent Specification 2129796A.
Intermediate 5 [1 R-[1 a.(Z),2 P,3(x,5a]]-(+)-Methyl 7-[3-Hydroxy-5-[[4'-methoxy(1,1'- biphenyl)-4-yilmethoxy]-2-(1 45 piperidinyl)cyclopentyll-4-heptenoate, hydrochloride.
Intermediate 6 [1R-[loL(Z),2p,3p,5otll-(+)-MethyI 7-[5-[[(1, 1'-Biphenyl)-4-yllmethoxy]- 3-hydroxy-2-(4morpholinyl)cyclopentyll-4-heptenoate.
A solution of Intermediate 3, hydrochloride (1.35g) in 19:1 methanol conc. H2S04 (10M1) was kept at 50 ambient temperature for 18h, then diluted with 8% NaHC03 solution (100mi) and extracted with CH2C12 (3x25mi). The combined extracts were dried and evaporated and the residue was purified by chromatogra phy using ER then 19:1 ER - methanol as eluantto give the title compoundas an oil (0.969).
I.R. (CHBr3) 3550,3460-3200,1728cm-1 [,121.4 = +78.2'(CI-IC13) D Intermediate 7 [1R-[oi(Z),2p,5oL]]-(-)-Methyl 7-[[4-Methoxy(l, l biphenyl)-4-yllmethoxy]-3-oxo-2-(1piperidinyl)cyclopentyll-4-heptenoate A solution of pyridine-sulphurtrioxide complex (10.33g) in dry DMSO (17mi) was added to a cold (00) solution of Intermediate 5, base (8.47g) in Et3N (13.5mi), CH2C12 (30mi) and DMSO (20mi). After 1 h at O'the mixture was diluted with pH 6.5 phosphate buffer (140mi) and extracted with EA (3x50mi). The combined extracts were dried and evaporated and the residue was purified by chromatography using 1:3 EA-PE as eluant to give the title compound as a solid (5.69g). A portion was recrystallised from ER-PE m.p. 61.5-62.50.
[(X122.2 19.8' (CHC13) D 8 GB 2 146 023 A 8 Intermediate 8 [1R-[19-(Z),2p,3p,5a]]-(+)-MethyI 7-[3-Hydroxy-S-[[4'- methoxy(l, 1'1.biphenyl)-4-yljmethoxy]-2-(1piperidinyl)cyclopentyll-4- heptenoate Dibal (93mi) was added dropwise to a cold (-50) stirred solution of 2,6-di-tert-butyi-4-methylphenoI (30.75g) in dry toluene (350mi). After 1 h at -50 the mixture was cooled to -700 and a solution of Intermediate 7 (9.67g) in toluene (50mi) was added dropwise. After 1 h at -700 and 1 h at - 1 0'the mixture was washed with 2N HCI (7x60mi) and the toluene was discarded. The acidic extracts were neutralised with 5N Na0H solution (200mi) and extracted with CH2C12 (4x80mi). The combined extracts were dried and evaporated and the residue was purified by chromatography using 17:3 ER-methanol as eluant to give the title compound 10 (7.02g) as an oil. Analysis Found: C,715; H,8.5; N, 23. C32H43NO5 requires C,733; H,83; N,23% [UJ21 = +612'(CHC13) D Intermediate 9 [1R-(1u,2p,3a,5ot)]-(+)-Methyl 5-ff(1, 1'1-Biphenyl)-4-yllmethoxy]-3- hydroxy-2-(1-piperidinyl)cyclopentaneacetate A solution of Intermediate 1 (3.5g) in methanol (50mi) and ethereal HCI (50mi) was kept at ambient temperature for 20h. The solvents were removed in vacuo and the residue in 8% NaHC03 solution (100mi) was extracted with CH2C12 (4x75m]). The combined extracts were dried and evaporated to give a solid 20 (3.78g).
A portion was crystallised from EA-PE to give the title compound m.p. 105107' [(YID = +66' (CHC13) Intermediate 10 a) [1R-[lct(Z),2p,3p,5ctll-()-Methyl7-5-[[(1,1-Biphenyl)-4-yljmethoxy]-3[(1H-i midazol-l-yl)thioxomethoxy]2-(1-piperidinyl)cyclopentyll-4-heptenoate A solution of Intermediate 2 (3.1g) and 1,1'-thiocarbonyidiimidazole (1. 35g) in dry THF (12mi) was kept at ambient temperature for 2h then the solvent was removed in vacuo. The residue in EA (1 00mi) was washed with pH6 phosphate buffer, dried and the solvent evaporated to give the title compound as an oil (3.7g). T.I.c. 30 ER Rf 0.37.
The following compounds were prepared in a similar manner:
b) [1R-(1(x,2p,3ot,5ot)]-()-Methyt[5-[[(1,1'1-Biphenyl)-4-yllmethoxy]-3[(1H-im idazol-l-yl)thioxomethoxy]-2(1-piperidinyl)jcyclopentane-acetate, m.p. 94-98'from Intermediate 9.
c) [1R-[lct(Z),2p,3p,5u-]]-()-Methyl7-[5-[[(1,1-BiphenYI)4-yllmethoxy]-3[(1H -imidazol-lyl)thioxomethoxy]-2-(4-morpholinyl) cyclopentyll-4heptenoate, from Intermediate 6. T.I.c. EA Rf 0.47.
d) [1R-[1(Y(Z),2p,3p,5otll-()-Methyl7-[3-[(1H-Imidazol-lyl)thioxomethoxy]-5-[[ 4-methoxy(1,1'-biphenyl)-4- 40 yllmethoxy]-2(1piperidinyl)cyclopentyll-4-heptenoate, from intermediate 8. T.I.c. ER Rf 0.36.
Intermediate 11 [IR-(lu,2u,5p)]-(+)-Methyl2-[[(l, l-Biphenyl)-4-yljmethoxyj-5-(l- piperidinyI)cyclopentaneacetate A solution of AIBN (0.91g) and tri-n-butyltin hydride (22.72g) in toluene (80ml) was added over 10 min to a stirred suspension of Intermediate 10b (25.5g) in toluene (250ml) at 95- 1000 under nitrogen. After a further 15min at 1 000the mixture was concentrated in vacuo and the mixture was purified by chromatography eluting initiallywith 19:1 PE-ER to remove impurities then with 25:25:1 PE-ER-Et3N to give the title compound as a solid (9.12g). A portion was crystal lised from ethanol-PE m.p. 113-116'.
[(X]23 = +74.4(CHC13) D Intermediate 12 [1R-(lot,2ct,5p)]-(+)-2-[[(1, i'-Biphenyl)4-yllmethoxy]-5-(1- piperidinyl)cyclopentaneethanol, hydrochloride Dibal (75m0was added overO.5hto a cooled (-65% stirred solution of Intermediate 11 (8.27g) in CH2C12 55 (200mi) under nitrogen. The solution was allowed to warm to 00 over 2h then methanol (200mi) was added.
After a further 1 h, the mixture was filtered and the filtrate was evaporated in vacuo. The residue was dissolved in ER (300mi), filtered and evaporated to give the title compound, base (7.06g). A portion in ER was treated wih an excess of ethereal HCI and the resulting solid was crystallised from CH2C12 - IPA to to give the title compound m.p. 165-168'.
[,]22 = +56'(CHC13) D Intermediate 13 [1R-(let,2oc,50)]-(+)-2-[[(1, 1'1-Biphenyl)-4-yllmethoxy]-5-(1- piperidinyl)cyclopentaneacetaldehyde A solution of pyridine-sulphur trioxide complex (0.5g) in DMSO (3mi) was added to a cooled (5% stirred 65 9 GB 2 146 023 A 9 solution of Intermediate 12 (0.397g) and Et.3N (0.72mi) in CH2C12 (5m]). After 1 h the mixture was diluted with 30% NH4C1 solution (10m I) and the layers separated. The aqueous layer was extracted with CH2C12 (2x7m]) and the combined extracts were dried and evaporated. The residue was purified by chromatography to give the title compound as an oil (0.189). 5 I.r. (CHBr3)2740,1710cm-1 [UJ25 = +100.7'(CHC13) D Intermediate 14 a) (3aa,4ct,6aa)( )-3,3ot,4,6a-Tetrahydro-4-(1piperidinyl)-2H-cyclopenta[blfur an-2-one Piperidine (8.49) was added to a cold (0% stirred solution of (3act,6eL, 6au-)-6-bromo-3,3a,6,6a-tetrahydro- 10 2H-cyclopenta[blfuran-2-one (5.19) in acetone (60mi) and the mixture was stirred at ambient temperature for 20h. The mixture was poured into water (200mi) and saturated NaCI (100mi) and extracted with EA (3x100mi). The aqueous layerwas adjusted to pH 9 and re-extracted with EA (2x 100mi). The combined extracts were dried and evaporated and the residue was purified by chromatography using 4:1 EA-methanol as eluant to give the title compound as an oil 3.2g). I.r. (CHBr3) 1760cm- 1.
The following compounds were prepared in a similar manner:
b) 3aa,4a,6act)-( )-3,3a,4,6a-Tetrahydro-4-(4-thiomorpholinyl)-2Hcyclopenta[blf uran-2-one, m.p. 87-890 using thiomorpholine and diisopropylethylamine. Purification by crystallisation from CH2C12-ER-PE 20 c) (3a(Y,4a,6aa)-(.t)-3,3a,4,6a-Tetrahydro-4-(4-methyl-l-piperazinyl)-2Hcyclop enta[bjfuran-2-one,m.p.6264' using N-m ethyl pi perazi ne and diisopropylethyla mine. Purification by crystallisation from PE-ER.
d) (3au,4a,6aoL)-(.t:)-3,3a,4,6a-Tetrahydro-4-(4-methyl-l-piperidinyl)-2Hcyclo penta[blfuran-2-one, using 4- 25 methyl pi peridine. Purification by chromatography on Et3N deactivated silica using EA as eluant. I.r. (CHBr3) 1760cm e) (3aot,4(x,6aoL)-( )-3,3a,4,6a-Tetrahydro-4-(1-pyrrolidinyl)-2Hcyclopenta[blf uran-2-one, using pyrrolidine.
Purification by chromatography using 79:20:1 EA-methanol-Et3N as eluant.
I.r. (CHBr3) 1765cm-1 f) (3act,4(x,6aot)-( )-3,3a,4,6a-Tetrahydro-4-(Hexahydro1H-azepin-l-yl)2H-cycl openta[blfuran-2-one, using hexahydro-1H-azepine. Purification by chromatography on Et3N deactivated silica using initially 1:1 CH2C12-ER then ER as eluant.
I.r. (CHBr3) 1760cm-1 Intermediate 15 (3act,4u,6au-)-( )-3,3a,4,6a-Tetrahydro-4-(4-thiomorpholinyl)-2Hcyclopenta[ blfuran-2one, SS-dioxide Peracetic acid (6.14 molar in acetic acid; 5mi) was added dropwise to a stirred solution of Intermediate 14b 40 (1 g) in CH2C12 (1 Orni). After 72h the mixture was added dropwise to 20% Na2S03 solution (20mi) and the mixture was stirred at ambient temperature for 1 h. The layers were separated and the aqueous layer was extracted with CH2C12 (2 x20mi). The combined organic layers were washed with 8% Nal-IC03 solution (20mi) dried and evaporated. A portion of the residual solid (1.02g) was crystallised from EA - methanol to give the title compound m.p. 147-150'.
