WO1994012493A1 - 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals - Google Patents

2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals Download PDF

Info

Publication number
WO1994012493A1
WO1994012493A1 PCT/EP1992/002719 EP9202719W WO9412493A1 WO 1994012493 A1 WO1994012493 A1 WO 1994012493A1 EP 9202719 W EP9202719 W EP 9202719W WO 9412493 A1 WO9412493 A1 WO 9412493A1
Authority
WO
WIPO (PCT)
Prior art keywords
benzopyran
oxide
hydrogen
formula
group
Prior art date
Application number
PCT/EP1992/002719
Other languages
French (fr)
Inventor
Paul W. Manley
Original Assignee
Sandoz, Ltd.
Sandoz-Patent-Gmbh
Sandoz-Erfindungen Verwaltungsgesellschaft Mbh
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Priority to AU30826/92A priority Critical patent/AU665040B2/en
Priority to EP92924604A priority patent/EP0623129A1/en
Priority to CA002122494A priority patent/CA2122494A1/en
Priority to RU94035761A priority patent/RU2104277C1/en
Priority to PL92304013A priority patent/PL172371B1/en
Priority to SK889-94A priority patent/SK88994A3/en
Application filed by Sandoz, Ltd., Sandoz-Patent-Gmbh, Sandoz-Erfindungen Verwaltungsgesellschaft Mbh filed Critical Sandoz, Ltd.
Priority to PCT/EP1992/002719 priority patent/WO1994012493A1/en
Priority claimed from CA002122494A external-priority patent/CA2122494A1/en
Priority to TW081109738A priority patent/TW223636B/zh
Publication of WO1994012493A1 publication Critical patent/WO1994012493A1/en
Priority to FI943489A priority patent/FI943489A/en
Priority to NO942744A priority patent/NO942744L/en

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D405/00Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom
    • C07D405/14Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom containing three or more hetero rings

