AZ AB I C YCLO [3 . 1 . 0] HEXANE DERIVATIVES AS MODULATORS OF DOPAMINE D3 RECEPTORS-

The present invention relates to novel compounds, processes for their preparation, intermediates used in these processes, pharmaceutical compositions containing them and 5 their use in therapy, as modulators of dopamine D ₃ receptors.

Recently a patent application has been published as WO2005/080382 and discloses the compounds of the following formula or salts thereof:

0 wherein

• G is selected from a group consisting of: phenyl, pyridyl, benzothiazolyl, indazolyl;

• p is an integer ranging from 0 to 5;

• R ₁ is independently selected from a group consisting of: halogen, hydroxy, cyano, 5 C _1-4 alkyl, haloC _1-4 alkyl, C _1-4 alkoxy, haloC _1-4 alkoxy, C^alkanoyl; or corresponds to a group

R ₅ ;

• R ₂ is hydrogen or C _1-4 alkyl;

• R ₃ is C _1-4 alkyl;

• R ₄ is hydrogen, or a phenyl group, a heterocyclyl group, a 5- or 6-membered 0 heteroaromatic group, or a 8- to 11-membered bicyclic group, any of which groups is optionally substituted by 1 , 2, 3 or 4 substituents selected from the group consisting of: halogen, cyano, C _1-4 alkyl, haloC^alkyl, C^alkoxy, C _1-4 alkanoyl;

• R ₅ is a moiety selected from the group consisting of: isoxazolyl, -CH ₂ -N-pyrrolyl, 1 , 1 -dioxido-2-isothiazolidinyl, thienyl, thiazolyl, pyridyl, 2-pyrrolidinonyl, and such a group 5 is optionally substituted by one or two substituents selected from: halogen, cyano, C _{1- 4} alkyl, haloC^alkyl, C _1-4 alkoxy, C^alkanoyl; and when R ₁ is chlorine and p is 1 , such R ₁ is not present in the ortho position with respect to the linking bond to the rest of the molecule; and when R ₁ corresponds to R ₅ , p is 1.

A new class of compounds which have affinity for dopamine receptors, in particular the dopamine D ₃ receptor has been found. These compounds have potential in the treatment of conditions wherein modulation, especially antagonism/inhibition, of the D ₃ receptor is beneficial, e.g. to treat drug dependency or as antipsychotic agents.

The present invention provides a compound of formula (I) or a pharmaceutically acceptable salt thereof:

wherein

• G is selected from a group consisting of: phenyl, a 5- or 6-membered monocyclic heteroaryl group, or a 8- to 11-membered heteroaryl bicyclic group;

• p is an integer ranging from 0 to 5; • R ₁ is halogen, hydroxy, cyano, C _1-4 alkyl, haloCi _-4 alkyl, C _1-4 alkoxy, haloC _1-4 alkoxy,

Ci _-4 alkanoyl and SF ₅ ; or corresponds to a group R ₈ ; and when p is an integer ranging from 2 to 5, each R ₁ may be the same or different;

• R ₂ is hydrogen or C _1-4 alkyl;

• n is 3, 4, 5 or 6; • R ₃ is selected in the group consisting of: hydrogen, halogen, hydroxy, cyano, C _1-

₄ alkyl, C _3-7 cycloalkyl, haloC _1-4 alkyl, C ₁ ^aIkOXy, haloCi_ ₄ alkoxy, C _1-4 alkanoyl and NR'R"; or R ₃ is a phenyl group, a 5-14 membered heterocyclic group; and any of such phenyl or heterocyclic group is optionally substituted by 1 , 2, 3 or 4 substituents selected from the group consisting of: halogen, cyano, C _1-4 alkyl, halod- ₄ alkyl, C _1-4 alkoxy, C _1-4 alkanoyl and SF ₅ ;

• R ₄ is selected in the group consisting of: hydrogen, halogen, hydroxy, cyano, C _{1- 4} alkyl, C _3-7 cycloalkyl, halod. ₄ alkyl, Ci_ ₄ alkoxy, haloC^alkoxy, C _1-4 alkanoyl and NR'R"; or R ₃ is a phenyl group, a 5-14 membered heterocyclic group; and any of such phenyl or

heterocyclic group is optionally substituted by 1 , 2, 3 or 4 substituents selected from the group consisting of: halogen, cyano, C _1-4 alkyl, haloC^alkyl, C _1-4 alkoxy, C ₁ _ ₄ alkanoyl and SF ₅ ;

• R ₅ is selected in the group consisting of: hydrogen, halogen, hydroxy, cyano, Ci_ ₄ alkyl, C ₃ -7 cycloalkyl, haloC _1-4 alkyl, d. ₄ alkoxy, haloC _1-4 alkoxy, C^alkanoyl and NR'R"; or

R ₃ is a phenyl group, a 5-14 membered heterocyclic group; and any of such phenyl or heterocyclic group is optionally substituted by 1 , 2, 3 or 4 substituents selected from the group consisting of: halogen, cyano, C _1-4 alkyl, haloC _1-4 alkyl, C _1-4 alkoxy, C^alkanoyl and SF ₅ ; • R ₆ is selected in the group consisting of: hydrogen, halogen, hydroxy, cyano, C ₁ .

₄ alkyl, C ₃ - ₇ cycloalkyl, and NR'R"; or R ₃ is a phenyl group, a 5-14 membered heterocyclic group; and any of such phenyl or heterocyclic group is optionally substituted by 1 , 2, 3 or 4 substituents selected from the group consisting of: halogen, cyano, C _1-4 alkyl, haloCi _-4 alkyl, C _1-4 alkoxy, C^alkanoyl and SF ₅ ;

• R ₇ is hydrogen or C _1-2 alkyl;

• R ₈ is a moiety selected from the group consisting of: isoxazolyl, -CH ₂ -N-pyrrolyl, 1 , 1 -dioxido-2-isothiazolidinyl, thienyl, thiazolyl, pyhdyl, 2-pyrrolidinonyl, and such R ₈ group is optionally substituted by one or two substituents selected from: halogen, cyano, C ₁ . ₄ alkyl, haloCi _-4 alkyl, C _1-4 alkoxy, C^alkanoyl;

• R' is H, C _1-4 alkyl or Ci. ₄ alkanoyl;

• R" is defined as R';

• R' and R" taken together with the interconnecting nitrogen atom may form a 5-, 6- membered saturated or unsaturated heterocyclic ring; wherein at least one of R ₃ , R ₄ , R ₆ and R ₅ is hydrogen; and wherein only one R ₂ group ma be different from hydrogen.

Because of the presence of the fused cyclopropane, compounds of formula (I) are believed to have a "cis" disposition of the substituents (both groups linked to the bicyclic ring system are on the same face of this bicyclic ring system).

In one embodiment of the present invention compounds of formula (I)' are provided which correspond to the compounds of formula (I), or salts thereof, having "cis" disposition, represented by the bold highlight of the bonds

wherein G, p, n, R ₁ , R ₂ , R ₃ , R ₄ , R ₅ , Re and R ₇ are defined as above for compounds of formula (I), or a salt thereof.

It will be appreciated that compounds of formula (I)' possess at least two chiral centres, namely at position 1 and 5 in the 3-azabιcyclo[3.1 0]hexane portion of the molecule. Because of the fixed cis disposition, the compounds may exist in two stereoisomers which are enantiomers with respect to the chiral centres in the cyclopropane. It will also be appreciated, in common with most biologically active molecules that the level of biological activity may vary between the individual stereoisomers of a given molecule. It is intended that the scope of the invention includes all individual stereoisomers (diastereoisomers and enantiomers) and all mixtures thereof, including but not limited to racemic mixtures, which demonstrate appropriate biological activity with reference to the procedures described herein.

In compounds of formula (I)' there are at least two chiral centres, which are located in the cyclopropane portion, as depicted below (the bold highlight of the bonds means the "cis" configuration); through optical resolution of a mixture containing the two stereoisomers which are enantiomers with respect to the chiral centres in the cyclopropane, single steroisomers of compounds of formula (I)' may be obtained as shown in the scheme below

Absolute configuration of chiral center at position named 1 and 5 may be assigned using Cahn-lngold-Prelog nomenclature based on groups' priorities.

In one embodiment of the present invention compounds of formula (IA) are provided that correspond to stereochemical isomers of compounds of formula (I)', enriched in configuration shown in the picture below at chiral centers at position named 1 and 5:

wherein G, p, n, R ₁ , R ₂ , R ₃ , R ₄ , Rs, R ₆ and R ₇ are defined as above for compounds of formula (I), or a salt thereof.

It is intended in the context of the present invention that stereochemical isomers of formula (IA) enriched in one configuration at centers named 1 and 5, correspond in one embodiment to at least 90% e.e. (enantiomeric excess). In another embodiment the isomers correspond to at least 95% e.e. In another embodiment the isomers correspond to at least 99% e.e.

In another embodiment of the present invention compounds of formula (IH) are provided that correspond to stereochemical isomers of compounds of formula (I)', enriched in configuration (1 S, 5R) or (1 R,5R)

wherein G, A, p, n, R ₁ , R _2, R ₃ , R ₄ , R ₅ and R ₆ are defined as above for compounds of formula (I) and R ₇ is hydrogen, or a salt thereof.

Different nomenclature for absolute configuration assigned to chiral center named 1 [(1 R) or (1S)] may be generated by different meanings for G group.

For example, when the group G is a phenyl group, absolute configuration nomenclature for compounds of formula (IH) is (1 S, 5R).

It is intended in the context of the present invention that stereochemical isomers enriched in configuration (1 S,5R) or (1 R.5R) of formula (IH) correspond in one embodiment to at least 90% e.e. (enantiomeric excess). In another embodiment the isomers correspond to at least 95% e.e. In another embodiment the isomers correspond to at least 99% e.e.

In another embodiment of the present invention the stereochemical isomers enriched in configuration (1 R.5S) are provided.

In another embodiment of the present invention compounds of formula (IL) are provided that correspond to stereochemical isomers of compounds of formula (I)', enriched in configuration shown in the picture below at chiral centers at position named 1 and 5:

wherein G, A, p, n, R ₁ , R ₂ , R ₃ , R ₄ , R ₅ ,Re and R ₇ are defined as above for compounds of formula (I), or a salt thereof.

The term 'C ₁ - ₄ alkyl' as used herein as a group or a part of the group refers to a linear or branched alkyl group containing from 1 to 4 carbon atoms; examples of such groups include methyl, ethyl, propyl, isopropyl, n-butyl, isobutyl, tert butyl.

The term 'C ₃ - ₇ cycloalkyl group' as used herein means a non aromatic monocyclic hydrocarbon ring of 3 to 7 carbon atom such as, for example, cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl or cycloheptyl; while unsaturated cycloalkyls include cyclopentenyl and cyclohexenyl, and the like.

The term 'C ₁ - ₄ alkoxy group' as used herein may be a linear or a branched chain alkoxy group, for example methoxy, ethoxy, propoxy, prop-2-oxy, butoxy, but-2-oxy or methylprop-2-oxy and the like.

The term 'C _T4 alkanoyl group' as used herein may be a linear or a branched chain alkanoyl group, for example acetyl, ethylcarbonyl, n-propylcarbonyl, /-propyl carbonyl, n- butylcarbonyl or f-butylcarbonyl and the like.

The term 'halogen' as used herein refers to a fluorine, chlorine, bromine or iodine atom.

The term 'halo C ₁ - ₄ alkyl' as used herein means an alkyl group having one or more carbon atoms and wherein at least one hydrogen atom is replaced with halogen such as for example a trifluoromethyl group and the like.

The term 'halo C _r4 alkoxy group' as used herein may be a Cr ₄ alkoxy group as defined before substituted with at least one halogen, preferably fluorine, such as OCHF ₂ , or OCF ₃ .

The term 'aryl' as used herein means an aromatic carbocyclic moiety such as phenyl, biphenyl or naphthyl.

The term '5,6-membered monocyclic heteroaryl' as used herein means an aromatic monocyclic heterocycle ring of 5 or 6 members and having at least one heteroatom selected from nitrogen, oxygen and sulfur, and containing at least 1 carbon atom.

Representative 5, 6 membered monocyclic heteroaryl groups include (but are not limited to): furyl, thiophenyl, pyrrolyl, pyridyl, oxazolyl, isooxazolyl, pyrazolyl, imidazolyl, thiazolyl, isothiazolyl, pyridazinyl, pyrimidinyl, pyrazinyl, triazinyl, triazolyl and tetrazolyl.