Intermediate 16 a) 3aot,4ot,6act)-(:t)-Hexahydro-4-(1-piperidinyl)-2H-cyclopenta[blfuran2-one, hydrochloride A solution of Intermediate 14a (7.8g) in EA (100mi) was hydrogenated over a pre-reduced suspension of 5% Rhodium on charcoal in EA (1 00mi) for 5h at atmospheric pressure and ambient temperature. The 50 catalyst was removed by filtration (Hyflo) and the filtrate was washed with 8% Nal-IC03 solution (50mi) dried and evaporated to give an oil (2.9g). A portion in ER was treated with an excess of ethereal HCI and the resulting solid was recrystallised from methanol-EA to give the title compound m.p. 1981199'.
The following compounds were prepared in a similar manner:
b) (3aot,4ot,6aa)-(:t)-Hexahydro-4-(4-methyl)-1-piperazinyl)-2Hcyclopentafbjfu ran-2-one, m.p. 93-960 from Intermediate 14c using 5% Rhodium on alumina. Purification by crystallisation from EA - PE.
c) (3au,4ot,6a(x)-( )-Hexahydro-4-(4-methyl-l-piperidinyl)-2Hcyclopenta[bjfuran -2-one, from Intermediate 14d using 5% Rhodium on alumina in ethanol.
I.R. (CHBr3) 1760cm-1.
d) 3au,4u,6au)-(.- )-Hexahydro-4-(l-pyrrolidinyl)-2H-cyclopentafbjfuran-2one, m.p. 47-50o from Intermedi ate Me using 5% Rhodium on alumina in ethanol. Purification by chromatography on Et3N deactivated silica using EA as eluant.
GB 2 146 023 A e) (3aot,4ot,6act)-(-t)-Hexahydro-4-(4-thiomorpholinyl)-2Hcyclopenta[blfuran-2 -oneSS-dioxide,m.p.1671710 from Intermediate 15 using 5% Rhodium on charcoal in methanol -water. Purification by crystallisation from EA - methanol.
Intermediate 17 (3act,4ot,6act)-(.t)-Hexahydro-4-(Hexahydro-1H-azepin-lyl)-2H-cyclopenta[bj furan-2-one Asolution of Intermediate 14f (1.1g) in 5N NaOH (10mi) andwater(60mi) was hydrogenated over pre-saturated 5% Rhodium on charcoal (250rng) in water (30mi). After uptake of hydrogen had ceased the catalyst was removed by filtration (Hyflo) and conc. HCI (1 5mi) was added to the filtrate. After 3h the solution was basified with 25% K2C03 solution and extracted with CH2C12 (3x40mi). The combined extracts were dried and evaporated and the residue in ER was filtered and the solvent removed to give the title compound as an oil (1. 049). I.r. (CHBr3) 1760cm-1 Intermediate 18 a) (3aot,4ot,6aoL]-(-!::)-Hexahydro-4-(1-piperidinyl)-2Hcyclopentafbjfuran-2-o I A solution of Intermediate 16a (8.3g of base) in CH2C12 (40mi) was stirred at -78' under nitrogen whilst Dibal (60mi) was added slowly. After 2h methanol (40m1) was added slowly and the mixture was allowed to attain ambient temperature and then was stirred for 18h. The solids were removed by filtration (Hyflo) and the filtrate was evaporated in vacuo to give the title compound (7.6g) m. p. 77-81'.
The following compounds were prepared in a similar manner:- b) (3act,4et,6act)-(--i:)-Hexahydro-4-(4-methyl-l-piperidinyl)-2Hcyclopenta[bl furan-2-olm.p.80-85'fromlntermediate 16c.
c) (3act,4a,6aa)-(:t)-Hexahydro-4-(4-methyl-l-piperazinyl)-2Hcyclopenta[blfura n-2-ol, from Intermediate 16b. I.r. (CHBr3) 3580cm-1 d) (3aa,4a,6aa-)-(:t)-Hexahydro4-(4-thiomorpholinyl)-2Hcyclopenta[blfuran-2-a lSS-dioxide, from Inter- 30 mediate 16e.
I.r. (CHBr3) 3580cm-1.
16d.
e) (3a(Y,4ot,6aa)-(:)-Hexahydro-4-(1 yrrolidinyl)-2H-cyclopenta[blfuran2ol, m.p. 79-820 from Intermediate f) 3aa,4u,6aa)-(-t)-Hexahydro-4-(hexahydro-1H-azepin-l-yl)-2Hcyclopenta[bjfura n-2-ol, from Intermediate 17. I.r. (CHBr3) 3580cm Intermediate 19 a) (let,2(Y,3p)-(.t)-2-(3-Methoxy-2-propenyl)-3-(1piperidinyl)cyclopentanoI (Methoxymethyl)tri phenyl phosphon W m chloride (1 6.5g) was added in portions to a stirred solution of potassium t-butoxide (5.69) in dry THF at 0'. After 0.5h a solution of Intermediate 18a (3.5g) in dry THF (20m1) was added dropwise and stirring continued for 2h. The mixture was poured into 8% Nal-IC03 solution (250mi) and the organic layer separated. The aqueous layer was extracted with CH2C12 (3x 1 00mi) and the combined organic layers were dried and evaporated. The residue was purified by chromatography using initially 9:1 EA-methanol then 85:10:5 EA-methanol- ET3N as eluant to give the title compound as an oil (3.5g).
I.r.(CHBr3)3600,3500,1655cm-1.
The following compounds were prepared in a similar manner:
b) [2R-(lot,2p,3p)]-(+)-1-[3-11(1,1'-Biphenyl)-4-yljmethoxy]-2-(3-methoxy2-pr openyl)cyclopentyllpiperidine, m.p. 44-47'from Intermediate 13. Purification by chromatography using initially 1:1 55 PE-ER then 25:75.1 PE-ER-Et3N as eluant. [a125 = +74.5' (CHC13) D c) (lct,2u,3p)-(-!:)-2-(3-Methoxy-2-propenyl)-3-(4-methyl-lpiperidinyl)cyclope ntanol, from Intermediate 18b. Purification by chromatography using 99:1 EA-Et3N as eluant then rechromatography using 19: 1:0.1 60 CH2C12-methanol-Et3N as eluant. I.r. (Film) 3400,1652cm-1 d) let,2(Y,3p)-(-!:)-2-(3-Methoxy-2-propenyl)-3-(4-methyl-lpiperazinyl)cyclope ntanol, from Intermediate 18c. Purification by chromatography using initially 49:1 EA-Et3N then 75:25:2 EA-methanol-ET3N as eluant.
I.r. (Film) 3400(br), 1660cm-1.
11 GB 2 146 023 A 11 e) (lot,2ot,3p-("-,h)-2-(3-Methoxy-2-propenyl)-3-(4-thiomorpholinyl) cyclopentanol, SS-dioxide, from Intermediate 18d. Purification by chromatography using initially 4:1 EA-PE then EA as eluant. I.r. (Film) 3400 (br), 1655cm-1 f) (let,2(Y,3p)-( )-2-(3-Methoxy-2-propenyl)-3-(1pyrrolidinyl)cyclopentanol, from Intermediate 18e. Purification by chromatography using 80:20:1 EA-methanol-IEt3N as eluant. I.r. (Film) 3400(br), 1650cm-1.
g) (la.,2ot,3p)-(-t)-3-(Hexahydro-lH-azepin-1-yl)-2-(3-methoxy-2propenyl)cyclo pentanol, from Intermediate 10 18f. Purification by chromatography on activity 2 alumina using ER as eluant. I.R. (Film) 3450(br), 1655cm-1.
Intermediate 20 (1a,2p,3p)-( )- 1-[3-[[(1, 1'-Biphenyl)-4-yllmethoxy]-2(3-methoxy-2-propenyl)cyclopentyllpiperidine 4-Bromomethyi(1,1'-biphenyi) (4.99) was added to a cold (09 stirred mixture of Intermediate 19a (1.79) and 15 sodium hydride (0.64g, 80% dispersion in oil) in dry DMF (3mi). After 3h at ambient temperature the mixture was poured carefully into water (30mi) and extracted with CH2C12 (3x30mi). The combined extracts were dried and evaporated and the residue was purified by chromatography using initially 9:1 EA-methanol then 85:10:5 EA-methanol-R31M as eluant to give the title compound as an oil (1.45g).
Analysis Found:
C2H35NO2 requires C, 79.7; H, 8.6; N, 3.6.
C, 80.0; H, 83; N, 3.45%.
Intermediate 21 (1(x,20,3p)-(:t)- 1-[3-[4-(1, 1-Dimethylethyl)phenylmethoxy]-2-(3-methoxy2-propenyl)cyclopentyllpiperidin e NaOH powder (403mg) was added under nitrogen to a stirred solution of Intermediate 19a (20Orng) in dry DIVISO (2mi). After 10 min 1 -bromomethyl-4-(1,1 -dim ethyl ethyl) benzene (21 Orng) was added and stirring continued for 4h. The mixture was diluted with pH 6.5 phosphate buffer (30mi) and extracted with EA (3x20mi). The combined extracts were dried and evaporated and the residue was purified by chromatogra- 30 phy using 4:1 EA-methanol to give the title compound (20Orng).
T.I.c. 4:1 EA-methanol Rf 0.41.
Intermediate 22 a) (1u-,2p,3p-(-L)-1-[2-(3-Methoxy-2-propenyl)-3-[[4(phenylmethyl)phenyllmetho xyIcyclopentyllpiperidine 35 Sodium Hydride [(60% dispersion in oil) 240rng] was added to a stirred solution of Intermediate 19a (0.72g) in dry DMF (10mi). The mixture was heated to ca. 80'to complete hydrogen evolution and then cooled (0') whilst 1 -(b ro m o methyl)-4-(p henyl m ethyl) benzene (0.78g) was added. After 2h the mixture was diluted with brine (200mi) and extracted with EA (3x75m1). The combined extracts were washed with brine (100mi) dried and evaporated and the residue was purified by chromatography using 99:1 EA-IEt3N as eluant to give the title compound as an oil (0.855g).
Analysis Found: C, 79.8; H, 8.9; N, 3.7.
C28HA02 requires C, 80.2; H, 8.9; N, 3.3%. 45 The following compounds were prepared in a similar manner:
b) (lot,2p,3p)-(-t)-1-[2-(3-Methoxy-2-propenyl)-3-[[4'1-methyl(1,1'biphenyl) 4-yllmethoxy]- cyclopentyllpiperidine, from Intermediate 19a and 4-bromomethyi-4'- methyi(1,1'-biphenyi). Purification by 50 chromatography using 99: 1 EA-IEt3N as eluant.
Analysis Found: C, 80.1; H, 8.9; IN, 3.7.
C28H37NO2 requires C, 80.2; H, 8.9; Nf 3.3%. 55 c) flu,2p,3p(E)]-( )-1-[2-(3-Methoxy-2-propenyl)-3-[(3-phenyl-2propenyl)oxylcyc lopentyllpiperidine, from Intermediate 19a and cinnamyl bromide. Purification by chromatography using initially 199:1 EA-IEt3N followed by 197: 1:1 EA-methanol-R3N as eluant.
Analysis Found:
C23H33NO2 requires C, 77.8; H, 9.5; N, 4.0.
C, 773; H, 9.4; N, 3.9%.
d) (1u-,2p,30)-( )-1-[2-(3-Methoxy-2-propenyl)-3-(phenylmethoxy) cycopentyllpiperidine, from Intermedi- 65 12 GB 2 146 023 A 12 ate 19a and benZY1 chloride. Purification by chromatography using initially EA followed by 199:1 EA-Et3N.