Definitions

  • the present invention relates to novel 2,2-dial yl- and 2, 2-dialkyl-3, 4-dihydro-3-hydroxy- -2H-l-benzopyrans and salts, esters and N-oxides thereof and to processes for their production, as well as to their use as pharmaceuticals and pharmaceutical compositions comprising them.
  • Alkyl groups and moieties of compounds as defined under 1. above may be branched or straight chain. Preferred significances for substituents at the 2-position of the benzopyran nucleus as well as at the 2 and/or 3 position of the pyridinyl group are as set forth below in relation to formula I for R 6 and R 7 , and R and R .
  • compounds of the present invention e.g. as defined under 1 above, have potassium (K + ) channel opening activity [see e.g. Cook et al., "Potassium Channels: Structure, Classification, Function and Therapeutic Potential", ed. N.S.Cook, Ellis Horwood, Chichester (1990), p.p. 181-255].
  • Benzopyran derivatives which are carboxamido-substituted at the 4-position, having K + -channel opening activity are extensively described in the art and comprise a substantial and recognisable compound class.
  • the 4-carboxamido moiety in the compounds of the invention may comprise any of those known and described in the art in relation to K + -channel opening benzopyrans, including N-substituted, for example cyclic, carboxamido moieties.
  • Preferred carboxamido moieties in relation to the compounds of the invention are those of the formula -N(R 9 )-CORio as defined below.
  • benzopyran nucleus of compounds defined under 1 may bear substituents in addition to those specifically defined.
  • they may, for example, be 7-C ⁇ '_ 5 alkyl substituted, especially 7-methyl substituted, e.g. as hereinafter indicated in relation to formula I.
  • Ri and R 2 are independently, hydrogen, C ⁇ _salkyl,
  • Ci_ 5 alkoxyalkyl
  • R 3 is a group of formula -N(R 9 )-C ⁇ R ⁇ o wherein R 9 is hydrogen and R ⁇ 0 is pyridyl or R 9 and Rio together are 1,3-butadienylene or represent a group of formula -(CH 2 ) n - or -(CH 2 ) m — - in which n is an integer of from 3 to 5 ⁇ inclusive and m is 1 or 2,
  • R 4 is hydrogen and R 5 is hydroxy in the trans position with respect to R 3 , or
  • R 4 and R 5 together represent an additional bond as indicated by the dotted line
  • R_ and R are, independently, C ⁇ _salkyl
  • R 8 is hydrogen or C ⁇ _salkyl, or N-oxide thereof; or physiologically-hydrolysable and -acceptable ester of such a compound or N-oxide, or acid addition or quarternary ammonium salt of such a compound, N-oxide or ester.
  • Alkyl groups as Ri , R 2 , R 6 , R 7 and R 8 , as well as alkyl moieties of hydroxyalkyl and alkoxyalkyl groups as R and R 2 may be branched or straight chain.
  • Alkoxyalkyl groups are preferably (Ci_ 4 alkoxy) -methyl, in particular methoxymethyl.
  • Preferred hydroxyalkyl groups are hydroxymethyl.
  • R 6 and R 7 are both preferably methyl.
  • R 8 is preferably hydrogen or methyl, most preferably hydrogen.
  • R x has any of the meanings given above in relation to formula I and R 2 is hydrogen or C ⁇ _ 5 alkyl (especially methyl), preferably hydrogen.
  • R 9 is hydrogen and Rio is pyridyl (especially 3-pyridyl) or R 9 and Rio together are 1, 3-butadienylene, trimethylene or tetramethylene. Most preferably R 9 and Rio together are tetramethylene.
  • R 4 is hydrogen and R 5 is hydroxy.
  • Benzopyrans of the invention for example compounds of formula I, form N-oxides, e.g. at the nitrogen atom of the 6-pyridinyl group. Such N-oxides have comparable activity (as hereinafter described) and tolerability to the parent compounds and also form part of the present invention.
  • physiologically-hydrolysable and -acceptable ester as used herein is meant an ester in which a hydroxy group (e.g., in relation to formula I, hydroxy groups R 5 and/or the hydroxy moiety of any hydroxyalkyl group present as Ri and/or R 2 ) is esterified and which is hydrolysable under physiological conditions to yield an acid which is itself physiologically tolerable at doses to be administered.
  • esters are pro-drug forms of conventional type and have comparable activity and tolerability to the parent compounds. Examples of such esters include, e.g. acetates.
  • Acid addition salts e.g. of compounds of formula I, their N-oxides and defined esters thereof, include salts with both inorganic and organic acids. Such salts also have comparable activity to the free compounds, N-oxides and esters.
  • Pharmaceutically acceptable acid addition salts for pharmaceutical use in accordance with the present invention as hereinafter described include e.g. hydrochloric, sulphuric and fumaric acid salts.
  • Quarternary ammonium salts e.g. of compounds of formula I, their N-oxides and defined esters thereof, include e.g. salts with organo-halides, e.g. alkyl halides.
  • Pharmaceutically acceptable quarternary ammonium salts for pharmaceutical use in accordance with the present invention include e.g. such salts with methyl iodide.
  • ester forms as aforesaid are generally less preferred.
  • the present invention also provides:
  • Ri , R 2 , R 6 , R 7 and R 8 have the meanings for formula I above, with an alkali metal salt of a carboxamide, for example a compound of formula III
  • R 9 and Rio have the meanings given for formula I above and M + is a lithium, sodium or potassium ion; or ) acylating and, when required, alkylating the amino group of a 2,2-di (C ⁇ _ 5 alkyl)- or trans-2, 2-di (Ci_ 5 alkyl) - -3, 4-dihydro-3-hydroxy- -4-amino-6- (pyridin-4-yl) - 2H-l-benzopyran wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two members selected from the group comprising C ⁇ _ 5 alkyl, Ci_ 5 hydroxyalkyl and Ci_ 5 (alkoxyalkyl) , for example, reacting a compound of formula IV
  • R'i 0 is pyridyl and X 1 and X 2 are leaving groups
  • Process step i 1 ) above may be carried out in accordance with methods known in the art, for example by reaction at ambient temperatures to reflux in the presence of an inert solvent or diluent such as tetrahydrofuran or dimethylsulfoxide.
  • an inert solvent or diluent such as tetrahydrofuran or dimethylsulfoxide.
  • the required alkali metal salt e.g. compound of formula III
  • the required alkali metal salt e.g. compound of formula III
  • the required alkali metal salt e.g. compound of formula III
  • the required alkali metal salt e.g. compound of formula III
  • the required alkali metal salt e.g. compound of formula III
  • the required alkali metal salt e.g. compound of formula III
  • benzopyrans and dihydro-benzopyrans of the invention may be obtained, e.g. as illustrated in Examples 11 and 12 hereinafter.
  • Use of lithium salts leads primarily or exclusively to
  • Process step i 2 may also be carried out in accordance with methods known in the art.
  • Suitable leaving groups X 1 are halogen and activated ester groups and suitable leaving groups X 2 are halogen.
  • Reaction is suitably carried out at temperatures of from 0° to 100°C in an inert solvent or diluent such as acetonitrile or dichloromethane, preferably in the presence of an acid binding agent, e.g. trialkylamine or alkali metal carbonate.
  • an acid binding agent e.g. trialkylamine or alkali metal carbonate.
  • Process step ii) may be carried out in accordance with conventional acylation/N-oxidation procedures, e.g. for the obtention of N-oxides by treatment with hydrogen peroxide, m-chloroperbenzoic acid or Collin's reagent (Cr0 3 .Py 2 ) as hereinafter illustrated in Example 23.
  • free bases may be converted into acid addition or quarternary ammonium salts by reaction with acids or e.g. alkyl, for example methyl, halides, and vice versa.
  • racemates of the formula II and formula IV compounds 4-carboxamido-3, 4-dihydro-3-hydroxy- -benzopyrans obtained will be in the form of the trans-racemate [i.e. comprising the (3S,4R) plus (3R, S) isomers) .
  • Obtained racemates may be separated to provide the individual (3R, 4S) or (preferred) (3S,4R) enantiomer, e.g. chromatographically using a chiral stationary phase.
  • 3S,4R) enantiomers are desired, however, this is preferably achieved using the corresponding isomer as starting material, i.e. in relation to formula II, the 3S,4S-antipode and, in relation to formula IV, the 3S,4R-antipode.
  • Process steps (iii) through (vi) may be carried out by conventional means, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.A.4, A.5, A.5'a, and A.5'b.
  • Starting materials of formula IV may be prepared from the corresponding compounds of formula II by reaction with ammonia, e.g. in accordance with the general procedures hereinafter illustrated in Example 24.A.6' . Proceeding via steps (iii) and (iv) , the formula II compound is obtained as the cis-racemate, i.e. comprising the (3R, 4R) and (3S,4S) antipodes. Step v involves introduction of an appropriate chiral acyl group [in sequence A, by way of example, (R)- ⁇ - -methoxyphenylacetyl] .
  • the chiral racemate VIII may readily be separated by column chromatography or fractional recrystallisation into its individual (3R,4S) and (3S,4R) antipodes.
  • compound II starting materials may be obtained in pure or substantially pure (3S,4S) enantiomeric form.
  • Steps (vii) to (ix) may be carried out by conventional means, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.A.2 and A.3, steps (viii) and (ix) being carried out in Example 24.A.3 without purification of the intermediate.
  • step (vii) is suitably carried out in an aprotic solvent such as acetone, in the presence of a base such as K 2 C0 3 and a catalyst such as KI.
  • Process steps (x) and (xi), and (xii) through (xiv), may be carried out by conventional means, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.A.la and b and 24.A.la' and b' respectively. In general, procedure via steps (x) and (xi) will be preferred for larger scale synthesis.
  • the mixture is stirred for 2 hours at room temperature after which the mixture is treated with aqueous Na 2 C0 3 (100ml/2M) and extracted with 3:1 CH 2 C1 2 /CH 3 0H (3x100ml) .
  • the combined extracts are washed with brine, dried (Na 2 S0 ) , filtered and the solvent evaporated off under reduced pressure to yield an oil.
  • the oil is purified by chromatography (silica gel, 2% C 2 H 5 0H in CH 2 C1 2 ) and recrystallised from C 2 HsOH-diethyl ether to give the title compound in enantiomerically pure or substantially pure form, m.p. 247-248°C, [o] D 20 - +19.8 (c-0.965, C 2 H 5 0H) .
  • Ethyl chloroformate (10.85 g) is added to a stirred mixture of 2-picoline (9.30 g) and copper (I) iodide (0.77 g) in dry tetrahydrofuran (150 ml), at -20°C under argon. The whole is stirred for 3 hours at -20°C and then treated dropwise with a solution of 4-methoxyphenyl magnesium bromide, prepared from 4-bromoanisole (18.7 g) and Mg turnings (2.64 g) in dry tetra ⁇ hydrofuran (100 ml) at such a rate that the temperature remains between -15° and -20°C.
  • step A.l.a (16.9 g) and sulphur (2.0 g) in decahydronaphthalene (100 ml) is stirred at 200°C for 3 hours.
  • the solvent is evaporated off under reduced pressure and the residue dissolved in ethyl acetate (500 ml) and extracted with HCl (3 x 200 ml of 2M) .
  • the combined extracts were washed with ethyl acetate (2 x 100 ml), basified with ice-cooling to pH 11 with NaOH and extracted with CH 2 C1 2 (3 x 200 ml) .
  • the combined extracts are dried (Na 2 S0 4 ), filtered and the solvent evaporated off under reduced pressure to yield the crude product.
  • the title compound may alternatively be produced via the following route:
  • 2-Methylpyridine (111.7g) is added to a freshly prepared solution of hydroxylamine-O-sulphonic acid (45.2 g, 90%) in H 2 0 (260 ml) at 0°C.
  • the mixture is heated to 95°C, stirred for a further 45 min, cooled to 10°C and cautiously treated with K 2 C0 3 (55 g) .
  • the mixture is washed with diethyl ether (2 x 100 ml) and the water evaporated off at 40°C under reduced pressure.
  • the residue is treated with C 2 H 5 0H (600 ml) and the K 2 S0 precipitate removed by filtration.
  • the filtrate is treated with HCl (120 ml of 18M) and evaporated to dryness at 50°C under reduced pressure to give a residue which is treated with dehydroacetic acid (68.6g) and HCl (150 ml of 18M) and heated under reflux for 90 min.
  • the solution is evaporated to dryness at 50° under reduced pressure and the residue stirred for 15 min with C 2 H 5 0H (200 ml), filtered and the precipitate washed with C 2 H 5 0H (200 ml) .
  • the combined filtrate and washings are treated with tetrafluoroboric acid in ethyl ether (50 ml of 50%) and diluted with diethyl ether (250 ml) . On standing the title compound crystallises out and is filtered off and dried in vacuo at 20°C, m.p. 206-208°C.
  • Example A.3. To a stirred solution of the product of Example A.3. (5.02g) in dry tetrahydrofuran (50ml) at -25°C under argon is added a solution of n-butyl lithium (12.5ml, 1.6M) in hexane. The resulting mixture is stirred at 10°C for 40 min, cooled to -5°C and treated with ethyl iodide (2.4ml) . The mixture is allowed to warm to room temperature, stirred for an additional 2h and then treated with saturated aqueous NH 4 C1 (100ml) and extracted with ethyl acetate (2 x 100ml) .
  • step G.3.a (4.8g) and acetic anhydride (50ml) is heated at 80°C under argon for lh. The solvent is evaporated off under reduced pressure to yield the crude product which is purified by chromatography (silica gel, 10% ethyl acetate in toluene) to give the title compound as an oil.
  • H.3. Preparation of 2, 2-Dimethyl-6- (2-methoxymethylpyridin- -4-yl) -2H-l-benzopyran
  • a stirred mixture of 4-bromo-3-methylphenol (184.lg) and aqueous NaOH (850 ml, 2M) at 20°C is treated with acetic anhydride (136 ml) and stirred at room temperature for lh.
  • the suspension is extracted with diethyl ether (3 x 300 ml) and the combined extracts are washed with aqueous NaOH (2 x 100 ml 2M) , dried (Na 2 S0 4 ) and filtered.
  • the solvent is evaporated off under reduced pressure to yield the title compound as an oil.
  • step a A mixture of the product of step a (195.6g) and aluminium chloride (152.6g) is stirred under argon at 165°C for 45 min.
  • the cooled mixture is treated with ice-cold HCl (2000 ml, 2 M) and extracted with CH 2 C1 2 (4 x 600ml) .
  • the combined extracts are washed with brine, dried (Na 2 S0 4 ), filtered and the solvent is evaporated off under reduced pressure to yield the crude product.
  • This is purified by chromatography (silica gel, 10% toluene in hexane) and recrystallised from diethyl ether-hexane to give the title compound, m.p. 81-82°C.
  • a mixture of the product of step b (48g) , acetone (31ml) and pyrrolidine (21ml) in dry benzene (500ml) is stirred at room temperature for 3h and then at reflux for 6h with water formed being removed via a Dean-Stark apparatus.
  • the cooled mixture is treated with HCl (200ml, 2M) , stirred for 10 min, basified with aqueous NaOH (1M) and extracted with CH 2 C1 2 (3x300ml) .
  • the combined extracts are dried (K 2 C0 3 ), filtered and the solvent is evaporated off under reduced pressure to yield the crude product.
  • a stirred solution of the product of step d (27.lg) in dry toluene (300ml) is treated with p-toluenesulphonic acid (1.15g) and heated under reflux for 2h with water formed being removed via a Dean-Stark apparatus.
  • the cooled solution is washed with aqueous sodium carbonate (100ml, 2M) , dried (Na 2 S0 4 ), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, hexane) to give the title compound as an oil.
  • step e A solution of the product of step e (7.60g) in dry tetrahydrofuran (30ml) is added over 15 min. to a stirred mixture of magnesium turnings (0.85g) and iodine (0.06g) in dry tetrahydrofuran (25ml) at 45°C under an argon atmosphere. The mixture is heated under reflux for 3h, cooled to 5°C, treated with bis- (triphenylphosphine)nickel (II) chloride (0.32g) and a solution of 4-bromopicoline (4.8g) in dry tetrahydrofuran (50ml) and stirred at room temperature for 18h.
  • magnesium turnings (0.85g) and iodine (0.06g) in dry tetrahydrofuran (25ml) at 45°C under an argon atmosphere.
  • the mixture is heated under reflux for 3h, cooled to 5°C, treated with bis- (triphenylphosphine)nic
  • the mixture is treated with HCl (140ml, 1M) and extracted with diethyl ether (2x60ml) .
  • the combined ether extracts are washed with HCl.
  • the combined acid solutions are basified to pH 10 with K 2 C0 3 , extracted with diethyl ether (3x100ml) , dried (Na 2 S0 ), filtered and the solvent is evaporated off under reduced pressure to yield the crude product.
