New arylglycinamide derivatives, processes for the manufacture thereof and pharmaceutical compositions containing these compounds

Abstract
The invention relates to new arylglycinamide derivatives of general formula I 1
Description


[0001] The invention relates to new arylglycinamide derivatives of general formula I
3


[0002] and the pharmaceutically acceptable salts thereof, processes for preparing them and pharmaceutical compositions containing these compounds. The compounds are valuable neurokinin (tachykinin) antagonists.


[0003] The abbreviations used in the specification and claims are explained as follows:


[0004] CDI=Carbonyldiimidazole


[0005] DCCI=Dicyclohexylcarbodiimide


[0006] HOBt=1-Hydroxybenzotriazole


[0007] THF=Tetrahydrofuran


[0008] DMF=Dimethylformamide


[0009] RT=Room temperature


[0010] DMAP=4-Dimethylaminopyridine


[0011] TBTU=O-Benzotriazolyl-tetramethyluronium-tetrafluoroborate


[0012] In order to show the formulae, a simplified representation is used. In the representation of the compounds all CH3-substituents are represented by a single bond, and for example the following formula
4


[0013] The invention relates to new arylglycinamide derivatives of general formula I
5


[0014] or the pharmaceutically acceptable salts thereof, wherein


[0015] Ar denotes unsubstituted or mono- to penta-substituted phenyl, or unsubstituted or mono- or di-substituted naphthyl, [in which the substituents of the phenyl and naphthyl independently of each other denote halogen (F, Cl, Br, I), OH, (C1-4)alkyl, O—(C1-4)alkyl, CF3, OCF3 or NR9R10 (wherein R9 and R10 independently of each other denote H, methyl or acetyl)] or Ar is phenyl substituted by —OCH2O— or —O(CH2)2O—;


[0016] R1 and R2 together with the N to which they are bound form a ring of the formula
6


[0017] wherein


[0018] p is 2 or 3,


[0019] X denotes oxygen, N(CH2)nR6 or CR7R8, wherein


[0020] n is 0, 1 or 2,


[0021] R6 is (C3-7)cycloalkyl, phenyl or naphthyl, wherein the phenyl may be mono- to tri-substituted by halogen (F, Cl, Br, I), (C1-4)alkyl, O—(C1-4)alkyl, CF3, OCF3 or NR15R16 (wherein R15 and R16 independently of each other denote H, methyl or acetyl);


[0022] R7 and R8 have one of the following meanings:


[0023] a) R7 and R8 represent H if R3 is unsubstituted or substituted phenyl,


[0024] b) R7 is phenyl, phenyl substituted by 1 to 3 substituents [wherein the substituents independently of one another denote halogen (F, Cl, Br, I), (C1-4)alkyl, O—(C1-4)alkyl, CF3 or OCF3], piperidinyl, 1-methylpiperidinyl,
7


[0025]  if R8 is H, —CONH2, —NHC(O)CH3, —N(CH3)C(O)CH3, CN
8


[0026]  or —C(O)N((C1-3)alkyl)2


[0027] or


[0028] c) R7 and R8 together form the group
9


[0029] R3 denotes H, (C1-4) alkyl, unsubstituted or mono- to tri-substituted phenyl, wherein the substituents independently of one another represent halogen (F, Cl, Br, I), (C1-4)alkyl, O—(C1-4) alkyl, CF3, OCF3 or NR17R18 (wherein R17 and R18 independently of one another denote H, methyl or acetyl);


[0030] R4 denotes phenyl(C1-4)alkyl or naphthyl (C1-4)alkyl, wherein phenyl may be substituted by 1 to 3 substituents, wherein the substituents independently of one another are halogen (F, Cl, Br, I), (C1-4)alkyl, O—(C1-4)alkyl, CF3, OCF3 or NR19R20 (wherein R19 and R20 independently of one another denote H, methyl or acetyl);


[0031] and


[0032] R5 denotes H, (C1-4)alkyl, (C3-6)cycloalkyl, CH2COOH, —CH2C(O)NH2, —OH or phenyl(C1-4)alkyl.


