IL191271A

IL191271A - Pharmaceutical compositions for treating a condition of dry eye comprising an a3 adenosine receptor agonist

Info

Publication number: IL191271A
Application number: IL191271A
Authority: IL
Original assignee: Can Fite Biopharma Ltd
Priority date: 2006-01-27
Filing date: 2008-05-06
Publication date: 2014-03-31
Also published as: JP2009524647A; KR20080090517A; CA2622975A1; CN101365430B; EP1976494A1; AU2006336834B2; JP2013032396A; CN101365430A; JP5185139B2; BRPI0621052A2; IL191271A0; WO2007086044A1; CA2622975C; AU2006336834A1; KR101037095B1

Description

Adenosine A3 receptor agonists for the treatment of dry eye disorders Can-Fite Biopharma Ltd. »"va fl»*» BACKGROUND OF THE INVENTION The preocular tear film plays an important role in the maintenance of corneal integrity, the protection against infection and the preservation of visual acuity. These functions, in turn, are critically dependent upon the stability, tonicity and/or composition of the tear film structure. Alteration, deficiency or absence of the tear film may lead to undesired dryness of the corneal epithelium, ulceration and perforation of the cornea, an increased incidence of infectious disease, and ultimately, severe visual impairment and blindness.

The condition of dry eye is often referred to as a syndrome, or a disease; and it is likewise known by a variety of terms. Keratoconjunctivitis sicca (KCS), or more commonly keratitis sicca, refers to any eye with some degree of dryness.

In dry eye the eye becomes dry either because there is abnormally high rate of evaporation of tears or because there is not enough tears being produced.

Throughout the world, countless individuals suffer from dry eye syndrome. The abnormalities leading to tear film dysfunction may be subdivided into four general categories: (a) aqueous tear deficiencies, which are most frequently responsible for dry eye states, originate from lacrimal gland disorders and include autoimmune disease, congenital alacrima, paralytic hyposecretion or excretory duct obstruction; (b) mucin deficiency, which is observed in various conjunctival cicatrization conditions, such as Stevens- Johns on syndrome, 2 191271/2 trachoma, pemphigoid, thermal and chemical burns, as well as hypovitaminosis A; (c) lipid abnormalities, which may occur during eyelid inflammation (e.g. chronic blepharitis); and (d) diminished eyelid function [Holly, F.J., Tear film physiology. Internal Ophthalmol. Clin. 27:2-6 (1987)].

The first line of treatment is usually eye drops, preferably preservative free, that act as artificial tears. Most artificial tears are hydrogels that increase the moisture content on the eye surface and give some temporary relief. These solutions and ointments give some temporary relief, but do little to arrest or reverse any damaging conditions. A recently introduced artificial tear product is based on Castor oil emulsion {Refresh Endura tears).

In addition, warm moist compresses applied to the skin of the closed eyelids are also used to reduce tear loss due to evaporation.

For more severe cases of dry eye, in which the cornea is inflamed, antiinflammatory agents, such as topical steroids (in eye drops) are sometimes prescribed. One example includes the combination of castor oil with cyclosporine (Restasis).

Oral medicine for dry eye is also available. For example, pilocarpine, the active ingredient in Salagen™ or cevimeline, the active ingredient in Evoxac™, are known to stimulate specific receptors in lacrimal gland and cause increased secretion of tears.

Other remedies include punctal plugs and punctal closure (which block the tears from flowing down the tear duct into the nose), and food supplements, such as the commercially available Flaxseed oil supplement (Omega-3 Supplement, TheraTears).

SUMMARY OF THE INVENTION In accordance with a first aspect, the invention provides a pharmaceutical composition for treating dry eye syndrome comprising as active ingredient an 01824556\9-02 3 191271/2 amount of A3AR agonist and a physiologically acceptable carrier, the amount of said A3AR agonist being effective to ameliorate dry eye symptoms.

In accordance with a second aspect, the present invention provides the use of an A3AR agonist for the preparation of a pharmaceutical composition for treating dry eye condition.

Passages of the description which are out of ambit of the claims do not constitute part of the invention.

DETAILED DESCRIPTION OF EXEMPLARY EMBODIMENTS Dry eye syndromes encompass a constellation of diverse disease processes that produce objective clinical signs of keratoconjunctivitis sicca (KCS). The classic prototype of the dry eye syndrome is Sjogren's syndrome, but there are many other causes of KCS including cicatrising conjunctival diseases such as trachoma and pemphigoid, non-cicatrising syndromes causing specific dry eye findings, and atypical syndromes such as keratomalacia in which the eye is symptomatically and objectively dry but tear production is paradoxically normal.