  • N-Bromosuccinimide (2-20 g) is added in portions to a stirred solution of the product of Example A.3. (2-50g) in dimethylsulphoxide (6 ml) and H 2 0 (0-36 ml) at 0°C. After exothermic reaction has subsided, stirring is continued for an additional lh and the reaction is quenched with saturated aq ⁇ ueous NH 4 C1 (200 ml) and extracted with CH 2 C1 2 (3x100 ml). The combined extracts are dried (Na 2 S0 4 ) , filtered and the solvent is evaporated off under reduced pressure to yield the crude product.
  • Benzopyrans and dihydrobenzopyrans as defined under 1. above, for example compounds of formula I as hereinbefore defined, and their N-oxides, and physiologically-hydrolysable and -acceptable esters thereof, as well as pharmaceutically acceptable acid addition and quarternary ammonium salts of said benzopyrans/dihydrobenzopyrans/N-oxides/esters, (hereinafter collectively AGENTS OF THE INVENTION) are useful as pharmaceuticals.
  • AGENTS OF THE INVENTION possess smooth muscle relaxant activity and exhibit potassium channel opening activity in relation to the plasmalemma membrane as demonstrated by their influence at concentrations in the region of 1 to 500nM on tension in, and of Rb + efflux from, various smooth muscle preparations in accordance with or analogously to the methods described in Quast, Brit. J. Pharmac, 9 ⁇ , 569-578 (1987) .
  • AGENTS OF THE INVENTION are thereby characterised as K + channel opening agents.
  • K + channel opening agents are accordingly useful for the treatment of conditions or disorders for which therapy employing a K + channel opening agent is indicated.
  • Therapeutic utility as K + channel opening agents may further be demonstrated in standard pharmacological tests, e.g. of cardio-vascular activity, in vitro or in vivo.
  • influence on blood-pressure may be demonstrated in the anaesthetised, cannulated normotensive rat following intra duodenal administration 1 hr post cannulation.
  • Anti-ischemic activity may be demonstrated in accordance with the methods described in Hof et al., Circ. Res., 6 , 679 (1988) .
  • AGENTS OF THE INVENTION exhibit hypotensive activity in the former test method at threshold doses of from about 0.03 to about 1.0 mg/kg i.d. and anti-ischemic activity in the latter test method at doses of from about 0.001 to about 0.03 mg/kg i.v..
  • AGENTS OF THE INVENTION are accordingly useful, e.g. as smooth muscle relaxants, in particular for use as vasodilating agents, for example for the treatment of hypertension or chronic cardiac insufficiency. They are further useful as anti-ischaemic and anti-vasospastic agents, e.g. for use in the treatment of disturbed blood supply, for example to the heart, skeletal muscle or brain. They are thus useful e.g. for the treatment of angina pectoris, myocardial ischaemia or myocardial infarction; as antifibrillatory agents; for the treatment of disorders of peripheral circulation, e.g.
  • AGENTS OF THE INVENTION are yet further indicated for use as gastro-intestinal, uterine and urinary tract antispastic agents, e.g. for the treatment of duodenal or peptic ulcer, irritable colon, diverticulitis, danger of miscarriage following premature labour and urinary incontinence.
  • AGENTS OF THE INVENTION are yet further indicated for use as hair-growth stimulating agents, e.g. for the treatment of hair loss due to ageing, e.g. male alopecia or pattern baldness, or disease-related hair loss for example consequent to infection or disturbance of the immune system.
  • Suitable dosages for such use will of course vary, e.g. depending on the particular condition to be treated, the particular AGENT OF THE INVENTION employed the mode of administration and the effect desired.
  • a suitable oral daily dosage e.g. for anti-hypertensive uses, will be from about 0.03 to about 2.0 mg/kg and for, e.g. anti-ischemic uses, from about 0.015 to about 0.3 mg/kg.
  • an indicated oral daily dosage will thus be from about 2 to about 150 mg for anti-hypertensive uses, or from about 1 to about 20 mg for anti-ischemic uses, administered once or in divided doses 2x daily.
  • Oral dosage forms for use in the above indications will thus suitably comprise from about 0.5 or 1.0 to about 20 or 150 mg AGENT OF THE INVENTION together with a pharmaceutically acceptable diluent or carrier therefor.
  • AGENTS OF THE INVENTION will appropriately be applied topically, e.g. in an appropriate cream, gel or emulsion base or the like as known in the art.
  • AGENTS OF THE INVENTION possess bronchodilator activity and reduce or reverse airways hyperreactivity. These activities may also be demonstrated in pharmaceutical test models in vivo and in vitro, for example as follows: TEST 1. BRONCHODILATOR ACTIVITY
  • Guinea-pigs (Dunkin-Hartley, male, 400-600g) are anaesthetised with phenobarbital (100 mg/kg i.p.) and pentobarbital (30 mg/kg i.p.) and paralysed with gallamine (8 mg/kg i.m.) and ventilated with a mixture of air and oxygen (45:55, v/v) .
  • Animals are ventilated via a tracheal cannula (10 ml/kg, 1Hz) .
  • Blood pressure and heart rate are recorded from the carotid artery. Ventilation is monitored by a flow transducer.
  • coincident pressure changes in the thorax are monitored directly via an intrathoracic trochar, permitting display of differential pressure relative to the trachea. From this information resistance and compliance are calculated at each inspiration.
  • Intravenous infusion of bombesin induces sustained bronchospasm.
  • Capacity of test substance to reverse response when administered by the intratracheal route serves as a measure of efficacy in reversing established broncho ⁇ spasm.
  • the bronchodilator response is taken as the percentage reduction of the maximal response to bombesin, measured at regular intervals.
  • Rhesus monkeys male and female, body wt 6.8-11.8kg known to be normal responders to methacholine (MeCH) , are anaesthetised (initial:• ketamine 20mg/kg i.m., maintenance: thiopental 8mg/kg/h i.v.) .
  • a cuffed pediatric endotracheal tube (5.0 cm) is then introduced into the trachea (xylocaine: topical administration at the epiglottus) and basal lung resistance measured .
  • xylocaine 1% w/v solution
  • Xylocaine has no effect on base-line resistance.
  • Test substance is administered in a similar manner to xylocaine pretreatment, in a lactose vehicle suspension (lmg/ml, 1ml delivered volume) in a cumulative manner at 30 min. intervals.
  • a single MeCH challenge 0.6 to 2.5 mg/ml solution, estimated to produce approximately a 50-100% change from baseline
  • % inhibition calculated from the response after vehicle administration.
  • AGENTS OF THE INVENTION produce potent, dose-dependent bronchodilator effect in the above test method at dosages of from about 10 ng/kg to about 10 ⁇ g/kg.
  • Guinea-pigs are prepared for recording of lung function as described under Test 1.1 above. Intravenous injection of histamine (1.8-3.2 ⁇ g/kg) establishes airways sensitivity to spasmogen. Following infusion of PAF (platelet activating factor) over 1 hour (total dose 600 ng/kg) , repeated injection of histamine reveals development of airways hyperreactivity, which can conveniently be expressed as the paired difference between the response amplitude before and after PAF exposure.
  • PAF platelet activating factor
  • Guinea pigs are prepared for recording of lung-function as described under Test 1.1 above.
  • An allergic reaction is initiated by intravenous injection of preformed immune-complexes (prepared by adding 30 ⁇ g of bovine gamma globulin in 0.05 ml of saline to 0.05 ml of guinea pig anti-bovine gamma globulin anti-serum) at regular (10 min) intervals for 30 min.
  • Intravenous injections of histamine (1.0-3.2 ⁇ g/kg at 10 min intervals) are used to define the sensitivity of the airways prior to and following the last exposure to immune-complex.
  • Airways hyperreactivity is expressed as the paired difference for the maximal value of lung resistance in response to histamine before and after repeated injection of immune-complex.
  • Test compounds are administered intratracheally.
  • Induced airways hyperreactivity is significantly reduced in the above test method by prior treatment with AGENTS OF THE INVENTION, at dosages of from about lOng/kg to about 10.0 ⁇ g/kg.
  • AGENTS OF THE INVENTION are accordingly useful in particular as bronchodilator agents and as agents for the therapy of airways hyperreactivity e.g. as agents for the symptomatic as well as prophylactic treatment of obstructive or inflammatory airways disease, in particular asthma.
  • bronchodilator agents AGENTS OF THE INVENTION may be employed, in particular as rescue therapy, to treat bronchoconstrictor attack, e.g. in asthma.
  • rescue therapy to treat bronchoconstrictor attack, e.g. in asthma.
  • AGENTS OF THE INVENTION may be used for the control, restriction or reversal of airways hyperreactivity or to provide advance protection against recurrence of bronchoconstrictor attack consequential to obstructive or inflammatory airways disease, in particular asthma.
  • treatment and “treating” as used throughout the present specification and claims in relation to use of AGENTS OF THE INVENTION for the treatment of obstructive or inflammatory airways disease, in particular asthma, are accordingly to be understood as embracing both prophylactic as well as symptomatic (i.e. bronchodilator) modes of therapy, unless otherwise specified.
  • the present invention also provides:
  • a method for the prophylactic treatment of inflammatory or obstructive airways disease e.g. for the treatment of airways hyperreactivity
  • An AGENT OF THE INVENTION for use as a pharmaceutical, e.g. for use in the treatment of any disease or condition as herein specified, in particular for use in the treatment of obstructive or inflammatory airways disease, e.g. as indicated under 4.a.l or 4.a.2 above; or
  • a pharmaceutical composition comprising an AGENT OF THE INVENTION, or use of an AGENT OF THE INVENTION for use in the preparation of a pharmaceutical composition, for use in the treatment of any disease or condition herein specified, in particular for use as set forth under 5 above.
  • Inflammatory or obstructive airways diseases to which the present invention is applicable include asthma of whatever type or genesis including both intrinsic and, especially, extrinsic asthma. They are useful for the treatment of aller ⁇ gic asthma, whether atopic, (i.e. IgE-mediated) or non-atopic, as well as, for example, bronchitic asthma, exercise induced asthma, occupational asthma, asthma induced following bacterial infection and other non-allergic asthmas. Treatment of asthma is also to be understood as embracing treatment of subjects, e.g.
  • Prophylactic efficacy in the treatment of asthma will be evidenced by reduced frequency or severity of symptomatic attack, e.g. of acute asthmatic or bronchoconstrictor attack.
  • symptomatic therapy i.e. therapy for or intended to restrict or abort symptomatic attack when it occurs, for example anti-inflammatory (e.g. corticosteroid) or bronchodilatory (e.g. ⁇ 2 adrenergic) therapy.
  • anti-inflammatory e.g. corticosteroid
  • bronchodilatory e.g. ⁇ 2 adrenergic
  • Prophylactic benefit in asthma may in particular be apparent in subjects prone to "morning dipping".
  • "Morning dipping” is a recognised asthmatic syndrome, common to a substantial percentage of asthmatics and characterised by asthma attack, e.g. between the hours of about 4 to 6 am, i.e. at a time normally substantially distant from any previously administered symptomatic asthma therapy,
  • Inflammatory or obstructive airways diseases to which the present invention is applicable also include pneumoconiosis (an inflammatory, commonly occupational, disease of the lungs, frequently accompanied by airways obstruction, whether chronic or acute, and occasioned by repeated inhalation of dusts) of whatever type or genesis, including, for example, aluminosis, anthracosis, asbestosis, chalicosis, ptilosis, siderosis, silicosis, tabacosis and, in particular, byssinosis.
  • pneumoconiosis an inflammatory, commonly occupational, disease of the lungs, frequently accompanied by airways obstruction, whether chronic or acute, and occasioned by repeated inhalation of dusts
  • pneumoconiosis an inflammatory, commonly occupational, disease of the lungs, frequently accompanied by airways obstruction, whether chronic or acute, and occasioned by repeated inhalation of dusts
  • pneumoconiosis an inflammatory, commonly occupational, disease of the
  • inflammatory or obstructive airways diseases and conditions to which the present invention is applicable include adult respiratory distress syndrome (ARDS) , chronic obstructive pulmonary or airways disease (COPD or COAD), and bronchitis, as well as exacerbation of airways hyperreactivity consequent to other drug therapy, in particular other inhaled drug therapy, e.g. ⁇ -agonist bronchodilator therapy, including in particular usage of AGENTS OF THE INVENTION as bronchodilators for the treatment of chronic or acute airways obstruction as well as dyspnea, associated with any of the said diseases or conditions.
  • ARDS adult respiratory distress syndrome
  • COAD chronic obstructive pulmonary or airways disease
  • bronchitis as well as exacerbation of airways hyperreactivity consequent to other drug therapy, in particular other inhaled drug therapy, e.g. ⁇ -agonist bronchodilator therapy, including in particular usage of AGENTS OF THE INVENTION as bronchodilators for the treatment of
  • inflammatory or obstructive airways disease may be administered by any conventional route, in particular AGENTS OF THE INVENTION enterally, e.g. orally, for example in the form of tablets or capsules, or parenterally, e.g. in the form of injectable solutions or suspensions .
  • enterally e.g. orally
  • parenterally e.g. in the form of injectable solutions or suspensions .
  • they will be administered by the pulmonary route, e.g. by inhalation from an appropriate nebulizer, inhaler or like device as known in the art.
  • Dosages employed in the treatment of inflammatory or obstructive airways disease will of course vary depending, e.g. on the particular condition to be treated, the particular AGENT OF THE INVENTION employed, the mode of administration and the effect desired.
  • a suitable daily dosage delivered to the lungs will be of the order of from about O.l ⁇ g to about lOO ⁇ g, in particular from about 1.O ⁇ g to about 50.0 ⁇ g, suitably administered from an inhaler device with administration effected once or from 2 to 4x daily, in a series of from 1 to 4 puffs at each administration.
  • a suitable daily dosage will generally be of the order of from about 0.1 to about 30 ⁇ g/kg.
  • a suitable oral daily dosage for larger mammals, e.g. humans will thus be of the order of from about 7 ⁇ g to about 2.1mg, administered in a single dose, in divided doses administered from 2 to 4x daily, or in sustained release form.
  • Oral unit dosage forms for such use will thus suitably comprise from about 1.75 ⁇ g to about 2.1mg AGENT OF THE INVENTION together with a pharmaceutically acceptable diluent or carrier therefor.
  • AGENTS OF THE INVENTION are generally active as bronchodilators or as agents for the treatment of airways hyperreactivity at dosages, in particular inhaled dosages, at which cardiovascular effects which would be undesirable in relation to such therapy, e.g. hypotensive/tachycardial effect are non-significant or within acceptable limits of tolerability in relation to the therapy practiced.
  • the present invention also provides:
  • a pharmaceutical composition comprising an AGENT OF THE INVENTION together with a pharmaceutically acceptable diluent or carrier therefor.
  • compositions may be manufactured in conventional manner, e.g. for pulmonary administration by compounding AGENT OF THE INVENTION in finely divided disperse particulate form, e.g. together with finely divided lactose as a carrier/diluent to form an inhalable powder.
  • an established ID 50 in one test run carried out in accordance with Test 1.1 hereinbefore is 0.02 mg/kg, i.t..
  • [ ⁇ 1 -[ [ (1, 1-Dimethyl ethyl)amino] -methyl]-4-hydroxy-l, 3-benze- nemethanol] is 0.001 mg/kg, i.t..
  • Appropriate dosages of the Example 1 compound for administration by inhalation, e.g. for bronchodilator effect in asthma therapy, will thus be anticipated to be ca. 20x those conventionally required using Salbutamol.