[0033] The compounds according to the invention are valuable neurokinin (tachykinin) antagonists which have both substance P-antagonism and also neurokinin A- or neurokinin B-antagonistic properties. They are useful for the treatment and prevention of neurokinin-mediated diseases.


[0034] Compounds of general formula I may contain acid groups, chiefly carboxyl groups, and/or basic groups such as, for example, amino functions. Compounds of general formula I may therefore be obtained either as internal salts, as salts with pharmaceutically acceptable inorganic acids such as hydrochloric acid, sulphuric acid, phosphoric acid or sulphonic acid or organic acids (such as, for example, maleic acid, fumaric acid, citric acid, tartaric acid or acetic acid) or as salts with pharmaceutically acceptable bases such as alkali or alkaline earth metal hydroxides or carbonates, zinc or ammonium hydroxides or organic amines such as, for example, diethylamine, triethylamine or triethanolamine, etc.


[0035] The compounds according to the invention may occur as racemates but may also be obtained as pure enantiomers, i.e. in (R)- or (S)-form. They may also occur as diastereoisomers or mixtures thereof.


[0036] The preferred compounds of general formula I are those wherein


[0037] R1 and R2 together with the N to which they are bound form a 6-membered ring of the formula
10


[0038] wherein


[0039] X denotes N(CH2)nR6 or CR7R8,


[0040] wherein n, R6, R7 and R8 are defined as in claim 1.


[0041] Particular mention should be made of compounds of formula I wherein


[0042] X is N(CH2)nR6 wherein n is 0, 1 or 2 and R6 is (C3-7)cycloalkyl or phenyl, particularly those compounds wherein n is 0 and R6 is (C3-7)cycloalkyl, particularly those compounds wherein R6 is cyclobutyl or cyclohexyl.


[0043] Mention should also be made of compounds of formula I wherein


[0044] R7 and R8 have one of the following meanings:


[0045] a) R7 and R8 denote H when R3 is unsubstituted or substituted phenyl,


[0046] b) R7 is phenyl, piperidinyl
11


[0047]  if R8 is H, —CONH2, —NHC(O)CH3, —N(CH3)C(O)CH3 or CN,


[0048] or


[0049] c) R7 and R8 together form the group
12


[0050]  particularly those wherein


[0051] R7 and R8 have one of the following meanings:


[0052] a) R7 and R8 denote H when R3 is unsubstituted or substituted phenyl,


[0053] b) R7 is phenyl,
13


[0054]  when R8 is H, —CONH2 or CN,


[0055] or


[0056] c) R7 and R8 together form the group
14


[0057] The preferred compounds are those wherein


[0058] R7 denotes phenyl,
15


[0059] and R8 is H or CN, particularly those wherein R7 is pyridino and R8 is H.


[0060] Of the compounds defined above, the preferred ones are those wherein


[0061] Ar denotes unsubstituted or mono- or di-substituted phenyl, or unsubstituted naphthyl [wherein the substituents of the phenyl independently of one another are halogen (F, Cl, Br, I), OH, methyl, methoxy, CF3, OCF3 or dimethylamine] or Ar is phenyl substituted by —OCH2O—, this group connecting positions 2 and 3 or 3 and 4 of the phenyl, particularly those wherein


[0062] Ar denotes unsubstituted or mono- or di-substituted phenyl, or unsubstituted naphthyl [wherein the substituents of the phenyl independently of one another are halogen (F, Cl, Br), methoxy or CF3] or Ar is phenyl substituted by —OCH2O—, this group connecting positions 2 and 3 or 3 and 4 of the phenyl.


[0063] The preferred compounds are those wherein Ar is phenyl, 3,4-dichlorophenyl, 3,4-dimethoxyphenyl or 3,4-methylenedioxyphenyl.


[0064] Of the compounds defined above, particular mention should be made of those wherein R3 is phenyl or preferably H.