Analysis Found: C, 76.5; H, 93; N, 4.2.
C211-131NO2 requires C, 76.6; H, 9.5; N, 4.25%. 5 e) (la,2p,3p)-(-t)-1-[2-(3-Methoxy-2-propenyl)-3-(2-naphthalenyl-methoxy) cyclopentyllpiperidine, from Intermediate 19a and 2-(brom o methyl) na phthylen e. Purification by chromatography on Et3N deactivated silica using EA as eluant.
Analysis Found: C25H33NO2 requires C, 78.9; H, 8.6; N, 3.5.
C, 79.1; H, 8.8; N, 3.7%.
f) (lot,2p,3p)-(:L)-1-[2-(3-Methoxy-2-propenyl)-3-[[4-(2thienyl)phenyllmethoxy lcyclopentyllpiperidine, from Intermediate 19a and 2-[4-(bro mo methyl) phenyl Ith io p hene. Purification by chromatography on Et3N 15 deactivated silica using EA as eluant.
Analysis Found: C, 73.0; H, 8.2; N, 3.3.
C25H33NO2S requires C, 73.0; H, 8.1; N, 3.4% 20 g) (leL,2p,3p)-(-t:)-1-[3-[3-[(1,1'-Biphenyl)-4-yllpropoxy]-2-(3-methoxy2-pro penyl)cyclopentyllpiperidine, from Intermediate 19a and 3-[1,1'biphenyl)-4-yilpropanol, 4-m ethyl benzenesu 1 p h onate. Purification by chromatography on Et3N deactivated silica eluting with EA.
Analysis Found: C, 80.0; H, 9.0; N, 3.2. 25 C29H39NO2 requires C, 80.3; H, 9.1; N, 3.2%.
h) (Ioc,2p,3p)-(.t)-1-[2-(3-Methoxy-2-propenyl)-3-[(5-phenyl-3thienyl)methoxyI cyclopentyllpiperidine, from Intermediate 19a and 4(bromomethyl)-2-phenyithiophene. Purification by chromatography on Et3N deactivated silica eluting with EA. 30 Analysis Found: C, 72.4; H, 8.0; N, 3.3.
C25H33NO2 requires C, 72.95; H, 8.1; N, 3.4% i) (let,2p,3p)-(--t)-1-[3-[[(1,1-Biphenyl)-4-yljmethoxy]-2-(3-methoxy-2propen yl)cyclopentyll-4-methyl- 35 piperidine, from Intermediate 19c and 4-bromo methyl (1, V-bi phenyl). Purification by chromatography using 1: 1 ER-PE as eluant.
Analysis Found: C, 79.9; H, 83; N, 3.7.
C28HA02 requires C, 80.15; H, 8.9; N, 3.3%. 40 j) (let,2p,3p)-(:t)-1-[3-[[(1,1'-Biphenyl)-4-yljmethoxy]-2-(3-methoxy-2propen yl)cyclopentyll-4 methylpiperazine, from Intermediate 19d and 4bromomethyl (1,1'-biphenyl). Purification by chromatography using initially 50:1 EA-Et3N followed by 85:15:1 EA-methancil-Et3N as eluant. 45 I.r. (Neat) 1653cm-1 k) (1a,2p,30)-(.t:)4-[3-[[(1,1'1-Biphenyl)-4-yllmethoxy]-2-(3methoxy-2propen yl)cyclopentyllthiomorpholine 1, 1-dioxide, m.p. 92-93'from Intermediate 19e and 4-bro mo methyl (1,1'-bi phenyl). Purification by chromatography using ER as eluant.
from Intermediate 19f and 4-bro mo methyl (1, V-bi phenyl). Purification by chromatography using 94:5A EA-methanol-Et3N as eluant.
Analysis Found: C26H33NO2 requires C, 80.0; H, 85.; N, 3.8.
C, 79.75; H, 8.5; N, 3.6%.
m) (1a,2p,3p)-(.t)-1-[3-[[(1,1'-Biphenyl)-4-yllmethoxy]-2-(3-methoxy-2propeny l)cyclopentyllhexahydroW-azepine, from Intermediate 19g and 4bromo methyl (1,1'-biphenyi). Purification by chromatography on 60 Et3N deactivated silica eluting initially with 1: 1 CHP2-ER then ER.
Analysis Found: C28HA02 requires C, 79.9; H, 83; N, 3.5.
C, 80.15; H, 8.9; N, 3.3%.
13 GB 2 146 023 A 13 Intermediate 23 a) (lot,2ct,5p)-(:L)-2-[[(1, 1'1.Biphenyl)-4-yllmethoxy]-5-(1- piperidinyllcyclopentanepropanaI A solution of Intermediate 20 (1.3g) in analar acetone (10mi) and 5N HCI (3m]) was stirred at ambient temperature for 5h. The mixture was adjusted to ca. pH 8 using 5N NaOH (3mi) and 8% Nal-IC03 solution (20m1) and extracted with CH2C12 (3x50m1). The combined extracts were dried and evaporated to give the 5 title cornpound(l.18g) m.p. 65-680.
The following compounds were prepared in a similar manner:
b) [1R-(1a-,2(x,50)]-(+)-2-[[(1,1-Biphenyl)-4-yllmethoxy]-5-(1piperidinyl)cyc lopentanepropanalm.p.88-920 from Intermediate 19b.
[0J24 = +76.10 (CHC13) D c) (lot,2a,5p)-( )-2-[4(1, 1-Dimethylethyl)phenylmethoxyj5-(1- piperidinyl)cyclopentanepropanal, from In termediate 21 I.r. (CHBr3) 1715cm-1 d) (lot,2a,5p)-( )-2-[[4-(Phenylmethyl)phenyllmethoxy]-5-(1piperidinyl)cyclopen tanepropanal, from Intermediate 22a I.r. (CHBr3) 2730,1720cm-1 e) (1u,2ot,5p)-(t)-2-[[4'-Methyl(l, 1'.biphenyl)-4-yllmethoxy]-5-(1- piperidinyl)cyclopentanepropanal, from Intermediate 22b I.r. (CHBr3) 2725, 1715cm-1 f) [lot,2u-(E),5p)-( )-2-[(3-Phenyl-2-propenyl)-oxy]-5-(1piperidinyl)cyclopenta nepropanal, from Intermedi- 25 ate 22c I.r. (CHBr3) 2740,1722, 970cm-1 g) (1a,2a,5P)-( )-2-(Phenylmethoxy)-5-(1-piperidinyl)cyclopentanepropanal, from Intermediate 22d I.r. (CHBr3) 2740,1720cm h) (lct,2(Y,5p)-( )-2-(2-Naphthalenylmethoxy)-5-(1piperidinyl)cyclopentanepropa nal, from Intermediate 22e I.r. (CHBr3) 2720,1720cm-1 i) (la,2p,5oL)-(:L)2-(1-Piperidinyl)-5-[[4(2thienyl)phenyllmethoxylcyclopent anepropanal, from Intermediate 22f I.r. (CHBr3) 2720, 1720cm-1 j) (loi,2a,5p)-( )-2-[3-[(1,1-Biphenyl)-4-yllpropoxy]-5(1piperidinyl)cyclopen tanepropanal, from Intermedi- 40 ate 22g I.r. (CHBr3) 2720,1720cm-1 k) (la,2oc,5p-( )-2-[(5-Phenyl-3-thienyl)methoxy]-5-(1piperidinyl)cyclopentanep ropanal, from Intermediate 22h I.r. (CHBr3) 2730,1715cm-1 1) 1'Biphenyl)-4-yllmethoxy]-5-(4-methyl-lpiperidinyl)cyclopentanepropanal, from Intermediate 22i 50 I.r. (CHBr3) 2720,1720cm-1 m) (la,2ot,5p)-( )-2-[[(1, 1'-Biphenyl)-4-yllmethoxy]-5-(4-methyl-lpiperazinyl)cyclopentanepropanal, from Intermediate 22j I.r. (CHBr3) 1720cm-1 n) (lot,2(Y,5p)-(:t)-2-[[(1,1'1-Biphenyl)-4-yllmethoxy]-5-(4thiomorpholinyl)cy clopentanepropanalSSdioxide, from Intermediate 22k. 1. r. (CHBr3) 2720,1720,1330cm-1 o) l.Biphenyl)-4-yllmethoxy]-5-(1-pyrrolidinyl)cyclopentanepropanal, from Intermediate 22 1 I.r. (CHBr3) 2720,1715cm-1 p) (lu,,2a,5p)-(:t)-2-[[(1,1-Biphenyl)-4-yllmethoxy]-5-(hexahydro-1Hazepin-l-y l)cyclopentanepropanal, from Intermediate 22m. I.r. (CHBr3) 2720,1715cm-1 14 GB 2 146 023 A 14 Intermediate 24 [lR-[lot(Z),2ot,5p]]-(+)-7-[2-[[(l, l-Biphenyl)-4yljmethoxyj-5-(l-piperidinyl)cyclopentyll-4-heptenenitrile 3-Cyanopropyltriphenylphosphonium bromide (2.1g) was added to a cold (0'), stirred solution of potassium t-butoxide (0.58g) in dry THF (20ml) under nitrogen. After 20 min a solution of Intermediate 23b (0.65g) in THF (1 Oml) was added dropwise. After a further 45 min methanol (30ml) was added and the solvents were removed in vacuo. The residue in pH 6.5 phosphate buffer was extracted with EA (2x50ml). The combined extracts were dried and evaporated and the residue was purified by chromatography on activity 2 alumina using 3:2 ER-PE as eluant to give the title compound (0.64g) m.p. 39-40'. [U]23.6 = + 87.20 (CHC13) D Intermediate 25 [1R-[1u-(Z),2ot,5p]]-(+)-(Triphenylmethyl) 7-[2-[[(1, 1'1Biphenyl)-4-yllmethoxy]-5-(1-piperidinyl)cyclopentyll-4heptenoate A mixture of trityl chloride (0.18g),the product of Example 3, base (0. 31g) and Et3N (2.02g) in CH2C12 (5mi) was stirred at ambient temperature for 66h. The mixture was diluted with pH 6.5 phosphate buffer (40mi) and15 extracted with ER (3x3Oml). The combined extracts were dried and evaporated and the residue was purified by chromatography on Et3N deactivated silica eluting with 2:3 ER-PE to give the title compound as an oil (0.31 g). I.r. (CHBr3) 1735cm-1 22.6 = + 52'(CHC13) [(YID Intermediate 26 [1R-[1a(Z),2ot,5p]]-(+)-(Diphenylmethyl) 7-[2-[[(1, l -Biphenyl)-4yllmethoxy]-5-(1-piperidinyl)cyclopentyll-4- heptenoate A mixture of the compound of Example 3, base (0.31 g) and diphenyl- diazomethane (0.39g) in benzene (1 Orril) was stirred at ambient temperature for 22h then heated to 50'for 9h. The solvent was removed in 25 vacuo and the residue was purified by chromatography on Et3N deactivated silica eluting with 2:1 PE-ER to give the title compound as an oil (0.36g). I.r. (CHBr3) 1730cm-1.