Landscapes

  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Plural Heterocyclic Compounds (AREA)

Abstract

2,2-Di(C1-5alkyl)- and trans-2,2-di(C1-5alkyl)-3,4-dihydro-3-hydroxy- -6-(pyridin-4-yl)-2H-1-benzopyrans, e.g. of formula (I) in which R1 and R2 = H, alkyl, hydroxyalkyl or alkoxyalkyl, at least one being other than H, R3 = typically a 2-piperidinone group, R4 = H and R5 = -OH or R4 + R5 = an additional bond, and R6, R7 are alkyl and R8 is H or alkyl, and N-oxides, esters and salts thereof, processes for their production and their uses as pharmaceuticals e.g. as K+-channel openers, bronchodilators and asthma prophylactic agents.

Description

,2-DIALKYL- AND 2.2-DIALKYL-3.4-DIHYDR0-3-HYDR0XY- 2H-1-BENZ0PYRANS, THEIR E AS PHARMACEUTICALS
The present invention relates to novel 2,2-dial yl- and 2, 2-dialkyl-3, 4-dihydro-3-hydroxy- -2H-l-benzopyrans and salts, esters and N-oxides thereof and to processes for their production, as well as to their use as pharmaceuticals and pharmaceutical compositions comprising them.
More particularly the present invention provides in its broadest aspect:
1. A 2,2-di(C1_5alkyl)- or trans-2, 2-di (Ci-salkyl) - -3, 4-dihydro-3-hydroxy- -6-(pyridin-4-yl) -2H- 1-benzopyran having a carboxamido moiety at the 4-position and wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two members selected from the group comprising Cι_5alkyl, Cι_5hydroxyalkyl and Ci_5 (alkoxyalkyl) , or N-oxide thereof; or physiologically-hydrolysable and -acceptable ester of such a benzopyran or N-oxide or acid addition or quarternary ammonium salt of such a benzopyran, N-oxide or ester.
Alkyl groups and moieties of compounds as defined under 1. above may be branched or straight chain. Preferred significances for substituents at the 2-position of the benzopyran nucleus as well as at the 2 and/or 3 position of the pyridinyl group are as set forth below in relation to formula I for R6 and R7 , and R and R . As hereinafter described, compounds of the present invention, e.g. as defined under 1 above, have potassium (K+) channel opening activity [see e.g. Cook et al., "Potassium Channels: Structure, Classification, Function and Therapeutic Potential", ed. N.S.Cook, Ellis Horwood, Chichester (1990), p.p. 181-255]. Benzopyran derivatives which are carboxamido-substituted at the 4-position, having K+-channel opening activity are extensively described in the art and comprise a substantial and recognisable compound class. The 4-carboxamido moiety in the compounds of the invention may comprise any of those known and described in the art in relation to K+-channel opening benzopyrans, including N-substituted, for example cyclic, carboxamido moieties. Preferred carboxamido moieties in relation to the compounds of the invention are those of the formula -N(R9)-CORio as defined below.
As will be appreciated, the benzopyran nucleus of compounds defined under 1 may bear substituents in addition to those specifically defined. In particular they may, for example, be 7-Cι'_5alkyl substituted, especially 7-methyl substituted, e.g. as hereinafter indicated in relation to formula I.
In accordance with the present invention 2,2-di- (Cx_5alkyl)-3, -dihydro-3-hydroxy-6- (pyridin-4-yl)-2H-1- -benzopyrans and/or -oxides, esters, and salts thereof as defined under 1 above are preferred. The 3-hydroxy group and the 4-carboxamido moiety in such compounds are disposed in the trans-configuration as specified under 1. For this compound group (3S,4R) -enantiomers will generally be preferred, whether in pure or substantially pure form or in isomeric, e.g. racemic, mixture as hereinafter described in relation to compounds of formula I .
In a more specific aspect the present invention provides: 2 . A compound of formula I
Figure imgf000005_0001
wherein
Ri and R2 are independently, hydrogen, Cι_salkyl,
Cι_5hydroxyalkyl or Ci_5 (alkoxyalkyl) , whereby at least one of Ri and R2 is other than hydrogen,
R3 is a group of formula -N(R9)-CθRχo wherein R9 is hydrogen and Rχ0is pyridyl or R9 and Rio together are 1,3-butadienylene or represent a group of formula -(CH2)n- or -(CH2)m— - in which n is an integer of from 3 to 5 ~ inclusive and m is 1 or 2,
R4 is hydrogen and R5 is hydroxy in the trans position with respect to R3 , or
R4 and R5 together represent an additional bond as indicated by the dotted line,
R_ and R are, independently, Cι_salkyl, and
R8 is hydrogen or Cι_salkyl, or N-oxide thereof; or physiologically-hydrolysable and -acceptable ester of such a compound or N-oxide, or acid addition or quarternary ammonium salt of such a compound, N-oxide or ester.
Alkyl groups as Ri , R2 , R6 , R7 and R8 , as well as alkyl moieties of hydroxyalkyl and alkoxyalkyl groups as R and R2 may be branched or straight chain. Alkoxyalkyl groups are preferably (Ci_4alkoxy) -methyl, in particular methoxymethyl. Preferred hydroxyalkyl groups are hydroxymethyl. R6 and R7 are both preferably methyl. R8 is preferably hydrogen or methyl, most preferably hydrogen.
In a preferred group of compounds of formula I, Rx has any of the meanings given above in relation to formula I and R2 is hydrogen or Cι_5alkyl (especially methyl), preferably hydrogen.
In a further preferred group of compounds of formula I, in the definition of R3 , R9 is hydrogen and Rio is pyridyl (especially 3-pyridyl) or R9 and Rio together are 1, 3-butadienylene, trimethylene or tetramethylene. Most preferably R9 and Rio together are tetramethylene.
Preferably R4 is hydrogen and R5 is hydroxy. Benzopyrans of the invention, for example compounds of formula I, form N-oxides, e.g. at the nitrogen atom of the 6-pyridinyl group. Such N-oxides have comparable activity (as hereinafter described) and tolerability to the parent compounds and also form part of the present invention.
By "physiologically-hydrolysable and -acceptable ester" as used herein is meant an ester in which a hydroxy group (e.g., in relation to formula I, hydroxy groups R5 and/or the hydroxy moiety of any hydroxyalkyl group present as Ri and/or R2 ) is esterified and which is hydrolysable under physiological conditions to yield an acid which is itself physiologically tolerable at doses to be administered. As will be appreciated such esters are pro-drug forms of conventional type and have comparable activity and tolerability to the parent compounds. Examples of such esters include, e.g. acetates.
Acid addition salts, e.g. of compounds of formula I, their N-oxides and defined esters thereof, include salts with both inorganic and organic acids. Such salts also have comparable activity to the free compounds, N-oxides and esters. Pharmaceutically acceptable acid addition salts for pharmaceutical use in accordance with the present invention as hereinafter described include e.g. hydrochloric, sulphuric and fumaric acid salts.
Quarternary ammonium salts, e.g. of compounds of formula I, their N-oxides and defined esters thereof, include e.g. salts with organo-halides, e.g. alkyl halides. Pharmaceutically acceptable quarternary ammonium salts for pharmaceutical use in accordance with the present invention include e.g. such salts with methyl iodide.
For pharmaceutical use in accordance with the present invention ester forms as aforesaid are generally less preferred.
Compounds of formula I in which R4 is hydrogen and R5 is hydroxy, as well as their N-oxides, esters and salts as aforesaid, have the configuration (3S*,4R*), i.e. the configuration of the groups R3 and R5 at the 3- and 4-ρositions is trans. Compounds of the invention thus exist in enantiomeric form, i.e. as optically active antipodes having the [3S,4R] or [3R,4S] configuration. The present invention is to be understood as embracing both the individual enantiomers (optically active, [3S,4R] or [3R,4S], antipodes) as well as mixtures, e.g. racemic mixtures, thereof.
In that pharmaceutical utility in accordance with the invention is believed to reside, or reside predominantly, in the [3S,4R] enantiomers, these are preferred. Suitably the said [3S,4R] enantiomers will be, or will be employed in accordance with the invention, in purified form, i.e. comprising less than 50% enantiomeric contaminants, more suitably in pure or substantially pure form, e.g. comprising less than 10%, preferably 5% or less, e.g. 1 or 2% or less of [3R, 4S] enantiomeric contaminants.
In addition to the foregoing the present invention also provides:
3. A process for the production of a benzopyran as defined under 1 above, for example a compound of formula I as defined under 2 above, or N-oxide thereof, or physiologically-hydrolysable and -acceptable ester of such a benzopyran or N-oxide or acid additon or quarternary ammonium salt of such a benzopyran, N-oxide or ester, which process comprises:
i) for the production of a benzopyran as aforesaid:
i1 ) reacting a la, 7b-dihydro-2, 2-di (Ci-salkyl) -6- (pyridin- -4-yl) -2H-oxireno[c] [1]benzopyran wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two memebers selected from the group comprising Ci-salkyl, Ci_5hydroxyalkyl and Cι_5~ (alkoxyalkyl) , for example a compound of formula II
Figure imgf000008_0001
wherein Ri , R2 , R6 , R7 and R8 have the meanings for formula I above, with an alkali metal salt of a carboxamide, for example a compound of formula III
Figure imgf000008_0002
wherein R9 and Rio have the meanings given for formula I above and M+ is a lithium, sodium or potassium ion; or ) acylating and, when required, alkylating the amino group of a 2,2-di (Cι_5alkyl)- or trans-2, 2-di (Ci_5alkyl) - -3, 4-dihydro-3-hydroxy- -4-amino-6- (pyridin-4-yl) - 2H-l-benzopyran wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two members selected from the group comprising Cι_5alkyl, Ci_5hydroxyalkyl and Ci_5 (alkoxyalkyl) , for example, reacting a compound of formula IV
Figure imgf000009_0001
wherein Ri , R2 and R4 to R8 have the meanings given for formula I, with a compound of formula V, V or V
R'I O-CO-X1 (V) X2-(CH2)n-C0X1 (V )
Figure imgf000009_0002
wherein R'i0 is pyridyl and X1 and X2 are leaving groups;
for the production of a benzopyran N-oxide or physiologically-hydrolysable and -acceptable ester of a benzopyran or benzopyran N-oxide as aforesaid, esterifying a benzopyran or benzopyran N-oxide as defined under 1 above having a free hydroxy group or moiety to introduce an appropriate ester grouping, for example reacting a compound of formula I as herein- before defined wherein R5 is hydroxy and/or at least one of Ri and R2 is Cι_5 hydroxyalkyl or N-oxide thereof with an appropriate acid halide or anhydride, and/or oxidising a benzopyran or physiologically-hydrolysable and -acceptable ester thereof as defined under 1 above, for example oxidising a compound of formula I as hereinbefore defined or physiologically-hydrolysable and -acceptable ester thereof; and recovering the obtained benzopyran, benzopyran N-oxide or physiologically-hydrolysable and-acceptable ester thereof in free or in acid addition or quarternary ammonium salt form.
Process step i1 ) above may be carried out in accordance with methods known in the art, for example by reaction at ambient temperatures to reflux in the presence of an inert solvent or diluent such as tetrahydrofuran or dimethylsulfoxide. Suitably the required alkali metal salt, e.g. compound of formula III, is pre-formed in situ, for example as described in Examples 1 to 11 and 21 hereinafter. By appropriate use of e.g. Na salts, both benzopyrans and dihydro-benzopyrans of the invention may be obtained, e.g. as illustrated in Examples 11 and 12 hereinafter. Use of lithium salts leads primarily or exclusively to the preferred dihydro- -benzopyrans of the invention as illustrated in Examples 1 to 10 hereinafter.
Process step i2 ) may also be carried out in accordance with methods known in the art. Suitable leaving groups X1 are halogen and activated ester groups and suitable leaving groups X2 are halogen. Reaction is suitably carried out at temperatures of from 0° to 100°C in an inert solvent or diluent such as acetonitrile or dichloromethane, preferably in the presence of an acid binding agent, e.g. trialkylamine or alkali metal carbonate. The procedure is illustrated in Examples 13 to 20 hereinafter.
Process step ii) may be carried out in accordance with conventional acylation/N-oxidation procedures, e.g. for the obtention of N-oxides by treatment with hydrogen peroxide, m-chloroperbenzoic acid or Collin's reagent (Cr03.Py2) as hereinafter illustrated in Example 23.
Initially obtained free bases may be converted into acid addition or quarternary ammonium salts by reaction with acids or e.g. alkyl, for example methyl, halides, and vice versa.
Employing racemates of the formula II and formula IV compounds, 4-carboxamido-3, 4-dihydro-3-hydroxy- -benzopyrans obtained will be in the form of the trans-racemate [i.e. comprising the (3S,4R) plus (3R, S) isomers) . Obtained racemates may be separated to provide the individual (3R, 4S) or (preferred) (3S,4R) enantiomer, e.g. chromatographically using a chiral stationary phase. Where individual (3S,4R) enantiomers are desired, however, this is preferably achieved using the corresponding isomer as starting material, i.e. in relation to formula II, the 3S,4S-antipode and, in relation to formula IV, the 3S,4R-antipode. These are suitably produced as hereinafter described in relation to reaction sequence A.
As will be appreciated, variants of or alternatives to the above procedures may be employed as known in the art, e.g. for the interconversion of initially obtained compounds or for the introduction of alternative carboxamido groups at the 4-position. Labile groups may be protected e.g. during acylation procedures, employing conventional protecting, e.g. hydroxy-protecting groups. In addition, initially obtained benzopyrans may, if desired, be converted to corresponding benzopyrans by dehydration across the 3,4-linkage, again in accordance with standard techniques. Further alternatives will be apparent to those skilled in the art.
Compounds of the formula II may be prepared in accord¬ ance with the following general reaction sequence A
Figure imgf000012_0001
(ID (Vi)
Process steps (iii) through (vi) may be carried out by conventional means, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.A.4, A.5, A.5'a, and A.5'b.
Starting materials of formula IV may be prepared from the corresponding compounds of formula II by reaction with ammonia, e.g. in accordance with the general procedures hereinafter illustrated in Example 24.A.6' . Proceeding via steps (iii) and (iv) , the formula II compound is obtained as the cis-racemate, i.e. comprising the (3R, 4R) and (3S,4S) antipodes. Step v involves introduction of an appropriate chiral acyl group [in sequence A, by way of example, (R)-α- -methoxyphenylacetyl] . The chiral racemate VIII may readily be separated by column chromatography or fractional recrystallisation into its individual (3R,4S) and (3S,4R) antipodes. By use of the (3R,4S) antipode and proceeding via step (vi) compound II starting materials may be obtained in pure or substantially pure (3S,4S) enantiomeric form.
Compounds of formula VI may be prepared in accordance with the following general reaction sequence B
Figure imgf000013_0001
in which X' ' is a leaving group, suitably a halogen atom, e.g. chlorine. Steps (vii) to (ix) may be carried out by conventional means, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.A.2 and A.3, steps (viii) and (ix) being carried out in Example 24.A.3 without purification of the intermediate. As in Example 24.A.2 step (vii) is suitably carried out in an aprotic solvent such as acetone, in the presence of a base such as K2C03 and a catalyst such as KI.