[0065] Of the compounds defined above, mention should also be made of those wherein


[0066] R4 denotes phenyl(C1-3)alkyl, wherein phenyl may be substituted by 1 or 2 substituents, the substituents independently of one another being halogen (F, Cl, Br, I), methyl, methoxy, CF3 or OCF3;


[0067] and


[0068] R5 denotes H, (C1-3)alkyl, CH2COOH, —CH2C(O)NH2 or phenethyl,


[0069] particularly those compounds wherein
16


[0070]  and R5 denotes H or CH3.


[0071] The following compounds are preferred:
17


[0072] The term naphthyl used above includes both 1-naphthyl and 2-naphthyl.


[0073] Test results for compounds according to the invention:


[0074] The receptor affinity for the NK1-receptor (substance P-receptor) is determined on human lymphoblastoma cells (IM-9) with cloned NK1-receptors, measuring the displacement of 125I-labelled substance P. The Ki-values thus obtained demonstrate the efficacy of the compounds:
1KiCompound of Example 3:1.4 nMCompound of Example 4:1.0 nMCompound of Example 5:1.3 nMCompound of Example 33:1.3 nMCompound of Example 45:1.6 nMCompound of Example 46:1.4 nMCompound of Example 52:1.1 nMCompound of Example 53:2.3 nMCompound of Example 58:6.4 nMCompound of Example 59:4.2 nMCompound of Example 65:9.2 nMCompound of Example 66:1.4 nMCompound of Example 68:1.5 nMCompound of Example 70:2.8 nMCompound of Example 71:2.1 nMCompound of Example 72:6.8 nMCompound of Example 73:1.7 nMCompound of Example 74:11.8 nM Compound of Example 75: 180 nM Compound of Example 76:7.0 nM


[0075] The compounds according to the invention are valuable neurokinin (tachykinin) antagonists which have, in particular, NK1-antagonism, but also NK2- and NK3-antagonistic properties.


[0076] The compounds according to the invention are valuable neurokinin (tachykinin) antagonists which have both substance P-antagonism and also neurokinin A- or neurokinin B-antagonistic properties. They are useful for the treatment and prevention of neurokinin-mediated diseases: treatment and prevention of inflammatory and allergic diseases of the respiratory tract, such as asthma, chronic bronchitis, emphysema, rhinitis or coughs, eye diseases such as conjunctivitis and iritis, skin diseases such as dermatitis in contact eczema, urticaria, psoriasis, sunburn, insect bites and stings, neurodermitis, itching and postherpetic pain,


[0077] diseases of the gastrointestinal tract such as gastric and duodenal ulcers, ulcerative colitis, Crohn's disease, irritable bowel, Hirschsprung's disease;


[0078] diseases of the joints such as rheumatoid arthritis, reactive arthritis and Reiter syndrome;


[0079] for treating diseases of the central nervous system such as dementia, Alzheimer's disease, schizophrenia, psychosis, depression, headaches (e.g. migraine or tension headaches) and epilepsy;


[0080] for the treatment of tumours, collagenosis, dysfunction of the urinary tract, haemorrhoids, nausea and vomiting, triggered for example by radiation or cytostatic therapy or motion and pain of all kinds.


[0081] The invention therefore also relates to the use of the compounds according to the invention as remedies and pharmaceutical preparations which contain these compounds. They are preferably for use in humans. The compounds according to the invention may be administered by intravenous, subcutaneous, intramuscular, intraperitoneal or intranasal route or by inhalation, by transdermal route, if desired with the aid of iontophoresis or enhancers known from the literature, and by oral route.


[0082] For parenteral administration, the compounds of formula I or the physiologically acceptable salts thereof, optionally with conventional substances such as solubilisers, emulsifiers or other adjuvants, may be made into solutions, suspensions or emulsions. Suitable solvents include, for example, water, physiological saline solutions or alcohols, e.g. ethanol, propanediol or glycerol, sugar solutions such as glucose or mannitol solutions or a mixture of various solvents.