[0123.7 = + 56'(CI-IC13) D Intermediate 27 [1R-[1a(Z),2(Y,5p]]-(+)-[(1, 1-Dimethylethyl)diphenylsilyll 7-[2-[[(1, 1'Biphenyl)-4-yllmethoxy]-5-(1- piperidinyl)cyclopentyll-4-heptenoate A mixture of the compound of Example 3, base, (0.31 g), Et3N (121 mg) and (1,1 Dimethylethyi)diphenyisilylchloride (0.275g) in CH2C12 (5m]) was stirred at ambient temperature for 21 h. The mixture was diluted with pH 6.5 phosphate buffer (30mi) and extracted with ER (3x35m1). The combined 35 extracts were washed with saturated NaCI solution, dried and evaporated to give the title compound as an oil.
I.r. (CHBr3) 1720cm-1.
Intermediate28 [1R-[lcL(Z),2ot,5011(+)-7-[2-[[(1, 1'1-Biphenyl)-4-yllmethoxy]-5- (1piperidinyl)cyclopentyll-4-heptynoic acid, hyrochloride A solution of bromine in CH2C12 (5% vlv; 8.1 mi) was added over 0.5h to a cooled (0') stirred solution of the compound of Example 1 a (3.657g) in CH2C12 (15 mi). After a further 1 h the mixture was washed with 7% Na2S203 solution (2x 10 m]) and 8% Nal-IC03 Solution (2x10 mi), dried and treated with an excess of ethereal 45 HCL The solvents were removed in vacuo to give a solid (4.75g).
The solid (5.5g) in dry DMSO (120 mi) was cooled (0% and stirred under nitrogen while potassium t-butoxide (12.329) was added. The mixture was stirred at ambient temperature for 19h then diluted with water (30 mO, 5N HCI (20 mi) and pH 6.5 phosphate buffer (100mi) and extracted with EA (3x80 m]). The combined extracts were washed with brine (2x50 mi) dried and evaporated and the residue was purified by 50 chromatography (twice), using 17:2A CH2C12-ethanol-Et3N, then 13:6A ER- ethanol-Et3N as eluant. The product in pH 6.5 phosphate buffer (40 m]) was extracted with CH2C12 (2x25 m]) and the combined, dried extracts were treated with an excess of ethereal I-ICI. The solvents were removed in vacuo and the residue was co-evaporated with ER to give the title compound as a foam (1.1 7g).
T.I.c. 17:2A CH2C12-ethanol-Et3N Rf 0.42 [(X123.6 = + 90' (CHC13) D EXAMPLE 1 a)[1R-[1u--(Z),2ct,5pjl-(+)-Methyl7-[2-[[(1,1'-Biphenyl)4-yllmethoxy]-5(l-p iperidinyl)cyclopentyll-4- heptenoate A solution of tri-n-butyltin hydride (18.729) and A1BN (847mg) in toluene (55m]) was added over 10min to a solution of Intermediate 10a (25.8g) in toluene (140mi) at 100' under nitrogen. The mixture was heated under ref lux for 15min., cooled and evaporated in vacuo. The residue was purified by chromatography (twice), firstly using 19:1 PE-ER as eluant and secondly using gradient elution from 40:15:1 PE-ER-Et3N upto 25:25:1 PE-ER-Et3N to give the title compound as an oil (13.31g). I.r. (CHBr3) 1730cm-1 GB 2 146 023 A 15 Analysis Found: C, 78.11; H, 8.5; N, 2.9.
C31 H41 N 03 req u i res C, 78.3; H, 83; N, 2.95%.
[UJ23 + 75.80 (CHC13) D The following compounds were prepared in a similar manner:
b) [1R-[1a(Z),2et,5l3J1-(+)-Methy1 7-[2-[[(l, l-Biphenyl)-4-yljmethoxyl-5(4-morpholinyl)cyclopentylj-4heptenoate, from Intermediate 1 Oc. Purification by chromatography initially on activity 2 alumina eluting with 3:2 ER-PE then on silica eluting with ER. I.r. (CHBr3) 1728cm-1 Analysis Found: C, 74.9; C30H39NO4 requires C, 75.4; [0,121.2 = + 80.41 (CHC13) D H, 8.5; N, 3.3.
H, 8.2; N, 2.9.
c) [1R-[lot(Z),2(x,5p]]-(+)-Methyl7[2-[[4'-Methoxy(1,1'-biphenyl)-4yllmetho xy1-5-(1piperidinyl)cyclopentyll-4-heptenoate, from Intermediate 10d. Purification by chromatography using initially 1:1 PE:ER then 49:49:2 PE-ER-Et3N as eluant. I.r. (CHBr3) 1730cm-1 Analysis Found: C32H43NO4 requires C, 76.0; [UJ25 = + 680 (CHC13) D C, 7 5.9; H, 8.6; N, 3.2.
H, 8.6; N, 2.8%.
EXAMPLE 2 a) [lcL(Z),2ot,5p]-(:)-Methyl 7-[2-ff(1, 1'-Biphenyl)-4yllmethoxy]-5-(1-piperidinyl)cyclopentyll-4-heptenoate (3Carboxypropyl)triphenylphosphonium bromide (3.9g) was added to a stirred solution of potassium t-butoxide (1,95g) in dry THF (30mi). After 0.5h a solution of Intermediate 23a (1.1g) in dry THF (5mi) was added and the mixture stirred for 2h at ambient temperature. Methanol (10mi) was added and the mixture 30 was concentrated in vacuo. The residue, which contained [1u-(Z),2a,5p]-(- :)-7-[2-[[(1,1'-Biphenyl)-4yilmethoxy]-5-(1 piperidinyi)cyclopentyll-4-heptenoic acid, in methanol (30mi) containing conc. H2S04 (5mi) was kept at ambient temperature for 18h then concentrated in vacuo. The residue was adjusted to pH 8 with 5N NaOH (5mi) and 8% NaHCO3 solution (200mi). The mixture was extracted with CH2C12 (3x 1 00mi) and the combined extracts were dried and evaporated. The residue was purified by chromatography using 49:1 35 ER-Et3N as eluantto give the title compound as an oil (0.64g). I.r. (CHBr3) 1730cm-1 Analysis Found: C, 78.25; H, 8.8; N, 2.8.
C311-141NO3 requires C, 78.3; H, 8.7; N, 2.9%.
The following compounds were prepared in a similar manner.
b) [1u-(Z),2a.,5p]-(:t)-Methyl 7-[2-[4-(1, 1-Dimethylethyl)phenylmethoxy]5-(1-piperidinyl)cyclopentyll-4heptenoate, from Intermediate 23c. Purification by chromatography using 80:20:1 EA-PE-C3N as eiuant. I.r. (CHBr3) 1730cm.
Analysis Found: C, 76.5; H, 10.0; N, 3. 1.
C29H45NO3 requires C, 76.4; H, 10.0; N, 3.1 %.
c) [Iot(Z),2ot,5P]-( )-Methyl 7-[2-[[4-(Phenylmethyl)phenyllmethoxy]-5-(1piperidinyl)cyclopentyll4- heptenoate, from Intermediate 23d. Purification by chromatography on Et3N deactivated silica using ER as 50 eluant. I.r. (CHBr3) 1725cm-1 Analysis Found: C, 783; C32H43NO3 requires C, 78.5; H, 83; N, 3.2.
H, 8.9; N, 2.9%.
d) [loL(Z),2ot,5p]-(-!:)-Methyl7-[2-[[4'-Methyl(1,1'.biphenyl)-4yllmethoxyl-5 -(1piperidinyl)cyclopentyll-4heptenoate, from Intermediate 23e. Purification by chromatography on Et3N deactivated silica using ER as eluant. I.r. (CHBr3) 1725cm-1.
Analysis Found: C, 78.3; C32H43NO3 requires C, 785; H, 86.; N, 2.6.
H, 8.9; N, 2.9%.
e) [lu(Z),2a(E),5p]-( )-Methyl7-[2-(3-Phenyl-2-propenyl)oxy]5-(1piperidinyl)cyc lopentyll-4-heptenoate, from Intermediate 23f. Purification by chromatography on Et3N deactivated silica eluting initially with 1: 1 65 CH2C12-ER then ER. I.r. (CHBr3),1730,970cm-1.
16 GB 2 146 023 A 16 Analysis Found: C, 76.2; H, 9.5; N, 3.4.
C2,,H39NO3 requires C, 76.2; H, 9.2; N, 3.3%.
f) flet(Z),2et,5p]-(-t:)-Methyl7-[2-(Phenylmethoxy)-5-(1piperidinyl)cyclopenty ll-4-heptenoate, from Interme diate 23g. Purification by chromatography on Et3N deactivated silica eluting initially with 1:1 CHP2-ER 5 then ER. I.r. (CHBr3) 1730cm-1 Analysis Found: C, 75.1; H, 9.7; N, 3.8.
C25H37NO3 requires C, 75.15; H, 9.3; N, 3.5%.
g) [1a-(Z),2ot,5p]-(-)-Methyl 7-[2-(2-Naphthalenyimethoxy)-5-(1piperidinyl)cyclopentyll-4-heptenoate, from Intermediate 23h. Purification by chromatography on Et3N deactivated silica using ER as eluant. I.r. (CHBr3) 1726cm-1.
Analysis Found: C, 77.4; H, 8.5; N, 2.9.
C29H39NO3 requires C, 77.5; H, 83; N, 3.1 %.
h) [la(Z),2p,50L]-(-t:)-MethYl 7-[2-(1-Piperidinyl)-5-[[4-(2thienyl)phenyllmethoxylcyclopentyll-4-heptenoa te, from Intermediate 23i. Purification by chromatography on Et3N deactivated silica using ER as eluant. I.r.
(CH13r3)1725cm-1.
Analysis Found: C, 72.8; H, 8.2; N, 2.8.
C29H39NO3S requires C,72.3; H, 8.1; N, 2.9% 0 [lu(Z),2(Y,5p]-( )-Methyl7-[2-[3-[(1,1'-Biphenyl)-4-yllpropoxy]-5-(1piperid inyl)cyclopentyll-4heptenoate, from Intermediate 23j. Purification by chromatography on Et3N deactivated silica using ER as eluant. I.r. (CHBr3) 1725cm-1 Analysis Found: C, 78.5; H, 9.0; N, 2.8.
C33H45NO3 requires C, 783; H, 9.0; N, 2.8%.
j) [let(Z),2a,5p]-(-f:)-MethYI7-[2-[(5-Phenyl-3-thienyl)methoxy]-5-(1piperidin yl)cyclopentyll-4-heptenoate, from Intermediate 23k. Purification by chromatography on Et3N deactivated silica eluting with 1:1 CH2C12 ER then ER. I.r. (CHBr3) 1730 cm-1.
Analysis Found: C, 72.65; H, 8.4; N, 2.9.
C29H39NO3S requires C,72.3; H, 8.2; N, 2.9%.
k) [1R-[1u.(Z),2(Y,5p]]-(-±)-Methyl9-[2-[[(1,1'-Biphenyl)-4-yllmethoxy]5-(1-p iperidinyl)cyclopentyll-6- nonenoate, from Intermediate 23b and (5carboxypentyi)triphenylphosphonium bromide. Purification by 40 chromatography using 50:1 ER-Et3N as eluant.
I.r. (CHBr3) 1730cm.
Analysis Found: C, 78.3; H, 8.6; N, 2.5.
C33H45NO3 requires C, 783; H, 9.0; N, 2.8%.