Compounds of formula (IX) may be prepared by a variety of possible routes, for example as shown in the following general reaction sequence C
Figure imgf000014_0001
(IX)
Process steps (x) and (xi), and (xii) through (xiv), may be carried out by conventional means, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.A.la and b and 24.A.la' and b' respectively. In general, procedure via steps (x) and (xi) will be preferred for larger scale synthesis.
When it is desired to produce compounds of the invention in which Ri and/or R2 are hydroxyalkyl or alkoxyalkyl, this can also be achieved by conversion of alkyl substituents as Ri /R2. Similarly methyl substituents as Ri /R2 can if desired, be converted to higher alkyl substituents. Conveniently such conversion reactions are carried out at the formula VI stage of synthesis employing conventional techniques, e.g. in accordance with the general procedures hereinafter illustrated in Examples 24.E.3, F.3, G.3.a + G.3.b and H.3.a + H.3.b.
Compounds of formula VI wherein R8 is other than hydrogen may more conveniently be prepared in accordance with the following reaction sequence D.
Figure imgf000015_0001
in which Hal is halogen, e.g. bromine, and R8 is Cι_5alkyl. Process steps (xv) through (xxi) may be carried out by conventional means, e.g. in accordance with the procedures hereinafter illustrated in Example 24.1. Intermediates illustrated above and in the accompanying Examples, notably intermediates of formulae II, IV and VI to VIII are new. Such intermediates, in particular the intermediates of formulae II and IV, and processes for their production also constitute part of the present invention.
The following Examples are illustrative of the processes of the present invention. All NMR spectra are recorded at 360 MHz. All temperatures are in degrees celsius and are uncorrected.
EXAMPLE 1
Production of (-) - (3S, R) -1-[3,4-dihydro-2,2-dimethyl-3- -hydroxy-6- (2-methylpyridin-4-yl) -2H-l-benzopyran-4-yl] -2- -piperidinone [FORMULA I : Rι_ = Rg_ = Rη_ = CH^; R2 = R4 = Rg_ = H; Rs_ = -OH; Rj_ = yC : pure or substantially pure
(3S,4R) enantiomers] . N' )
A. stirred solution of 2-piperidinone (19.8g) in dry tetrahydrofuran (400ml) at 10°C under argon is treated with a solution of lithium bi (trimethylsilyl)amide (200ml/1.0M) in tetrahydrofuran and stirred at room temperature for 2h. The resulting suspension is treated with a solution of (-) - (3S,4S) -4- (la, 7b-dihydro-2, 2-dimethyl-2H-oxireno[c] [1] - benzopyran-6-yl) -2-methylpyridine (26.7g see Example 24.A.5' hereinafter) in dry tetrahydrofuran (150ml) and heated under reflux for 31h. The mixture is cooled to 15°C, treated with a saturated aqueous solution of NH CI (300ml) and extracted with ethyl acetate (2 x 150ml) . The combined extracts are washed with brine (300ml), dried (Na2S04) and filtered. The solvent is evaporated off under reduced pressure to give a crude product which is purified by chromatography (silica gel, 5% C2H50H in CH2C12) and recrystallised from C2H50H - pentane to give the title compound, m.p. = 192°C, [α]D 20 = -83.2° (c= 1.06, C2H50H) . M.P. for the hemimaleate salt = 146-148 ° C .
The following compounds of formula la
Figure imgf000017_0001
are prepared analogously, production of the required oxireno starting material being illustrated in the Example indicated in the right-hand column of the table.
All compounds listed in the table are in the form of the trans racemate.
Figure imgf000017_0002
EXAMPLE 11
Production of 1- [2,2-Dimethyl-6- (2-methylpyridin-4-yl) - -2H-l-benzopyran-4-yl] -2-piperidinone [Formula I: Ri = R6 = R7 = CH3_-; R2 = R8 = H; R^_ + R5 = additional bond; Rj_ = [ ∑.
A stirred solution of 2-piperidinone (0.90g-in dry dimethylsulphoxide (20ml) is treated with NaH (0.48g of a 55% dispersion in oil) and stirred at 50°C for 30 min. under argon. The mixture is cooled to 10°C and treated with a solution of (±) -4- (la, 7b-dihydro-2,2-dimethyl-2H-oxireno- [c] [l]benzopyran-6-yl) -2-methylpyridine (2.67g, see Example 24.A.5) and stirred for 14h at room temperature under argon. The solvent is evaporated off under reduced pressure and the residue treated with saturated aqueous NH4CI (200ml) and extracted with CH2C12 (3x100ml) . The combined extracts are dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield a mixture. This is separated by chromatography (silica gel, 2% C2H50H in CH2C12) to yield a less polar product (A) which is recrystallised from ethyl ether-pentane to give the title compound and a more polar compound (B) which is recrystallised from CH2C12-diethyl ether to give the same product as that of Example 2 above. M.P. for the title compound = 95-98°C.
EXAMPLE 12
Production of 1-[2,2-dimethyl-6-(3-methylpyridin-4-yl) -
Figure imgf000018_0001
The title compound is obtained together with the product of Example 3 above, starting from the product of Example 24.D.5. hereinafter and proceeding analogously to Example 11 above. Physical characteristics for the title compound: !H-NMR (δ-d6 DMSO) : 1.41 (s,3H), 1.45 (s,3H), 1.77-1.96 (m,3H), 2.26 (s,3H), 2.27-2.68 (m, 3H) , 3.37-3.58 (m,2H), 5.83 (s,lH), 6.92 (d,lH), 7.14-7.20 (m,2H) , 7.36 (m, 1H) , 8.39 (d,lH) and 8.45 (s,lH) .
EXAMPLE 13
Production of (+) - (3S, 4R)-[3,4-dihydro-2,2-dimethyl-3- -hydroxy-6- (2-methylpyridin-4-yl)-2H-l-benzopyran]-3-pyridine-
Figure imgf000019_0001
A stirred solution of (+)-(3S,4R)-4-amino-3,4-dihydro-2,2- -dimethyl-6-(2-methylpyridin-4-yl)-2H-l-benzopyran-3-ol (0.65g: see Example 24.A.6' hereinafter), triethylamine (0.50g) and 4-dimethylaminopyridine (0.002g) in dry CH2C12 (30ml) at 2°C under argon is treated with nicotinoyl chloride, hydrochloride (0.445g) . The mixture is stirred for 2 hours at room temperature after which the mixture is treated with aqueous Na2C03 (100ml/2M) and extracted with 3:1 CH2C12/CH30H (3x100ml) . The combined extracts are washed with brine, dried (Na2S0 ) , filtered and the solvent evaporated off under reduced pressure to yield an oil. The oil is purified by chromatography (silica gel, 2% C2H50H in CH2C12) and recrystallised from C2HsOH-diethyl ether to give the title compound in enantiomerically pure or substantially pure form, m.p. 247-248°C, [o]D 20 - +19.8 (c-0.965, C2H50H) .
The following compounds of formula lb
(lb)
Figure imgf000019_0002
are prepared analogously, production of the required 4-amino-benzopyran-3-ol starting material being illustrated in the example indicated in the right hand column of the table.
All compounds listed in this table are in the form of the trans racemate.
Figure imgf000020_0002
EXAMPLE 21
Production of trans-(±)-1-[3,4-dihydro-2,2-dimethyl-3- -hydroxy-6-(2-methylpyridin-4-yl)-2H-l-benzopyran-4-yl]-2(1H)- -pyridinone [Formula I: Rτ_ « R^ = ^ = CH^-; R?_ = RΛ_ = R^ = H; R3 » j—if Q as the trans racemate]
Figure imgf000020_0001
A stirred solution of 2-hydroxypyridine (0.42g) in dry C2H50H (20ml) is treated with NaH (0.21g of a 55% dispersion in oil) and stirred at room temperature for 15 min. under argon. The mixture is then cooled to 2°C and treated with a solution of (±) -4- (la, 7b-dihydro-2, 2-dimethyl-2H-oxireno[c] [l]benzopyran- -6-yl)-2-methylpyridine (1.07g (see Example 24.A.5) and stirred for 96h at room temperature. The solvent is evaporated off under reduced pressure and the residue treated with saturated aqueous NH4C1 (100ml) and extracted with CH2C12 (3x100ml) . The combined extracts are dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product which is purified by chromatography (silica gel, 2% C2H50H in CH2C12) and recrystallised from C2H50H-diethyl ether to give the title compound, m.p. 213-214°C.
EXAMPLE 22
Production of Trans-(±) -2-[3, 4-Dihydro-2,2-dimethyl-3- hydroxy-6-(2-methyl-pyridin-4-yl)-2H-l-benzopyran-4-yl] -2,3-di hydro-lH-isoindol-1-one [Formula I: Rι_ = R. = R^ = CH^-; Rg_ = Ri_ ~ RiL = H; R_ *" I N- as the trans racemate]
A stirred solution of trans-(±)-4-amino-3,4-dihydro-2,2- -dimethyl-6- (2-methylpyridin-4-yl)-2H-l-benzopyran-3-ol
(2-84g) (see Example 24.A.6) and 2-bromomethylbenzoic acid methyl ester (2-30g) in dry acetonitrile (100 ml) is treated with KI (0-84g) and then K2C03 (4-20g) under argon. The reaction mixture is stirred for lh at 20°C, lh at 60°C and then 15h at 85°. The solvent is evaporated off under reduced pressure and the residue treated with H20 (300ml) and extracted with 2% CH30H in CH2C12 (4x150ml) . The combined extracts are washed with sodium thiosulphate solution
(100ml/2%) , dried (Na2S04) and filtered. The solvent is evaporated off under reduced pressure to yield a crude product which is purified by chromatography (silica gel, 5% C2H50H in CH2C12) and recrystallised from C2Hs0H-acetone to give the title compound, m.p. 222-224°C. EXAMPLE 23
Production of (-)- (3S, R)-4- [3, -Dihydro-2,2-dimethyl- -3-hydroxy-4- (2-oxo-piperidin-l-yl) -2H-l-benzopyran-6-yl] -2- methylpyridine-N-oxide
A solution of the product of Example 1 (2.6g) in CH2C12 (40 ml) is treated with 3-chloroperoxybenzoic acid (1.92 g of 90%) and stirred at room temperature for 18 h. The solvent is evaporated off under reduced pressure to yield the crude product which is purified by chromatography (silica gel, 5% C2H50H in CH C12) and recrystallised from acetone-diethyl ether to give the title compound, m.p. 202-205°C.
EXAMPLE 24
Production of starting materials for Examples 1 through 23
A.l. Preparation of 4- (4-methoxyphenyl) -2-methylpyridine
A.l.a. ,4- (4-Methoxyphenyl) -2-methyl-l (4H) -pyridinecarboxylic acid ethyl ester
Ethyl chloroformate (10.85 g) is added to a stirred mixture of 2-picoline (9.30 g) and copper (I) iodide (0.77 g) in dry tetrahydrofuran (150 ml), at -20°C under argon. The whole is stirred for 3 hours at -20°C and then treated dropwise with a solution of 4-methoxyphenyl magnesium bromide, prepared from 4-bromoanisole (18.7 g) and Mg turnings (2.64 g) in dry tetra¬ hydrofuran (100 ml) at such a rate that the temperature remains between -15° and -20°C. The mixture is stirred at -15° for 1 hour, and 16 hours at 20°C and then treated with a saturated aqueous solution of NH4CI (300 ml) and extracted with ethyl acetate (4 x 200 ml) . The combined extracts are dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 50% toluene in hexane) to give the title compound as a pale yellow oil.
A.l.b 4- (4-Methoxyphenyl) -2-methylpyridine
The product of step A.l.a (16.9 g) and sulphur (2.0 g) in decahydronaphthalene (100 ml) is stirred at 200°C for 3 hours. The solvent is evaporated off under reduced pressure and the residue dissolved in ethyl acetate (500 ml) and extracted with HCl (3 x 200 ml of 2M) . The combined extracts were washed with ethyl acetate (2 x 100 ml), basified with ice-cooling to pH 11 with NaOH and extracted with CH2C12 (3 x 200 ml) . The combined extracts are dried (Na2S04), filtered and the solvent evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 2% C2H50H/CH C12 ) and recrystallised from C2H50H-ethyl acetate to yield the title compound, m.p. 88-91°C.
The title compound may alternatively be produced via the following route:
Figure imgf000023_0001
-tetrafluoroborate
2-Methylpyridine (111.7g) is added to a freshly prepared solution of hydroxylamine-O-sulphonic acid (45.2 g, 90%) in H20 (260 ml) at 0°C. The mixture is heated to 95°C, stirred for a further 45 min, cooled to 10°C and cautiously treated with K2C03 (55 g) . The mixture is washed with diethyl ether (2 x 100 ml) and the water evaporated off at 40°C under reduced pressure. The residue is treated with C2H50H (600 ml) and the K2S0 precipitate removed by filtration. The filtrate is treated with HCl (120 ml of 18M) and evaporated to dryness at 50°C under reduced pressure to give a residue which is treated with dehydroacetic acid (68.6g) and HCl (150 ml of 18M) and heated under reflux for 90 min. The solution is evaporated to dryness at 50° under reduced pressure and the residue stirred for 15 min with C2H50H (200 ml), filtered and the precipitate washed with C2H50H (200 ml) . The combined filtrate and washings are treated with tetrafluoroboric acid in ethyl ether (50 ml of 50%) and diluted with diethyl ether (250 ml) . On standing the title compound crystallises out and is filtered off and dried in vacuo at 20°C, m.p. 206-208°C.
A.l.b' 4- (4-Methoxyphenyl)-2-methyl-pyridine
A stirred solution of 4-methoxyphenylmagnesium bromide prepared from 4-bromoanisole (56-1 g) and Mg turnings (7.92 g) in dry tetrahydrofuran (400 ml) at 0-5° is treated with the product of step (A.l.a') (30.2 g) under an argon atmosphere. The mixture is stired at room temperature for 48h, washed with saturated aqueous NH4C1 (300 ml) and the aqueous phase is extracted with CH2C12 (3x100 ml) . The combined tetrahydrofuran solution and CH2C12 extracts are dried (Na2S0 ), filtered and the solvent is evaporated off under reduced pressure to yield crude 4' - (4-methoxyphenyl) -2,2' , 6'-trimethyl-[1, 1' (4H,4'H)- -bipyridin]-4-one. The crude product is dissolved in dry dimethylformamide (400 ml) and heated under reflux for 4 h. The solvent is evaporated off under reduced pressure to give a residue which is purified by chromatography (silica gel, 2% C2H50H in CH2C12) and recrystallised from C2H50H to yield the title compound m.p. 88-91°.
A.2. Preparation of 4-(4-hydroxyphenyl)-2-methylpyridine
A solution of the product of Example A.l. (6-45 g) in HBr (100 ml of 48 %) is heated at 135° for 3h. The excess HBr is evaporated off under reduced pressure to give a residue which is neutralised with aqueous NaHC03 and extracted with 3:1 CH2C12 /C2H50H (3x150 ml) . The combined extracts are dried (Na2S04 ) , filtered and the solvent is evaporated off under re¬ duced pressure to give the crude product. This is recrystallised from C2HsOH-diethyl ether to give the title compound, m.p. 203-204°. A.3. Preparation of 2, 2-dimethyl-6- (2-methylpyridin-4-yl) - -2H-l-benzopyran.
A stirred mixture of the product of Example A.2. (4-07 g) , anhydrous K2C03 (6-9 g) and KI (1-0 g) in dry acetone (75 ml) under argon is treated with 3-chloro-3-methylbutyne (5-65 g) and heated under reflux for 120 h. The mixture is filtered and the solvent evaporated off under reduced pressure to yield crude 4-[4- (1, l-dimethyl-2-propynyl)oxyphenyl] -2-methylpyri- dine. This is dissolved in 1,2-dichlorobenzene (50 ml) and heated at 170° for 1 h. The solvent is evaporated off under reduced pressure to give the crude title compound which is purified by chromatography (silica gel, 2% C2H50H in CH2C12), to give the title compound, m.p. 37-40°C.
The following compounds may be prepared analogously to Example A.l to A.3 above proceeding either via steps (A.l.a) + (A.l.b) or (A.l.a' + (A.l.b'); all are recovered as oils:
B.3. 2, 2-Dimethyl-6- (2-ethylpyridin-4-yl) -2H-l-benzopyran;
C.3. 2, 2-Dimethyl-6- (2, 3-dimethylpyridin-4-yl) -2H-l-benzopyran;
D.3. 2,2-Dimethyl-6- (3-methylpyridin-4-yl) -2H-l-benzopyran.
E.3. Preparation of 2,2-dimethyl-6- (2-propylpyridin-4-yl) - -2H-1-benzopyran
To a stirred solution of the product of Example A.3. (5.02g) in dry tetrahydrofuran (50ml) at -25°C under argon is added a solution of n-butyl lithium (12.5ml, 1.6M) in hexane. The resulting mixture is stirred at 10°C for 40 min, cooled to -5°C and treated with ethyl iodide (2.4ml) . The mixture is allowed to warm to room temperature, stirred for an additional 2h and then treated with saturated aqueous NH4C1 (100ml) and extracted with ethyl acetate (2 x 100ml) . The combined extracts are dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product which is purified by chromatography (silica gel, 10% acetone in hexane) to yield the title compound as an oil.