[0083] In addition, the compounds may be administered by means of implants, e.g. of polylactide, polyglycolide or polyhydroxybutyric acid or by means of intranasal preparations.


[0084] The oral effectiveness of compounds of general formula I can be demonstrated using the following standard test:


[0085] Inhibition of the lowering of blood pressure caused by NK1 in anaesthetised guinea pigs.


[0086] Guinea pigs weighing 300-500 grams were anaesthetised with pentobarbital (50 mg/kg i.p.), intubated and mechanically ventilated with 10 ml of ambient air per kg of body weight at a rate of 60 breaths per minute. The blood pressure was measured in the blood flow through the carotid artery. In order to introduce substances intravenously, the jugular vein was cannulated.


[0087] By the intravenous administration of the NK1-agonist [βAla4, Sar9, Met(O2)11] SP(4-11) (0.2 μmol/kg) a brief lowering of the blood pressure was triggered which was repeated at 10 minute intervals by repeatedly giving the NK1-agonist.
18


[0088] The neurokinin-antagonist was then administered by intraduodenal route and at 10 minute intervals a lowering of blood pressure was induced by means of the NK1-agonist.


[0089] The inhibition of the lowering of blood pressure caused by the above-mentioned NK1-agonist was measured before and after treatment with the neurokinin-antagonist.


[0090] The compound of Example 5 yielded an ID50 of 1.4 mg/kg. (ID50 is the dose which inhibits the lowering of blood pressure caused by the NK1-agonist by 50%.)


[0091] The compounds according to the invention may be prepared by generally known methods.


[0092] The compounds may be prepared in various ways. The two commonest methods are shown in the following scheme:
19


[0093] Method A.


[0094] The carboxylic acid may be linked to the amine HN (R5) R4 in various ways. The usual methods are coupling methods such as those used in peptide chemistry. A coupling reagent such as TBTU, DCCI/HOBt, CDI, etc., is added to the coupling partners in an approximately equivalent amount. Suitable solvents are DMF, THF, CH2Cl2, CHCl3, acetonitrile or other inert solvents or mixtures thereof. The appropriate temperature range is between −50° C. and +120° C., preferably between 0° C. and 40° C.


[0095] The carboxylic acid may also initially be converted by means of SOCl2, SO2Cl2, PCl3, PCl5 or PBr3 or mixtures thereof, by known methods, into the corresponding acid halide which is subsequently reacted with the amine HN(R5)R4 in an inert solvent such as CH2Cl2, THF or dioxane at temperatures between −50° C. and +100° C., typically between 0° C. and 20° C.


[0096] Another alternative is to convert the carboxylic acid initially into the alkylester, usually the methylester, by known methods and then to react this ester with the amine HN(R5)R4 in an inert solvent such as DMF, dioxane or THF. The reaction temperatures are between 20° C. and 150° C., typically between 50° C. and 120° C. The reaction may also be carried out in a pressurised container.


[0097] Process B.


[0098] In this, the α-halo-arylacetamide derivative obtained according to known procedures is reacted with the amine R1(R2)NH, thereby generating hydrogen halide. In order to mop up the cleaved (or excess) hydrogen halide, inorganic bases are used such as K2CO3, NaHCO3 or CaCO3, or organic bases may be used such as triethylamine, Hünig base, pyridine or DMAP, or an excess of the amine R1(R2)NH may be used. DMF, THF, dioxane or other inert solvents are used. The temperature range for the reaction is from 0 to 100° C., typically from 10 to 80° C.


[0099] Process C.


[0100] The compounds according to the invention in which R5 is not H may also be prepared as follows: first of all, the corresponding compound in which R5 is H is synthesised according to process A or B. Then N-alkylation is carried out as follows in order to introduce alkyl, cycloalkyl or CH2COOH. The compound according to the invention wherein R5 is H is deprotonated with an equivalent quantity of NaH, NaNH2, KOH, NaOCH3 or some other strong base. Anhydrous inert solvents such as THF, dioxane or diethylether are used. Then the corresponding alkylating agent is added slowly in the form of the corresponding halide, tosylate or mesylate. The reaction is carried out in the temperature range from −50° C. to +100° C., typically between 0° C. and +50° C. The method is described in detail in Example 33.