The main symptom of dry eye is usually a scratchy or sandy feeling as if something is in the eye. Other symptoms may include stinging or burning of the eye; episodes of excess tearing that follow periods of very dry sensation; a stringy discharge from the eye; and pain and redness of the eye. Sometimes individuals with dry eye experience heaviness of the eyelids or blurred, changing, or decreased vision, although loss of vision is uncommon. 01824556\9-02 Some individuals with dry eye may have tears that run down their cheeks. This is because the eye may be producing less of the lipid and mucin layers of the tear film, which help keep tears in the eye. When this happens, tears do not stay in the eye long enough to thoroughly moisten it.

The present invention provides a method for treating dry eye condition, specifically dry eye syndrome, comprising providing an individual exhibiting one or more dry eye symptoms and signs with an amount of A3 adenosine receptor (A3AR) agonist, the amount being effective to treat the dry eye condition.

As appreciated, while the invention is described in the following detailed description with reference to the above method, it is to be understood that also encompassed within the present invention are compositions comprising the A3AR agonist for use in said treatment.

In the context of the present invention the term "dry eye condition" denotes any condition or syndromewhich results in the manifestation of dry eye symptoms. It includes an already existing condition as well as pseudo dry eye conditions, i.e. conditions high predisposition of developing dry eye syndromes. Dry eye syndrome may be as a result of another underlying condition causing dry eye, for example, Sjogren's syndrome, menopause or rheumatoid arthritis. Dry eye may also be a complication of inflammation, e.g. Blepharitis or of a foreign body in the eye. Yet dry eye may be a result of infection, or a side effect of medications, or exposure to toxins, chemicals, or other substances may cause a symptom or condition of dry eye.

The term "dry eye symptoms" which may be used interchangeably with the term "dry eye signs" is used herein to denote any sensation or change in normal function or structure of the eye that is experienced by an individual. Anon-limiting list of signs which may be perceived by a subject and be indicative of an dry eye syndrome includes, dry eye feeling, sandy eye feeling, scratchy eye feelmg, burning eye, stinging or itching eye, excessive tearing, eye pain, redness of the eye, blurred vision, degraded vision.

The terms "treating" or "treatment", and the like are used herein to refer to obtaining a desired pharmacological and physiological effect. The effect may be prophylactic in terms of preventing or partially preventing a disease, symptom or condition of dry eye and/or may be therapeutic in terms of a partial or complete cure of a disease, condition, symptom or adverse effect attributed to dry eye syndrome. The term "treatment", as used herein, covers any treatment of a disease in a mammal, particularly a human, and includes: (a) preventing dry eye syndrome from occurring in an individual which may be predisposed to develop dry eye syndrome but has not yet been diagnosed as having it, i.e., causing the clinical symptoms of dry eye syndrome not to develop in a subject that may be predisposed to dry eye syndrome but does not yet experience or display symptoms of dry eye syndrome; (b) inhibiting dry eye syndrome, i.e., arresting or reducing the development of dry eye syndrome or its clinical symptoms; or (c) relieving diy eye syndrome, i.e., causing regression of dry eye syndrome and/or its symptoms or conditions.

The term "A3 adenosine receptor agonist" (A3AR agonist) in the context of the present invention refers to any molecule capable of specifically binding to the A3AR, thereby fully or partially activating said receptor. The A3AR agonist is thus a molecule that exerts its prime effect through the binding and activation of the A3AR. This means that at the doses it is being administered it essentially binds to and activates only the A3AR. In a preferred embodiment, an A3AR agonist has a binding affinity (Κ;) to the human A3AR in the range of less than 100 nM, typically less than 50 nM, preferably less than 20 nM, more preferably less than 10 nM and ideally less than 5 nM. Particularly preferred are A3AR agonists that have a ¾ to the human A3R of less than 2 nM and desirably less than 1 nM.

It should be noted that some A3AR agonists can also interact with and activate other receptors with lower affinities (namely a higher Ki). A molecule will be considered an A3AR agonist in the context of the invention (namely a molecule that exerts its prime effect through the binding and activation A3 AR) if its affinity to the A3AR is at least 3 times (i.e. its Ki to the A3AR is at least 3 times lower), preferably 10 times, desirably 20 times and most preferably at least 50 times larger than the affinity to any other of the adenosine receptors (i.e. Al5 A2a and A2b).

The affinity of an A3AR agonist to the human A3AR as well as its relative affinity to the other human adenosine receptors can be determined by a number of assays, such as a binding assay. Examples of binding assays include providing membranes containing a receptor and measuring the ability of the A3AR agonist to displace a bound radioactive agonist; utilizing cells that display the respective human adenosine receptor and measuring, in a functional assay, the ability of the A3AR agonist to activate or deactivate, as the case may be, downstream signaling events such as the effect on adenylate cyclase measured through increase or decrease of the cAMP level; etc. Clearly, if the administered level of an A3AR agonist is increased such mat its blood level reaches a level approaching that of the Ki of the Ai, A2a and A2b adenosine receptors, activation of these receptors may occur following such administration, in addition to activation of the A3A . An A3AR agonist is thus preferably administered at a dose such that the blood level is such so that essentially only the A3AR will be activated.