F.3. Preparation of 2, 2-dimethyl-6- (2-i.butylpyridin-4-yl) - -2H-1-benzopyran
The title compound, prepared analogously to Example E.3. employing isopropyl iodide in lieu of ethyl iodide, is obtained as an oil.
G.3. Preparation of 2, 2-dimethyl-6- (2-hydroxymethylpyridin- -4-yl) -2H-l-benzbpyran acetate
G.3.a 4- (2, 2-Dimethyl-2H-l-benzopyran-6-yl) -2-methylpyridine- -N-oxide
A solution of the product of Example A.3. (13.4g) in CH2C12 (200ml) is treated with 3-chloroperoxybenzoic acid (13.5g of 70%) and stirred at room temperature for lh. The solvent is evaporated off under reduced pressure to give a residue which is purified by chromatography (silica gel, 5% C2HsOH in CH2C1 ) to give the title compound as a yellow gum.
G.3.b (2, 2-Dimethyl-6- (2-hydroxymethylpyridin-4-yl) -2H-1 -benzopyran acetate
A mixture of the product of step G.3.a (4.8g) and acetic anhydride (50ml) is heated at 80°C under argon for lh. The solvent is evaporated off under reduced pressure to yield the crude product which is purified by chromatography (silica gel, 10% ethyl acetate in toluene) to give the title compound as an oil. H.3. Preparation of 2, 2-Dimethyl-6- (2-methoxymethylpyridin- -4-yl) -2H-l-benzopyran
H.3.a (2, 2-Dimethyl-2H-l-benzopyran-6-yl) -2-pyridinemethanol
A mixture of the product of Example G.3. (69.5g), Na2C03 (95.4g), H20 (160ml) and C2H50H (600ml) is stirred at room temperature for 22h. The mixture is filtered and the filtrate evaporated to dryness under reduced pressure to give a residue which is treated with H20 (400ml) and extracted with CH2C12 (3x150ml) . The combined extracts are dried (Na2S04) and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, ethyl acetate) and recrystallised from pentane to give the title compound, m.p. 86-88°C.
H.3.b (2,2-Dimethyl-2H-l-benzopyran-6-yl) -2-methoxymethyl pyridine
A stirred solution of the product of step H.3.a (8.0g) in dry tetrahydrofuran (150ml) at 15°C under argon is treated with NaH
(0.90g of an 80% dispersion in oil) and stirred at room temperature for 45 min. Methyl iodide (4.26g) is added and the mixture is stirred at room temperature for 18h. The mixture is treated with saturated aqueous NH4C1 (200ml) and extracted with ethyl acetate (2x200ml) . The combined extracts are dried
(Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 20% acetone in hexane) to give the title compound as an oil.
I . Preparation of 6-(2-methylpyridin-4-yl) -2,2, 7-trimethyl- -2H-1-benzopyran
a. 4-Bromo-3-methylphenol acetate
A stirred mixture of 4-bromo-3-methylphenol (184.lg) and aqueous NaOH (850 ml, 2M) at 20°C is treated with acetic anhydride (136 ml) and stirred at room temperature for lh. The suspension is extracted with diethyl ether (3 x 300 ml) and the combined extracts are washed with aqueous NaOH (2 x 100 ml 2M) , dried (Na2S04) and filtered. The solvent is evaporated off under reduced pressure to yield the title compound as an oil.
b. 1- (3-Bromo-2-hydroxy-5-methylphenyl)ethanone
A mixture of the product of step a (195.6g) and aluminium chloride (152.6g) is stirred under argon at 165°C for 45 min. The cooled mixture is treated with ice-cold HCl (2000 ml, 2 M) and extracted with CH2C12 (4 x 600ml) . The combined extracts are washed with brine, dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 10% toluene in hexane) and recrystallised from diethyl ether-hexane to give the title compound, m.p. 81-82°C.
c. 6-Bromo-3, 4-dihydro-2,2, 7-trimethyl-2H-l-benzopyran-4-one
A mixture of the product of step b (48g) , acetone (31ml) and pyrrolidine (21ml) in dry benzene (500ml) is stirred at room temperature for 3h and then at reflux for 6h with water formed being removed via a Dean-Stark apparatus. The cooled mixture is treated with HCl (200ml, 2M) , stirred for 10 min, basified with aqueous NaOH (1M) and extracted with CH2C12 (3x300ml) . The combined extracts are dried (K2C03), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 50% toluene in hexane) and recrystallised from diethyl ether-pentane to give the title compound, m.p. 95-96°C. d. 6-Bromo-3, 4-dihydro-4-hydroxy-2, 2, 7-trimethyl-2H-l- -benzopyran
A stirred solution of the product of step c (26.9g) in C2H50H (200 ml) at 5°C is treated with sodium borohydride (1.95g) and stirred at room temperature for 12h. The solvent is evaporated off under reduced pressure to give a residue which is treated with H20 (500 ml) and extracted with diethyl ether (3x200ml) . The combined extracts are dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 10% acetone in hexane) and recrystallised from diethyl ether-pentane to give the title compound, m.p. 92-93°C.
e. 6-Bromo-2, 2, 7-trimethyl-2H-l-benzopyran
A stirred solution of the product of step d (27.lg) in dry toluene (300ml) is treated with p-toluenesulphonic acid (1.15g) and heated under reflux for 2h with water formed being removed via a Dean-Stark apparatus. The cooled solution is washed with aqueous sodium carbonate (100ml, 2M) , dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, hexane) to give the title compound as an oil.
f. 6- (2-methylpyridin-4-yl)-2,2, 7-trimethyl-2H-l-benzopyran
A solution of the product of step e (7.60g) in dry tetrahydrofuran (30ml) is added over 15 min. to a stirred mixture of magnesium turnings (0.85g) and iodine (0.06g) in dry tetrahydrofuran (25ml) at 45°C under an argon atmosphere. The mixture is heated under reflux for 3h, cooled to 5°C, treated with bis- (triphenylphosphine)nickel (II) chloride (0.32g) and a solution of 4-bromopicoline (4.8g) in dry tetrahydrofuran (50ml) and stirred at room temperature for 18h. The mixture is treated with HCl (140ml, 1M) and extracted with diethyl ether (2x60ml) . The combined ether extracts are washed with HCl. The combined acid solutions are basified to pH 10 with K2C03, extracted with diethyl ether (3x100ml) , dried (Na2S0 ), filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This purified by chromatography (silica gel, 10% acetone in hexane) to give the title compound as an oil, having the following physical characteristics: iH-NMRfδ-CDCls) : 1.44 (s,6H), 2.21 (s,3H), 2.59 (s,3H), 5.60 (d,lH), 6.31 (d,lH), 6.70 (S,1H), 6.82 (s,lH), 7.04 (dd,lH), 7.09 (d,lH) and 8.49 (d,lH) .
A.4. Preparation of trans- (±) 3-Bromo-3, 4-dihydro-2, 2-
-dimethyl-6-(2-methylpyridin-4-yl) -2H-l-benzopyran-4-ol
N-Bromosuccinimide (2-20 g) is added in portions to a stirred solution of the product of Example A.3. (2-50g) in dimethylsulphoxide (6 ml) and H20 (0-36 ml) at 0°C. After exothermic reaction has subsided, stirring is continued for an additional lh and the reaction is quenched with saturated aq¬ ueous NH4C1 (200 ml) and extracted with CH2C12 (3x100 ml).. The combined extracts are dried (Na2S04 ) , filtered and the solvent is evaporated off under reduced pressure to yield the crude product. This is purified by chromatography (silica gel, 2% C2H50H in CH2C12) and recrystallised from C2H50H-diethyl ether to give the title compound, m.p. 212-214°C.
A.5. Preparation of (±) -4- (la, 7b-Dihydro-2,2-dimethyl-2H-oxi- reno[c] [l]benzopyran-6-yl) -2-methylpyridine
A solution of the product of Example A.4. (3-5 g) in dry tetra¬ hydrofuran (80 ml) is treated with NaH (0- 90 g of a 55 % dispersion in oil) and stirred at room temperature under argon for 1 h. The reaction is quenched with a saturated aqueous solution of NH4C1 (150 ml) and extracted with diethyl ether (3x100 ml) . The combined extracts are dried (Na2S04 ) , filtered and the solvent is evaporated off under reduced pressure to give a residue which is purified by chromatography (silica gel, 2% C H5UH in CH2C12) to give the title compound as an oil having the following physical characteristics:
!H-NMR (δ-d6 DMSO) : 1-23 (s,3H), 1-50 (s,3H) , 2-52 (s,3H) , 3-75 (d,lH) , 4-14 (d,lH) , 6-89 (d, 1H) , 7-47 (dd, 1H) , 7-56 (s,lH), 7- 19 (dd,lH) , 7- 96 (d, 1H) and 8-47 (d,lH) .
The following compounds of formula II in which Rg and R are each methyl and Rx , R2 and R8 have the significances indicated may be prepared analogously to Examples A4 and A5 above, but carrying out reaction by a one-pot procedure. This is done by diluting the mixture obtained subsequent to exothermic reaction and stirring according to Example A.4. with dioxan, treating with aqueous NaOH (0.6M) and stirring at room temperature for ca. lh further. Purification then proceeds analogously to Example A.5. following evaporation of dioxan. The starting materials are as shown in column 2 of the table. All products are obtained as the (±) racemate in the form of an oil.
Figure imgf000031_0001
CHARACTERISING DATA
B.5. XHNMR (δ-CDCl3) : 1.31 (S,3H), 1.37 (t,3H), 1.62 (s,3H), 2.89 (q,2H), 3,56 (d, 1H) , 3.99 (d, 1H) , 6.91 (d, 1H) , 7.28 (dd,lH), 7.34 (m,lH), 7,54 (dd, 1H) 7.63 (d, 1H) and 8.54 (dd, 1H) .
C.5. XH-NMR (δ-CDCla) : 1.32 (s,3H), 1.61 (s,3H), 2.20 (s,3H), 2.61 (s,3H), 3.54 (d,lH), 3.39 (d, 1H) , 6.87 (d, 1H) , 6.98 (d,lH), 7.17 (dd,lH), 7.26 (d, 1H) and 8.32 (d,lH) .
D.5. iH-NMR (δ-CDCl3) : 1.33 (s,3H), 1.62 (s,3H), 2.31 (s,3H), 3.55 (d,lH), 3.95 (d,lH), 6.89 (d,lH), 7.13 (d, 1H) , 7.23 (dd,lH), 7.31 (S,1H), 8.45 (d, 1H) and 8.49 (s,lH) .
E.5. iH-NMR (δ-CDCl3) : 1.01 (t,3H), 1.30 (s,3H), 1.62 (s,3H), 1.82 (sex,2H), 2.82 (t,2H), 3.54 (d, 1H) , 3.98 (d, 1H) , 6.91 (d,lH), 7.28 (dd, 1H) , 7.32 (d, 1H) , 7.53 (dd,lH), 7.63 (d,lH) and 8.54 (d, 1H) .
F.5. ^-NMR (δ-CDCl3) : 0.96 (d, 6H) , 1.30 (s,3H), 1.62 (s,3H), 2.15 (dt,lH), 2.70 (d,2H), 3.54 (d,lH), 3.93 (d, 1H) , 6.90 (d,lH), 7.22-7.30 (m, 2H), 7.53 (dd, 1H) , 7.63 (d, 1H) and 8.54 (d,lH) .
G.5. XH-NMR (δ-CDCl3) : 1.31 (s,3H), 1.63 (s,3H), 3.55 (d, 1H) , 3.98 (d,lH), 4.83 (s,2H), 6.92 (d, 1H) , 7.35-7.45 (m, 2H) , 7.54 (dd,lH), 7.64 (d,lH) and 8.57 (d, 1H) .
1.5. iH-rNMR (δ-CDCl3) : 1.29 (s,3H), 1.59 (s,3H), 2.21 (s,3H), 2.60 (s,3H), 3.50 (d,lH), 3.89 (d, 1H) , 6.74 (s,lH), 7.04 (dd,lH), 7.10 (d,lH), 7.18 (s,lH) and 8.50 (d,lH) .
A.5' Preparation of (-) - (3S, 4S) -4- (la, 7b-dihydro-2, 2- dimethyl-2H-oxireno[c] [l]benzopyran-6-yl) -2-methyl- pyridine
A.5. 'a [lR-[lα(3R,4S) ,4β]- and [1R- [la (3S, 4R) , 4β ] -
-α-methoxybenzene acetic acid, 3-bromo-3, 4-dihydro- -2, 2-dimethyl-6- (2-methylpyridin-4-yl) -2H-l-benzopyran- -4-yl, ester.
A solution of the product of Example A.4. (9-80 g) , (-) - (R) -α-methoxyphenylacetic acid (5-65 g) and 4-dimethylaminopyridine (0,45 g) in dry CH2C12 (330 ml), is treated with N,N-dicyclohexylcarbodiimide (6-81 g) and stirred for 90 min at room temperature. The mixture is filtered and the solvent evaporated off under reduced pressure to give a crude mixture of diastereoisomers which is purified by chromatography (silica gel, 5% acetone in CH2C12) to yield a less polar product (A) which is recrystallised from acetone-pentane to give the [1R-[lα (3R, 4S) , 4β] isomer of the title compound, m.p. 137-138°C, [α]D 20 = -75.4° (c = 0.955, C2H50H) and, as a more polar product, (B) the [1R-[lα (3S, 4R) , - 4β] isomer of the title compound as an oil, [α]D 20 = -22° (c = 0.975, C2H50H) .
A.5' .b (-) - (3S, 4S) -4- (la, 7b-Dihydro-2,2-dimethyl-2H-
-oxireno[c] [l]benzopyran-6-yl) -2-methylpyridine
A solution of [1R-[lα (3R, 4S) , 4β] isomer product of step (A.5' .a) (3.16 g) in dioxan (75 ml) at 20°C is treated with aqueous NaOH (45 ml of 0-58 M) and stirred for 10 min at 20°C. The dioxan is evaporated off under reduced pressure and the residue treated with H 0 (100 ml) and extracted with CH2C12 (3 x 100 ml) . The combined extracts are dried (Na2S04), filtered and the solvent is evaporated off under reduced pressure to give a residue which is purified by column chromatography (silica gel, 5% C2H50H in CH2C12) to give the title compound in pure or substantially pure enatiomeric form as a colourless oil, [α]D 20 72° (c = 1-125, C2H50H) .
A.6'. Preparation of (+) - (3S, 4R) -4-amino-3,4-dihydro-2,2-
-dimethyl-6- (2-methylpyridin-4-yl)-2H-l-benzopyran-3-ol
A solution of the product of Example A.5' (0.64 g) is treated with saturated NH3 in C2H50H (15 ml) and heated at 80°C in autoclave for 15 hours. The solvent is evaporated off under reduced pressure to yield the crude product which is purified by chromatography (silica gel, 5% C2H50H in CH2C12) to give the title compound as a foam: [α]20 D = +100°, (c = 1.00, C2H50H) .
The following compounds of formula IV in which R4 is H, R5 is hydroxy, R6 and R7 are each methyl and Rx , R2 and R8 have the meanings shown may be produced analogously from the indicated starting material. All compounds listed in this table are in the form of the trans racemate and, except for the product of Example B6, are obtained as an oil.
PHYSICAL DATA
A.6. 1H-NMR (δ6-DMSO): 1.12 (s,3H), 1.38 (s,3H), 2.06 (broad, 2H), 2.50 (s,3H), 3.23 (dd,1H) , 3.59 (d,1H) , 5.47 (d,1H) , 6.81 (d,lH), 7.43 (dd,lH), 7.51 (s,lH), 7.55 (dd,1H) , 7.99 (m,1H) and 8.44 (d,lH)
B.6. M.P. = 140-141°C.
C.6. iH-NMR (δ-CDCl3): 1.27 (s,3H), 1.54 (s,3H), 2.15 (s,3H), 2.2-2.5 (br.s,3H), 2.57 (s,3H), 3.41 (d,1H) , 3.71 (d,1H) , 6.85 (d,lH), 6.99 (d,lH), 7.10 (dd,lH), 7.31 (dd,lH) and 8.31 (d,lH). E.6. -H-NMR (δ-CDCl3) : 1.00 (t,3H), 1.27 (s,3H), 1.55 (s,3H), 1.80 (s,2H), 2.0-2.4 (br.s,3H), 2.80 (t,2H), 3.41 (d, 1H) , 3.74 (d,lH), 6.89 (d, 1H) , 7.25-7.36 (m, 2H) , 7.47 (dd,lH), 7.70 (d,lH) and 8.51 (d, 1H) .
F.6. XH-NMR (δ-DMSO) : 0.90 (d, 6H) , 1.13 (s,3H), 1.41 (s,3H), 2.0-2.2 (br.s,2H), 2.09 (dt,lH), 2.65 (d,2H), 3.24 (dd,lH), 3.63 (d,lH), 5.45 (br.d,lH), 6.84 (d, 1H) , 7.48 (m,2H), 7.58 (dd,lH), 8.00 (d, 1H) and 8.46 (d,lH) .
1.6. iH-NMR (δ-CDCl3) : 1.24 (s,3H), 1.53 (s,3H), 2.1-2.4
(br.s,3H), 2.20 (s,3H), 2.60 (s,3H), 3.38 (d, 1H) , 3.67 (d,lH), 6.73 (S,1H), 7.05 (d,lH), 7.10 (s,lH), 7.21 (s,lH) and 8.49 (d,lH) .
Benzopyrans and dihydrobenzopyrans as defined under 1. above, for example compounds of formula I as hereinbefore defined, and their N-oxides, and physiologically-hydrolysable and -acceptable esters thereof, as well as pharmaceutically acceptable acid addition and quarternary ammonium salts of said benzopyrans/dihydrobenzopyrans/N-oxides/esters, (hereinafter collectively AGENTS OF THE INVENTION) are useful as pharmaceuticals.
AGENTS OF THE INVENTION possess smooth muscle relaxant activity and exhibit potassium channel opening activity in relation to the plasmalemma membrane as demonstrated by their influence at concentrations in the region of 1 to 500nM on tension in, and of Rb+ efflux from, various smooth muscle preparations in accordance with or analogously to the methods described in Quast, Brit. J. Pharmac, 9∑, 569-578 (1987) . AGENTS OF THE INVENTION are thereby characterised as K+ channel opening agents.
AGENTS OF THE INVENTION are accordingly useful for the treatment of conditions or disorders for which therapy employing a K+ channel opening agent is indicated. Therapeutic utility as K+ channel opening agents may further be demonstrated in standard pharmacological tests, e.g. of cardio-vascular activity, in vitro or in vivo. Thus influence on blood-pressure may be demonstrated in the anaesthetised, cannulated normotensive rat following intra duodenal administration 1 hr post cannulation. Anti-ischemic activity may be demonstrated in accordance with the methods described in Hof et al., Circ. Res., 6 , 679 (1988) . AGENTS OF THE INVENTION exhibit hypotensive activity in the former test method at threshold doses of from about 0.03 to about 1.0 mg/kg i.d. and anti-ischemic activity in the latter test method at doses of from about 0.001 to about 0.03 mg/kg i.v..