The term '8, 1 1 -membered bicyclic heteroaryl' as used herein means an aromatic bicyclic heterocycle ring of 8 to 11 members and having at least one heteroatom selected from nitrogen, oxygen and sulfur, and containing at least 1 carbon atom.

Representative 8, to 11 membered bicyclic heteroaryl groups include (but are not limited to): benzofuranyl, benzothiophenyl, indolyl, isoindolyl, azaindolyl, quinolinyl, isoquinolinyl, benzoxazolyl, benzimidazolyl, benzothiazolyl, quinazolinyl and phthalazinyl.

The term 5-14 membered heterocycle means a 5 to 7-membered monocyclic, or 7-to 14- membered polycyclic, heterocycle ring which is either saturated, unsaturated or aromatic, and which contains from 1 to 4 heteroatoms independently selected from nitrogen, oxygen and sulfur, and wherein the nitrogen and sulfur heteroatoms may be optionally oxidized, and the nitrogen heteroatom may be optionally quaternized, including bicyclic rings in which any of the above heterocycles are fused to a benzene ring as well as tricyclic (and higher) heterocyclic rings. The heterocycle may be attached via any heteroatom or carbon atom. Heterocycles include heteroaryls as defined above. Thus, in addition to the aromatic heteroaryls listed above, heterocycles also include (but are not limited to) morpholinyl, pyrrolidinonyl, pyrrolidinyl, piperidinyl, hydantoinyl, valerolactamyl, oxiranyl, oxetanyl, tetrahydrofuranyl, tetrahydropyranyl, tetrahydropyridinyl, tetrahydropyrimidinyl, tetrahydrothiophenyl, tetrahydrothiopyranyl, tetrahydropyrimidinyl, tetrahydrothiophenyl, tetrahydrothiopyranyl, and the like.

Any of these groups may be attached to the rest of the molecule at any suitable position.

As used herein, the term "salt" refers to any salt of a compound according to the present invention prepared from an inorganic or organic acid or base, quaternary ammonium salts and internally formed salts. Physiologically acceptable salts are particularly suitable for medical applications because of their greater aqueous solubility relative to the parent compounds. Such salts must clearly have a physiologically acceptable anion or cation. Suitably physiologically acceptable salts of the compounds of the present invention include acid addition salts formed with inorganic acids such as hydrochloric, hydrobromic, hydroiodic, phosphoric, metaphosphoric, nitric and sulfuric acids, and with organic acids, such as tartaric, acetic, trifluoroacetic, citric, malic, lactic, fumaric, benzoic, formic, propionic, glycolic, gluconic, maleic, succinic, camphorsulfuric, isothionic, mucic, gentisic, isonicotinic, saccharic, glucuronic, furoic, glutamic, ascorbic, anthranilic, salicylic, phenylacetic, mandelic, embonic (pamoic), methanesulfonic, ethanesulfonic, pantothenic, stearic, sulfinilic, alginic, galacturonic and arylsulfonic, for example benzenesulfonic and p-toluenesulfonic, acids; base addition salts formed with alkali metals and alkaline earth metals and organic bases such as N,N-dibenzylethylenediamine, chloroprocaine, choline, diethanolamine, ethylenediamine, meglumaine (N-methylglucamine), lysine and procaine; and internally formed salts. Salts having a non-physiologically acceptable anion or cation are within the scope of the invention as useful intermediates for the preparation of physiologically acceptable salts and/or for use in non-therapeutic, for example, in vitro, situations.

In one embodiment, R ₁ is halogen, cyano, acetyl, trifluoromethyl, trifluoromethoxy.

In one embodiment, R ₂ is hydrogen. In another embodiment R ₂ is C _1-4 alkyl (e.g. methyl).

In one embodiment R ₃ may be hydrogen, C _1-4 alkyl, haloC _1-4 alkyl, C^alkoxy, (IaIoC ₁ . ₄ alkoxy, C _1-4 alkanoyl or halogen.

In one embodiment R ₄ may be hydrogen, C ₁ . ₄ alkyl, haloC _1-4 alkyl, C ₁ ^aIkOXy, (IaIoC ₁ . ₄ alkoxy, C^alkanoyl or halogen.

In one embodiment R ₅ may be hydrogen, C _1-4 alkyl, haloC _1-4 alkyl, C ₁ ^aIkOXy, (IaIoC ₁ . ₄ alkoxy, C^alkanoyl or halogen.

In one embodiment R ₆ may be hydrogen, C _1-4 alkyl, haloC _1-4 alkyl, C _1-4 alkoxy, 1IaIoC _{1- 4} alkoxy, C^alkanoyl or halogen.

In one embodiment R ₇ is hydrogen or methyl.

In one embodiment, R ₈ is a group selected from: isoxazolyl, 2-pyrrolidinonyl, -CH ₂ -N- pyrrolyl, 1 , 1 -d ioxido-2-isothiazolidinyl , 2-thienyl, 2-pyridyl, 2-thiazolyl which is optionally substituted by one or two substituents selected from: halogen, cyano, C _1-2 alkyl (e.g. methyl), haloCi. ₂ alkyl (e.g. trifluoromethyl), C _1-2 alkoxy (e.g. methoxy), C _1-3 alkanoyl (e.g. acetyl).

In one embodiment, p is 0, 1 or 2.

In another embodiment p is 1.

In one embodiment n is 3 or 4.

In one embodiment, n is 3. In another embodiment n is 4.

In another embodiment Ri trifluoromethyl.

In another embodiment R ₂ is hydrogen.

In another embodiment R ₃ and R ₄ are hydrogen or methyl.

In one embodiment R ₃ is hydrogen, C _1-4 alkyl, cyano, C _1-4 alkoxy or an optionally substituted 5, 6 membered heteroaryl group.

In another embodiment R ₃ is hydrogen, methyl, optionally substituted pyridyl, optionally substituted pyrimidyl, methoxy or cyano.

In one embodiment R ₄ is hydrogen or methyl.

In another embodiment R ₅ and R ₆ are hydrogen.

In another embodiment R ₇ is hydrogen.

In another embodiment R ₈ is isoxazolyl, 2-pyrrolidinonyl, - 1 ,1-dioxido-2-isothiazolidinyl.

In one embodiment G is a phenyl group.

In one embodiment, a compound of formula (IB) or a salt thereof is provided, wherein R ₁ , p, n, R ₃ , R ₄ , R ₅ , R ₆ and R ₇ are as defined for formula (I):

In Formula (IB), in one embodiment, n may be 3 or 4, p is 1 , R ₁ is trifluoromethyl, R ₂ is hydrogen, R ₃ and R ₄ may be hydrogen or methyl, R ₅ and R ₆ are hydrogen and R ₇ is hydrogen.

In Formula (IB), in another embodiment, n may be 3 or 4, p is 1 , R ₁ is trifluoromethyl, R ₂ is hydrogen, R ₃ may be hydrogen, methyl, optionally substituted pyridyl, optionally substituted pyrimidyl, methoxy or cyano, R ₄ may be hydrogen or methyl, R ₅ and R ₆ are hydrogen and R ₇ is hydrogen.

The absolute configuration of the compounds of the present invention was may be assigned in agreement with the method described in the PCT International Publication WO2005/080382.

Further embodiments of the present invention are compounds of formula (IB)' which correspond to the stereochemical isomers of compounds of formula (IB) as defined above enriched in configuration (1S, 5R).

In one embodiment, a stereochemical isomer enriched in the (1 S.5R) configuration of formula (IB)' or a salt thereof is provided, wherein R ₁ , p, n, R ₃ , R ₄ , R ₅ , R ₆ and R ₇ are as defined for formula (I):

In Formula (IB)', in one embodiment, n may be 3 or 4, p is 1 , R ₁ is tπfluoromethyl, R ₂ is hydrogen, R ₃ and R ₄ may be hydrogen or methyl, R ₅ and R ₆ are hydrogen and R ₇ is hydrogen

In Formula (IB)', in another embodiment, n may be 3 or 4, p is 1 , R ₁ is trifluoromethyl, R ₂ is hydrogen, R ₃ may be hydrogen, methyl, optionally substituted pyridyl, optionally substituted pyπmidyl, methoxy or cyano, R ₄ may be hydrogen or methyl, R ₅ and R ₆ are hydrogen and R ₇ is hydrogen

Certain of the compounds of the invention may form acid addition salts with one or more equivalents of the acid The present invention includes within its scope all possible stoichiometric and non-stoichiometric forms

Pharmaceutical acceptable salts may also be prepared from other salts, including other pharmaceutically acceptable salts, of the compound of formula (I) using conventional methods

Those skilled in the art of organic chemistry will appreciate that many organic compounds can form complexes with solvents in which they are reacted or from which they are precipitated or crystallized These complexes are known as "solvates" For example, a complex with water is known as a "hydrate" Solvates of the compound of the invention are within the scope of the invention The compounds of formula (I) may readily be isolated in association with solvent molecules by crystallisation or evaporation of an appropriate solvent to give the corresponding solvates

In addition, prodrugs are also included within the context of this invention As used herein, the term "prodrug" means a compound which is converted within the body, e g by

hydrolysis in the blood, into its active form that has medical effects Pharmaceutically acceptable prodrugs are described in T Higuchi and V Stella, Prodrugs as Novel Delivery Systems, VoI 14 of the A C S Symposium Series, Edward B Roche, ed , Bioreversible Carriers in Drug Design, American Pharmaceutical Association and Pergamon Press, 1987, and in D Fleisher, S Ramon and H Barbra "Improved oral drug delivery solubility limitations overcome by the use of prodrugs", Advanced Drug Delivery Reviews (1996) 19(2) 115-130, each of which are incorporated herein by reference

Prodrugs are any covalently bonded carriers that release a compound of structure (I) in vivo when such prodrug is administered to a patient Prodrugs are generally prepared by modifying functional groups in a way such that the modification is cleaved, either by routine manipulation or in vivo, yielding the parent compound Prodrugs include, for example, compounds of this invention wherein hydroxy, amine or sulfhydryl groups are bonded to any group that, when administered to a patient, cleaves to form the hydroxy, amine or sulfhydryl groups Thus, representative examples of prodrugs include (but are not limited to) acetate, formate and benzoate derivatives of alcohol, sulfhydryl and amine functional groups of the compounds of structure (I) Further, in the case of a carboxylic acid (-COOH), esters may be employed, such as methyl esters, ethyl esters, and the like

Esters may be active in their own right and /or be hydrolysable under in vivo conditions in the human body Suitable pharmaceutically acceptable in vivo hydrolysable ester groups include those which break down readily in the human body to leave the parent acid or its salt

Furthermore, some of the crystalline forms of the compounds of structure (I) may exist as polymorphs, which are included in the present invention

Hereinafter, compounds of formula (I) and their pharmaceutically acceptable salts, solvates and prodrugs defined in any aspect of the invention (except intermediate compounds in chemical processes) are referred to as "compounds of the invention"

Those skilled in the art will appreciate that in the preparation of the compounds of the invention, it may be necessary and/or desirable to protect one or more sensitive groups in the molecule to prevent undesirable side reactions Suitable protecting groups for use according to the present invention are well known to those skilled in the art and may be used in a conventional manner See, for example, "Protective groups in organic synthesis"

by T. W. Greene and P. G. M. Wuts (John Wiley & sons 1991) or "Protecting Groups" by PJ. Kocienski (Georg Thieme Verlag 1994). Examples of suitable amino protecting groups include acyl type protecting groups (e.g. formyl, thfluoroacetyl, acetyl), aromatic urethane type protecting groups (e.g. benzyloxycarbonyl (Cbz) and substituted Cbz), aliphatic urethane protecting groups (e.g. 9-fluorenylmethoxycarbonyl (Fmoc), t- butyloxycarbonyl (Boc), isopropyloxycarbonyl, cyclohexyloxycarbonyl) and alkyl type protecting groups (e.g. benzyl, trityl, chlorotrityl). Examples of suitable oxygen protecting groups may include for example alky silyl groups, such as trimethylsilyl or tert- butyldimethylsilyl; alkyl ethers such as tetrahydropyranyl or tert-butyl; or esters such as acetate.

The present invention also includes isotopically-labelled compounds, which are identical to those recited in formula (I) and following, but for the fact that one or more atoms are replaced by an atom having an atomic mass or mass number different from the atomic mass or mass number usually found in nature. Examples of isotopes that can be incorporated into compounds of the invention and pharmaceutically acceptable salts thereof include isotopes of hydrogen, carbon, nitrogen, oxygen, phosphorous, sulphur, riuorine, iodine, and chlorine, such as ² H, ³ H, ¹¹ C, ¹³ C, ¹⁴ C, ¹⁵ N, ¹⁷ O, ¹⁸ 0, ³¹ P, ³² P, ³⁵ S, ¹⁸ F, ³⁶ CI, ¹²³ I and ¹²⁵ I.