The characteristic of some adenosine A3AR agonists and methods of their preparation are described in detail in, inter alia, US 5,688,774; US 5,773,423, US 5,573,772, US 5,443,836, US 6,048,865, WO 95/02604, WO 99/20284, WO 99/06053, WO 97/27173 and applicant's co-pending patent application no. 09/700,751 (corresponding to WO 01/19360), all of which are incorporated herein by reference.

The following examples are specified in US 5,688,774 at column 4, lines 67-column 6, line 16; column 5, lines 40-45; column 6, lines 21-42; column 7, lines 1-11; column 7, lines 34-36; and column 7, lines 60-61: N6-(3-iodobenzyl)-9-methyladenine; N6-(3-iodobenzyl)-9-hydroxyemyladenine; R— N6-(3-iodoberizyl)-9-(2,3-dihydroxypropyl)adenine; S— N6-(3-iodoben2yl)-9-(2,3-dihydroxypropyl)adenine; N6-(3 -iodoben2yladenin-9-yl)acetic acid; N6-(3-iodoben2yl)-9-(3-cyanopropyl)adenine; 2-chloro-N6-(3-iodoben2yl)-9-methyladeniiie; 2-amino-N6-(3-iodobenzyl)-9-methyladenine; 2-hydrazido-N6-(3-iodoben2yl)-9-metliyladenine; N6-(3-iodobenzyl)-2-methylamino-9-methyladenine; 2-dmiethylamino-N6-(3-iodoberi2yl)-9-met_ yladenine; N6-(3-iodobenzyl)-9-methyl-2-propylaminoadenine; 2-hexylamino-N6-(3-iodobenzyl)-9-methyladenine; N6-(3-iodobeiizyl)-2-methoxy-9-metl yladenine; N6-(3-iodoben2yl)-9-methyl-2-methylthioadenine; N6-(3-iodobeii2yl)-9-methyl-2-(4-pyridylthio)adenine; (1 S,2R,3 S,4R)-4-(6-amino-2-phenylethylamino-9H-purin-9-yl)cyclopentane-l,2 ,3-triol; (lS,2R,3S,4R)-4-(6-amino-2-chloiO-9H-pui-in-9-yl) cyclopentane- 1,2,3 triol; (±)-9-[2a,3a-dihydroxy-4a-(N-methylcai-banioyl)cyclopent-la-yl)]-N6-(3-iodoben2yl)-adenine; 2-chloro-9-(2,-mnino-2, ,-dideoxy-a-D-5'-metliyl-arabino-furonmTiido)-N6-(3 -iodobenzyl)adenine; 2-chloro-9-(2' ,-dideoxy-2'-fluoro-a-D-5'-methyl-arabino furonamido)-N6 (3-iodobenzyl)adenine; 9-(2-acetyl-3 -deoxy-a-D-5-methy l-ribofuronamido)-2-chloro-N6(3 -iodoben2yl)adenine; 2-chloro-9-(3-deoxy-2-methanesulfonyl-a-D-5-methyl-ribofuronaiiiido)-N6-(3-iodoben2yl)adenine; 2-chloro-9-(3 -deoxy-a-D-5-methy l-ribofuronamido)-N6-(3 -iodoben2yl)adenine; 2-chloro-9-(3,5-l,l53,3-tetraisopropyldisiloxyl-a-D-5-ribofi.iranosyl)-N6-(3-iodobenzyl)adenine; 2-chloro-9-(2^3,-0-thiocarbonyl-a-D-5-methyl-ribofuronamido)-N6-(3-iodobenzyl)adenine; 9-(2-phenoxythiocarbonyl-3-deoxy-a-D-5-methyl-ribofuronamido)-2-chloro-N6-(3-iodobenzyl)adenine; 1- (6-benzylamho-9H-purin-9-yl)-l-deoxy-N,4-dimethyl-a-D-ribofuranosiduronamide; 2- cWoro-9-(2,3-dideoxy-a-D-5-metiiyl-ri^ 2-chloro-9 2'-azido-2^3'-dideoxy-a-D-5'-methyl-arabino-iuronamido)- N6-benzyladenine; 2-chloro-9-(a-D-ei throfui¾noside)-N6-(3-iodoben2yl)adenine; N6-(benzodioxanemethyl)adenosine; 1 -(6-furfurylamino-9H-purin-9-yl)- 1 -deoxy-N-methyl-a-D-ribofuranosiduronamide; N6-[3-(L-prolylamino)ben2yl]adenosine-5'-N-methyluronamide; N6-[3 -(N-T-B oc-a-alany lamino)benzyl] adenosine-5'-N-methy luronamide 6-(N'-phenylhyckazinyl)purine-9-a-ribofuranoside-5,-N-m^ 6-(0-phenyUiyd xylamino)purine-9-a-ribofLu*anoside-5'-N-methyluronamide; 9-(a-D-2,93,-dideoxyerythrofuranosyl)-N6-[(3-a-alanylamino)beri2yl]adenosine; 9-(a-D-erythrofuranoside)-2-me lamino-N6-(3-iodoben2yl)adenine; 2-chloro-N-(3-iodobenzyl)-9-(2-te1rahydrofiiryl)-9H-purin-6-amine; 2-chloro-(2'-deoxy-6'-tl io-L-arabinosyl)adenine; and 2-chloro-(6'-tliio-L-arabinosyl)adenine.