1) [1u-(Z),2ot,5p]-(-t)-Methyl7-[2-[[(1,1'.Biphenyl)-4-yllmethoxy]-5(hexahydr o-1H-azepin-l-yl)cyclopentyll4-heptenoate, from Intermediate 23p. Purification by chromatography on Et3N deactivated silica eluting initially with CH2C12 then with 9:1 CH2C12-ER increasing to 2:1 CH2C12-ER. I.r. (CHBr3) 1730cm-1.
Analysis Found: C, 78.6; H, 8.9; N, 3.25.
C32H43NO3 requires C, 78.5; H, 8.85; N, 2.9%.
m) [let(Z),2u-,5p]-(:t)-Methyl7-[2-[[(1,1'-Biphenyl)-4yljmethoxy]-5-(4thiomo rpholinyl)cyclopentyll-4- heptenoate SS-dioxide, from Intermediate 23n. Purification by chromatography using ER as eluant. 55 T.I.c. ER Rf 0.4 I.r. (CHBr3) 1725cm-1 n) [1u-(Z),2ot,501-(:t)-Methyl7-[2-[[(1,1-Biphenyl)-4-yljmethoxy]-5-(4methyl-1 -piperidinyl)cyclopentyll-4- heptenoate, from Intermediate 231. Purification by chromatography using 75:25:1 PE-ER-Et3N as eluant. I.r. 60 (CHBr3) 1730cm-1.
Analysis Found: C32H43NO3 requires C, 783; H, 8.6; N, 3.2.
C, 78.5; H, 8.85; N, 2.9%.
17 GB 2 146 023 A 17 o) [lot(Z),2u.,5p]-( )Methyl7-[2-[[(1,1-Biphenyl)-4-yllmethoxy]-5-(1pyrrolidin y1)cyclopentyll-4-heptenoate, from Intermediate 23o. Purification by chromatography on Et3N deactivated silica using 2:1 ER-E as eluant. I.r. (CHBr3) 1730cm-1 Analysis Found: C, 78.1; H, 8.8; N, 3.4.
C30H39NO3 requires C, 78.05; H, 8.5; N, 3.0%.
p) [1u-(Z),2ct,5p]-( )-Methyl7-[2-[[(1,1-Biphenyl)-4-yllmethoxy-5-(4methyl-l-p iperazinyl)cyclopentyll-4heptenoate, from Intermediate 23m. Purification by chromatography using ER followed by 90:10:1 10 ERmethanol-Et3N as eluant. I.r. (CHBr3) 1725cm-1 Analysis Found: C, 75.6; H, 8.6; N, 5.4.
C311-142N203 requires C,75.9; H, 8.6; N, 5.7%.
EXAMPLE 3 a) [1R-[lct(Z),2a,5p]]-(+)-7-[2-[[(1, 1'1-Biphenyll-4yljmethoxy]-5-(1-piperidiny1)cyclopentyll-4-heptenoic acid, hydrobromide 5N NaOH (0.5mi) was added to the compound of Example la (0.4g) in methanol (2mi) and the mixture was stirred at ambient temperature for 24h. Most of the methanol was removed in vacuo and the residue was 20 adjusted to pH 6 using 5N HCI (0.5mi) and pH 6 phosphate buffer. The mixture was extracted with CH2C12 (3x50mi) and the combined extracts were dried and evaporated. The residue was purified by chromatography using 85:10:5 CH2C12-methanol-Et3N as eluant to give an oil. A solution of the oil in CH2C12 (20mi) was washed with pH 6 phosphate buffer (1 Orni) dried, and evaporated. The residue in CH2C12 (2mi) was treated with an excess of ethereal hydrogen bromide. The resulting solid was washed with ER and dried to give the title compound (0.275 g) m.p. 134-136' [U123.5 = + 69' (CHC13). D Analysis Found: C,663; H, 7.4; N, 2.6.
C30H39NO3.HBr requiresC, 66.4; H, 7-A; N, 2.6%.
b)[1R-[1(x(Z),2oL,5p]]-(+)-7-[2-[[(1, 1'1-Biphenyl)-4-yllmethoxy]-5-(1piperidinyl)cyclopentyll-4heptenoic acid, hydrochloride MethodA 5N NaOH (25mi) was added to the compound of Example la (20.1g) in methanol (130mi) and the mixture 35 was stirred vigorously overnight. The mixture was neutralised with 5N HCI (25mi) and pH 6.5 phosphate buffer (25mi) then concentrated in vacuo.
The solution was extracted with CH2C12 (3x125mi) and the combined organic extracts were dried and evaporated in vacuo to give a foam, which was dissolved in CH2C12 (80mi), treated with excess ethereal HCI (2M, 40mi), and evaporated in vacuo followed by co-evaporation with dry ER (50mi). The oily residue was 40 triturated with dry ER (4x 1 00mi) causing crystallisation. The mixture was filtered and dried in vacuo to afford the title compound (20.47g) m.p. 144-146'.
T.I.c. 17:2A CH2C12 - Ethanol - Et3N Rf 0.18.
[allg = + 79.90 (CHC13) D Method 8 (3-Carboxypropyl)triphenylphosphonium bromide (1.44g) was added to a stirred solution of potassium t-butoxide (0.735g) in dry THF (25mi). After 2h a solution of Intermediate 23b (0.43g) in dry THF (1 Orni) was added and the mixture stirred for 2h at ambient temperature. Water (2m]) was added and the solvents removed in vacuo. The residue in water (100mi) was extracted with ER (2x60mi, discarded), neutralised with 50 conc. HCI and pH 6.5 phosphate buffer and extracted with EA (3x60mi). The EA extracts were dried and evaporated and the residue in CH2C12 (4mi) was treated with an excess of ethereal HCL The solvents were removed in vacuo and the residue was triturated with ER until solid (0. 29g). A portion was crystallised from CH2C12 - IPA to give the title compound m.p. 143-146'.
T.I.c. Identical mixed spot with the product of Method A.
Method C A solution of the compound of Example 6 (0.26g) in ethanoi (1 Orni) and 2N NaOH (5mi) was heated under reflux for 20h. The cooled solution was concentrated in vacuo and extracted with EA (2 x 5mi., discarded).
The aqueous layer was neutralised with 2N HCI (5mi) and pH 6.5 phosphate buffer (1 5mi) and extracted with 60 CH2C12 (2x60m0. The combined organic layers were dried and treated with an excess of ethereal HCL The solvents were removed in vacuo and the residue triturated with ER to give the title compound (0.23g) m.p.
*144-146'.
T.I.c. Identical mixed spot with the product of Method A.
18 GB 2 146 023 A 18 MethodD A stirred suspension of the compound of Example 7 (0.26g) in acetone was treated with Jones reagent (2.67M, 0.5mi) at O'and the mixture was stirred at O'for 2h. Propan-2-ol (3mi) was added at 00 and 0.5h later the mixture was diluted with pH 6.5 phosphate buffer (40mi) and extracted with EA (3x 13mi). The combined 5 extracts were dried and evaporated and the residue was purified by chromatography using 17:2A CH2C12 ethanol - Et3N as eluant. The product in pH 6.5 phosphate buffer (1 Omi) was extracted with CH2C12 (3x 5mi). The combined extracts were washed with 2N HCI (6mi), dried and evaporated and the residue was triturated with ER until solid. The solid was crystallised from CH2C12 - IPA to give the title compound (36mg) m.p. 144.5-146.5'.
T.I.c. Identical mixed spot with the product of Method A.
MethodE A stirred solution of the compound of Example 8 (115mg) in acetone (4m[) at 00 was treated with Jones reagent (0.5M, 1.1 mi) and the mixture was stirred at O'for 1.5h. Propan-2-ol (0.5mi) was added and 1 h later the solution was concentrated in vacuo, diluted with pH 6.5 phosphate buffer and extracted with EA (3x7m1).15 The combined extracts were dried and evaporated and the residue in CH2C12 (3mi) was treated with an excess of ethereal HCL The solvents were removed in vacuo to give a solid (56mg). A portion was crystallised from CH2C12 - IPA to give the title compound m.p. 142-145'. T.I.c. Identical mixed spot with the product of Method A.
MethodF A solution of Intermediate 24 (0.41 g) in 1: 1 methanol - ethanol (20ml) and 5N NaOH (5ml) was heated under reflux for 5.5h. The cooled solution was concentrated in vacuo, diluted with water and acidified with conc. hydrochloric acid. The solution was extracted with CH2CI2 (3x4Oml) and the dried solvents were evaporated. The residue was triturated with ER until solid and the solid was crystal I ised from CH2CI2 -IPA to give the title compound (0.145g) m. p. 142-145'. T.I.c. identical mixed spot with the product of Method A.
Method G A solution of Intermediate 4 (0.375g) and thiocarbonyidiimidazole (0. 315g) in THF (5mi) was stirred at ambient temperature for 17h. Water (4mi) was added, the mixture was stirred for a further 0.5h then concentrated in vacuo. The residue was diluted with water (1 Oml), extracted with CH2C12 (2x 1 Omi) and the combined extracts were dried and evaporated. The residue in toluene (1 Omi) was maintained at 95' under nitrogen whilst a solution of tri-n-butyltin hydride (0.35mi) and A1BN (35mg) in toluene (4m[) was added over 1 Omin. After a further 15min at 100' the solution was cooled, evaporated and the residue in acetonitrile (35mi) was extracted with PE (2x20mi). The extracts were washed with 2N HU (2x15mi) and the aqueous layers were extracted with CH2C12 (2x 15mi). The CH2C12 extracts were washed with pH 6.5 phosphate buffer, dried and evaporated and the residue was purified by chromatography (twice) firstly using 17:2A CHC13 - ethanol - Et3N as eluant and secondly using 25:2A CHC13- ethanol - Et3N as eluant. The product in CH2C12 (8m1) was washed with pH 6.5 phosphate buffer, dried and treated with an excess of ethereal HCL The solvents were removed in vacuo and the residue was triturated with ER until solid. The solid was crystallised from CH2C12- IPAto give the title compound (42mg) m.p. 142-145'.
T.I.c. Identical mixed spot with the product of Method A.
MethodH A mixture of Intermediate 25 (0.269), acetone (5mi) and 2N HCI (4mi) was stirred at ambient temperature for 4h. The mixture was concentrated in vacuo and the residue was diluted with 2N HCI (5m1) and extracted with ER (20ml., discarded). The aqueous layerwas extracted with CH2C12 (6x 1 Orni) and the combined extracts were dried and evaporated. The residue was triturated with ER to give the title compoundas a solid (0.112g).A portion was crystallised from CH2C12- IPA m.p. 141-144'. T.I.c. Identical mixed spot with the product of Method A.
Methodl Intermediate 26 was converted into the title compound following the procedure described for Method H m.p. 140-14C. T.I.c. Identical mixed spot with the product of Method A.
Method,l Intermediate 27 was converted into the title compound following the procedure described for Method H.
m.p. 145-147'. T.I.c. Identical mixed spot with the product of Method A.
EXAMPLE 4 a) [IR-[1a(ZJ,2ot,5p]]-(+)-7-[2-[[4'-Methoxy(1,1'-biphenyl)-4yljmethoxy]-5-( 1-piperidinyl)cyclopentyll-4- heptenoic acid, hydrochloride 19 GB 2 146 023 A 19 A mixture of the compound of Example l c (1.159), methanol (10mi) and 5N NaOH (2ml) was vigorously stirred at ambient temperature for 5h. The mixture was concentrated in vacuo, neutralised with 5N HCI (2mi) and pH 6.5 phosphate buffer (10mi) and extracted with CH2C12 (3x10mi). The combined extracts were dried and evaporated and the residue in CH2C12 (4mi) was treated with an excess of ethereal HCL The solvents were removed in vacuo and the residue was triturated with ER until solid. Recrystallisation from CH2C12- IPA 5 gave the title compound (0.83g) m.p. 127.5-1310.