AGENTS OF THE INVENTION are accordingly useful, e.g. as smooth muscle relaxants, in particular for use as vasodilating agents, for example for the treatment of hypertension or chronic cardiac insufficiency. They are further useful as anti-ischaemic and anti-vasospastic agents, e.g. for use in the treatment of disturbed blood supply, for example to the heart, skeletal muscle or brain. They are thus useful e.g. for the treatment of angina pectoris, myocardial ischaemia or myocardial infarction; as antifibrillatory agents; for the treatment of disorders of peripheral circulation, e.g. claudicatio intermittens, Morbus Raynaud or venous ulcer; as well as for the treatment, including prophylaxis, of cerebral ischaemia, senile dementia, stroke, subarachnoidal hemorrhage and other related or consequential diseases or disorders.
AGENTS OF THE INVENTION are yet further indicated for use as gastro-intestinal, uterine and urinary tract antispastic agents, e.g. for the treatment of duodenal or peptic ulcer, irritable colon, diverticulitis, danger of miscarriage following premature labour and urinary incontinence.
AGENTS OF THE INVENTION are yet further indicated for use as hair-growth stimulating agents, e.g. for the treatment of hair loss due to ageing, e.g. male alopecia or pattern baldness, or disease-related hair loss for example consequent to infection or disturbance of the immune system.
Suitable dosages for such use will of course vary, e.g. depending on the particular condition to be treated, the particular AGENT OF THE INVENTION employed the mode of administration and the effect desired. In general however a suitable oral daily dosage, e.g. for anti-hypertensive uses, will be from about 0.03 to about 2.0 mg/kg and for, e.g. anti-ischemic uses, from about 0.015 to about 0.3 mg/kg. For larger mammals, e.g. humans, an indicated oral daily dosage will thus be from about 2 to about 150 mg for anti-hypertensive uses, or from about 1 to about 20 mg for anti-ischemic uses, administered once or in divided doses 2x daily. Oral dosage forms for use in the above indications will thus suitably comprise from about 0.5 or 1.0 to about 20 or 150 mg AGENT OF THE INVENTION together with a pharmaceutically acceptable diluent or carrier therefor.
For use as hair-growth stimulating agents AGENTS OF THE INVENTION will appropriately be applied topically, e.g. in an appropriate cream, gel or emulsion base or the like as known in the art.
More importantly it has in accordance with the present invention been found that AGENTS OF THE INVENTION possess bronchodilator activity and reduce or reverse airways hyperreactivity. These activities may also be demonstrated in pharmaceutical test models in vivo and in vitro, for example as follows: TEST 1. BRONCHODILATOR ACTIVITY
1.1 In the Guinea-Pig
Guinea-pigs (Dunkin-Hartley, male, 400-600g) are anaesthetised with phenobarbital (100 mg/kg i.p.) and pentobarbital (30 mg/kg i.p.) and paralysed with gallamine (8 mg/kg i.m.) and ventilated with a mixture of air and oxygen (45:55, v/v) . Animals are ventilated via a tracheal cannula (10 ml/kg, 1Hz) . Blood pressure and heart rate are recorded from the carotid artery. Ventilation is monitored by a flow transducer. When making measurements of flow, coincident pressure changes in the thorax are monitored directly via an intrathoracic trochar, permitting display of differential pressure relative to the trachea. From this information resistance and compliance are calculated at each inspiration.
Intravenous infusion of bombesin (100 ng/kg/h) induces sustained bronchospasm. Capacity of test substance to reverse response when administered by the intratracheal route serves as a measure of efficacy in reversing established broncho¬ spasm. The bronchodilator response is taken as the percentage reduction of the maximal response to bombesin, measured at regular intervals.
In the above test model, AGENTS OF THE INVENTION effect dose related abrogation of bronchospasm at dosages of from about 0.001 to about 1.0 mg/kg.
1.2 In the Rhesus Monkey
Rhesus monkeys (male and female, body wt 6.8-11.8kg) known to be normal responders to methacholine (MeCH) , are anaesthetised (initial:• ketamine 20mg/kg i.m., maintenance: thiopental 8mg/kg/h i.v.) . A cuffed pediatric endotracheal tube (5.0 cm) is then introduced into the trachea (xylocaine: topical administration at the epiglottus) and basal lung resistance measured .
Following these manoeuvres, 2ml xylocaine (1% w/v solution) is administered at the carina with a pediatric fibreoptic bronchoscope. 10 minutes later, lung resistance is again measured. Xylocaine has no effect on base-line resistance. Test substance is administered in a similar manner to xylocaine pretreatment, in a lactose vehicle suspension (lmg/ml, 1ml delivered volume) in a cumulative manner at 30 min. intervals. At the 15 minute time point, a single MeCH challenge (0.6 to 2.5 mg/ml solution, estimated to produce approximately a 50-100% change from baseline) is performed and the % inhibition calculated from the response after vehicle administration.
AGENTS OF THE INVENTION produce potent, dose-dependent bronchodilator effect in the above test method at dosages of from about 10 ng/kg to about 10 μg/kg.
TEST 2. SUPPRESSION OF AIRWAYS HYPERREACTIVITY
2.1 PAF-induced hyperreactivity
Guinea-pigs are prepared for recording of lung function as described under Test 1.1 above. Intravenous injection of histamine (1.8-3.2 μg/kg) establishes airways sensitivity to spasmogen. Following infusion of PAF (platelet activating factor) over 1 hour (total dose 600 ng/kg) , repeated injection of histamine reveals development of airways hyperreactivity, which can conveniently be expressed as the paired difference between the response amplitude before and after PAF exposure.
On administration of AGENTS OF THE INVENTION intratracheally after PAF exposure at dosages of from about 0.1 to about lOOμg/kg, reversal of airways hyperreactivity induction is observed. 2.2 Immune-complex-induced hyperreactivity
Guinea pigs are prepared for recording of lung-function as described under Test 1.1 above. An allergic reaction is initiated by intravenous injection of preformed immune-complexes (prepared by adding 30 μg of bovine gamma globulin in 0.05 ml of saline to 0.05 ml of guinea pig anti-bovine gamma globulin anti-serum) at regular (10 min) intervals for 30 min. Intravenous injections of histamine (1.0-3.2 μg/kg at 10 min intervals) are used to define the sensitivity of the airways prior to and following the last exposure to immune-complex. Airways hyperreactivity is expressed as the paired difference for the maximal value of lung resistance in response to histamine before and after repeated injection of immune-complex. Test compounds are administered intratracheally.
Induced airways hyperreactivity is significantly reduced in the above test method by prior treatment with AGENTS OF THE INVENTION, at dosages of from about lOng/kg to about 10.0 μg/kg.
AGENTS OF THE INVENTION are accordingly useful in particular as bronchodilator agents and as agents for the therapy of airways hyperreactivity e.g. as agents for the symptomatic as well as prophylactic treatment of obstructive or inflammatory airways disease, in particular asthma. As bronchodilator agents, AGENTS OF THE INVENTION may be employed, in particular as rescue therapy, to treat bronchoconstrictor attack, e.g. in asthma. In addition, by continued administration, AGENTS OF THE INVENTION may be used for the control, restriction or reversal of airways hyperreactivity or to provide advance protection against recurrence of bronchoconstrictor attack consequential to obstructive or inflammatory airways disease, in particular asthma. The words "treatment" and "treating" as used throughout the present specification and claims in relation to use of AGENTS OF THE INVENTION for the treatment of obstructive or inflammatory airways disease, in particular asthma, are accordingly to be understood as embracing both prophylactic as well as symptomatic (i.e. bronchodilator) modes of therapy, unless otherwise specified.
In accordance with the foregoing the present invention also provides:
4. A method for the treatment of any disease or condition herein specified; in particular
4.a A method for the treatment of obstructive or inflammatory airways disease; including
4.a.l A method for the symptomatic treatment of inflammatory or obstructive airways disease, e.g. of effecting bronchodilatation; or
4.a.2 A method for the prophylactic treatment of inflammatory or obstructive airways disease, e.g. for the treatment of airways hyperreactivity;
- in a subject in need thereof, which method comprises administering to said subject an effective amount of an AGENT OF THE INVENTION:
or, in the alternative:
5. An AGENT OF THE INVENTION for use as a pharmaceutical, e.g. for use in the treatment of any disease or condition as herein specified, in particular for use in the treatment of obstructive or inflammatory airways disease, e.g. as indicated under 4.a.l or 4.a.2 above; or
6. A pharmaceutical composition comprising an AGENT OF THE INVENTION, or use of an AGENT OF THE INVENTION for use in the preparation of a pharmaceutical composition, for use in the treatment of any disease or condition herein specified, in particular for use as set forth under 5 above.
Inflammatory or obstructive airways diseases to which the present invention is applicable include asthma of whatever type or genesis including both intrinsic and, especially, extrinsic asthma. They are useful for the treatment of aller¬ gic asthma, whether atopic, (i.e. IgE-mediated) or non-atopic, as well as, for example, bronchitic asthma, exercise induced asthma, occupational asthma, asthma induced following bacterial infection and other non-allergic asthmas. Treatment of asthma is also to be understood as embracing treatment of subjects, e.g. of less than 4 or 5 years of age, exhibiting wheezing symptoms, in particular at night, and diagnosed or diagnosable as "wheezy infants", an established patient category of major medical concern and now more correctly identified as incipient or early-phase asthmatics. (For convenience this particular asthmatic condition is referred to as "wheezy-infant syndrome".)
Prophylactic efficacy in the treatment of asthma will be evidenced by reduced frequency or severity of symptomatic attack, e.g. of acute asthmatic or bronchoconstrictor attack.
It may further be evidenced by reduced requirement for other, symptomatic therapy, i.e. therapy for or intended to restrict or abort symptomatic attack when it occurs, for example anti-inflammatory (e.g. corticosteroid) or bronchodilatory (e.g. β2 adrenergic) therapy.
Prophylactic benefit in asthma may in particular be apparent in subjects prone to "morning dipping". "Morning dipping" is a recognised asthmatic syndrome, common to a substantial percentage of asthmatics and characterised by asthma attack, e.g. between the hours of about 4 to 6 am, i.e. at a time normally substantially distant from any previously administered symptomatic asthma therapy,
Inflammatory or obstructive airways diseases to which the present invention is applicable also include pneumoconiosis (an inflammatory, commonly occupational, disease of the lungs, frequently accompanied by airways obstruction, whether chronic or acute, and occasioned by repeated inhalation of dusts) of whatever type or genesis, including, for example, aluminosis, anthracosis, asbestosis, chalicosis, ptilosis, siderosis, silicosis, tabacosis and, in particular, byssinosis.
Further inflammatory or obstructive airways diseases and conditions to which the present invention is applicable include adult respiratory distress syndrome (ARDS) , chronic obstructive pulmonary or airways disease (COPD or COAD), and bronchitis, as well as exacerbation of airways hyperreactivity consequent to other drug therapy, in particular other inhaled drug therapy, e.g. β-agonist bronchodilator therapy, including in particular usage of AGENTS OF THE INVENTION as bronchodilators for the treatment of chronic or acute airways obstruction as well as dyspnea, associated with any of the said diseases or conditions.
For use in the treatment of inflammatory or obstructive airways disease may be administered by any conventional route, in particular AGENTS OF THE INVENTION enterally, e.g. orally, for example in the form of tablets or capsules, or parenterally, e.g. in the form of injectable solutions or suspensions . Preferably however they will be administered by the pulmonary route, e.g. by inhalation from an appropriate nebulizer, inhaler or like device as known in the art.
Dosages employed in the treatment of inflammatory or obstructive airways disease will of course vary depending, e.g. on the particular condition to be treated, the particular AGENT OF THE INVENTION employed, the mode of administration and the effect desired. In general however, for pulmonary administration for larger mammals, e.g. humans, a suitable daily dosage delivered to the lungs will be of the order of from about O.lμg to about lOOμg, in particular from about 1.Oμg to about 50.0μg, suitably administered from an inhaler device with administration effected once or from 2 to 4x daily, in a series of from 1 to 4 puffs at each administration.
For oral administration a suitable daily dosage will generally be of the order of from about 0.1 to about 30μg/kg. A suitable oral daily dosage for larger mammals, e.g. humans, will thus be of the order of from about 7μg to about 2.1mg, administered in a single dose, in divided doses administered from 2 to 4x daily, or in sustained release form. Oral unit dosage forms for such use will thus suitably comprise from about 1.75μg to about 2.1mg AGENT OF THE INVENTION together with a pharmaceutically acceptable diluent or carrier therefor.
In this connection it is in particular to be noted that AGENTS OF THE INVENTION are generally active as bronchodilators or as agents for the treatment of airways hyperreactivity at dosages, in particular inhaled dosages, at which cardiovascular effects which would be undesirable in relation to such therapy, e.g. hypotensive/tachycardial effect are non-significant or within acceptable limits of tolerability in relation to the therapy practiced.
In accordance with the foregoing the present invention also provides:
7. A pharmaceutical composition comprising an AGENT OF THE INVENTION together with a pharmaceutically acceptable diluent or carrier therefor.
Such compositions may be manufactured in conventional manner, e.g. for pulmonary administration by compounding AGENT OF THE INVENTION in finely divided disperse particulate form, e.g. together with finely divided lactose as a carrier/diluent to form an inhalable powder.
As previously indicated, therapeutic dosage requirements in practicing the present invention will vary depending on a variety of factors. Dosaging for any particular AGENT OF THE INVENTION will also depend on its relative potency of action. For the preferred AGENT OF THE INVENTION, namely the product of Example 1 in pure or substantially pure (3S,4R) enantiomeric form an established ID50 in one test run carried out in accordance with Test 1.1 hereinbefore is 0.02 mg/kg, i.t.. An established ID50 in the same test method for the known inhaled bronchodilator drug salbutamol
1-[ [ (1, 1-Dimethyl ethyl)amino] -methyl]-4-hydroxy-l, 3-benze- nemethanol] is 0.001 mg/kg, i.t.. Appropriate dosages of the Example 1 compound for administration by inhalation, e.g. for bronchodilator effect in asthma therapy, will thus be anticipated to be ca. 20x those conventionally required using Salbutamol.