In US 5,773,423 at column 6, line 39, to column 7, line 14, specifically disclosed are compounds which include the fonnula: wherein Xi is RaRbNC(=0), wherein Ra and Rb may be the same or different and are selected from the group consisting of hydrogen, - o allcyl, amino, CrC10 haloalkyl, CpCio aminoalkyl, and C3-C10 cycloallcyl; R2 is selected from the group consisting of hydrogen, halo, Ci-C10 allcyoxy, amino, C2-C10 alkenyl, and C2-Ci0 allcynyl; and R5 is selected from the group consisting of R- and S-l-phenylethyl, an unsubstituted benzyl group, and a benzyl group substituted hi one or more positions with a substituent selected from the group consisting of Ci-C10 allcyl, amino, halo, CJ-CJO haloalkyl, nitro, hydroxy, acetamido, CrC10 alkoxy, and sulfo.

More specific compounds include those of the above formula wherein Ra and Rb may be the same or different and are selected from the group consisting of hydrogen and CrC10 allcyl, particularly when R2 is hydrogen or halo, especially hydrogen.

Additional specific compounds are those compounds wherein R" is hydrogen and R2 is hydrogen, particularly when R5 is unsubstituted benzyl.

More specific compounds are such compounds wherein Rb is a CrC10 allcyl or C3-C10 cycloallcyl, particularly a CrCio allcyl, and more particularly methyl.

Especially specific are tliose compounds where Ra is hydrogen, Rb is CrC10 allcyl or C3-C10 cycloallcyl, and R5 is R- or S-l-phenylethyl or a benzyl substituted in one or more positions with a substituent selected from the group consisting of halo, amino, acetamido, CrCi0 haloalkyl, and sulfo, where the sulfo derivative is a salt, such as a triethylammonium salt.

An example of an especially preferred compound disclosed in US 5,773,423 is IB-MECA. In addition, those compounds in which R2 is a C2-C10 alkenylene of the formula Rd— C=C— where Rd is a CrC8 allcyl are particularly noted in this publication. Also specific are those compounds wherein R2 is otlier than hydrogen, particularly those wherein R2 is halo, CrCi0 allcylamino, or CrC10 alkylthio, and, more preferably, when additionally Ra is hydrogen, Rb is a Ci-Ci0 alky I, and/or R5 is a substituted ben2yl.

Such specifically disclosed compounds include 2-chloro-N6-(3-iodobenzyl)-9-[5-(methylmm^o)-a-D-ribofuranosyl]-adenine, N6-(3-iodobenzyl)-2-memylaniino-9-[5-(methylamido)-a-D-ribofliranosyl]-adenine, and N6-(3-iodobenzyl)-2-methylthio-9-[5-(methylamido)-a-D-iibofuranosyl]-adenine.

Further US 5,773,423 discloses at column 7, line 60, through column 8, line 6, A3AR agonists as modified xanthine-7-ribosides having the formula: wherein X is O; Re is ^^C^O), wherein Ru and Rb may be the same or different and are selected from the group consisting of hydrogen, C Cio all yl, amino, C C10 haloalkyl, CpC10 aminoalkyl, and C3-Ci0 cycloalkyl; R7 and Re may be the same or different and are selected from the group consisting of Ci-C10 allcyl, R- and S-l-phenylethyl, an unsubstituted benzyl group, and a benzyl group substituted in one or more positions with a substituent selected from the group consisting of Q-Cio allcyl, amino, halo, C C10 haloalkyl, nitro, hydroxy, acetamido, CrC10 alkoxy, and sulfo; and R9 is selected from the group consisting of halo, benzyl, phenyl, and C3-C10 cycloalkyl.