Analysis Found: C311-141NO4MC1 requires C, 70.4; H, 7.8; N, 2.75.
C, 70.5; H, 8.0; N, 2.65%.
[,Xl22 = + 79.70 (CHC13).
D The following compounds were prepared in a similar manner:
b) [IR-[lot(Z),2a,,5p]]-(+)-7-[2-[[(1,1'-Biphenyl)-4-yllmethoxy]-5-(4morpholi ny1)cyclopentyll-4-heptenoic 15 acid, hydrochloride, m.p. 138-1390 from the compound of Example lb.
Analysis Found:
C29H3,N04.HCI requires [,122 = + 65.5'(CHC13) D C, 69.2; H, 7.7; N, 2.7.
C, 69.65; H, 73; N, 2.8%.
c) [1(x(Z),2a,5P]-(-t)-7-[2-[[(1, 1'1-Biphenyl)-4yljmethoxyj-S-(1piperidinyl)cyclopentyll-4-heptenoic acid, hydrobromide, m.p. 110-1 19'from the compound of Example 2a. Initial purification by chromatography using 17:2A 25 CH2C12-ethanol-Et3Naseiuant.
I.r. (CHBr3) 3480,3300-2400,1720cm-1.
d) [1(x(Z),2a,5p]-( )-7-[2[4-(1, 1-Dimethylethyl)phenylmethoxy]-5-(1piperidinyl)cyclopentyll-4-heptenoic acid, hydrochloride, m.p. 108-1 10'from the compound of Example 2b.
Analysis Found: C2BH43NO3MC1 requires C, 70.2; H, 9.2; N, 2.7.
C, 70.3; H, 9.3; N, 2.9%.
e) [leL(Z),2ot,5p]-( )-7-12-[4-(Phenylmethyl)phenylmethoxyl5-(1piperidinyl)cyc lopentyll-4-heptenoic acid, hydrochloride, m.p. 111-1 12'from the compound of Example 2c. Purification by crystallisation from methanol - EA.
Analysis Found: C, 72.3; H, 8.2; N, 2.6. 40 C311-141NO3MC1 requires C, 723; H, 8.3; N, 2.7%.
f) [I(Y(Z),2u.,5p]-(: )-7-[2-[(4'-Methyl(1,1-biphenyl)-4-yllmethoxy]-5-(1pipe ridinyl)cyclopentyll-4-heptenoic acid, hydrochloride, m.p. 133-134'from the compound of Example 2d. Purification by crystallisation from methanol - EA. 45 Analysis Found: C3,H41NO3.HCI requires C, 72.8; H, 8.2; N, 2.6.
C, 723; H, 8.3; N, 2.7%.
9) [1u-(Z),2(Y.(E),5p]-(-i:)-7-[2-[(3-Phenyl-2-propenyl)oxy]-5-(1piperidinyl)c yclopentyll-4-heptenoic acid, hyd- 50 rochloride, m.p. 123A 25'from the compound of Example 2e.
I.r. (CHBr3) 2700,2250,1720cm-1.
h) [la(Z),2(x,5p]-(:t)7-[2(Phenylmethoxy)-,r-(,-piperidinyl)cyclopentyll4-he ptenoic acid, from the corn- 55 pound of Example 2f.
T.I.c. 25:15:8:2 EA-iPrOH-H20-NH40H Rf 0.3 I.r. (Film) 3200-1900,1710,1600-1550cm-1.
i) [let(Z),2oL,5p]-( )-7-[2-(2-Naphthalenylmethoxy)-5-(1piperidinyl)cyclopentyl l-4-heptenoic acid, hydroch- 60 loride, m.p. 154'from the compound of Example 2g. Purification by crystallisation from CH2CIAPA.
Analysis Found: C28H3,N03.HCI requires C, 70.9; H, 81; N, 2.8.
C, 71.2; H, 8.11; N, 3.0%.
GB 2 146 023 A j) [lu(Z),2p,5a]-(-L)-7-[2-(1-Piperidinyl)-5-[[4-(2thienyl)phenyllmethoxylcycl opentyll-4-heptenoic acid, from the compound of Example 2h. T.I.c. 25:15:8:2 EA-iPrOH-H20-NH40H Rf 0.49 I.r. (CHBr3) 1720,1705,1596cm-1 k) 1'-Biphenyl)-4-yllpropoxy]-5-(1-piperidinyljcyclopentyll-4-heptenoic acid, from the compound of Example 2i. T.I.c. 25:15:8:2 EA-WrOH-H20-NH40H Rf 0.55 I.r. (CHBr3) 3100-2200,1705,1598cm-1.
1) [1(Y.(Z),2a,5p]-(-t)-7-[2-[(5-Phenyl-3-thienyl)methoxy-5-(1piperidinyl)cycl opentyll-4-heptenoic acid, hydrochloride, m.p. 120123'from the compound of Example 2j. I.r. (CHBr3) 3480,1716cm-1.
m) [1R-[1a(Z),2a,5P]]-(+)-9-[2-[[(1,1'Biphenyl)-4-yllmethoxy]-5-(1piperidinyl) cyclopentyll-6-nonenoic acid, 15 hydrochloride, m.p. 99.5-101'from the compound of Example 2k. Purification by crystallisation from CH2C12 - IPA.
Analysis Found:
C321---143NO3MC1 requires [,124 = + 80.80 (CHC13) D C, 72.85; H, 8.2; N, 2.5.
C, 73.05; H, 8.4; N, 2.7%.
n) [IR-[loL(E),2a,5p]]-(+)-7-[2-[[(1,1-Biphenyl)-4-yljmethoxy]-5-(1piperidiny l)cyclopentyll-4-heptenoic 25 acid, hydrochloride, m.p. 103.5107'from the compound of Example 5.
Analysis Found: C30H39NO3 requires [122 + 71.3o (CHC13) D C, 72.1; H, 7.75; N, 2.8.
C, 72.3; H, 8.1; N, 2.8%.
o) [1u-(Z),2a,5p]-(-t)-7-[2-[[(1,1'1-Biphenyl)4-yllmethoxy]-5-(hexahydro1H-az epin-l-yl)cyclopentyll-4heptenoic acid, from the compound of Example 21. T.I.c. 25:15:8:2 EA-WrOH-HA-NH40H Rf 0.36 35 I.r. (CHBr3) 1700,1595cm-1.
p) [la(Z),2(x,5p]-( )-7-[2-[[(1,1'-Biphenyl)-4-yljmethoxyj-5-(4thiomorpholinyl)cyclopentyll-4-heptenoic acid SS-dioxide, hydrochloride, M.P. 110-11 Yfrom the compound of Example 2m.
Analysis Found: C29H3,N05S.HCI requires C, 63.1; H, 6.8; N, 2.4.
C, 63.5; H, 7.0; N, 2.6%.
q) [lu(Z),2u,5p)-(-t)-7-[2-[[(1,1'-Biphenyl)-4-yllmethoxy]-5-(4-methyl-lpiper idinyl)cyclopentyll-4-heptenoic acid, hydrochloride, from the compound of Example 2n. Trituration with PE gave the title compound as an 45 amorphous solid. T.I.c. 25:15:8:2 EA-WrOH-HA-NH40H Rf 0.52 I.r. (CHBr3) 3500-2200,1715 em-'.
r) [1u-(ZJ,2(Y,5p]-(-!:)-7-[2-[[(1, i'-Biphenyl)-4-yljmethoxy]-5-(1pyrrolidinyl)cyclopentyll-4-heptenoic acid, 50 from the compound of Example 2o. T.I.c. 25:15:8:2 EA-iPrOH-H20-NH40H Rf 0.37 I.r. (CHBr3) 2380(br), 1705,1597 cm-1.
s) 1'1-Biphenyl)-4-yllmethoxy]-5-(4-methyl-l-piperazinyl)cyclopentyll-4hepteno ic 55 acid, dihydrochloride, from the compound of Example 2p. Trituration with ER gave the title compoundas a hygroscopic solid. T.I.c. 25:15:8:2 EA-iPrOH-H20-NH40H Rf 0.36 I.r. (CHdr3) 2300 (br), 1715,1595cm.
EXAMPLE 5 [1R-[1(x(E),2(x,5p]]-(+)-Methyl 7-[2-[[(1, 1'1-Biphenyl)-4yllmethoxy]-5-(1-piperidinyl)cyclopentyll-4-heptenoate A solution of the compound of Example la (0.915g) and 4-toluenesulphinic acid (0.38g) in dioxan (100mi) was heated at ref lux temperature under nitrogen for 5h. The cooled solution was diluted with EA (150mi), washed with 8% NaHC03 solution (100m1) then dried and evaporated. The residue was purified by 65 chromatography on silica (300g) impregnated with silver nitrate (30g) using 12:1 followed by 10:1 21 GB 2 146 023 A 21 EA-ethanol as eluant. The product in EA (30mi) was washed with water (25mi), dried and evaporated and the residue was purified by chromatography using 49:49:2 PE-ER-Et3N as eluant to give the title compound as a gum (0.38g). 1r. (CHBr3) 1730cm-1 Analysis Found: C, 78.3; H, 8.6; N, 3. 1. 5 C311-141NO3 requires C, 78.3; H, 83; N, 2.95%.
[0t123 = + 62.70 (CHC13) D EXAMPLE 6 [1R-[1(Y(Z),2ot,5011-(+)-7-[2-[[(1, l-Biphenyl)-4-yllmethoxy]-5-(1- piperidiny1)cyclopentyll-4-heptenamide Isobutylchloroformate (0.9mi) was added to a cooled (-10% stirred solution of the compound of Example 3, hydrochloride (1.01 2g) and Et3N (1.1 mi) in acetonitrile (1 5mi). After 0.5h liquid ammonia (2mi) was added and the mixture was stirred at -10'for 1 h and ambient temperature for 0.5h. The mixture was diluted with 30% NH4C1 sol.ution (50m1) and extracted with EA (3x30mi). The combined extracts were dried and evaporated and the residue was purified by chromatography using 50: 10:1 ER- methanol -Et3N as eluant to give the title compound (0.755g) m.p. 87-90' Analysis Found: C, 77.9; H, 8.9; N, 6. 1.
C3oH4oN202 requires C, 78.2; H, 8.75; N, 6.1 %. 20 121 OLID = + 791 (CHC13) EXAMPLE 7 [1R-[lct(Z),2ot,5P]]-(+)-7-[2-[[(1, 1 -Biphenyl)-4-yllmethoxy]-5-(1- piperidinyl)cyclopentyll-4-hepten- 1-ol, hyd- 25 rochloride The co m pou n d of Exa m p le 1 a (1 g) i n d ry TH F (6m 1) was added si owly at a m bient tem peratu re to a sti rred sol uti on of LiAl H4 (267 m 9) i n d ry TH F (30 m 1) u nd er n itrog en. After 1 h 9:1 TH F - water (1 5m 1) was add ed cautiously then the mixture was filtered and the filtrate evaporated in vacuo The oil in ER (4m]) was treated with an excess of ethereal HCI and the solvents were evaporated in vacuo. The residual gum was triturated 30 with ER to give the title compound (0.915g) m.p. 127-132'.
Analysis Found: C3oH41NO2.HCI requires [,122.5 = + 79'WHC13) D C ' 73.9; H, 8.5; N, 2.9.