Compounds of the present invention and non-pharmaceutically acceptable salts thereof that contain the aforementioned isotopes and/or other isotopes of other atoms are within the scope of the present invention. Isotopically-labelled compounds of the present invention, for example those into which radioactive isotopes such as ³ H, ¹⁴ C are incorporated, are useful in drug and/or substrate tissue distribution assays. Tritiated, i.e., ³ H, and carbon-14, i.e., ¹⁴ C, isotopes are particularly preferred for their ease of preparation and detectability. ¹¹ C and ¹⁸ F isotopes are particularly useful in PET (positron emission tomography), and ¹²⁵ I isotopes are particularly useful in SPECT (single photon emission computerized tomography), all useful in brain imaging. Further, substitution with heavier isotopes such as deuterium, i.e., ² H, can afford certain therapeutic advantages resulting from greater metabolic stability, for example increased in vivo half-life or reduced dosage requirements and, hence, may be preferred in some circumstances, lsotopically labelled compounds of the present invention and non-pharmaceutically acceptable salts thereof can generally be prepared by carrying out the procedures disclosed in the

Schemes and/or in the Examples below, by substituting a readily available isotopically labelled reagent for a non-isotopically labelled reagent.

Certain groups/substituents included in the present invention may be present as isomers. The present invention includes within its scope all such isomers, including racemates, enantiomers, tautomers and mixtures thereof. Certain of the substituted heteroaromatic groups included in compounds of formula (I) may exist in one or more tautomeric forms.

The present invention includes within its scope all such tautomeric forms, including mixtures.

Example compounds of the invention include:

3-methyl-1-(4-{(1S,5R)-1-[4-(trifluoromethyl)phenyl]-3-az abicyclo[3.1.0]hex-3-yl}butyl)-

2(1 H)-pyridinone;

4-methyl-1 -(4-{(1 S,5R)-1 -^-(trifluorometriyOphenyO-S-azabicycloβ.1.0]hex-3-yl}butyl )- 2(1 H)-pyridinone; or a pharmaceutically acceptable salt thereof.

Further examples of the invention include:

6'-methyl-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)pheny|]-3-azabicyclo[3.1.0]hex-3 -yl}butyl)- 3,3'-bipyridin-2(1 H)-one;

2'-fluoro-1 -(4-{(1 S,5R)-1 -^(trifluoromethyOphenyO-S-azabicyclop.1.0]hex-3-yl}butyl)-3 ,4'- bipyridin-2(1 H)-one;

2'-fluoro-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex-3 -yl}butyl)-3,3'- bipyhdin-2(1 H)-one; 6'-fluoro-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex-3 -yl}butyl)-3,3 ¹ - bipyridin-2(1 H)-one;

3-(5-pyrimidinyl)-1 -(4-{(1 S,5R)-1 -[4-(trifluoromethyl)pheny|]-3-azabicyclo[3.1.0]hex-3- yl}butyl)-2(1 H)-pyhdinone;

3-(methyloxy)-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex-3 - yl}butyl)-2(1 H)-pyridinone;

2-0X0-1 -(4-{(1 S,5R)-1 -^-(trifluoromethyOphenyll-S-azabicyclo^.1.0]hex-3-yl}butyl) -1 ,2- dihydro-3-pyridinecarbonitrile;

3-methyl-1 -(4-{(1 S,5R)-1 -[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex-3-yl}but yl)-

2(1 H)-pyridinone;

4-methyl-1-(4-{(1 S,5f?)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex- 3-yl}butyl)- 2(1 H)-pyridinone;

3-methyl-1 -(3-{(1 S,5R)-1 -^-(trifluoromethyOphenyll-S-azabicyclofS.1.0]hex-3-yl}propy l)- 2(1 H)-pyridιnone; or a pharmaceutically acceptable salt thereof.

In another embodiment, the compounds of formula (I) are selected from the group consisting of hydrochloride salts, of the compounds listed below:

6'-methyl-1 -(4-{(1 S,5R)-1 -^-(trifluoromethyOphenyO-S-azabicycloβ.1.0]hex-3-yl}butyl) - 3,3'-bipyridin-2(1 H)-one;

2'-fluoro-1-(4-{(1 S,5R)-1-[4-(trιfluoromethyl)phenyl]-3-azabicyclo[3.1.0Jhex- 3-yl}butyl)-3,4'- bιpyridin-2(1 H)-one;

2'-fluoro-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0Jhex-3 -yl}butyl)-3,3'- bipyridin-2(1 H)-one, 6'-fluoro-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0Jhex-3 -yl}butyl)-3,3 ¹ - bipyridin-2(1 H)-one;

3-(5-pyrimidinyl)-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0Jhex-3 - yl}butyl)-2(1 H)-pyrιdιnone;

3-(methyloxy)-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex-3 - yl}butyl)-2(1 H)-pyrιdιnone;

2-0X0-1 -(4-{(1 S,5R)-1 -^-(trifluoromethyOphenyll-S-azabicyclotS.1.0]hex-3-yl}butyl )-1 ,2- dihydro-3-pyridinecarbonitπle;

3-methyl-1-(4-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex-3 -yl}butyl)-

2(1 H)-pyridιnone; 4-methyl-1-(4-{(1 S,5f?)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hex- 3-yl}butyl)-

2(1H)-pyridinone;

3-methyl-1-(3-{(1 S,5R)-1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1 0]hex-3-yl}propyl)-

2(1 H)-pyridinone.

Some of the compounds of the present invention may be prepared following some of the procedures described in PCT International Publication WO2005/080382.

The present invention also provides a process for preparing a compound of formula (I)' or a salt thereof as defined above, which comprises the steps of:

a) reacting a compound of formula (II):

wherein R ₁ , R ₇ and p are as defined for formula (I), with a compound of formula (III):

wherein R ₂ , R ₃ , R ₄ , R5, Re and n are as defined for formula (I) and X is a leaving group,

Or

b) reacting a compound of formula (II) as above defined:

with a compound of formula (IV)

wherein R ₂ , R ₃ , R ₄ , R5, Re and n are as defined for formula (I);

and thereafter optionally for process (a) or process (b): (i) removing any protecting group(s); and/or (ii) forming a salt; and/or

(iii) converting a compound of formula (I)' or a salt thereof to another compound of formula (I)' or a salt thereof.

Process (a) may be performed using conventional methods for the formation of a tertiary amine. The leaving group X can be halogen such as chlorine. Alternatively X can be a sulfonyloxy group such C^alkylsulfonyloxy (e.g. methanesulfonyloxy), C-\. 4alkylsulfonyloxy or haloC^alkylsulfonyloxy (e.g. trifluoromethanesulfonyloxy); or arylsulfonyloxy wherein aryl is optionally substituted phenyl, an optionally substituted 5- or 6- membered heteroaromatic group, or an optionally substituted bicyclic group, for example optionally substituted phenyl, wherein in each case the optional substituents are one or more C^alkyl groups; e.g. para-toluenesulfonyloxy. When X is a halogen the reaction may be carried out using a base such as potassium carbonate in the presence of a source of iodide such as sodium iodide in a solvent such as /V,/V-dimethylformamide at a suitable temperature, e.g. 60 ⁰ C.

Process (b) may be performed using conventional methods for the formation of a tertiary amine by means of reductive ammination. For example when, for compounds of formula (IV) R ₂ is hydrogen, the reaction may be carried out using sodium thacetoxy borohydride in a suitable solvent such as 1 ,2 dichloroethane at O ⁰ C.

In another embodiment the present invention provides a process for the preparation of compounds of formula (Ia), i.e. a compound of formula (I)' wherein p is 1 or 2 and one R ₁ is a group R _6, comprises the following steps:

c) reacting a compound of formula (V):

wherein R ₁ , and R ₇ are as defined for formula (I), Pg is a suitable amine protecting group such as for example tert-buthoxy carbonyl group, p is 0 or 1 and Y is halogen, a perfluoroalkylsulfonyloxy group (e.g. trifluoromethylsulfonyloxy), or Y is a group M selected from a boron derivative (e.g. a boronic acid function B(OH) ₂ ) or a metal function

such as trialkylstannyl (e.g. SnBu ₃ ), zinc halide or magnesium halide; with a compound of formula FVYi, wherein R ₆ is an optionally substituted isoxazolyl, thienyl, thiazolyl or pyridyl, group, Y ₁ is halogen when Y is a group M; or, when Y is halogen or a perfluoroalkylsulfonyloxy group, Y ₁ is a group M as defined above or hydrogen that can be activated by a suitable base (e.g. Cs ₂ CO ₃ ) in the presence of a suitable transition metal (e.g. Pd); "leaving group" is as understood by a skilled chemist, i.e. a group which can be displaced by a nucleophile in e.g. a S[sj2, S _[ \ _| 1 or SpgAr type reaction; to form a compound of formula (XXXIV)

wherein R ₁ , and R ₇ are as defined for formula (I), Pg is a suitable amine protecting group such as for example tert-buthoxy carbonyl group, p is 0 or 1 and R ₆ is an optionally substituted isoxazolyl, thienyl, thiazolyl or pyridyl, group;

d) removing the Pg group;

e) reacting the obtained product with a compound of formula (III) or (IV), as above defined, under the conditions described for processes a) or b);

and thereafter optionally:

(i) removing any protecting group(s); and/or

(ii) forming a salt; and/or

(iii) converting a compound of formula (Ia) or a salt thereof to another compound of formula (Ia) or a salt thereof.

Reaction of a compound of formula (V) with R ₁ -Y ₁ according to process (c) may be effected in the presence of a transition metal e.g., palladium catalyst such as bis- triphenylphosphinepalladium dichloride, tefr-a/c/s-triphenylphosphinepalladium (0) or the complex formed in situ from ths(dibenzylideneacetone) dipalladium(O) and 4,5- bis(diphenylphosphino)-9,9-dimethylxanthene. When M is a boronic acid function such as B(OH) ₂ the reaction may be carried out under basic conditions, for example using

aqueous sodium carbonate in a suitable solvent such as dioxane. When M is trialkylstannyl the reaction may be carried out in an inert solvent, such as xylene or dioxane optionally in the presence of LiCI. When M is a zinc or magnesium halide the reaction may be effected in an aprotic solvent such as tetrahydrofuran. When M is hydrogen that can be activated by a suitable base (e.g. Cs ₂ CO ₃ ) in the presence of a suitable transition metal (e.g. Pd) the reaction may be carried out in an inert solvent such as dioxane in the presence of a suitable base such as Cs ₂ CO ₃ . The substituent Y may be halogen such as bromine, or a sulfonyloxy group such as trifluoromethylsulfonyloxy; and Y ₁ is may be a group M, such as hydrogen that can be activated by a suitable base (e.g. Cs ₂ CO ₃ ) in the presence of a suitable transition metal (e.g. Pd).

Compounds of formula (II) may be prepared by methods well known in the art (e.g. J. Med. Chem. 1981 , 24, 481-490 or PCT International Publication WO2005/080382). Interconversion of groups Ri may be affected by methodology well known in the art (e.g. demethylation of a methoxy group resulting in a hydroxy group using a suitable Lewis acidic reagent such as boron tribromide in an inert solvent such as dichloromethane).

In one aspect of the present invention there is provided a process for the preparation of compounds of formula (Ha), i.e. a compound of general formula (II) wherein R ₇ is hydrogen and G is a phenyl ring and R ₁ is defined as for compounds of formula (I).

The process may be conveniently performed also for preparing compounds of formula (Mb), wherein the phenyl moiety of compound (Ma) is replaced by pyridine. This process comprises the following steps:

wherein: step(a') means diazotation of an aniline (Vl) followed by reaction with maleimide to give 3- arylmaleimide (VII); step (b ¹ ) means cycloropanation of (VII) to provide bicyclic imide (VIII); step (c ¹ ) means reduction of imide (VIII) to give compounds of formula (Ilia).

Step (a ¹ ) may be effected using conventional methods for the Meerwein reaction (e.g. J. Am. Chem. Soc. 1955, 77, 2313 describes the formation of arylmaleimides using this approach). Alternatively, in many cases this step is suitably performed applying a procedure where to a mixture of maleimide, an apropriate copper (II) salt such as anhydrous CuCI ₂ , and a suitable organonitrite, such as terf-butyl nitrite, in a compatible solvent, such as acetonitrile, is slowly added a solution of a compound of formula (Vl). This is followed by allowing time to react as appropriate and a suitable workup.