EXAMPLE 1

[0101]

20






[0102] 1st Step:


[0103] 2.2 g of 1-cyclohexylpiperazine were dissolved in 150 ml of anhydrous DMF, mixed with 2 g of K2CO3, stirred at room temperature for 20 minutes and then cooled to 5° C. 2.7 g of methyl (R,S)-α-bromophenylacetic acid were added and the suspension was stirred overnight at RT. The precipitate was filtered off and the filtrate was evaporated down. The residue was taken up in ethyl acetate, extracted twice with 10% KHCO3 solution and once with saturated NaCl solution. The organic phase was dried over Na2SO4, filtered and evaporated down, and 3.7 g of (R,S)-1-cyclohexyl-4-(methyl 2-phenylacetate)-piperazine were obtained in the form of a yellow oil.


[0104] Yield: about 100%.


[0105] 2nd Step:


[0106] 2.3 g of the product of the first step were dissolved in 10 ml of methanol, mixed with 14 ml of 1N NaOH and the resulting emulsion was stirred overnight at room temperature. The clear reaction solution was neutralised by the addition of 14 ml of 1N HCl, evaporated to dryness, the residue was treated with isopropanol and the solid matter was collected by suction filtration. The filtrate was evaporated down and the residue was triturated again with isopropanol, the solid matter was suction filtered and combined with the solid obtained earlier. In this way, 1.6 g of (R,S)-1-cyclohexyl-4-(2-phenylacetic acid)-piperazine were obtained as a white solid.


[0107] Yield: 75%.


[0108] 3rd Step:


[0109] 0.6 g of the product of the second step, 0.48 g of 3,5-bis-(trifluoromethyl)-benzylamine and 0.32 g of HOBT were suspended in 60 ml of THF/CH2Cl2 (1:1) and adjusted to pH 8.5 by the addition of about 0.7 ml of Hünig base. 0.77 g of TBTU were added and the mixture was stirred overnight at room-temperature. The clear reaction solution was evaporated down in vacuo, the residue was taken up in CH2Cl2 and extracted twice with 10% KHSO4 solution, once with saturated NaCl solution, twice with 10% KHCO3 solution and once more with saturated NaCl solution. The organic phase was dried over Na2SO4, filtered and evaporated down, whereupon crystallisation took place. 0.685 g of (R,S)-1-cyclohexyl-piperazinyl-4-[2-phenylacetic acid-N-(3,5-bis-trifluoromethylbenzyl)amide] were obtained as a yellowish solid. Yield 64%.


[0110] Mp: 124-129° C. FAB-MS: (M+H)+=528.2.



EXAMPLE 2

[0111]

21






[0112] 1st Step:


[0113] 0.49 g of 3,5-bis-(trifluoromethyl)-benzylamine were dissolved in 30 ml of anhydrous CH2Cl2, 0.3 ml of triethylamine were added, the mixture was cooled in an ice bath and over 20 minutes a solution of 0.46 g of (R,S)-α-bromophenylacetyl chloride in 10 ml of CH2Cl2 was added dropwise. After the mixture had stood at room temperature over a weekend, the solvent was eliminated and the solid residue was triturated with diethylether, suction filtered and the filtrate was evaporated down. 0.6 g of α-bromophenylacetic acid N-(bis-trifluoromethyl-benzyl)-amide were obtained as a light beige solid.


[0114] Yield: 43.5%.