C, 74.4; H, 83; N, 2.9%.
EXAMPLE 8 [IR-[1u.(Z),2cy,5p]]-(+)-7-[2-[[(1, l -Biphenyl)-4-yllmethoxy]5-(1-piperidinyl)cyclopentyll-4-heptenal A solution of the compound of Example 7 (0.306g) in CH2Q2 (5mi) was washed with 2N Na2C03 solution (1 Orni). The aqueous layer was extracted with CH2C12 (5mi) and the combined organic layers were dried and evaporated in vacuo to ca. 4mi. Et3N (0.5mi) was added to the solution which was then cooled to (-150). Pyridine-sulphur trioxide complex (0.51 g) in DIVISO (4mi) as added and the mixture was stirred at -1 5'for 1 h then quenched with 30% NI-140 solution (1 5ml). The aqueous layer was extracted with CH2CJ2 (2x 1 Omi) and the combined organic layers were dried and evaporated. The residue was purified by chromatography using 45 60:40:1 then 50:50:1 PE-ER-Et3N as eluant to give the title compound as an oil (0.164g). I.r. (CHBr3) 2730, 1720cm-1.
Analysis Found: C, 80.9; H, 9.0; N, 3. 1.
C30H39NO2 requires C, 80.9; H, 8.8; N, 3.1 %. 50 [(X12 = + 80' (CHC13) D EXAMPLE 9 [1R-[1a.(Z),2ot,5p]]-(+)-7-[2-[[(1,1-Biphenyl)-4-yllmethoxy]-5-[1piperidin y1)cyclopentyll-4-heptenoic acid, 55 hydrochloride Lindlar catalyst (5% I'd on CaC03 poisoned with lead; 60rng) in EA (4m]) was pre-saturated with hydrogen for 0.5h. Intermediate 28 MOrng) in EA (4m]) was added and stirring continued at ambient temperature under hydrogen for 2h. The presence of the title compound in the reaction mixture was demonstrated by t.l.c. (Si02 impregnated with AgN03) using 8:1 EA-AcOH. 0.17; Identical mixed spot with the product of Example 3b) 60 Method A.
The term "active ingredient" as used below refers to a compound of the invention and may be for example a compound according to one of the previous examples, such as [1 R-[1o(Z),2u-,5p]]-(+)-7-[2-[[(1,1'-biphenyi)4-yilmethoxy]-5-(1-piperidinyi)cyclopentyll-4-heptenoic acid.
22 GB 2 146 023 A 22 Pharmaceutical Examples Tablets These may be prepared by direct compression or wet granulation. The direct compression method is preferred but may not be suitable in all cases as it is dependent upon the dose level and physical 5 characteristics of the active ingredient.
Direct Compression Active Ingredient Microcrystalline Cellulose B.P.C. Magnesium Stearate Compression Weight mg/tablet 100.00 298.00 2.00 400.00mg The active ingredient is sieved through a 250m -6 sieve, blended with the excipients and compressed using 15 10.Omm punches. Tablets of other strengths may be prepared by altering the compression weight and using punches to suit.
B. Wet Granulation rng/tablet Active Ingredient 100.00 20 Lactose B.P. 238.00 Starch BY. 40.00 Pregelatinised Maize Starch BY. 20.00 Magnesium Stearate BY. 2.00 Compressed Weight 400.00mg 25 The active ingredient is sieved through a 250m -6 sieve and blended with the lactose, starch and pre-gelatinised starch. The mixed powders are moistened with purified water, granules are made, dried, screened and blended with the magnesium stereate. The lubricated granules are compressed into tablets as 30 described for the direct compression formula.
The tablets may be film coated with suitable film forming materials, e.g. methyl cellulose or hydroxylpropyi methyl cellulose using standard techniques. Alternatively the tablets may be sugar coated.
Capsules mg/capsule 35 Active Ingredient 100.00 STA-RX 1500 99.00 Magnesium Stearate B.P. 1.00 Fill Weight 200.00mg 40 A form of directly compressible starch supplied by Colorcorn Ltd., Orpington, Kent.
The active ingredient is sieved through a 250m-6 sieve and blended with the other materials. The mix is 45 filled into No. 2 hard gelatin capsules using a suitable filling machine. Other doses may be prepared by altering the fill weight and if necessary changing the capsule size to suit.
Inhalation cartridges rnglcartridge Active Ingredient (micronised) 3.00 50 Lactose BY. to 25.00 The active ingredient is micronised in a fluid energy mill to a fine particle size range prior to blending with normal tabletting grade lactose in a high energy mixer. The powder blend is filled into No. 3 hard gelatin capsules on a suitable encapsulating machine.
The contents of the cartridge are administered 23 GB 2 146 023 A 23 MetredDose Pressurised Aerosol rng/metered dose PerCan Active Ingredient (micronised) 0.500 120rng 5 Oleic Acid B.P. 0.050 12mg Trichlorofluoromethane B. P. 22.25 5.34g 10 D i eh 1 o ro cl iff u o ro m eth a n e 13.P. 60.90 14.62g The active ingredient is micronised in a fluid energy mill to a fine particle size range. The oleic acid is mixed with the trichlorofluoromethane at a temperature of 10-15'C and the micronised drug is mixed into this solution with a high shear mixer. The suspension is metered into aluminium aerosol cans and suitable metering valves, delivering a metered dose of 85mg of suspension, are crimped onto the cans and the dichlorodifluoromethane is pressure filled into the cans through the valves.
Syrup mg/5mi dose Active Ingredient 100.00 Buffer 25 1 Flavour Colour Preservative Thickening Agent as required Sweetening Agent Purified Water to 5.00mi The active ingredient, buffer, flavour, colour, preservative, thickening agent and sweetening agent ae dissolved in some of the water, the solution is adjusted to volume and mixed. The syrup produced is clarified 40 by f i Itrati o n.
Injection for Intravenous Administration Active Ingredient 50rng 45 Waterfor injections B.P. to 5mi Sodium chloride orany othersuitable material may be added to adjust the tonicity of the solution and the pH maybe adjusted to that of maximum stability of the active ingredient using dilute acid or alkali or by the 50 addition of suitable buffer salts. The solution is prepared, clarifed and filled into appropriate sized ampoules sealed by fusion of the glass. The injection is sterilised by heating in an autoclave using one of the acceptable cycles. Alternatively the solution may be sterilised by filtration and filled into sterile ampoules under aseptic conditions. The solution may be packed under an inert atmosphere of nitrogen.
24 GB 2 146 023 A 24 Suspensions mg/5mi dose Active i ng redient 100.00 Aluminium monostearate 75.00 5 Sweetening agent) Flavour as required 10 Colour Fractionated coconut oil to 5.00m] The aluminium monostearate is dispensed in about 90% of the fractionated coconut oil. The resulting 15 suspension is heated to 11 YC while stirring and then cooled. The sweetening agent, flavour and colour are added and the active ingredient is suitably dispersed. The suspension is made up to volume with the remaining fractionated coconut oil and mixed.
Claims (21)
1. Compounds of the general formulae (1a) and (1b) OR2 OR2 1 1 25 1,.,e(CH2)2XWCOORI 1,.,02)2XWZ (W v v (1 b) 30 wherein R' is a hydrogen atom, ora Cl-6 alkyl orC7-10 aralkyi group; 35 W is straight or branched Cl-7 alkylene; Xis cis ortrans -CH=CH-; Y is a saturated heterocyclic amino group (attached to the cyclopentane ring via the nitrogen atom) which has 5-8 ring members and (a) optionally contains in the ring -0-, -S-, -S02-, or NR 3 (where R 3 is a hydrogen atom, Cl-7 alkyl oraralkyl having a Cl-4 alkyl portion); and/or (b) is optionally substituted by one 40 or more Cl-4alkyl groups; R 2 is (1) straight or branched Cl-5 alkyl substituted by (a) phenyl [optionally substituted by Cl-6 alky], C5-7 cycloalkyl, phenylalkyl having a Cl-3 alkyl portion, thienyl, phenyl (optionally substituted by Cl-4 alkyl, Cl-4 alkoxy, or phenyl)], (b) thienyl [optionally substituted by C5-7 cycloalkyl or phenyl (optionally substituted by Cl-3 alkyl, Cl-3 alkoxy or halogen)], or (c) naphthyl (optionally substituted by Cl -4 alkyl or Cl-4 alkoxy) or (H) 45 cinnamyl; and Z is -CH20H, -CHO or -CONHR 4 where R 4 is a hydrogen atom or a methyl group; and the physiologically acceptable salts and solvates thereof.
2. Compounds as claimed in claim 1 of the formula (1a).
3. Compounds as claimed in claim 1 or2 in which Y is pyrrolidino, piperidino, hexamethyleneimino or 50 4-methylpiperidino.
4. Compounds as claimed in claim 1 or2 in which Yis piperidino.
5. Compounds as claimed in any preceding claim in which Xis cis -CH=CH-.
6. Compounds as claimed in any preceding claim in which Xis cis -CH=CHand W is -(CH2)2- or -(CH2)4_.
7. Compounds as claimed in any preceding claim in which R' isa hydrogen atom ora methyl group. 55
8. Compounds as claimed in any preceding claim in which R' is a hydrogen atom.
9. Compounds as claimed in claim 2 in which:
R' is a hydrogen atom or a methyl group, W is -(CHA2-, Xiscis-CH=CH-,and Y is piperidino, and their physiologically acceptable salts and solvates.
10. Compounds as claimed in any preceding claim in which R 2 is (i) Cl-5 alkyl substituted by (a) phenyl or phenyl substituted by phenyl (Cl-3)aiky], thienyl, phenyl, Cl-4 alkylphenyl or Cl-4 alkoxyphenyl, (b) thienyl or phenylthienyl or (c) naphthyl, or (ii) cinnamyi.
GB 2 146 023 A 25
11. Compounds as claimed in claim 9 or claim 10 in which R 2 is (i) methyl, ethyl, or propyl substituted by phenyl (itself substituted by benzyi, thienyl, phenyl, methylphenyl or methoxyphenyl), phenylthienyl or naphthyl, or (ii) cinnamyi.
12. Compounds as claimed in claim 9 in which R 2 is benzyi substituted by phenyl, methylphenyl or methoxyphenyl.
13. Compounds as claimed in any preceding claim in the form of their 1 Risomers.
14. Compounds as claimed in claim 2, said compounds being: [lot(Z),2et, 5p]-( )-7-[2-[[4'-methoxy(1,1'-biphenyi)-4-yilmethoxy]-5-(1-pipe ridinyi)cyclopentyll-4-heptenoic acid, or its 1 R isomer; [ 1 oL(Z),2et,5 p]-( )-7-[2-[4-(ph enyl methyl) phenyl m eth oxy]-5-(1 - pi perid i nyl)cyclo pentyll-4-1h epteno ic acid, or 10 its 1 R isomer; [ 1 oL(Z),2u,5p] -( )-7-[2-[ [4'-m ethyl (1, V-1bi ph enyi)-4-yll methoxy]-5-(1 -pi perid i nyi)cycl opentyl 1-4-hepten oic acid, or its 1 R isomer; [1 ot(Z),2p,5a.]-( )-7-[2-(1 -piperidinyi)-5-[(4-thien-2yl)phenyimethoxyI cyclopentyll-4-heptenoic acid, or its 1 R isomer; [1 u,(Z),2a,5P]-( )-7-[2-[3-[(1,1'-biphenyl)-4-yilpropoxy]-5-(1 piperidinyi)cyclopentyll-4-heptenoic acid, or its 1 R isomer; and their physiologically acceptable salts and solvates.