WO 99/06053 discloses in examples 19-33 compounds selected from: N6-(4-biphenyl-carbonylammo)-adenosine-5'-N-ethyluronamide; N6-(2,4-dichlorobenzyl-carbonylamino)-adenosine-5'-N-ethyluronamide; N6-(4-methoxyphenyl-carbonylammo)-adenosme-5'-N-ethyluronamide; N6-(4-chlorophenyl-carbonylamino)-adenosine-5'-N-ethyluronamide; N6-(phenyl-carbonylaniino)-adenosine-5,-N-ethyluiOnamide; N6-(benzylcarbamoylaniMo)-adenosine-5 '-N-emyluronamide; N6-(4-sulfonamido-phenylcarbamoyl)-adenosine-5'-N-ethyluiOi amide; N6-(4-acetyl-phenylcarbamoyl)-adenosine-5'-N-ethyluronamide; N6-((R)-a-phenylethylcarbamoyl)-adenosine-5'-N-ethyluronamide; N6-((S)-a-phenylethylcarbamoyl)-adenosine-5'-N-ethylui iiamide; N6-(5-methyl-isoxazol-3-yl-carbamoyl)-adenosine-5'-N-etliyluronamide; N^Cl^^-thiadiazol^-yl-carbamoyO-adenosine-S'-N- ethyluronamide; N6-(4-n-propoxy-phenylcarbamoyl)- adenosine-5'-N-ethyluronamide; N6-bis-(4-nihOphenylcarbanioyl)-adenosine-5'-N-ethyluronamide; and N6-bis-(5-chloro-pyridin-2-yl-carbamoyl)-adenosine-5'-N-ethyluronamide.

According to one embodiment of the invention, the A3AR agonist is a compound that exerts its prime effect through the binding and activation of the adenosine A3A and is a purine derivative falling within the scope of the general formula (I): wherein, - Rn represents an allcyl, hydroxyalkyl, carboxyallcyl or cyanoallcyl or a group of the following general formula (II): in which: Y represents oxygen, sulfur or CH2; Xu represents H, allcyl, R¾faC(=0 or HOR -, wherein - Re and Rf may be the same or different and are selected from the group consisting of hydrogen, allcyl, amino, haloalkyl, aminoalkyl, BOC-aminoallcyl, and cycloallcyl or are joined together to form a heterocyclic ring containing two to five carbon atoms; and - R is selected from the group consisting of allcyl, amino, haloalkyl, aminoalkyl, BOC-aminoallcyl, and cycloallcyl; Xi2 is H, hydroxyl, allcylamino, allcylamido or hydroxyalkyl; Xi3 and Xi4 represent independently hydrogen, hydroxyl, amino, amido, azido, halo, allcyl, allcoxy, carboxy, nitrilo, nitro, trifluoro, aryl, allcaryl, thio, thioester, thioether, -OCOPh, -OC(=S)OPh or both Xi3 and Xi4 are oxygens connected to >C=S to form a 5-membered ring, or X12 and Xi3 form the ring of formula (III): where R' and R" represent independently an allcyl group; - Ri2 is selected from the group consisting of hydrogen, halo, alkylether, amino, hydrazido, allcylamino, alkoxy, thioalkoxy, pyridylthio, allcenyl; alkynyl, thio, and alkylthio; and - R13 is a group of the formula -NR15R16 wherein - Ris is a hydrogen atom or a group selected from allcyl, substituted allcyl or aryl-NH-C(Z)-, with Z being 0, S, or NRa with Re having the above meanings; wherein when R15 is hydrogen than - Ri6 is selected from the group consisting of R- and S-l-phenylethyl, benzyl, phenylethyl or anilide groups unsubstituted or substituted in one or more positions with a substituent selected from the group consisting of allcyl, amino, halo, haloallcyl, nitro, hydroxyl, acetoamido, alkoxy, and sulfonic acid or a salt thereof; benzodioxanemethyl, fururyl, L-propylalanyl- aminobenzyl, β-alanylamino- benzyl, T-BOC-P-alanylaminobenzyl, phenylamino, carbamoyl, phenoxy or cycloallcyl; or Ri6 is a group of the following formula: or when Ri5 is an allcyl or aryl-NH-C(Z , then, R16 is selected from the group consisting of heteroaryl- ^-C Z)-, heteroaryl-C(Z)-, allcaryl-lSn .a-C(Z)-, alkaryl-C(Z)-, aryl-NR-C(Z)- and aryl-C(Z)-; Z representing an oxygen, sulfor or amine; or a physiologically acceptable salt of the above compound.

According to one preferred embodiment, the A3AR agonist is a nucleoside derivative of the general formula (IV): wherein Xi, R2' and R5 are as defined above, and physiologically acceptable salts of said compound.

The non-cyclic carbohydrate groups (e.g. alkyl, alkenyl, alkynyl, alkoxy, arall yl, alkaryl, aU ylamine, etc) forming part of the substituent of the compounds of the present invention are either branched or unbranched, preferably containing from one or two to twelve carbon atoms.