[0115] 2nd Step:


[0116] 0.21 g of 4-propionylamino-piperidine hydrochloride were dissolved in 30 ml of anhydrous DMF, 0.33 g of K2CO3 were added and the mixture was stirred for 30 minutes at room temperature. Over 20 minutes a solution of 0.68 g of the product of the first step in 10 ml of DMF were added dropwise to this mixture, which was then stirred overnight at room temperature. The suspension was filtered, the filtrate was evaporated down, the oily residue obtained was taken up in ethyl acetate, extracted twice with 10% KHCO3 solution and once with saturated NaCl solution. The organic phase was dried over Na2SO4, filtered, the filtrate was evaporated down and the semi-solid residue obtained was triturated with diethylether and suction filtered. 0.33 g of (R,S)-4-propionylamino-1-[2-phenylacetic acid-N(3,5-bis-trifluoromethyl-benzyl)-amide]-piperidine were obtained as a white solid.


[0117] Yield: 64%. Mp: 189-191° C.


[0118] FAB-MS: (M+H)+=516.4.



EXAMPLE 33

[0119]

22






[0120] Mp: >240° C.; FAB-MS: (M+H)+=556.4


[0121] 0.3 g of the compound according to Example 25 were converted into the corresponding base by treatment with KHCO3 and dried. The resulting product was dissolved in 5 ml of anhydrous THF, 34 mg of NaH (60% in oil) were added and the mixture was stirred for 1.5 hours at room temperature. Then 0.1 g of methyliodide were added and the mixture was stirred overnight. The reaction mixture was mixed with 2 ml of THF/water (1:1) then with 25 ml of water and extracted 3 times with ether. The combined ether extracts were dried over Na2SO4 and evaporated down in vacuo, thereby obtained 170 mg of the desired compound in the form of a free base (oil). This was converted into the dihydrochloride by the addition of an excess of ethereal HCl, the dihydrochloride being obtained in the form of yellow crystals.


[0122] Yield: 113 mg (36%).


[0123] The other compounds of the invention may be prepared analogously, e.g. as follows:



EXAMPLE 3

[0124]

23






[0125] Mp: 235-238° C. FAB-MS: (M+H)+=542.2.



EXAMPLE 4

[0126]

24






[0127] Mp: >240° C. (Decomp.). FAB-MS: (M+H)+=542.3.



EXAMPLE 5

[0128]

25






[0129] Mp: 158-164° C.; FAB-MS: (M+H)+=556.4.



EXAMPLE 6

[0130]

26






[0131] Mp: 97-99° C.; FAB-MS: (M+H)+=556.3.



EXAMPLE 7

[0132]

27






[0133] Mp: >240° (Decomp.); FAB-MS: (M+H)+=528.4.



EXAMPLE 8

[0134]

28






[0135] Mp: 102105° C.; FAB-MS: (M+H)+=640.3.



EXAMPLE 9

[0136]

29






[0137] Mp: 141-149° C.; FAB-MS: (M+H)+=579.2.



EXAMPLE 10

[0138]

30






[0139] Mp: 218-223° C.; FAB-MS: (M+H)+=579.3.



EXAMPLE 11

[0140]

31






[0141] Mp: >220° (Decomp.); FAB-MS (M+H)+=571.3



EXAMPLE 12

[0142]

32






[0143] Mp: 205-210° C.; FAB-MS: (M+H)+=591.3.



EXAMPLE 13

[0144]

33






[0145] Mp: 87-95° C.; FAB-MS: (M+H)+=571.2



EXAMPLE 14

[0146]

34






[0147] Mp: 164166° C.; FAB-MS: (M+H)+=537.3.



EXAMPLE 15

[0148]

35






[0149] Mp: 208-210° C.; FAB-MS: (M+H)+=578.3.



EXAMPLE 16

[0150]

36







EXAMPLE 17

[0151]

37







EXAMPLE 18

[0152]

38







EXAMPLE 19

[0153]

39







EXAMPLE 20

[0154]

40







EXAMPLE 21

[0155]

41







EXAMPLE 22

[0156]

42







EXAMPLE 23

[0157]

43







EXAMPLE 24

[0158]

44







EXAMPLE 25

[0159]

45







EXAMPLE 26

[0160]

46







EXAMPLE 27

[0161]

47







EXAMPLE 28

[0162]

48







EXAMPLE 29

[0163]