Step (b') consists of slow addition of a solution of purified compound of formula (VII), or mixtures containing a compound of formula (VII), dissolved in a suitable solvent such as dimethylsulfoxide, to a solution of trimethylsulfoxonium iodide in a suitable solvent such as

dimethylsulfoxide and a suitable base, such as sodium hydride. This is followed by allowing time to react as appropriate and a suitable workup.

Step (c ¹ ) can be performed using a suitable reducing agent in a compatible solvent, such as borane in tetrahydrofuran or Red-AI ^® in toluene at an appropriate temperature, such as for example 65 ⁰ C in the case of borane as the reducing agent. This is followed by a suitable workup.

In another aspect of the present invention an alternative synthetic process for the preparation of compounds of formula (II), is provided. This process comprises the following steps:

(IX) (X) (Xl)

(Xi) (M)

wherein: R ₁ , p and G are as defined for formula (I), R ₈ O is a suitable alkoxy group, PG is an appropriate protecting group and Y may be halogen such as bromine, or a sulfonyloxy group such as trifluoromethylsulfonyloxy and comprising the following steps: step (a") means coupling reaction of a (2,5-dihydro-1 H-pyrrol-3-yl)boronate (IX) with the aromatic halogen or sulfonyloxy derivative (X); step (b") means cycloropanation of (Xl) followed by, if appropriate, deprotection to provide bicyclic amine (II).

Step (a") may be effected using conventional methods for the Suzuki coupling, e.g. using tetrakis(triphenylphosphine)palladium(0) as the source of catalytic palladium(O) in the presence of cesium fluoride in an appropriate solvent such as tetrahydrofuran at a

suitable temperature. (R ₈ O) ₂ B may suitably be 4,4,5,5-tetramethyl-1 ,3,2-dioxaborolan-2-yl and PG benzyl, representing a compound of structure (X) as reported in Synlett 2002, 5, 829-831.

Step (b") consists of a cyclopropanation reaction effected for example using the reagent generated from trimethylsulfoxonium iodide and a suitable base such as sodium hydride. This is followed by a deprotection reaction.

In another aspect of the present invention there is provided a synthetic process for the preparation of compounds of formula (lie), i.e. compounds of general formula (II) wherein R ₇ is C _L2 alkyl and G is a phenyl group. This process comprises the following steps:

d"

wherein: step (a") means bromuration of compound (XV) to give compound (XVI); step (b") means reaction of compound (XVI) with a benzylic amine with a benzylic amine (susceptible to afford benzylic cleavage in acidic conditions) to give irriide (XVII); step (c") means coupling of compound (XVII) with an aryl boronic acid to give compound (XVIII); step (d") means removal of the benzylic protecting group of compound (XVIII) to give compound (XIX);

step (e") means cycloropanation of (XIX) to provide bicyclic imide (XX); step (f") means reduction of imide (XX) to give compounds of formula (lie).

Step (a") may be effected using bromine in the presence of AICI3, and heating the mixture at high temperature, suitably 120 ⁰ C.

Step (b") may be performed heating compound (XVI) together with an appropriate benzylic amine (suitably as 3,4-(dimethoxy)benzylamine or 2,4-(dimethoxy)benzylamine) in the presence of AcONa and AcOH.

Step (c") may be effected using conventional methods for the Suzuki coupling, e.g. using Pd(PPh ₃ ) ₂ CI ₂ as the source of catalytic palladium(O) in the presence of cesium fluoride, BnEt ₃ NCI and a generic arylboronic acid in an appropriate mixture of solvents, (such as toluene/H ₂ O 1 :1) at a suitable temperature (such as 90 ⁰ C).

Step (d") may be perfomed through an appropriate method for acidic cleavage of benzylic protecting group, such as one of those reported in "Protective groups in organic synthesis" by T.W. Greene and P. G. M. Wuts (John Wiley & sons 1991) or "Protecting Groups" by PJ. Kocienski (Georg Thieme Verlag 1994). Suitably, if the benzylic group is represented by 3,4-(dimethoxy)benzyl, protection may be removed through reaction of compound (XVIII) with TFA and anisole in the presence of sulforic acid.

Step (e") consists of slow addition of a solution of purified compound of formula (XIX), or mixtures containing a compound of formula (XIX), dissolved in a suitable solvent such as dimethylsulfoxide, to a solution of trimethylsulfoxonium iodide in a suitable solvent such as dimethylsulfoxide and a suitable base, such as sodium hydride. This is followed by allowing time to react as appropriate and a suitable workup.

Step (f) can be performed using a suitable reducing agent in a compatible solvent, such as borane in tetrahydrofuran or Red-AI ^® in toluene at an appropriate temperature, such as for example 65 ⁰ C in the case of borane as the reducing agent. This is followed by a suitable workup.

A compound of formula (III) may itself be prepared by reacting a compound of formula (XXI):

wherein R ₃ , R ₄ , R ₅ and R ₆ are as defined as for formula (I),, with a compound of formula (XIII):

L(CHR ₂ )n X (XIII)

wherein R ₂ is defined as for formula (I), X is as above defined and L is a leaving group.

The leaving group L can be halogen, such as chlorine. Alternatively L can be a sulfonyloxy group such C-|_4alkylsulfonyloxy (e.g. methanesulfonyloxy), C-μ 4alkylsulfonyloxy or haloC-|^alkylsulfonyloxy (e.g. trifluoromethanesulfonyloxy); or arylsulfonyloxy wherein aryl is optionally substituted phenyl, an optionally substituted 5- or 6- membered heteroaromatic group, or an optionally substituted bicyclic group, for example optionally substituted phenyl, wherein in each case the optional substituents are one or more C- _| _2alkyl groups; e.g. para-toluenesulfonyloxy. When L is a halogen the reaction may be carried out using a base such as potassium carbonate in the presence of a source of iodide such as sodium iodide in a solvent such as λ/,λ/-dimethylformamide at a suitable temperature, e.g. 60 ⁰ C.

A compound of formula (IV) may itself be prepared through the following steps:

f) reacting a compound of formula (XXI):

wherein R ₃ , R ₄ , R ₅ and R ₆ are as defined as for formula (I), with a compound of formula (XXII)

MCR ₂ (CHR ₂ V ₁ X (XXH)

wherein R ₂ is defined as for formula (I), X is as above defined and M is an appropriate carbonylic protecting group (for example dimethylacetale or dioxalane);

and then

g) cleavage of the protecting group.

Cleavage of the protecting group may be carried out under appropriate conditions known to the man skilled in the art. For example, when M is dimethylacetale, the cleavage may carried out by treatment with a diluted solution of hydrochloric acid in dioxane or methanol under gentle heating (e.g. 6O ⁰ C).

Compound of formula (III), as above defined, may be prepared through the following steps:

h) reacting a compound of formula (XXI), as above defined:

with a compound of formula (XXIII)

NCR ₂ (CHR ₂ ) _H-1 X (XXIII)

wherein R ₂ is defined as for formula (I), X is as above defined and N is a protected alcoholic function (for example: terbutyldimethylsilyl);

and then

i) cleavage of the protecting group under appropriate conditions known to the man skilled in the art and subsequent oxidation of the free alcoholic function obtained to carbonyl group.

For example when N is a terbutyl dimethyl silyl protecting group the cleavage can be performed by treatment with a 1 N solution of hydrochloric acid in dioxane at O ⁰ C for 1 hour. Appropriate conditions for the oxidation step comprise Dess- Martin periodinane mediated oxidation in dry THF as solvent at O ⁰ C for 1 hour.

Alternatively compounds of formula (Ilia), i.e. compounds of formula (III) wherein R ₃ is a 5,6-membered heteroaryl, may be prepared through the following steps:

m) reacting a compound of formula (XXIV)

wherein R ₄ , R ₅ and R ₆ are defined as for formula (I), with a compound of formula (XIII) under standard alkylation conditions

and then

n) coupling the obtained product of formula (XXV), wherein n, R ₄ , R ₅ and R ₆ are defined as for formula (I) and X is as above defined for compounds of formula (XIII),

with the appropriate heteroaryl boronic acid or ester.

Step (n) may suitably be performed using convential method for the Suzuky coupling , using for example Pd(OAc)2 as the source of catalytic palladium (0), in the presence of Na ₂ CO ₃ as base and a suitable heteroaryl boronic acid or boronic ester in an appropriate solvent, such as nPrOH.

Compounds of formula (XIII), (XXII) and (XXIII) are commercially available or may be prepared through reactions known in the literature.

Compounds of formula (XXI) are either commercially available or may be prepared through reactions known in the literature or through the procedures herebelow described.

Compounds of formula (Ic), i.e. compounds of formula (I) where R ₁ , R ₂ , R ₃ , R ₄ , R ₅ , R ₆ , R7, n, G and p are as above defined and A is a group P1 , may be prepared by reacting a compound of formula (XIV):

wherein R ₁ , R ₂ , R ₇ , G, n and p are as defined for formula (I) and X is a leaving group, with a compound of formula (XXI) as above defined:

A compound of formula (XIV) wherein R ₁ , R ₇ , G and p are as defined for formula (I), X is a leaving group and R ₂ is hydrogen and n is 3, can be prepared by alkylation of a compound of formula (II) in the presence of a suitable base such as a tertiary amine, for example diisopropylethylamine, with a propyl derivative carrying two leaving groups of preferrably differential reactivity in positions 1 and 3, for example 1-bromo-3- chloropropane.

Interconversion reactions between compounds of formula (I)' and salts thereof may be performed using methods well known in the art. Examples include: (i) converting one or more of R ₁ from alkoxy (e.g.methoxy) to hydroxy, (ii) converting one or more of Ri from hydroxy to sulfonyloxy, such as alkylsulfonyloxy or haloalkylsulfonyloxy, e.g. methanesulfonyloxy or alkylsulfonyloxy or trifluoro- methanesulfonyloxy,

(iii) converting one or more of R ₁ from halogen or perfluoroalkylsulfonyloxy to cyano; and optionally thereafter forming a salt of formula (I)'.

When a specific enantiomer or diastereoisomer of a compound of formula (I) or salts thereof, is required, this may be obtained for example by resolution of a corresponding enantiomeric or diastereosiomeric mixture using conventional methods. Thus, for example, specific enantiomers or diastereoisomers of the compounds may be obtained from the corresponding enantiomeric or diastereoisomeric mixture using chiral chromatographic methods such as for example chiral HPLC.

Alternatively a specific enantiomer or diastereoisomer of a compound of general formula (I), or salts thereof, may be synthesised from the appropriate optically active intermediates using any of the general processes described herein.

Compounds of formula (I) or pharmaceutically acceptable salts thereof, have been found to exhibit affinity for dopamine receptors, in particular the D ₃ receptor, and are expected to be useful in the treatment of disease states which require modulation of such receptors, such as psychotic conditions.

Many of the compounds of formula (I) or pharmaceutically acceptable salts thereof have also been found to have greater affinity for dopamine D ₃ than for D ₂ receptors. The therapeutic effect of currently available antipsychotic agents (neuroleptics) is generally believed to be exerted via blockade of D ₂ receptors; however this mechanism is also thought to be responsible for undesirable extrapyramidal side effects (eps) associated with many neuroleptic agents. It has been suggested that blockade of the recently characterised dopamine D ₃ receptor may give rise to beneficial antipsychotic activity without significant eps. (see for example Sokoloff et al, Nature, 1990; 347: 146-151 ; and Schwartz et al, Clinical Neuropharmacology, VoI 16, No.4, 295-314, 1993). In one embodiment compounds of formula (I) or salts thereof are provided which have higher (e.g. >10x or >100x higher) affinity for dopamine D ₃ than dopamine D ₂ receptors (such affinity can be measured using standard methodology- see herein).

Compounds of the invention may suitably be used as selective modulators of D ₃ receptors.

From the localisation of D ₃ receptors, it could also be envisaged that the compounds could also have utility for the treatment of substance abuse where it has been suggested that D ₃ receptors are involved (e.g. see Levant, 1997, Pharmacol. Rev., 49, 231-252). Examples of such substance abuse include alcohol, cocaine, heroin and nicotine abuse. Other conditions which may be treated by the compounds include substance related disorders, dyskinetic disorders such as Parkinson's disease, neuroleptic-induced parkinsonism and tardive dyskinesias; depression; anxiety, cognitive impairment including memory disorders such as Alzheimers disease, sexual dysfunction, sleep disorders, emesis, amnesia, aggression, vertigo, dementia, circadian rhythm disorders and gastric motility disorders e.g. IBS.