When referring to "physiologically acceptable salts" of the compounds employed by the present invention it is meant any non-toxic alkali metal, alkaline earth metal, and ammonium salt commonly used in the pharmaceutical industry, including the sodium, potassium, lithium, calcium, magnesium, barium ammonium and protamine zinc salts, which are prepared by methods known in the art. The term also includes non-toxic acid addition salts, which are generally prepared by reacting the compounds of this invention with a suitable organic or inorganic acid. The acid addition salts are those which retain the biological effectiveness and qualitative properties of the free bases and which are not toxic or otherwise undesirable. Examples include, inter alia, acids derived from mineral acids, hydrochloric, hydrobromic, sulfuric, nitric, phosphoric, metaphosphoric and the like. Organic acids include, inter alia, tartaric, acetic, propionic, citric, malic, malonic, lactic, fumaric, benzoic, cinnamic, mandelic, glycolic, gluconic, pyruvic, succinic salicylic and arylsulphonic, e.g. p-toluenesulphonic, acids.

Specific examples of A3AR agonist which may be employed according to general formula (TV) of the present invention include, without being limited thereto, N6-2- (4-aminophenyl)ethyladenosine (APNEA), N6-(4-amino-3-iodoben2yl) adenosine- 5'-(N-methylui namide) (AB-MECA), N6-(3-iodobenzyl)-adenosine-5'-N- methyluronamide (IB-MECA) and 2-chloro-N6-(3-iodobenzyl)- adenosine-5'-N-methyluronamide (Cl-IB-MECA). IB-MECA is the most preferred compound in accordance with the invention.

According to another embodiment, the A3AR agonist may be an oxide derivative of adenosine, such as N6-benzyladenosine-5,-N-all yluronamide-N1-oxide or N^benzyladenosine-S'-N-diall yluronamide-N^oxide, wherein the 2-purine position may be substituted with an alkoxy, amino, alkenyl, alkynyl or halogen.

The terms "effective amount" or "amount effective to" in the context of the present invention refer to an amount of A3AR agonist which prevents or reduces symptoms of dry eye in patients. The "effective amount" can be readily determined, in accordance with the invention, by administering to a plurality of tested subjects various amounts of the A3AR agonist and then plotting the physiological response (for example an integrated "SS index" combining several of the therapeutically beneficial effects) as a function of the amount. Alternatively, the effective amount may also be determined, at times, through experiments performed in appropriate animal models and then extrapolating to human beings using one of a plurality of conversion methods; or by measuring the plasma concentration or the area under the curve (AUC) of the plasma concentration over time and calculating the effective dose so as to yield a comparable plasma concentration or AUC. As known, the effective amount may depend on a variety of factors such as mode of administration (for example, oral administration may require a higher dose to achieve a given plasma level or AUC than an intravenous administration); the age, weight, body surface area, gender, health condition and genetic factors of the subject; other adrninistered drugs; etc.

In the following, unless otherwise indicated, dosages are indicated in weight/Kg, meaning weight of administered A3AR agonist (e.g. IB-MECA) per kilogram of body weight of the treated subject in each admmistration. For example, mg/Kg and micrograrn/Kg denote, respectively, milligrams of administered agent and micrograms of administered agent per kilogram of body weight of the treated subject.

The effective amount is preferably less than about 1 mg/kg body weight, particularly less than about 500 \ig/kg or even less than about 200 ^ig/kg body weight or at times less than about 100 μg/kg body weight or even less than about less than 50 μg kg body weight. With respect to IB-MECA, the effective amount is preferably less than 5 mg each dose, for once daily administration (namely a dose less than about 70 g/kg body weight, assuming an average individual weight of about 70 kg), and less than about 4 mg each dose (i.e. less than about 57 g/kg body weight), for twice daily administration. The dose of IB-MECA is more preferably less than about 2 mg each dose and typically between about 0.1-1 mg each dose, for either once or twice daily administration (the corresponding dosages in weight per body weight being about. 29 μg/kg and about 1.5-15 body weight, respectively).

The administration of the A3AR agonist to an individual may be together with a pharmaceutically acceptable carrier. In the case where the administration is oral, the carrier is one that is acceptable for oral administration. In the case where the admmistration is topical, the canier is one that is acceptable for topical administration, one example being ocular administration.

By the term "pharmaceutically acceptable carder" it is meant any one of inert, non-toxic materials, which do not react with the A3AR agonist and which can be added to formulations as diluents or carriers or to give form or consistency to the formulation.