49







EXAMPLE 30

[0164]

50







EXAMPLE 31

[0165]

51







EXAMPLE 32

[0166]

52







EXAMPLE 33

[0167]

53







EXAMPLE 34

[0168]

54







EXAMPLE 35

[0169]

55







EXAMPLE 36

[0170]

56







EXAMPLE 37

[0171]

57







EXAMPLE 38

[0172]

58







EXAMPLE 39

[0173]

59







EXAMPLE 40

[0174]

60







EXAMPLE 41

[0175]

61







EXAMPLE 42

[0176]

62







EXAMPLE 43

[0177]

63







EXAMPLE 44

[0178]

64







EXAMPLE 45

[0179]

65







EXAMPLE 46

[0180]

66







EXAMPLE 47

[0181]

67







EXAMPLE 48

[0182]

68







EXAMPLE 49

[0183]

69







EXAMPLE 50

[0184]

70







EXAMPLE 51

[0185]

71







EXAMPLE 52

[0186]

72







EXAMPLE 53

[0187]

73







EXAMPLE 54

[0188]

74







EXAMPLE 55

[0189]

75







EXAMPLE 56

[0190]

76







EXAMPLE 57

[0191]

77







EXAMPLE 58

[0192]

78







EXAMPLE 59

[0193]

79







EXAMPLE 60

[0194]

80







EXAMPLE 61

[0195]

81







EXAMPLE 62

[0196]

82







EXAMPLE 63

[0197]

83







EXAMPLE 64

[0198]

84







EXAMPLE 65

[0199]

85







EXAMPLE 66

[0200]

86







EXAMPLE 67

[0201]

87







EXAMPLE 68

[0202]

88







EXAMPLE 69

[0203]

89







EXAMPLE 70

[0204]

90







EXAMPLE 71

[0205]

91







EXAMPLE 72

[0206]

92







EXAMPLE 73

[0207]

93







EXAMPLE 74

[0208]

94







EXAMPLE 75

[0209]

95







EXAMPLE 76

[0210]

96







EXAMPLE 77

[0211]

97







EXAMPLE 78

[0212]

98





2













Injectable solution









200 mg
of active substance*






1.2 mg

of monopotassium dihydrogen phospate = KH2PO4
)





0.2 mg

of disodium hydrogen phosphate =
) (buffer)



NaH2PO4.2H2O
)










 94 mg
of sodium chloride
)



or

)
(isotonic)


520 mg
of glucose
)


 4 mg
of albumin

(protease protection)










q.s.
     sodium hydroxide solution
)



q.s.
     hydrochloric acid
)
to adjust the pH





to pH 6







sufficient water to make a 10 ml solution for injection


Injectable solution









200 mg
of active substance*



 94 mg
of sodium chloride


or


520 mg
of glucose










 4 mg
     of albumin




q.s.
     sodium hydroxide solution
)


q.s.
     hydrochloric acid
)
to adjust the pH





to pH 9







sufficient water to make a 10 ml solution for injections


Lyophilisate








200 mg
of active substance*


520 mg
of mannitol (isotonic/structural component)


 4 mg
of albumin







Solvent 1 for lyophilisate








 10 ml
of water for injections







Solvent 2 for lyophilisate








 20 mg
of Polysorbate ®80 = Tween ®80



(surfactant


 10 ml
of water for injections






*Active substance: compound according to the invention, e.g. that of Examples 1 to 78.