A wide range of psychiatric and neuropsychiatric disorders appear to be related to Obsessive-Compulsive Disorder, and form a family of related disorders referred to as obsessive-compulsive (OC) spectrum disorders. The compounds of the invention may be used for the treatment of an obsessive-compulsive spectrum disorder, including somatoform disorders such as body dysmorphic disorder and hyperchondriasis, bulimia nervosa, anorexia nervosa, binge eating, paraphilia and nonparaphilic sexual addictions, Sydeham's chorea, torticollis, autism, compulsive hoarding, and movement disorders, including Tourette's syndrome. As used herein, the phrase "obsessive-compulsive spectrum disorder" is intended to include Obsessive- Compulsive Disorder.

The compounds of the invention are also useful for the treatment of premature ejaculation.

The terms describing the indications used herein are classified in the Diagnostic and Statistical Manual of Mental Disorders, 4th Edition, published by the American Psychiatric Association (DSM-IV) and/or the International Classification of Diseases, 10th Edition (ICD-10). The various subtypes of the disorders mentioned herein are contemplated as part of the present invention. Numbers in brackets after the listed diseases below refer to the classification code in DSM-IV.

The term "psychotic disorder" includes :

Schizophrenia including the subtypes Paranoid Type (295.30), Disorganised Type

(295.10), Catatonic Type (295.20), Undifferentiated Type (295.90) and Residual Type (295.60); Schizophreniform Disorder (295.40); Schizoaffective Disorder (295.70) including

the subtypes Bipolar Type and Depressive Type; Delusional Disorder (297.1 ) including the subtypes Erotomanic Type, Grandiose Type, Jealous Type, Persecutory Type, Somatic Type, Mixed Type and Unspecified Type; Brief Psychotic Disorder (298.8); Shared Psychotic Disorder (297.3); Psychotic Disorder Due to a General Medical Condition including the subtypes With Delusions and With Hallucinations; Substance- Induced Psychotic Disorder including the subtypes With Delusions (293.81 ) and With Hallucinations (293.82); and Psychotic Disorder Not Otherwise Specified (298.9).

The term "substance-related disorder" includes:

Substance-related disorders including Substance Use Disorders such as Substance Dependence, Substance Craving and Substance Abuse; Substance-Induced Disorders such as Substance Intoxication, Substance Withdrawal, Substance-Induced Delirium, Substance-Induced Persisting Dementia, Substance-Induced Persisting Amnestic Disorder, Substance-Induced Psychotic Disorder, Substance-Induced Mood Disorder, Substance-Induced Anxiety Disorder, Substance-Induced Sexual Dysfunction, Substance- Induced Sleep Disorder and Hallucinogen Persisting Perception Disorder (Flashbacks); Alcohol-Related Disorders such as Alcohol Dependence (303.90), Alcohol Abuse (305.00), Alcohol Intoxication (303.00), Alcohol Withdrawal (291.81 ), Alcohol Intoxication Delirium, Alcohol Withdrawal Delirium, Alcohol-Induced Persisting Dementia, Alcohol-Induced Persisting Amnestic Disorder, Alcohol-Induced Psychotic Disorder, Alcohol-Induced Mood Disorder, Alcohol-Induced Anxiety Disorder, Alcohol-Induced Sexual Dysfunction, Alcohol- Induced Sleep Disorder and Alcohol-Related Disorder Not Otherwise Specified (291.9); Amphetamine (or Amphetamine-I_ike)-Related Disorders such as Amphetamine Dependence (304.40), Amphetamine Abuse (305.70), Amphetamine Intoxication (292.89), Amphetamine Withdrawal (292.0), Amphetamine Intoxication Delirium, Amphetamine Induced Psychotic Disorder, Amphetamine-Induced Mood Disorder, Amphetamine- Induced Anxiety Disorder, Amphetamine-Induced Sexual Dysfunction, Amphetamine- Induced Sleep Disorder and Amphetamine-Related Disorder Not Otherwise Specified (292.9); Caffeine Related Disorders such as Caffeine Intoxication (305.90), Caffeine- Induced Anxiety Disorder, Caffeine-Induced Sleep Disorder and Caffeine-Related Disorder Not Otherwise Specified (292.9); Cannabis-Related Disorders such as Cannabis Dependence (304.30), Cannabis Abuse (305.20), Cannabis Intoxication (292.89), Cannabis Intoxication Delirium, Cannabis-lnduced Psychotic Disorder, Cannabis-lnduced Anxiety Disorder and Cannabis-Related Disorder Not Otherwise Specified (292.9);

Cocaine-Related Disorders such as Cocaine Dependence (304.20), Cocaine Abuse (305.60), Cocaine Intoxication (292.89), Cocaine Withdrawal (292.0), Cocaine Intoxication Delirium, Cocaine-Induced Psychotic Disorder, Cocaine-Induced Mood Disorder, Cocaine-Induced Anxiety Disorder, Cocaine-Induced Sexual Dysfunction, Cocaine- Induced Sleep Disorder and Cocaine-Related Disorder Not Otherwise Specified (292.9); Hallucinogen-Related Disorders such as Hallucinogen Dependence (304.50), Hallucinogen Abuse (305.30), Hallucinogen Intoxication (292.89), Hallucinogen Persisting Perception Disorder (Flashbacks) (292.89), Hallucinogen Intoxication Delirium, Hallucinogen-Induced Psychotic Disorder, Hallucinogen-Induced Mood Disorder, Hallucinogen-Induced Anxiety Disorder and Hallucinogen-Related Disorder Not Otherwise Specified (292.9); Inhalant-Related Disorders such as Inhalant Dependence (304.60), Inhalant Abuse (305.90), Inhalant Intoxication (292.89), Inhalant Intoxication Delirium, Inhalant-Induced Persisting Dementia, Inhalant-Induced Psychotic Disorder, Inhalant- Induced Mood Disorder, Inhalant-Induced Anxiety Disorder and Inhalant-Related Disorder Not Otherwise Specified (292.9); Nicotine-Related Disorders such as Nicotine Dependence (305.1 ), Nicotine Withdrawal (292.0) and Nicotine-Related Disorder Not Otherwise Specified (292.9); Opioid-Related Disorders such as Opioid Dependence (304.00), Opioid Abuse (305.50), Opioid Intoxication (292.89), Opioid Withdrawal (292.0), Opioid Intoxication Delirium, Opioid-lnduced Psychotic Disorder, Opioid-lnduced Mood Disorder, Opioid-lnduced Sexual Dysfunction, Opioid-lnduced Sleep Disorder and Opioid- Related Disorder Not Otherwise Specified (292.9); Phencyclidine (or Phencyclidine-Like)- Related Disorders such as Phencyclidine Dependence (304.60), Phencyclidine Abuse (305.90), Phencyclidine Intoxication (292.89), Phencyclidine Intoxication Delirium, Phencyclidine-lnduced Psychotic Disorder, Phencyclidine-lnduced Mood Disorder, Phencyclidine-lnduced Anxiety Disorder and Phencyclidine-Related Disorder Not Otherwise Specified (292.9); Sedative-, Hypnotic-, or Anxiolytic-Related Disorders such as Sedative, Hypnotic, or Anxiolytic Dependence (304.10), Sedative, Hypnotic, or Anxiolytic Abuse (305.40), Sedative, Hypnotic, or Anxiolytic Intoxication (292.89), Sedative, Hypnotic, or Anxiolytic Withdrawal (292.0), Sedative, Hypnotic, or Anxiolytic Intoxication Delirium, Sedative, Hypnotic, or Anxiolytic Withdrawal Delirium, Sedative-, Hypnotic-, or Anxiolytic-Persisting Dementia, Sedative-, Hypnotic-, or Anxiolytic- Persisting Amnestic Disorder, Sedative-, Hypnotic-, or Anxiolytic-lnduced Psychotic Disorder, Sedative-, Hypnotic-, or Anxiolytic-lnduced Mood Disorder, Sedative-, Hypnotic-, or Anxiolytic-lnduced Anxiety Disorder Sedative-, Hypnotic-, or Anxiolytic-lnduced Sexual Dysfunction, Sedative-, Hypnotic-, or Anxiolytic-lnduced Sleep Disorder and Sedative-,

Hypnotic-, or Anxiolytic-Related Disorder Not Otherwise Specified (292.9); Polysubstance- Related Disorder such as Polysubstance Dependence (304.80); and Other (or Unknown) Substance-Related Disorders such as Anabolic Steroids, Nitrate Inhalants and Nitrous Oxide.

Compounds of the invention may be useful for the treatment of cognition impairment.

The term "cognition impairment" includes cognition impairment in other diseases such as schizophrenia, bipolar disorder, depression, other psychiatric disorders and psychotic conditions associated with cognitive impairment, e.g. Alzheimer's disease.

In a further aspect therefore the present invention provides a method of treating a condition for which modulation of dopamine receptors (especially dopamine D ₃ receptors) is beneficial, which comprises administering to a mammal (e.g. human) in need thereof an effective amount of a compound of the invention.

Modulation, as used herein, especially refers to inhibition/antagonism (which may also translate into inverse agonism in constitutively active receptor systems).

In one embodiment, the condition is a substance-related disorder, a psychotic disorder, an obsessive compulsive spectrum disorder or premature ejaculation.

The invention also provides a compound of the invention for use in therapy.

The invention also provides a compound of the invention for use in the treatment of a condition in a mammal for which modulation of dopamine receptors (especially dopamine D ₃ receptors) is beneficial.

The invention also provides the use of a compound of the invention in the manufacture of a medicament for the treatment of a condition in a mammal for which modulation of dopamine receptors (especially dopamine D ₃ receptors) is beneficial.

In one embodiment, compounds of the invention are used in the treatment of psychoses such as schizophrenia, in the treatment of substance abuse, in the treatment of obsessive compulsive spectrum disorders, in the treatment of premature ejaculation.

Also provided is the use of a compound of the invention in the manufacture of a medicament for the treatment of a psychotic condition, substance abuse in a mammal, obsessive compulsive spectrum disorders, and premature ejaculation.

Also provided is a compound of the invention for use in the treatment of a psychotic condition (e.g. schizophrenia), substance abuse, obsessive compulsive spectrum disorders, and premature ejaculation in a mammal.

Also provided is a compound of the invention or for use as an active therapeutic substance in a mammal, e.g. for use in the treatment of any of the conditions described herein.

"Treatment" includes prophylaxis, where this is appropriate for the relevant condition(s).

For use in medicine, the compounds of the present invention are usually administered as a standard pharmaceutical composition. The present invention therefore provides in a further aspect a pharmaceutical composition comprising a compound of the invention and a pharmaceutically acceptable carrier. The pharmaceutical composition can be for use in the treatment of any of the conditions described herein.

Compound of the invention may be administered by any convenient method, for example by oral, parenteral (e.g. intravenous), buccal, sublingual, nasal, rectal or transdermal administration and the pharmaceutical compositions adapted accordingly.

Compound of the invention which are active when given orally can be formulated as liquids or solids, for example syrups, suspensions or emulsions, tablets, capsules and lozenges.

A liquid formulation will generally consist of a suspension or solution of the compound or pharmaceutically acceptable salt in a suitable liquid carrier(s) for example an aqueous solvent such as water, ethanol or glycerine, or a non-aqueous solvent, such as polyethylene glycol or an oil. The formulation may also contain a suspending agent, preservative, flavouring or colouring agent.

A composition in the form of a tablet can be prepared using any suitable pharmaceutical carrier(s) routinely used for preparing solid formulations. Examples of such carriers include magnesium stearate, starch, lactose, sucrose and cellulose.

A composition in the form of a capsule can be prepared using routine encapsulation procedures. For example, pellets containing the active ingredient can be prepared using standard carriers and then filled into a hard gelatin capsule; alternatively, a dispersion or suspension can be prepared using any suitable pharmaceutical carrier(s), for example aqueous gums, celluloses, silicates or oils and the dispersion or suspension then filled into a soft gelatin capsule.

Typical parenteral compositions consist of a solution or suspension of the compound or pharmaceutically acceptable salt in a sterile aqueous carrier or parenterally acceptable oil, for example polyethylene glycol, polyvinyl pyrrolidone, lecithin, arachis oil or sesame oil. Alternatively, the solution can be lyophilised and then reconstituted with a suitable solvent just prior to administration.

Compositions for nasal administration may conveniently be formulated as aerosols, drops, gels and powders. Aerosol formulations typically comprise a solution or Fine suspension of the active substance in a pharmaceutically acceptable aqueous or non-aqueous solvent and are usually presented in single or multidose quantities in sterile form in a sealed container, which can take the form of a cartridge or refill for use with an atomising device. Alternatively the sealed container may be a unitary dispensing device such as a single dose nasal inhaler or an aerosol dispenser fitted with a metering valve which is intended for disposal once the contents of the container have been exhausted. Where the dosage form comprises an aerosol dispenser, it will contain a propellant which can be a compressed gas such as compressed air or an organic propellant such as a fluoro- chlorohydrocarbon. The aerosol dosage forms can also take the form of a pump- atomiser.