An oral formulation may be in the form of a pill, capsule, in the form of a syrup, an aromatic powder, and other various forms. The carrier is selected at times based on the desired form of the formulation. The carrier may also at times have the effect of the improving the delivery or penetration of the active ingredient to the target tissue, for improving the stability of the drug, for slowing clearance rates, for imparting slow release properties, for reducing undesired side effects etc. The carrier may also be a substance that stabilizes the formulation (e.g. a preservative), for providing the formulation with an edible flavor, etc. The carriers may be any of those conventionally used and is limited only by chemical-physical considerations, such as solubility and lack of reactivity with the A3AR agonist, and by the route of administration. The carrier may include additives, colorants, diluents, buffering agents, disintegrating agents, moistening agents, preservatives, flavoring agents, and pharmacologically compatible carriers. In addition, the carrier may be an adjuvant, which, by definition are substances affecting the action of the active ingredient in a predictable way.

Typical examples of carriers suitable for oral administration comprise (a) liquid solutions, where an effective amount of the active substance is dissolved in diluents, such as water, saline, natural juices, alcohols, syrups, etc.; (b) capsules (e.g. the ordinary hard- or soft-shelled gelatin type containing, for example, surfactants, lubricants, and inert fillers), tablets, lozenges (wherein the active substance is in a flavor, such as sucrose and acacia or tragacanth or the active substance is in an inert base, such as gelatin and glycerin), and troches, each containing a predetermined amount of the tragacanth as solids or granules; (c) powders; (d) suspensions in an appropriate liquid; (e) suitable emulsions; (f) liposome formulation; and others.

A topical formulation may be in any form suitable for topical administration, including, without being limited thereto, an ophthalmic solution (e.g. eye drops), an ophthalmic gel or an ophthalmic ointment or oily lotion. Topical administration of the A3A agonist also comprises the use of ophthalmic patches carrying the A3AR agonist in a suitable drug containing layer and to be placed on top of the eyelid as well as to Ocular inserts which are devices containing the A3AR agonist and placed into the inferior or superior conjunctival sacs (see for example WO0059420).

Eye drops may be prepared by dissolving A3AR agonist in a sterile aqueous solution such as saline, buffering solution etc., or by combining powder compositions to be dissolved before use. Other additives may be included in the eye drops such as isotonizing agents (e.g., sodium chloride, etc.), buffer agent (e.g., boric acid, sodium monohydrogen phosphate, sodium dihydrogen phosphate, etc.), preservatives (e. g., benzalkonium chloride, benzethonium chloride, chlorobutanol, etc.), thickeners (e. g., saccharide such as lactose, mahnitol, maltose, etc.; e.g., hyaluronic acid or its salt such as sodium hyaluronate, potassium hyaluronate, etc.; e.g., mucopolysaccharide such as chondroitin sulfate, etc.; e.g., sodium polyacrylate, carboxyvinyl polymer, crosslinked polyacrylate, etc.).

Eye ointments may be prepared by mixing A3AR agonist into a base. Examples of the base for eye ointment include petrolatum, selen 50, Plastibase, macrogol, etc., but not limited thereto.

Some exemplary ophthalmic viscosity enhancers that can be used in the present formulation include: carboxymethyl cellulose sodium; methylcellulose; hydroxypropyl cellulose; hydroxypropylmethyl cellulose; hydroxyethyl cellulose; polyethylene glycol 300; polyetliylene glycol 400; polyvinyl alcohol; and providone.

Some natural products, such as veegum, alginates, xanthan gum, gelatin, acacia and tragacantli, may also be used to increase the viscosity of ophthalmic solutions.

A tonicity is important because hypotonic eye drops cause an edema of the cornea, and hypertonic eye drops cause deformation of the cornea. The ideal tonicity is approximately 300 mOsM. The tonicity can be achieved by methods described in Remington: The Science and. Practice of Pharmacy, known to those versed in the art.

As used herein, the forms "a", "an" and "the" include singular as well as plural references unless the context clearly dictates otherwise. For example, the term "an A3AR agonist" includes one or more compounds which are capable of specifically binding to the A3 AR, thereby fully or partially activating said receptor.

Further, as used herein, the term "comprising" is intended to mean that the composition include the recited active agent, i.e. A3AR agonist, but not excluding other elements, such as physiologically acceptable carriers and excipients as well as other active agents. The term "consisting essentially of is used to define compositions which include the recited elements but exclude other elements that may have an essential significance on treatment of dry eye syndrome. "Consisting of shall thus mean excluding more than trace elements of other elements. Embodiments defined by each of these transition terms are within the scope of this invention.

Further, all numerical values, e.g. when referring the amounts or ranges of the elements constituting the composition comprising the A3AR agonist as an active ingredient, are approximations which are varied (+) or (-) by up to 20%, at times by up to 10% of from the stated values. It is to be understood, even if not always explicitly stated that all numerical designations are preceded by the term "about".