15. Compounds as claimed in claim 2, said compounds being [19-,(Z),2ot, 5p]-( )-7-[2-[[(1,1'-biphenyi)-4yilmethoxyll-5-(1-piperidinyi)cyclopentyll-4-heptenoic acid and its physiologically acceptable salts and 20 solvates.
16. Compounds as claimed in claim 2, said compounds being [1R-[1(x(Z),2e,, 5p]]-(+)-7-[2-[[(1,1'biphenyl)-4-yilmethoxy]1-5-(1-piperidinyl)cyclopentyll-4-heptenoic acid and its physiologically acceptable salts and solvates.
17. The hydrochloride salts of the compounds of claims 15 and 16.
18. A pharmaceutical composition comprising a compound as claimed in any preceding claim together with one or more pharmaceutical carriers.
19. A process for the preparation of a compound as claimed in claim 1 which comprises:
(a) in the preparation of a compound of formula (1a), reacting a compound of formula (2) qR2 30 1 35 (2) 40 with a phosphorane of the formula R5p = CHWCOOR' (where R5 is Cl-6 alkyl or phenyl) or a salt thereof; 3 (b) in the preparation of a compound of formula (1a) in which R' is a hydrogen atom, hydrolysing a corresponding ester, amide or nitrile; (c) in the preparation of a compound of formula (1a) in which R' is C1-6 alkyl orC7-10 phenalkyl, esterifying the corresponding carboxylic acid; (d) in the preparation of a compound of formula (1a) dehydroxylating a corresponding alcohol of formula (9) OR2 50 ,(CH2)2XWCOOR1 HO A Y (9) 55 60 or a thioester thereof; (e) in the preparation of a compound of formula (1a), reducing the corresponding compound in which X is an acetylene group; (f) in the preparation of compounds of formula (1a) in which X is trans - CH=CH-, isomerising the corresponding cis compound; 26 GB 2 146 023 A 26 (9) in the preparation of compounds of formula (1a) in which R' isa hydrogen atom, oxidising a corresponding compound of formula (1 b) in which Z is -CH20H or -CHO; (h) in the preparation of a compound of formula (1b) in which Z is - CH2011, reducing the corresponding compound of formula (1 a) in which R' is a methyl group; (i) in the preparation of a compound of formula (1b) in which Z is -CHO, oxidising the corresponding 5 compound in which Z is -CH20F1; (j) in the preparation of a compound of formula (1b) in which Z is -CONHR 4, amidating the corresponding compound of formula (1a) in which R' is a hydrogen atom; or (k) in the preparation of a salt, treating a compound of formula (1a) or (1b) with an acid ora base or converting one salt of a compound of formula (1a) or (1b) into another.
20. A compound as claimed in claim 1, said compound being the title product of any of the Examples herein.
21. A pharmaceutical composition as claimed in claim 18, substantially as described herein in any of the pharmaceutical examples.
Printed in the UK for HMSO, D8818935, 2185, 7102.
Published by The Patent Office, 25 Southampton Buildings, London, WC2A lAY, from which copies may be obtained.
Applications Claiming Priority (2)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| GB838323830A GB8323830D0 (en) | 1983-09-06 | 1983-09-06 | Carbocyclic compounds |
| GB848414676A GB8414676D0 (en) | 1984-06-08 | 1984-06-08 | Carbocyclic compounds |
Publications (3)
| Publication Number | Publication Date |
|---|---|
| GB8422453D0 GB8422453D0 (en) | 1984-10-10 |
| GB2146023A true GB2146023A (en) | 1985-04-11 |
| GB2146023B GB2146023B (en) | 1987-03-25 |
Family
ID=26286823
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| GB08422453A Expired GB2146023B (en) | 1983-09-06 | 1984-09-05 | Aminocyclopentanes and their preparation and pharmaceutical formulation |
Country Status (21)
| Country | Link |
|---|---|
| US (1) | US4613597A (en) |
| KR (1) | KR850002476A (en) |
| AU (1) | AU574711B2 (en) |
| BE (1) | BE900502A (en) |
| CA (1) | CA1234811A (en) |
| CH (1) | CH662350A5 (en) |
| DE (1) | DE3432658A1 (en) |
| DK (1) | DK422984A (en) |
| ES (1) | ES8600241A1 (en) |
| FI (1) | FI843469A (en) |
| FR (1) | FR2551440B1 (en) |
| GB (1) | GB2146023B (en) |
| GR (1) | GR80294B (en) |
| IL (1) | IL72862A (en) |
| IT (1) | IT1177981B (en) |
| LU (1) | LU85528A1 (en) |
| NL (1) | NL8402713A (en) |
| NO (1) | NO843529L (en) |
| NZ (1) | NZ209447A (en) |
| PT (1) | PT79175B (en) |
| SE (1) | SE8404456L (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| GB2165235A (en) * | 1984-09-05 | 1986-04-09 | Glaxo Group Ltd | Carbocyclic compounds |
| GB2165535A (en) * | 1984-09-05 | 1986-04-16 | Glaxo Group Ltd | Carbocyclic compounds |
Families Citing this family (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CH667646A5 (en) * | 1984-05-18 | 1988-10-31 | Glaxo Group Ltd | AMINOCYCLOPENTYL ETHER, THEIR PRODUCTION AND PHARMACEUTICAL FORMULATION. |
| GB8625326D0 (en) * | 1986-10-22 | 1986-11-26 | Glaxo Group Ltd | Medicaments |
| US5039673A (en) * | 1987-06-22 | 1991-08-13 | Glaxo Group Limited | Aminocyclopentyl ethers and their preparation and pharmaceutical formulation |
Citations (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| GB2028805A (en) * | 1978-07-11 | 1980-03-12 | Glaxo Group Ltd | Prostanoid compounds |
| GB2075503A (en) * | 1980-04-30 | 1981-11-18 | Glaxo Group Ltd | Prostanoid aminocyclopentane alkenoic acids and esters and their preparation and pharmaceutical formulation |
| GB2097397A (en) * | 1981-04-29 | 1982-11-03 | Glaxo Group Ltd | Aminocyclopentanol acids and esters as prostaglandin analogues and their preparation and pharmaceutical formulation |
Family Cites Families (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| ES482357A1 (en) * | 1978-07-11 | 1980-08-16 | Glaxo Group Ltd | Prostanoid compounds and compositions |
| GB2079281B (en) * | 1980-07-04 | 1984-04-18 | Glaxo Group Ltd | Aminocyclopentanone amides and their preparation and pharmaceutical formulation |
| IL67041A (en) * | 1981-10-29 | 1988-03-31 | Glaxo Group Ltd | 2-aminocyclopentane alkanoic and alkenoic acid esters,process for their preparation and pharmaceutical compositions containing them |
-
1984
- 1984-09-05 KR KR1019840005434A patent/KR850002476A/en not_active Application Discontinuation
- 1984-09-05 IT IT48800/84A patent/IT1177981B/en active
- 1984-09-05 NO NO843529A patent/NO843529L/en unknown
- 1984-09-05 NZ NZ209447A patent/NZ209447A/en unknown
- 1984-09-05 GB GB08422453A patent/GB2146023B/en not_active Expired
- 1984-09-05 AU AU32753/84A patent/AU574711B2/en not_active Ceased
- 1984-09-05 DK DK422984A patent/DK422984A/en not_active Application Discontinuation
- 1984-09-05 IL IL72862A patent/IL72862A/en unknown
- 1984-09-05 SE SE8404456A patent/SE8404456L/en not_active Application Discontinuation
- 1984-09-05 US US06/647,537 patent/US4613597A/en not_active Expired - Fee Related
- 1984-09-05 NL NL8402713A patent/NL8402713A/en not_active Application Discontinuation
- 1984-09-05 PT PT79175A patent/PT79175B/en unknown
- 1984-09-05 CH CH4237/84A patent/CH662350A5/en not_active IP Right Cessation
- 1984-09-05 DE DE19843432658 patent/DE3432658A1/en not_active Withdrawn
- 1984-09-05 GR GR80294A patent/GR80294B/en unknown
- 1984-09-05 FI FI843469A patent/FI843469A/en not_active Application Discontinuation
- 1984-09-05 BE BE0/213592A patent/BE900502A/en not_active IP Right Cessation
- 1984-09-05 CA CA000462455A patent/CA1234811A/en not_active Expired
- 1984-09-05 LU LU85528A patent/LU85528A1/en unknown
- 1984-09-05 ES ES535674A patent/ES8600241A1/en not_active Expired
- 1984-09-06 FR FR8413706A patent/FR2551440B1/en not_active Expired
Patent Citations (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| GB2028805A (en) * | 1978-07-11 | 1980-03-12 | Glaxo Group Ltd | Prostanoid compounds |
| GB2075503A (en) * | 1980-04-30 | 1981-11-18 | Glaxo Group Ltd | Prostanoid aminocyclopentane alkenoic acids and esters and their preparation and pharmaceutical formulation |
| GB2097397A (en) * | 1981-04-29 | 1982-11-03 | Glaxo Group Ltd | Aminocyclopentanol acids and esters as prostaglandin analogues and their preparation and pharmaceutical formulation |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| GB2165235A (en) * | 1984-09-05 | 1986-04-09 | Glaxo Group Ltd | Carbocyclic compounds |
| GB2165535A (en) * | 1984-09-05 | 1986-04-16 | Glaxo Group Ltd | Carbocyclic compounds |
Also Published As
| Publication number | Publication date |
|---|---|
| SE8404456L (en) | 1985-03-07 |
| NZ209447A (en) | 1988-07-28 |
| PT79175B (en) | 1986-11-10 |
| GB8422453D0 (en) | 1984-10-10 |
| KR850002476A (en) | 1985-05-13 |
| IT8448800A1 (en) | 1986-03-05 |
| DE3432658A1 (en) | 1985-03-21 |
| FI843469A (en) | 1985-03-07 |
| CA1234811A (en) | 1988-04-05 |
| GB2146023B (en) | 1987-03-25 |
| FI843469A0 (en) | 1984-09-05 |
| IL72862A (en) | 1988-07-31 |
| AU574711B2 (en) | 1988-07-14 |
| FR2551440B1 (en) | 1986-12-26 |
| DK422984A (en) | 1985-03-07 |
| IT1177981B (en) | 1987-09-03 |
| NO843529L (en) | 1985-03-07 |
| AU3275384A (en) | 1985-03-14 |
| NL8402713A (en) | 1985-04-01 |
| SE8404456D0 (en) | 1984-09-05 |
| ES535674A0 (en) | 1985-10-01 |
| IL72862A0 (en) | 1984-12-31 |
| ES8600241A1 (en) | 1985-10-01 |
| DK422984D0 (en) | 1984-09-05 |
| FR2551440A1 (en) | 1985-03-08 |
| IT8448800A0 (en) | 1984-09-05 |
| GR80294B (en) | 1985-01-07 |
| PT79175A (en) | 1984-10-01 |
| CH662350A5 (en) | 1987-09-30 |
| BE900502A (en) | 1985-03-05 |
| US4613597A (en) | 1986-09-23 |
| LU85528A1 (en) | 1985-04-29 |
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Legal Events
| Date | Code | Title | Description |
|---|---|---|---|
| PCNP | Patent ceased through non-payment of renewal fee |