Compositions suitable for buccal or sublingual administration include tablets, lozenges and pastilles, wherein the active ingredient is formulated with a carrier such as sugar and acacia, tragacanth, or gelatin and glycerin.

Compositions for rectal administration are conveniently in the form of suppositories containing a conventional suppository base such as cocoa butter.

Compositions suitable for transdermal administration include ointments, gels and patches.

In one embodiment, the composition is in unit dose form such as a tablet, capsule or ampoule.

Each dosage unit for oral administration contains for example from 1 to 250 mg (and for parenteral administration contains for example from 0.1 to 25 mg) of a compound of the invention calculated as the free base.

The compounds of the invention will normally be administered in a daily dosage regimen (for an adult patient) of, for example, an oral dose of between 1 mg and 500 mg, for example between 10 mg and 400 mg, e.g. between 10 and 250 mg or an intravenous, subcutaneous, or intramuscular dose of between 0.1 mg and 100 mg, for example between 0.1 mg and 50 mg, e.g. between 1 and 25 mg of the compound of the formula (I) or a pharmaceutically acceptable salt thereof calculated as the free base, the compound being administered 1 to 4 times per day. Suitably the compounds will be administered for a period of continuous therapy, for example for a week or more.

Biological Test Methods

Functional potency of compounds of this invention can be measured by the following GTPS scintillation proximity assay (GTPS-SPA). Cells used in the study are Chinese Hamster Ovary (CHO) Cells.

Cell Line CHO_D2 CHO_D3

Dopamine CHO D ₃ (Biocat no 1060) transduced with bacmam GO G-protein (Biocat no 97886)

All steps are performed at 4°C. Cell membranes are prepared as follows. Cell pellets are resuspended in 10 volumes of 5OmM HEPES, 1 mM EDTA pH 7.4, using KOH.

Cells are homogenised within a glass waring blender for 2 bursts of 15secs in 20OmIs of buffer (5OmM HEPES, 1mM leupeptin, 25μg/ml bacitracin, 1 mM EDTA, 1 mM PMSF, 2μM Pepstatin A), (the latter 2 reagents added as fresh x100 and x 500 stocks respectively in ethanol). The blender is plunged into ice for 5 mins after the first burst and 10-40 mins after the final burst to allow foam to dissipate. The material is then spun at 50Og for 20 mins and the supernatant spun for 36 mins at 48,00Og. The pellet is resuspended in the same buffer as above but without PMSF and Pepstatin A. The material is then forced through a 0.6mm needle, made up to the required volume, (usually x4 the volume of the original cell pellet), aliquoted and stored frozen at -80°c

The final top concentration of test drug is 3μM in the assay and 1 1 points serial dilution curves 1 :4 in 100% DMSO are carried out using a Biomek FX. The test drug at 1 % (0.5ul) total assay volume (TAV) is added to a solid, white Greiner polypropylene 384-well assay plate. 50%TAV (25μl) of precoupled (for 60 mins at RT) membranes, 5μg/well, and Wheatgerm Agglutinin Polystyrene Scintillation Proximity Assay beads (RPNQ0260, Amersham), 0.25rηg/well, in 2OmM HEPES (pH 7.4, 10OmM NaCI, 1OmM MgCI2), 60μg/ml_ saponin and 3OuM GDP is added. The third addition is a 20% TAV(IOuI) addition of either buffer, (agonist format) or EC80 final assay concentration of agonist, Quinelorane, prepared in assay buffer (antagonist format). The assay is started by the addition of 29%TAV (15 ul) of GTP[35S] 0.38nM final (37MBq/mL, 1 160Ci/mmol, Amersham). After all additions assay plates are spun down for 1 min at 1 ,000rpm. . The final assay cocktail (45.5μl) is incubated at room temperature to equilibrate for 3-6 hours before reading on a ViewLux™ (613/55 filter) luminescence imager 5min/plate.

The effect of the test drug over the basal generates fpKi values of test drug are calculated from the IC50 generated by "antagonist format" experiment, using Cheng & Prusoff equation: fKi = IC50 / 1 +([A] / EC50) where: [A] is the concentration of the agonist Quinelorane in the assay and EC50 is the Quinelorane EC50 value obtained in the same experiment. fpKi is defined as -logfKi. pKi results are only estimated to be accurate to about 0.3-0.5.

In the context of the present invention functional pKi (fpKi, corresponding to the negative logarithm of fKi) is used instead of functional Ki (fKi) and the compounds of formula (I) and salts thereof typically show fpKi for D3 receptors comprised between approximately 7.0 and 8.5.

Here below a list of examples is provided which show at least 20 fold selectivity for D3 over D2 receptors: E1 , E2, E3, E4.

Here below a list of examples is provided which showed no activity in the D2 GTPS-SPA assay up to the highest concentration tested in the assay (3 μM) and thus considered to be selective for D3 over D2 receptors: E8 and E9.

Examples

The invention is further illustrated by the following non-limiting examples.

In the procedures that follow, after each starting material, reference to a Preparation or Example by number is typically provided. This is provided merely for assistance to the skilled chemist. The starting material may not necessarily have been prepared from the batch referred to.

Where reference is made to the use of a "similar" procedure, as will be appreciated by those skilled in the art, such a procedure may involve minor variation, for example reaction temperature, reagent/solvent amount, reaction time, work-up conditions or chromatographic purification conditions.

Compounds may be named using ACD/Name PRO 6.02 chemical naming software (Advanced Chemistry Development Inc., Toronto, Ontario, M5H2L3, Canada) or ISIS/Draw 2.5 SR 2 Autonom (MDL Information System, Inc)

All temperatures refer to ⁰ C.

Proton Magnetic Resonance (MMR) spectra may be typically recorded either on Varian instruments at 300, 400 or 500 MHz, or on a Bruker instrument at 300 and 400 MHz.

Chemical shifts are reported in ppm (δ) using the residual solvent line as internal standard. Splitting patterns are designed as s, singlet; d, doublet; t, triplet; q, quartet; m, multiplet; b, broad. The NMR spectra may be recorded at a temperature ranging from 25 to 9O ⁰ C. When more than one conformer was detected the chemical shifts for the most abundant one is reported.

Mass spectra (MS) may be typically taken on a 4 Il triple quadrupole Mass Spectrometer (Micromass UK) or on a Agilent MSD 1100 Mass Spectrometer, operating in ES (+) and ES (-) ionization mode or on an Agilent LC/MSD 1100 Mass Spectrometer, operating in ES (+) and ES (-) ionization mode coupled with HPLC instrument Agilent 1100 Series. In the mass spectra only one peak in the molecular ion cluster is reported.

For reactions involving microwave irradiation, a Personal Chemistry EmrysTM Optimizer or Biotage Initiator 60 may be used.

Flash silica gel chromatography may be carried out on silica gel 230-400 mesh (supplied by Merck AG Darmstadt, Germany) or over Varian Mega Be-Si pre-packed cartridges or over pre-packed Biotage silica cartridges.

In a number of preparations, purification may be performed using either Biotage manual flash chromatography (Flashí) or automatic flash chromatography (Horizon) systems. All these instruments work with Biotage Silica cartridges.

Optical rotations may be measured using a (Perkin Elmer Model 241 ) polarimeter operating at 589 nm (Sodium source). Measurements are made using a 1 decimeter microcell thermostated at 23o C. Concentrations are typically 10 rηg/ml (c=0.01 ). For ab initio OR assignments, the Dalton Quantum Chemistry Program may be used.

Column chromathography was carried out over silica gel (Merck AG Darmstaadt, Germany). The following abbreviations are used in the text: EtOAc = ethyl acetate, Et ₂ O = dietyl ether, THF = tetrahydrofuran, TIc refers to thin layer chromatography on silica plates, and dried refers to a solution dried over anhydrous sodium sulphate, r.t. (RT) refers to room temperature, Rt = retention time, DMSO = dimethyl sulfoxide; DMF = N ₁ N'- dimethylformamide, DCM = dichloromethane, TEA = triethylamine, SPE Cartridge = Solid Phase Extraction Cartridge; SCX Cartridge = Strong Cation Exchange Cartridge.

Preparation 1 : 3-[4-(trifluoromethyl)phenyl]-1H-pyrrole-2,5-dione (Prepi)

A mixture of hydrochloric acid (37% in water, 285 ml.) and water (190 mL) was added to 4-(trifluoromethyl)aniline (15O g, 116 mL) at room temperature with vigorous stirring and the formed precipitate was allowed to stir for further 30 minutes. Temperature was reduced to 0 ⁰ C and sodium nitrite (70.6 g) in 180 mL of water was added dropwise to the stirred suspension. At the end of diazotisation, a clear yellow solution was obtained. Maleimide (180 g) in acetone (1.1 L) was added dropwise at 0 ⁰ C and then the pH of the solution was adjusted to 3-3.5 by adding sodium acetate. Copper (II) chloride (18.8 g) was added to the vigorously stirred mixture. After a few minutes a gas started to develop (conspicuous foaming). The reaction mixture was allowed to stir at 0 ⁰ C for 1 h and overnight at room temperature. Acetone was removed in vacuo, the residue was filtered and dried overnight in vacuo to give the title compound (155 g) as a light brown solid. MS (mlz): 242.2 [MH] ⁺ .

Preparation 2: (1 R,5Sλ S,5R)-1 -[4-(trif luoromethyl)phenyl]-3-azabicyclo[3.1.0]- hexane-2,4-dione (Prep2)

Milled sodium hydroxide (40 g) was added in small portions to a stirred solution of thmethylsulfoxonium iodide (219 g) in DMSO (anhydrous, 2L). The resulting mixture was allowed to stir at room temperature for 1.5 h. 3-[4-(Tnriuoromethyl)phenyl]-1 H-pyrrole-2,5- dione (Prepi , 120 g) dissolved in DMSO (anhydrous, 0.5 L) was then added dropwise and the resulting mixture was allowed to stir at room temperature for 20 minutes. Temperature was then reduced to 0 ⁰ C and aqueous saturated NH ₄ CI (2 L) was slowly added, followed by Et ₂ O (1 L). After separation of the two phases, the aqueous layer was repeatedly extracted with Et ₂ O (3 x 1 L). Combined organic layers were washed with brine (2 x 1 L) and then dried over Na ₂ SO ₄ . Evaporation of the solvent gave a light brown solid which was suspended in 1 L of dichloromethane and 1 L of cyclohexane. The mixture was

allowed to stir at room temperature for 45 minutes and then filtered to give the title compound (116 g) as white solid. MS (mlz): 256.1 [MH] ⁺ .

Preparation 3: (1/?,5S/1S,5R)-1-[4-(trifluoromethyl)pheny|]-3-azabicyclo[3. 1.0]- hexane (Prep3)

Borane (1 M in tetrahydrofuran, 1.4 I) was charged into a 5 I reactor under N ₂ and cooled at 0 ⁰ C. (I R.SS/I S.S^-i-^^trifluoromethyOphenyO-S-azabicyclotS.I .OJhexane^^-dione (Prep2, 101 g) dissolved in anhydrous THF (1 L) was then added dropwise with vigorous stirring whereby the temperature was constantly kept below 5 ⁰ C and gas evolution was monitored. At the end of the addition the resulting mixture was allowed to stir at 0 ⁰ C for 1 h and then at room temperature overnight. The mixture was then cooled to 0 ⁰ C and methanol (200 mL) followed aqueous 6M hydrochloric acid solution (0.8 L) were cautiously added monitoring gas evolution. THF was then removed in vacuo, the residue was cooled to 0 ⁰ C and an aqueous 5M sodium hydroxide solution was added until pH 9- 10 had been reached. The aqueous layer was extracted with Et ₂ O (3 x 1 L). Removal of solvent in vacuo gave the title compound (140 g) as colorless oil. MS (mlz): 228.1 [MH] ⁺ .

Preparation 4: (1 S,5/?)-1 -[4-(trif luoromethyl)phenyl]-3-azabicyclo[3.1.OJhexane (Prep4)

(S)-(+)-Mandelic acid (94 g) was added in portions to a stirred solution of (1R,5S/1 S,5R)- 1-[4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hexane (Prep3, 140 g) in 1.4 L of THF.