Dosage for humans weighing 67 kg: 1 to 500 mg








Claims
  • 1. Arylglycinamide derivatives of general formula I
  • 2. Compounds according to claim 1, wherein R1 and R2 together with the N to which they are bound form a 6-membered ring of formula 104wherein X denotes N(CH2)nR6 or CR7R8, wherein n, R6, R7 and R8 are defined as in claim 1.
  • 3. Compounds according to claim 2, wherein X is N(CH2)nR6, wherein n is 0, 1 or 2 and R6 is (C3-7)cycloalkyl or phenyl.
  • 4. Compounds according to claim 3, wherein n is O and R6 is (C3-7) cycloalkyl.
  • 5. Compounds according to claim 4, wherein R6 is cyclobutyl or cyclohexyl.
  • 6. Compounds according to claim 2, wherein X is CR7R8, wherein R7 and R8 have one of the following meanings: a) R7 and R8 denote H when R3 is unsubstituted or substituted phenyl, b) R7 is phenyl, piperidinyl 105 if R8 is H, —CONH2, —NHC(O)CH3, —N(CH3)C(O)CH3 or CN or c) R7 and R8 together form the group 106
  • 7. Compounds according to claim 6, wherein R7 and R8 have one of the following meanings: a) R7 and R8 denote H when R3 is unsubstituted or substituted phenyl, b) R7 is phenyl, 107 when R8 is H, —CONH2 or CN, or c) R7 and R8 together form the group 108
  • 8. Compounds according to claim 7, wherein R7 is phenyl, 109and R8 is H or CN.
  • 9. Compounds according to claim 8, wherein R7 is pyridino and R8 is H.
  • 10. Compounds according to one of claims 1 to 9, wherein Ar denotes unsubstituted or mono- or di-substituted phenyl, or unsubstituted naphthyl [wherein the substituents of the phenyl independently of one another are halogen (F, Cl, Br, I), OH, methyl, methoxy, CF3, OCF3 or dimethylamine] or Ar is phenyl substituted by —OCH2O—, this group connecting positions 2 and 3 or 3 and 4 of the phenyl.
  • 11. Compounds according to claim 10, wherein Ar denotes unsubstituted or mono- or di-substituted phenyl, or unsubstituted naphthyl [wherein the substituents of the phenyl independently of one another are halogen (F, Cl, Br), methoxy or CF3] or Ar is phenyl substituted by —OCH2O—, this group connecting positions 2 and 3 or 3 and 4 of the phenyl.
  • 12. Compounds according to claim 11, wherein Ar is phenyl, 3,4-dichlorophenyl, 3,4-dimethoxyphenyl or 3,4-methylenedioxyphenyl.
  • 13. Compounds according to one of claims 1 to 12, wherein R3 is H.
  • 14. Compounds according to one of claims 1 to 12, wherein R3 is phenyl.
  • 15. Compounds according to one of claims 1 to 14, wherein R4 denotes phenyl(C1-3)alkyl, wherein phenyl may be substituted by 1 or 2 substituents, the substituents independently of one another being halogen (F, Cl, Br, I), methyl, methoxy, CF3 or OCF3; and R5 denotes H, (C1-3)alkyl, CH2COOH, —CH2C(O)NH2 or phenethyl.
  • 16. Compounds according to claim 15, wherein R4 is 110and R5 is H or CH3.
  • 17. Compounds according to claim 1 which are
  • 18. Process for preparing a compound of general formula I according to one of claims 1 to 17, characterised in that a) an acid 112 or a halide or alkylester thereof is reacted with an amine 113b) an α-haloarylacetamide 114 is reacted with an amine 115c) a compound I wherein R5 is H is N-alkylated; and a compound thus obtained is isolated as a free compound or as a pharmaceutically acceptable salt thereof.
  • 19. Pharmaceutical preparation containing a compound according to one of claims 1 to 17.
  • 20. Use of a compound according to one of claims 1 to 17 for preparing a pharmaceutical preparation for the treatment and prevention of neurokinin-mediated diseases.
  • 21. Use of a compound according to one of claims 1 to 17 for the treatment and prevention of neurokinin-mediated diseases.
Priority Claims (2)
Number Date Country Kind
195 14 112.1 Apr 1995 DE
195 19 245.1 May 1995 DE
Divisions (3)
Number Date Country
Parent 09752730 Jan 2001 US
Child 09971358 Oct 2001 US
Parent 09507581 Feb 2000 US
Child 09752730 Jan 2001 US
Parent 08930704 Oct 1997 US
Child 09507581 Feb 2000 US