Claims

A 2,2-di (Cι_5alkyl)- or trans-2, 2-di (Cx_5alkyl) - -3, 4-dihydro-3-hydroxy- -6- (pyridin-4-yl) -2H- -1-benzopyran having a carboxamido moiety at the 4-position and wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two members selected from the group comprising Cι_5alkyl, Cι_5hydroxyalkyl and Cι_5 (alkoxyalkyl) , or N-oxide thereof; or physiologically-hydrolysable and -acceptable ester of such a benzopyran or N-oxide or acid addition or quarternary ammonium salt of such a benzopyran, N-oxide or ester.
A compound of formula I
Figure imgf000046_0001
wherein
Ri and R2 are independently, hydrogen, Cι_5alkyl,
Cι_5hydroxyalkyl or Ci-5 (alkoxyalkyl) , whereby at least one of Ri and R2 is other than hydrogen, R3 is a group of formula -N(R9 ) -CORi0 wherein R9 is hydrogen and Riois pyridyl or R9 and R10 together are 1, 3-butadienylene or represent a group of formula -(CH2)n- or
Figure imgf000047_0001
in which n is an integer of from 3 to 5 inclusive and m is 1 or 2, R4 is hydrogen and R5 is hydroxy in the trans position with respect to R3 , or R4 and R5 together represent an additional bond as indicated by the dotted line, R6 and R are, independently, Ci-salkyl, and R8 is hydrogen or Cι_5alkyl, or N-oxide thereof; or physiologically-hydrolysable and -acceptable ester of such a compound or N-oxide, or acid addition or quarternary ammonium salt of such a compound, N-oxide or ester.
3. A compound of formula I as illustrated in claim 1 wherein:
R4 is hydrogen, R5 is hydroxy in the trans position with respect to R3 , R6 and R7 are each methyl and
A) R3 is a group of formula
Figure imgf000047_0002
and
A1) Ri is methyl, ethyl, n-propyl, i-butyl, hydroxymethyl or methoxymethyl and R2 and R8 are each hydrogen, or A2) Ri and R8 are each hydrogen and R2 is methyl, or A3) R and R8 are each methyl and R2 is hydrogen; or B) R3 is a group of formula
Figure imgf000048_0001
CO-NH- and
B1 ) Ri is methyl, ethyl, n-propyl, i-butyl or methoxy¬ methyl and R and R8 are each hydrogen, or B2 ) Ri and R8 are each hydrogen and R2 is methyl, or B3 ) Ri and R8 are each methyl and R8 is hydrogen; or
C) R3 is a group of formula
Figure imgf000048_0002
Ri is methyl and R2 and R8 are each hydrogen;
or wherein
Ri is methyl and R2 is hydrogen or Rj is hydrogen and R2 is methyl, R6 and R are each methyl, R8 is hydrogen, R4 and R5 together represent an additional bond and R3 is a group of formula
Figure imgf000048_0003
or N-oxide thereof; or physiologically-hydrolysable and -acceptable ester of such a compound or N-oxide or acid addition or quarternary ammonium salt of such a compound, N-oxide or ester.
A compound of formula I as illustrated in claim 1 wherein R , R6 and R are each methyl, R2 , R4 and R8 are each hydrogen R5 is hydroxy in the trans position with respect to R3 and R3 is a group of formula
Figure imgf000049_0001
or N-oxide thereof or acid addition salt of such a compound or N-oxide.
5. A trans-2,2-di (Ci-salkyl) -3, 4-dihydro-3-hydroxy-6-
- (pyridin-4-yl) -3H-l-benzopyran, N-oxide, ester or salt as claimed in claim 1 or compound of formula I as illustrated in claim 2 wherein R4 is hydrogen and R5 is hydroxy in the trans position with respect to R3 and Ri , R2 , R3 , R6 , R7 and R8 have the meanings given in claim 2 or N-oxide, ester or salt thereof as defined in claim 2, in (3S,4R) enantiomeric form.
6. A compound as claimed in claim 4 in (3S,4R) enantiomeric form.
7. A process for the production of a benzopyran, N-oxide, ester or salt as claimed in claim 1 which process comprises:
i) for the production of a benzopyran as aforesaid:
i1 ) reacting a la, 7b-dihydro-2,2-di (Ci_5alkyl) -6- (pyridin- -4-yl) -2H-oxireno[c] [1]benzopyran wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two memebers selected from the group comprising Ci-salkyl, Cι_5hydroxyalkyl and Cι_5- (alkoxyalkyl) , with an alkali metal salt of a carboxamide; or i2 ) acylating and, when required, alkylating the amino group of a 2,2-di(Cι_5alkyl)- or trans-2, 2-di (Cι_5al yl) - 3, 4-dihydro-3-hydroxy- -4-amino-6- (pyridin-4-yl) - 2H-l-benzopyran wherein the pyridin-4-yl group is substituted at the 2- and/or 3-position by one or two members selected from the group comprising C _5alkyl, Ci_5hydroxyalkyl and Ci_5 (alkoxyalkyl) ;
ii) for the production of a benzopyran N-oxide or physiologically-hydrolysable and -acceptable ester of a benzopyran or benzopyran N-oxide as aforesaid, esterifying a benzopyran or benzopyran N-oxide as aforesaid having a free hydroxy group or moiety to introduce an appropriate ester grouping and/or oxidising a benzopyran or physiologically-hydrolysable and -acceptable ester thereof as aforesaid;
and recovering the obtained benzopyran, benzopyran N-oxide or physiologically-hydrolysable and -acceptable ester thereof in free or in acid addition or quarternary ammonium salt form.
8. A benzopyran, N-oxide, ester or pharmaceutically acceptable salt as claimed in claim 1 for use as a pharmaceutical.
9. A pharmaceutical composition comprising a benzopyran, N-oxide, ester or pharmacetically acceptable salt as claimed in claim 1 together with a pharmaceutically acceptable diluent or carrier therefor.
10. A method of treating obstructive or inflammatory airways disease in a subject in need thereof which method comprises administering to said subject an effective amount of a benzopyran, N-oxide, ester or pharmaceutically acceptable salt as claimed in claim 1.
PCT/EP1992/002719 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals WO1994012493A1 (en)

Priority Applications (10)

Application Number Priority Date Filing Date Title
EP92924604A EP0623129A1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals
CA002122494A CA2122494A1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1- benzopyrans
RU94035761A RU2104277C1 (en) 1992-11-25 1992-11-25 2,2-dialkyl or trans-2,2-dialkyl-3,4-dihydro-3-hydroxy-6- (pyridin-4-yl)-2h-1-benzopyrans
PL92304013A PL172371B1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1- bewnzopyranes
SK889-94A SK88994A3 (en) 1992-11-25 1992-11-25 2,2-dialkyl-2h-1-benzopyrans and 2,2-dialkyl-3,4-dihydro- -3-hydroxy-2h-1-benzopyrans
AU30826/92A AU665040B2 (en) 1992-11-25 1992-11-25 4-carboxamido-6(pyridin-4-yl substituted benzopyran derivatives
PCT/EP1992/002719 WO1994012493A1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals
TW081109738A TW223636B (en) 1992-11-25 1992-12-04
FI943489A FI943489A (en) 1992-11-25 1994-07-22 2,2-dialkyl and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2H-1-benzopyrans
NO942744A NO942744L (en) 1992-11-25 1994-07-22 2,2-dialkyl and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2H-1-benzopyrans

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
CA002122494A CA2122494A1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1- benzopyrans
PCT/EP1992/002719 WO1994012493A1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals

Publications (1)

Publication Number Publication Date
WO1994012493A1 true WO1994012493A1 (en) 1994-06-09

Family

ID=25677227

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/EP1992/002719 WO1994012493A1 (en) 1992-11-25 1992-11-25 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals

Country Status (1)

Country Link
WO (1) WO1994012493A1 (en)

Cited By (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO1998000412A1 (en) * 1996-07-01 1998-01-08 Schering Corporation Muscarinic antagonists
US5935958A (en) * 1996-07-01 1999-08-10 Schering Corporation Muscarinic antagonists
WO2002079195A1 (en) * 2001-03-30 2002-10-10 Bayer Aktiengesellschaft Substituted 2-thio-3,5-dicyano-4-phenyl-6-aminopyridines with adenosine receptor-binding activity and their use as cardiovascular preparations
EP1284141A2 (en) * 2001-08-15 2003-02-19 Pfizer Products Inc. Pharmaceutical combinations comprising neuronal nitric oxide synthase inhibitors for the treatment of neurodegenerative diseases
US20120238579A1 (en) * 2007-04-23 2012-09-20 Yevgeni Besidki New Compounds 806
US8642536B2 (en) 2008-10-17 2014-02-04 Wisconsin Alumni Research Foundation Method of making biologically active alpha-beta peptides

Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0346724A1 (en) * 1988-06-16 1989-12-20 MERCK PATENT GmbH Chroman derivates
EP0488301A1 (en) * 1990-11-28 1992-06-03 J. URIACH & CIA. S.A. New benzopyran compounds with pharmacological activity

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0346724A1 (en) * 1988-06-16 1989-12-20 MERCK PATENT GmbH Chroman derivates
EP0488301A1 (en) * 1990-11-28 1992-06-03 J. URIACH & CIA. S.A. New benzopyran compounds with pharmacological activity

Cited By (12)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO1998000412A1 (en) * 1996-07-01 1998-01-08 Schering Corporation Muscarinic antagonists
US5935958A (en) * 1996-07-01 1999-08-10 Schering Corporation Muscarinic antagonists
WO2002079195A1 (en) * 2001-03-30 2002-10-10 Bayer Aktiengesellschaft Substituted 2-thio-3,5-dicyano-4-phenyl-6-aminopyridines with adenosine receptor-binding activity and their use as cardiovascular preparations
EP1589013A2 (en) * 2001-03-30 2005-10-26 Bayer Health Care Aktiengesellschaft Substituted 2-thio-3,5-dicyano-4-phenyl-6-aminopyridines with adenosine receptor-binding activity and their use as cardiovascular preparations
EP1589013A3 (en) * 2001-03-30 2005-11-09 Bayer Health Care Aktiengesellschaft Substituted 2-thio-3,5-dicyano-4-phenyl-6-aminopyridines with adenosine receptor-binding activity and their use as cardiovascular preparations
US7078417B2 (en) 2001-03-30 2006-07-18 Bayer Aktiengesellschaft Substituted 2-thio-3,5-dicyano-4-phenyl-6-aminopyridines with adenosine receptor-binding activity and their use as cardiovascular preparations
EP1284141A2 (en) * 2001-08-15 2003-02-19 Pfizer Products Inc. Pharmaceutical combinations comprising neuronal nitric oxide synthase inhibitors for the treatment of neurodegenerative diseases
EP1284141A3 (en) * 2001-08-15 2003-07-30 Pfizer Products Inc. Pharmaceutical combinations comprising neuronal nitric oxide synthase inhibitors for the treatment of neurodegenerative diseases
US20120238579A1 (en) * 2007-04-23 2012-09-20 Yevgeni Besidki New Compounds 806
US8642536B2 (en) 2008-10-17 2014-02-04 Wisconsin Alumni Research Foundation Method of making biologically active alpha-beta peptides
US9416156B2 (en) 2008-10-17 2016-08-16 Wisconsin Alumni Research Foundation Method of making biologically active alpha-beta peptides
US10647743B2 (en) 2008-10-17 2020-05-12 Wisconsin Alumni Research Foundation Method of making biologically active alpha-beta peptides

Similar Documents

Publication Publication Date Title
US5177085A (en) Dihydro-isoquinoline derivatives, processes for their production, pharmaceutical compositions containing them, and their use in treating asthma
US5071871A (en) Pharmaceutically useful benzo(β)pyranes and pyranopyridines
US4980359A (en) Isoquinoline derivatives and their use
EP0258191A1 (en) Xanthine derivatives
US5905156A (en) Benzopyrans and pharmaceutical compositions containing them
JPH0730072B2 (en) Substituted 3,4-dihydro-2H-benzopyran
WO1994012493A1 (en) 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1-benzopyr ans, their use as pharmaceuticals
US5574049A (en) 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2H-1-benzopyrans
US5189047A (en) 2-oxo-1,2-(dihydropyridyl)-2h-1-benzopyrans
JP2005523324A (en) Compounds useful for the preparation of camptothecin derivatives
AU665040B2 (en) 4-carboxamido-6(pyridin-4-yl substituted benzopyran derivatives
NZ245321A (en) Substituted 6-(pyridin-4-yl)-2h-1-benzopyran derivatives and pharmaceutical compositions thereof
JP2583028B2 (en) 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2-H-1-benzopyrans
RU2104277C1 (en) 2,2-dialkyl or trans-2,2-dialkyl-3,4-dihydro-3-hydroxy-6- (pyridin-4-yl)-2h-1-benzopyrans
WO2000021957A1 (en) Benzopyrans having potassium channel opening activity
CZ282091B6 (en) 6-(pyridin-4-yl)-2h-1-benzopyrans, process of their preparation, pharmaceutical compositions containing thereof and their use
MXPA97009004A (en) Benzopira
PL172371B1 (en) 2,2-dialkyl- and 2,2-dialkyl-3,4-dihydro-3-hydroxy-2h-1- bewnzopyranes
JPS62273972A (en) Novel compound, its production and pharmaceutical composition containing the same

Legal Events

Date Code Title Description
WWE Wipo information: entry into national phase

Ref document number: 2122494

Country of ref document: CA

WWE Wipo information: entry into national phase

Ref document number: 1992924604

Country of ref document: EP

AK Designated states

Kind code of ref document: A1

Designated state(s): AU CA CS FI HU JP KR KZ NO PL RO RU US

AL Designated countries for regional patents

Kind code of ref document: A1

Designated state(s): AT BE CH DE DK ES FR GB GR IE IT LU MC NL PT SE

WWE Wipo information: entry into national phase

Ref document number: 94-01242

Country of ref document: RO

ENP Entry into the national phase

Ref document number: 1994 256803

Country of ref document: US

Date of ref document: 19940722

Kind code of ref document: A

WWE Wipo information: entry into national phase

Ref document number: 943489

Country of ref document: FI

Ref document number: 88994

Country of ref document: SK

Ref document number: PV1994-1767

Country of ref document: CZ

121 Ep: the epo has been informed by wipo that ep was designated in this application
WWP Wipo information: published in national office

Ref document number: 1992924604

Country of ref document: EP

WWP Wipo information: published in national office

Ref document number: PV1994-1767

Country of ref document: CZ

EX32 Extension under rule 32 effected after completion of technical preparation for international publication

Free format text: GE

WWG Wipo information: grant in national office

Ref document number: PV1994-1767

Country of ref document: CZ

WWW Wipo information: withdrawn in national office

Ref document number: 1992924604

Country of ref document: EP