The resulting mixture was stirred at room temperature for 2 h until a white precipitate was formed. The mixture was then warmed up to reflux temperature, stirred for 45 minutes and then slowly cooled down to room temperature. The white solid was collected by filtration and dried in vacuo. This material was recrystallised 4 times from THF (10 volumes) to give 32.5 g of a white solid. This material was then suspended in sodium hydroxide (I M solution, 400 ml.) and Et ₂ O (400 ml.) and allowed to stir at room temperature until complete dissolution. After separation of the two phases, the aqueous layer was extracted again with Et ₂ O (3 x 250 ml_). Combined organic layers were washed with aqueous 1 M sodium hydroxide solution (3 x 200 mL) and then dried over Na ₂ SO ₄ . Evaporation of solvent in vacuo gave the title compound (19 g) as white solid. The absolute configuration of the optical isomers was assigned as described in PCT International Publication WO2005/080382.

NMR ( ¹ H, CDCI ₃ ): δ 7.51 (d, 2H), 7.25 (d, 2H), 3.20 (d, 1 H), 3.0-3.1 (m, 3H), 1.69 (m, 1 H),

0.8-1.0 (m, 2H), NH not observed. MS (mlz): 228.1 [MH] ⁺ . Analytical chromatography

Column: chiralcel OD 10 urn, 250 x 4.6 mm

Mobile phase: A: n-Hexane; B: lsopropanol +0.1 % lsopropyl amine

Gradient: isocratic 2% B

Flow rate: 1 imL/min UV wavelengh range: 200-400 nm

Analysis time 25 min ret. time (min) % a/a

16.5 0.4 (1 R,5S)-1-[4-(trifluoromethyl)pheny|]-3-azabicyclo[3.1.0]hexan e

21.7 99.6 title compound Specific Optical Rotation: [α] _D = - 10 ° (CDCI ₃ , T = 20 ⁰ C, c ≡ 0.004 g/0.8 mL).

Preparation 5: 1-(4-chlorobutyl)-3-methyl-2(1H)-pyridinone (Prep5)

To a solution of 3-methyl-2(1 H)-pyhdinone (commercial aldrich) (200 mg, 1.85 mmol), in dry DMF (5 mL), K ₂ CO ₃ (0.51 g) and 1-bromo-3-chlorobutane (0.32 mL) were added and

the resulting mixture was heated at 90° C for 5 hours After solvent elimination under reduced pressure, the residue was diluted with ethyl acetate and washed once with water and once with brine The organic phase was dried over anhydrous Na ₂ SO ₄ and concentrated under reduced pressure The crude product was purified by silica gel chromatography eluting with cyclohexane/EtOAc 8 2 to give the title compound as colourless oil (0 24 g) MS (m/z): 200 [MH]+

Preparation 6: 1-(4-chlorobutyl)-4-methyl-2(1 H)-pyridinone (Prepθ)

The title compound was prepared in 46% yield using a similar procedure as set out earlier in Prep5 starting from 4-methyl-2(1 H)-pyrιdιnone (commercial aldrich) (200 mg, 1 85 mmol)

MS (ES) 200 m/z [MH ⁺ ], C ₁₀ H ₁₄ CINO requires 199 68

1H NMR (400 MHz, CHLOROFORM-d) δ ppm 7 14 (d, 1 H) 6 38 (dd, 1 H) 6 01 (dd, 1 H)

3 95 (t, 2 H) 3 58 (t, 2 H) 2 16 - 2 21 (m, 3 H) 1 78 - 1 96 (m, 4 H)

Preparation 7: 3-bromo-1-(4-chlorobutyl)-2(1 H)-pyridinone (P7)

To a solution of 3-bromo-2(1 H)-pyrιdιnone (commercial source Alfa Aesar) (5 g, 28 7 mmol) in DMF (130ml) was added K ₂ CO ₃ (4 8 g, 34 5 mmol) The reaction mixture was stirred at room temperature for 1 hour, then 1-bromo-4-chlorobutane (3 3 ml, 28 7 mmol) was added and the reaction mixture was stirred for 18 hours at room temperature DMF was evaporated, water was added to the crude and the organic layers were extracted with DCM The organic layers were combined, dried over Na ₂ SO ₄ , filtered and concentrated in

vacuo The crude product was purified by column chromatography on silica gel eluting with a gradient of methanol in DCM (from 0 to 5%) to afford the title compound (4 82 g, 63%)

1 H NMR (400 MHz, CHLOROFORM-d) δ ppm 7 73 (d, 1 H) 7 29 (dd, 1 H) 6 10 (t, 1 H) 4 04 (t, 2 H) 3 58 (t, 2 H) 1 90 - 2 01 (m, 2 H) 1 79 - 1 89 (m, 2 H)

Preparation 8: 1-(4-chlorobutyl)-6'-methyl-3,3 ^l -bipyridin-2(1 H)-one (Prepδ)

3-Bromo-1-(4-chlorobutyl)-2(1 H)-pyrιdιnone (400 mg, 1 51 mmol and then 627 mg, 4 54 mmol) was added to a solution of (6-methyl-3-pyπdιnyl)boronιc acid (commercial Synchem OHG product list) (311 mg, 2 27 mmol) in dioxane (5 K ₂ CO ₃ ml) The mixture was degassed bubbling with N ₂ for 10' and then triphenylphosphine (120 mg, 0 45 mmol) and palladium (II) acetate (34 mg, 0 15 mmol) were added The reaction mixture was stirred at reflux for 5 h and then at room temperature for 18 hours Further (6-methyl-3- pyπdιnyl)boronιc acid (Synchem OHG product list) (60 mg, 0 43 mmol), triphenylphosphine (78 mg, 0 3 mmol) and palladium (II) acetate (22 mg, 0 1 mmol) were added and the reaction was stirred for additional 4 hours at 80 ⁰ C The reaction was cooled and concentrated by removing the solvent under reduced pressure Water was added to the crude and the organic layers were extracted with DCM The organic layers were combined, dried over Na ₂ SO ₄ , filtered and concentrated in vacuo The crude product was purified by column chromatography on silica gel eluting with a gradient of methanol in DCM (from 0 to 5%) to afford the title compound (280 mg, 67%) 1H NMR (400 MHz, CHLOROFORM-d) δ ppm 8 64 (br s , 1 H) 7 99 - 8 06 (m, 1 H) 7 59 - 7 69 (m, 1 H) 7 23 - 7 33 (m, 1 H) 7 1 1 - 7 20 (m, 1 H) 6 20 - 6 34 (m, 1 H) 3 94 - 4 07 (m, 2 H) 3 49 - 3 60 (m, 2 H) 2 5 (s, 3 H) 1 71 - 2 02 (m, 4 H)

Preparation 9: 1-(4-chlorobutyl)-6'-fluoro-3,3'-bipyridin-2(1 H)-one (Prep9)

The title compound was prepared in 82% yield using a similar procedure as set out earlier in Prepδ starting from 3-bromo-1-(4-chlorobutyl)-2(1 H)-pyridinone (Prep7) (400 mg, 1.51 mmol), (6-fluoro-3-pyridinyl)boronic acid (commercial Alfa Aesar) (426 mg, 3.02 mmol), K ₂ CO ₃ (627 mg, 4.54 mmol), triphenylphosphine (200 mg, 0.75 mmol) and palladium (II) acetate (68 mg, 0.30 mmol) dissolved in dioxane (5 ml).

1 H NMR (400 MHz, CHLOROFORM-d) δ ppm 8.40 (d, 1 H) 8.22 - 8.28 (m, 1 H) 7.50 (dd, 1 H) 7.35 (dd, 1 H) 6.94 (dd, 1 H) 6.30 (t, 1 H) 4.04 (t, 2 H) 3.57 (t, 2 H) 1.90 - 2.01 (m, 2 H) 1.79 - 1.90 (m, 2 H)

Preparation 10: i^-chlorobutyO-σ'-fluoro-S^'-bipyridin-∑ti HJ-one (PrepiO)

The title compound was prepared in 53% yield using a similar procedure as set out earlier in Prepδ starting from 3-bromo-1-(4-chlorobutyl)-2(1H)-pyridinone (Prep7) (400 mg, 1.51 mmol), (6-fluoro-3-pyridinyl)boronic acid (commercial Synchem OHG product list) (426 mg, 3.02 mmol), K ₂ CO ₃ (627 mg, 4.54 mmol), triphenylphosphine (200 mg, 0.75 mmol) and palladium (II) acetate (68 mg, 0.30 mmol) dissolved in dioxane (5 ml). 1H NMR (400 MHz, CHLOROFORM-cf) δ ppm 8.15 (d, 1 H) 7.60 (dd, 1 H) 7.49 (dt, 1 H) 7.41 (dd, 1 H) 7.34 - 7.38 (m, 1 H) 6.29 (t, 1 H) 4.01 (t, 2 H) 3.53 (t, 2 H) 1.86 - 1.97 (m, 2 H) 1.75 - 1.85 (m, 2 H)

Preparation 11 : 1 -(4-chlorobutyl)-2'-fluoro-3,3'-bipyridin-2(1 H)-one (Prepi 1 )

The title compound was prepared in 79% yield using a similar procedure as set out earlier in Prepδ starting from 3-bromo-1-(4-chlorobutyl)-2(1 H)-pyridinone (Prep7) (400 mg, 1.51 mmol), (6-fluoro-3-pyridinyl)boronic acid (commercial Alfa Aesar) (426 mg, 3.02 mmol), K ₂ CO ₃ (627 mg, 4.54 mmol), triphenylphosphine (200 mg, 0.75 mmol) and palladium (II) acetate (68 mg, 0.30 mmol) dissolved in dioxane (5 ml). 1 H NMR (400 MHz, CHLOROFORM-cf) δ ppm 8.07 - 8.19 (m, 2 H) 7.54 - 7.61 (m, 1 H) 7.35 - 7.40 (m, 1 H) 7.20 - 7.27 (m, 1 H) 6.30 (t, 1 H) 4.04 (t, 2 H) 3.58 (t, 2 H) 1.92 - 2.04 (m, 2 H) 1.78 - 1.91 (m, 2 H)

Preparation 12: 1-(4-chlorobutyl)-3-(5-pyrimidinyl)-2(1 H)-pyridinone (Prep12)

The title compound was prepared in 51 % yield using a similar procedure as set out earlier in Prepδ starting from 3-bromo-1-(4-chlorobutyl)-2(1 H)-pyridinone (Prep7) (400 mg, 1.51 mmol), (6-fluoro-3-pyridinyl)boronic acid (commercial Apollo Scientific Intermediates for Research and Development) (426 mg, 3.02 mmol), K ₂ CO ₃ (627 mg, 4.54 mmol), triphenylphosphine (200 mg, 0.75 mmol) and palladium (II) acetate (68 mg, 0.30 mmol) dissolved in dioxane (5 ml).

1 H NMR (400 MHz, CHLOROFORM-d) δ ppm 9.06 (br. s., 1 H) 9.01 (br. s., 2 H) 7.52 (dd, 1 H) 7.37 (dd, 1 H) 6.29 (t, 1 H) 4.00 (t, 2 H) 3.52 (t, 2 H) 1.70 - 1.96 (m, 4 H)

Preparation 13: 1-(4-chlorobutyl)-3-(methyloxy)-2(1H)-pyridinone (Prep13)

The title compound was prepared in 42% yield using a similar procedure as set out earlier in Prep7 starting from 3-(methyloxy)-2(1 H)-pyridinone (commercial Aldrich) (0.54 g, 4.31 mmol).