The invention will now be exemplified in the following description of experiments that were carried out in accordance with the invention. It is to be understood that these examples are intended to be in the nature of illustration rather man of limitation. Obviously, many modifications and variations of these examples are possible in light of the above teaching. It is therefore, to be understood that within the scope of the appended claims, the invention may be practiced otherwise, in a myriad of possible ways, than as specifically described hereinbelow.

EXAMPLE: IB-MECA improves dry eye symptoms in Rheumatoid Arthritis patients Drug: The A3AR agonist used was a clinical grade of the compound known generically as l-Deoxy-l-[6-[[(3-iodophenyl)methyl]amino]-9H-purine-9-yl]-N-metliyl-D-ribofuranuronamide or as N6-(3-iodobenzyl)-adenosine-5'-N-methyluronamide (IB-MECA), that was synthesized for Can-Fite BioPharma, under good clinical practice (GMP) by Albany Molecular Research Inc, Albany, NY, USA.

The IB-MECA was formulated in oval softgel capsules. The capsules contained solutions of IB-MECA in Cremophor RH 40 and Miglyol 812. The capsules contained a dose of 0.1, 1 or 4 mg of IB-MECA, the exact composition of each capsules' type is shown in the following Tabels 1-3: Table 1: Composition of 0.1 mg IB-MECA Softgel Capsules Table 3: Composition of 4 mg IB-MECA Softgel Capsules Ingredient Capsule %WAV Methods: The capsules with IB-MECA were given to patients orally twice daily. All patients had rheumatoid aiihiitis (RA) and were give ΓΒ-MECA within the framework of a clinical study aimed at testing the effect of IB-MECA in modifying RA disease symptoms in these patients. The patients received randomly capsules of one of the above there doses. The patients received the IB-MECA for a period of 12 weeks. 4 out of the treated patients also suffered from Sicca and the effect of IB-MECA on their dry eye symptoms was examined as well.

Results Table 1 summarizes the results of CF101 treatment of RA patients. Specifically, four patients at the age 58±4 years who suffered from RA for 8±2 years were followed. At base line, the patients had elevated levels of rheumatoid factor, i.e., 313±120 IU/ml (0 Table 1 - Effect of CFlOl treatment on RA patients 1 65 14 5 positive 4 6 9 2 58 7 7 positive 5 10 32 3 54 6 5 7 5 16 4 62 5_ 3 9 6 9 Mean 59.75 8.00 5 6.25 6.75 16 SE 2.4 0.51 0.82 1.11 1.11 5.

Claims

23 191271/2 CLAIMS:

1. A pharmaceutical composition for treating a condition of dry eye, comprising an amount of an A3 adenosine receptor (A3AR) agonist and a pharmaceutically acceptable carrier, the amount of said A3AR agonist being effective to ameliorate symptoms of dry eye in the individual.

2. The composition of Claim 1 , in a form suitable for oral administration.

3. The composition of Claim 1 , in a form suitable for topical administration.

4. The composition of Claim 3, in a form suitable for topical administration to the eye.

5. The composition of any one of Claims 1 to 4, for treating dry eye syndrome.

6. The composition of any one of Claims 1 to 5, wherein said A3RAg is selected from N6-2- (4-aminophenyl)ethyladenosine (APNEA), N6-(4-amino-3-iodobenzyl) adenosine- 5'-(N-methyluronamide) (AB-MECA), N6-(3-iodobenzyl)-adenosine-5'-N- methyluronamide (IB-MECA) and 2-chloro-N6-(3-iodobenzyl)-adenosine-5'-N-methyluronamide (Cl-IB-MECA).

7. The composition of Claim 6, wherein said A3RAg is IB-MECA.

8. Use of an A3 adenosine receptor (A3AR) agonist for the preparation of a pharmaceutical composition for treating dry eye condition.

9. The use of Claim 8, for treating dry eye syndrome.

10. The use of Claim 8 or 9, for the preparation of a pharmaceutical composition for oral administration.

11. The use of Claim 8 or 9, for the preparation of a pharmaceutical composition for topical administration. 01824556\9-02 24 191271/2

12. The use of Claim 11, for the preparation of a pharmaceutical composition for topical administration to the eye.

13. The use of any one of Claims 8 to 12, wherein said A3RAg is selected from N6-2- (4-aminophenyl)ethyladenosine (APNEA), N6-(4-amino-3-iodobenzyl) adenosine- 5'-(N-methyluronamide) (AB-MECA), N6-(3-iodobenzyl)-adenosine-5'-N- methyluronamide (IB-MECA) and 2-chloro-N6-(3-iodobenzyl)- adenosine-5'-N-methyluronamide (Cl-IB-MECA).

14. The composition of Claim 13, wherein said A3RAg is IB-MECA. For the Applicants Reinhold Cohn & Partners 01824556\9-02