1H NMR (400 MHz, CHLOROFORM-αf) δ ppm 6.88 (dd, 1 H) 6.60 (dd, 1 H) 6.1 1 (t, 1 H) 4.01 (t, 2 H) 3.80 - 3.83 (m, 3 H) 3.57 (t, 2 H) 1.87 - 1.97 (m, 2 H) 1.76 - 1.86 (m, 2 H)

Preparation 14: 1-(4-chlorobutyl)-2-oxo-1,2-dihydro-3-pyridinecarbonitrile (Prep14)

The title compound was prepared in 65% yield using a similar procedure as set out earlier in Prep7 starting from 2-oxo-1 ,2-dihydro-3-pyridinecarbonitrile (commercial RC Biomedical Research Chemicals) (0.36 g, 1.71 mmol) MS (ES) 211 m/z: [MH ⁺ ]; C ₁₀ H ₁₁ CIN ₂ O requires 210.66

1 H NMR (400 MHz, CHLOROFORM-αf) δ ppm 7.83 (dd, 1 H) 7.57 (dd, 1 H) 6.30 (t, 1 H) 4.05 (t, 2 H) 3.60 (t, 2 H) 1.91 - 2.03 (m, 2 H) 1.79 - 1.90 (m, 2 H)

Example 1 : 3-methyl-1-(4-{(1S,5R)-1-[4-(trifluoromethyl)phenyl]-3- azabicyclo[3.1.0]hex-3-yl}butyl)-2(1H)-pyridinone hydrochloride (E1)

A mixture of 1-(4-chlorobutyl)-3-methyl-2(1 H)-pyridinone (Prep5, 40 mg), (1 S,5R)-1-[4- (trifluoromethyl)pheny|]-3-azabicyclo[3.1.0]hexane (Prep4, 30 mg, reference procedure for

preparation reported in WO 2005080382), K ₂ CO ₃ (36 rηg) and NaI (33 mg) in DMF (anhydrous, 0.5 mL) was heated at 70 ⁰ C for 18 h. After elimination of the solvent under reduced pressure, the residue was dissolved in ethyl acetate and the organic layer was washed water and dried over Na ₂ SO ₄ . This solution was filtered and the filtrate was concentrated in vacuo. The crude was purified by flash chromatography (dichloromethane to 5% MeOH / 0,5% ammonium hydroxide [33% w/w] in dichloromethane) to give 30 mg of the free base of the title compound. To a solution of this material in dichloromethane (0.2 mL) was added 0.08 mmol of HCI (I M solution in Et ₂ O), the solvent evaporated in vacuo and the material obtained triturated with Et ₂ O to give 27 mg of the title compound as a white slightly hygroscopic solid (48% yield).

NMR ( ¹ H, DMSO): δ 10.36 (br. s., 1 H), 7.69 (d, 2 H), 7.54 (d, 1 H), 7.48 (d, 2 H), 7.29 (d, 1 H) ₁ 6.14 (t, 1 H), 4.03 (dd, 1 H), 3.89 (t, 2 H), 3.69 (dd, 1 H), 3.58 - 3.65 (m, 1 H), 3.45 - 3.51 (m, 1 H), 3.17 - 3.25 (m, 2 H), 2.25 - 2.32 (m, 1 H), 1.96 - 2.01 (m, 3 H), 1.61 - 1.73 (m, 5 H), 1.16 - 1.22 (m, 1 H). MS(mlz): 391 [MH] ⁺ .

Example 2: 4-methyl-1 -(4-{(1 S,5R)-1 -[4-(trif luoromethyl)phenyl]-3- azabicyclo[3.1.0]hex-3-yl}butyl)-2(1 H)-pyridinone hydrochloride (E2)

H

The title compound was prepared using a similar procedure as set out earlier in Example 1 in 40 mg yield as a white slightly hygroscopic solid starting from 30 mg of (1 S,5R)-1-(4- (trif luoromethyl)henyl)-3-azabicyclo[3.1.0]hexane.

NMR ( ¹ H, DMSO): δ 10.46 - 10.61 (m, 1 H), 7.72 (d, 2 H), 7.59 (d, 1 H), 7.50 (d, 2 H),

6.19 - 6.22 (m, 1 H), 6.11 (dd, 1 H), 4.04 (dd, 1 H), 3.86 (t, 2 H), 3.70 (dd, 1 H), 3.59 - 3.66 (m, 1 H), 3.47 - 3.53 (m, 1 H), 3.17 - 3.27 (m, 2 H), 2.28 - 2.31 (m, 1 H), 2.12 - 2.14

(m, 3 H), 1.73 - 1.78 (m, 1 H), 1.68 - 1.74 (m, 2 H), 1.62 - 1.69 (m, 2 H), 1.17 - 1.23 (m, 1

H). MS(m/z): 391 [MH] ⁺ .

Example 3: 6'-methyl-1-(4-{(1S,5R)-1-[4-(trifluoromethyl)phenyl]-3- azabicyclo[3.1.0]hex-3-yl}butyl)-3,3'-bipyridin-2(1 H)-one dihydrochloride (E3)

Step a

TEA (0.056 ml, 0.4 mmol) was added to a solution of 1-(4-chlorobutyl)-6'-rnethyl-3,3'- bipyridin-2(1 H)-one (55mg, 0.2 mmol, Prepδ) and (1 S, 5R)-1-[4-(trifluoromethyl)phenyl]-3- azabicyclo[3.1.0]hexane (Prep4, 70 mg, 0.31 mmol, reference procedure for preparation also reported in WO 2005080382) in anhydrous DMF (2 ml). The reaction mixture was heated at 9O ⁰ C for 1 hour and then at 100 ⁰ C for 24 hours, quenched with water and extracted with ethyl acetate. The combined organics layers were dried (Na ₂ SO ₄ ) and concentrated in vacuo. The crude product was purified by SCX cartridge (eluting with methanol followed by 2N ammonia solution in methanol) and then by SPE cartridge eluting with a gradient of methanol in DCM (from 0 to 5%) to afford the free base of the title compound (19 mg, 20%). 1 H NMR (400 MHz, CHLOROFORM-cf) δ ppm 8.69 (d, 1 H) 8.10 (dd, 1 H) 7.50 - 7.56 (m, 3 H) 7.34 (dd, 1 H) 7.18 - 7.25 (m, 3 H) 6.31 (t, 1 H) 4.05 (t, 2 H) 3.36 (d, 1 H) 3.12 (d, 1 H) 2.58 - 2.61 (m, 3 H) 2.52 - 2.58 (m, 3 H) 2.45 - 2.50 (m, 1 H) 1.82 - 1.91 (m, 2 H) 1.74 - 1.80 (m, 1 H) 1.55 - 1.59 (m, 2 H) 1.48 - 1.52 (m, 1 H) 0.82 - 0.87 (m, 1 H)

Step b

The free base of E3 (19 mg, 0.041 mmol) was dissolved in DCM (1 ml) and treated with HCI (0.071 ml of a 1.25 M solution in methanol, 0.092 mmol) at room temperature. The resulting mixture was stirred at room temperature for 1 hour. Evaporation of the solvent and trituration with diethyl ether (2 x 2 ml) gave the title compound (E3) (16 mg) as a solid. MS (ES) 468 m/z: [MH ⁺ ]; C ₂₇ H ₂₈ F ₃ N ₃ O requires 467.5

Examples E4-E10:

The following examples (E4-E10) were prepared using a similar procedure as set out earlier in Example 3.

Free bases of title compounds (data reported in the table below) were obtained using a similar procedure as set out earlier in Example 3, Step a starting from the appropriate pyridazinone (selected from Prep9-Prep14) and (1 S, 5R)-1-[4-(trifluoromethyl)phenyl]-3- azabicyclo[3.1.0]hexane (reference procedure for preparation reported in WO 2005080382).

E8 Free Base 1H NMR (400 MHz, CHLOROFORM-d) δ ppm 7.52 (d, 2 H) 7.21

3-(methyloxy)-1 -(4-{(1 S,5R)-1 -[4- (d, 2 H) 6.89 (dd, 1 H) 6.59 (dd, 1 H) 6.10 (t, 1 H) 4.00 (t, 2 H)

(tιϊfluoromethyl)phenyl]-3- 3.79 - 3.84 (m, 3 H) 3.35 (d, 1 H) 3.10 (d, 1 H) 2.48 - 2.60 (m, 3 H) 2.42 - 2.48 (m, 1 H) 1.73 - 1.86 (m, 3 H) 1.46 - 1.60 (m, 3 H) azabicyclo[3.1.0]hex-3-yl}butyl)- 0.78 - 0.88 (m, 1 H)

2(1 H)-pyridinone

MS (ES) 402 m/z: [MH ⁺ ]; C ₂₂ H ₂₂ F ₃ N ₃ O requires 401.43

E9 Free Base 1 H NMR (400 MHz, CHLOROFORM-d) δ ppm 7.81 (dd, 1 H)

2-OXO-1 -(4-{(1 S,5R)-1 -[4- 7.57 (dd, 1 H) 7.53 (d, 2 H) 7.22 (d, 2 H) 6.28 (t, 1 H) 4.03 (t, 2

(trifluoromethyl)phenyl]-3- H) 3.36 (d, 1 H) 3.12 (d, 1 H) 2.46 - 2.64 (m, 4 H) 1.75 - 1.89 (m, azabicyclo[3.1.0]hex-3-yl}butyl)-1 ,2- 3 H) 1.53 - 1.61 (m, 2 H) 1.47 - 1.54 (m, 1 H) 0.83 - 0.89 (m, 1 dihydro-3-pyridinecarbonitrile H)

Title compounds (data reported in the table below) were obtained using a similar procedure as set out earlier in Example 3, Step b starting from the title compounds' free bases. For compounds containing a pyridine ring 2.2 eq of HCI of a 1.25 M solution in methanol were added otherwise 1.1 eq of of HCI of a 1.25 M solution in methanol were added.

Examples Analytical data

MS (ES) 472 m/z: [MH ⁺ ]; C ₂₆ H ₂₅ F ₄ N ₃ O requires 471.50

E4 1H NMR (400 MHz, DMSO-d ₆ ) δ ppm 10.50 (br. s ., 1 H ) 8. 23 (d,

2'-fluoro-1 -(4-{(1 S,5R)-1 -[4- 1 H) 7.99 (dd, 1 H) 7.94 (dd, 1 H) 7. 76 (dt, 1 H) 7.70 (d 2 H)

(trifluoromethyl)phenyl]-3- 7.65 (br. s., 1 H) 7.49 (d, 2 H) 6.45 (t 1 H) 3.98 - 4.09 (m , 3 H) azabicyclo[3.1.0]hex-3-yl}butyl)- 3.67 - 3.74 (m, 1 H) 3.58 - 3.67 (m, 1 H) 3.46 - 3.55 (m 1 H)

3,4'-bipyridin-2(1 H)-one 3.17 - 3.29 (m, 2 H) 2.25 - 2.35 (m, 1 H) 1.66 - 1.82 (m 5 H) dihydrochloride 1.11 - 1.23 (m, 1 H)

Example 10: 3-methyl-1 -(3-{(1 S,5R)-1 -[4-(trif luoromethyl)phenyl]-3- azabicyclo[3.1.0]hex-3-yl}propyl)-2(1 H)-pyridinone hydrochloride (E10)

Step a

3-Methyl-2(1 H)-pyridinone (commercial source: Aldrich) (17 mg, 0.16 mmol), (1 S,5R)-1- [4-(trifluoromethyl)phenyl]-3-azabicyclo[3.1.0]hexane (40 mg, 0.13 mmol, reference procedure for preparation reported in WO 2005080382), K ₂ CO ₃ (27.6 mg, 0.0.2 mmol), NaI (33.2 mg, 0.2 mmol) in DMF (1 ml) were heated over night at 8O ⁰ C. The reaction was quenched with saturated solution of NaHCO ₃ and extracted with ethyl acetate. The organic layers were combined, dried over Na ₂ SO ₄ , filtered and concentrated in vacuo. The crude product was purified by column chromatography on silica gel eluting with a gradient of methanol in DCM (from 0 to 30%) with a 5% of NH3 to afford the free base of the title compound (30 mq, 61 %).

1H NMR (400 MHz, CHLOROFORM-cf) δ ppm 7.53 (d, 2 H) 7.16 - 7.26 (m, 4 H) 6.09 (t, 1 H) 4.02 (t, 2 H) 3.32 - 3.45 (m, 1 H) 3.10 - 3.21 (m, 1 H) 2.43 - 2.68 (m, 4 H) 2.13 - 2.20 (m, 3 H) 1.89 - 2.05 (m, 2 H) 1.75 - 1.85 (m, 1 H) 1.46 - 1.66 (m, 1 H) 0.78 - 0.96 (m, 1 H)

Step b

The free base of E10 (30 mg, 0.08 mmol) was dissolved in DCM (1 ml) and treated with HCI (0.08 ml of a 1 M solution in ether at room temperature. The resulting mixture was stirred at room temperature for 1 hour. Evaporation of the solvent and trituration with diethyl ether (3 x 2 ml) gave the title compound (27 mg) MS (ES) 377 m/z: [MH ⁺ ]; C ₂₁ H ₂₃ F ₃ N ₂ O requires 376.42

All publications, including but not limited to patents and patent applications, cited in this specification are herein incorporated by reference as if each individual publication were specifically and individually indicated to be incorporated by reference herein as though fully set forth.

It is to be understood that the present invention covers all combinations of particular groups described herein above.

The application of which this description and claims forms part may be used as a basis for priority in respect of any subsequent application. The claims of such subsequent application may be directed to any feature or combination of features described herein. They may take the form of product, composition, process, or use claims and may include, by way of example and without limitation, the following claims: