US20030181469A1 - Crystalline and amorphous form of a triazolo(4,5-d)pyrimidine compound - Google Patents

Crystalline and amorphous form of a triazolo(4,5-d)pyrimidine compound Download PDF

Info

Publication number
US20030181469A1
US20030181469A1 US10/296,990 US29699002A US2003181469A1 US 20030181469 A1 US20030181469 A1 US 20030181469A1 US 29699002 A US29699002 A US 29699002A US 2003181469 A1 US2003181469 A1 US 2003181469A1
Authority
US
United States
Prior art keywords
compound
formula
mixture
solvent
diffraction pattern
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Abandoned
Application number
US10/296,990
Inventor
Martin Bohlin
Steve Cosgrove
Bo Lassen
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
AstraZeneca AB
Original Assignee
AstraZeneca AB
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Family has litigation
First worldwide family litigation filed litigation Critical https://patents.darts-ip.com/?family=9892841&utm_source=google_patent&utm_medium=platform_link&utm_campaign=public_patent_search&patent=US20030181469(A1) "Global patent litigation dataset” by Darts-ip is licensed under a Creative Commons Attribution 4.0 International License.
Application filed by AstraZeneca AB filed Critical AstraZeneca AB
Assigned to ASTRA ZENCA AB reassignment ASTRA ZENCA AB ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: LASSEN, BO, BOHLIN, MARTIN, COGROVE, STEVE
Publication of US20030181469A1 publication Critical patent/US20030181469A1/en
Priority to US11/240,801 priority Critical patent/US7265124B2/en
Priority to US11/892,597 priority patent/US20070293513A1/en
Abandoned legal-status Critical Current

Links

Images

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D487/00Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, not provided for by groups C07D451/00 - C07D477/00
    • C07D487/02Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, not provided for by groups C07D451/00 - C07D477/00 in which the condensed system contains two hetero rings
    • C07D487/04Ortho-condensed systems
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P11/00Drugs for disorders of the respiratory system
    • A61P11/06Antiasthmatics
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P13/00Drugs for disorders of the urinary system
    • A61P13/02Drugs for disorders of the urinary system of urine or of the urinary tract, e.g. urine acidifiers
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P13/00Drugs for disorders of the urinary system
    • A61P13/12Drugs for disorders of the urinary system of the kidneys
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/06Antimigraine agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P29/00Non-central analgesic, antipyretic or antiinflammatory agents, e.g. antirheumatic agents; Non-steroidal antiinflammatory drugs [NSAID]
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • A61P35/04Antineoplastic agents specific for metastasis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P41/00Drugs used in surgical methods, e.g. surgery adjuvants for preventing adhesion or for vitreum substitution
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P43/00Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P7/00Drugs for disorders of the blood or the extracellular fluid
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P7/00Drugs for disorders of the blood or the extracellular fluid
    • A61P7/02Antithrombotic agents; Anticoagulants; Platelet aggregation inhibitors
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/04Inotropic agents, i.e. stimulants of cardiac contraction; Drugs for heart failure
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/10Drugs for disorders of the cardiovascular system for treating ischaemic or atherosclerotic diseases, e.g. antianginal drugs, coronary vasodilators, drugs for myocardial infarction, retinopathy, cerebrovascula insufficiency, renal arteriosclerosis
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/14Vasoprotectives; Antihaemorrhoidals; Drugs for varicose therapy; Capillary stabilisers

Definitions

  • the present invention relates to forms of a chemical compound, in particular to crystalline and amorphous forms, more particularly four crystalline forms and an amorphous form.
  • the invention further relates to processes for the preparation of such forms, to pharmaceutical compositions comprising the compound in crystalline and/or amorphous form and to the therapeutic use of such forms.
  • the drug substance In the formulation of drug compositions, it is important for the drug substance to be in a form in which it can be conveniently handled and processed. This is of importance, not only from the point of view of obtaining a commercially viable manufacturing process, but also from the point of subsequent manufacture of pharmaceutical formulations comprising the active compound. Chemical stability, solid state stability, and shelf life of the active ingredients are also very important factors.
  • the drug substance, and compositions containing it should be capable of being effectively stored over appreciable periods of time, without exhibiting a significant change in the active component's physico-chemical characteristics (e.g. its chemical composition, density, hygroscopicity and solubility). Moreover, it is also important to be able to provide drug in a form which is as pure as possible.
  • Amorphous materials may present significant problems in this regard. For example, such materials are typically more difficult to handle and to formulate than crystalline material, provide for unreliable solubility, and are often found to be unstable and chemically impure.
  • the skilled person will appreciate that, if a drug can be readily obtained in a stable crystalline form, the above problems may be solved.
  • drug compositions it is desirable, wherever possible, to provide drug in a substantially crystalline, and stable. form. It is to be noted, however, that this goal is not always achievable. Indeed, typically, it is not possible to predict, from molecular structure alone, what the crystallisation behaviour of a compound will be, and this can usually only be determined empirically.
  • the process of platelet adhesion to the sub-endothelial surface may have an important role to play in the repair of damaged vessel walls, the platelet aggregation that this initiates can precipitate acute thrombotic occlusion of vital vascular beds, leading to events with high morbidity such as myocardial infarction and unstable angina.
  • the success of interventions used to prevent or alleviate these conditions, such as thrombolysis and angioplasty are also compromised by platelet-mediated occlusion or re-occlusion.
  • ADP adenosine 5′-diphosphate
  • P 2T receptor subtype located on the platelet membrane.
  • the P 2T receptor also known as P2Y ADP or P2T AC
  • P2Y ADP or P2T AC is to primarily involved in mediating platelet aggregation/activation and is a G-protein coupled receptor which is as yet uncloned.
  • the pharmacological characteristics of this receptor have been described, for example, in the references by Humphries et al., Br. J. Pharmacology ( 1994), 113, 1057-1063, and Fagura et al., Br. J.
  • the compound of formula (I) is conventionally named: ⁇ 1S-[1 ⁇ , 2 ⁇ , 3 ⁇ (1S*,2R*),5 ⁇ ] ⁇ -3-(7- ⁇ [2-(3,4difluorophenyl)cyclopropyl[amino ⁇ -5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol.
  • the compound of formula (I) may exist in four different substantially crystalline forms referred to hereafter as Polymorph I, Polymorph II, Polymorph III and Polymorph IV.
  • a polymorph is a particular crystalline form of a compound.
  • the preferred crystalline form of the compound of formula (I) is in the form of Polymorph I, Polymorph II, Polymorph m and/or Polymorph IV.
  • a preferred crystalline form of the compound of formula (I) is Polymorph I.
  • a preferred crystalline form of the compound of formula (I) is Polymorph II.
  • a preferred crystalline form of the compound of formula (I) is Polymorph III.
  • the compound of formula (I) is in a substantially amorphous form.
  • an amorphous form the three dimensional long range order that normally exists in a crystalline form (for example in a polymorph) does not exist, and the positions of the molecules relative to one another in the amorphous form are essentially random (see B. C. Hancock and G. Zografi, J. Pharm. Sci. (1997) 86 1).
  • the amorphous form of the compound of formula (I) is referred to as Form ⁇ .
  • anhydrous form of the compound of formula (I) in a crystalline form or an amorphous form is provided.
  • anhydrous form of the compound of formula (I) in a crystalline form or an amorphous form By the use of the term “substantially pure and essentially in the anhydrous form”, we do not exclude the presence of some solvent, including water, within the crystal lattice structure or outside the crystal lattice structure.
  • An anhydrous form has less than 0.4 water molecules per compound molecule (less than 40% hydrated).
  • the anhydrous form contains less than 0.1 water molecules per compound molecule.
  • Polymorphs I, II, III and IV can be distinguished by reference to their onset of melting, powder X-ray diffraction patterns and/or single crystal X-ray data,
  • Polymorph I has an onset of melting which is in the range 146-152° C., for example about 151° C., when it is substantially pure and essentially in the anhydrous form.
  • Polymorph II has an onset of melting that is in the range 136-139° C., for example about 137.5° C., when it is substantially pure and essentially in the anhydrous form.
  • Polymorph III has an onset of melting that is in the range 127-132° C., for example about 132° C., when it is substantially pure and essentially in the anhydrous form.
  • Polymorph IV has an onset of melting which is typically about 139° C., when it is substantially pure and essentially in the anhydrous form.
  • Form ⁇ typically undergoes a glass transition followed by crystallisation into one of the above Polymorph forms, for example Polymorph II, prior to melting.
  • the melting points were determined using differential scanning calorimetry (DSC) using Perkin Elmer DSC7 instrumentation.
  • DSC differential scanning calorimetry
  • the onset of melting is defined as the point at which a significant change from the baseline occurs and was measured by Perkin Elmer Pyris software. It will be appreciated that alternative readings of melting point may be given by other types of equipment or by using conditions different to those described here. Hence the figures quoted are not to be taken as absolute values. The skilled person will realise that the precise value of the melting point will be influenced by the purity of the compound, the sample weight, the heating rate and the particle size.
  • Polymorph I when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 5.3° ( ⁇ 0.1°), 20.1° ( ⁇ 0.1), 20.7° ( ⁇ 0.1°), 21.0° ( ⁇ 0.1°) and 21.3° ( ⁇ 0.1°) 2 ⁇ .
  • substantially pure and essentially anhydrous Polymorph I has an X-ray powder diffraction pattern containing specific peaks at 5.3° ( ⁇ 0.1°), 8.0° ( ⁇ 0.1°), 9.6° ( ⁇ 0.1°), 13.9° ( ⁇ 0.1°), 15.3° ( ⁇ 0.1°), 20.1° ( ⁇ 0.1° ), 20.7° ( ⁇ 0.1°), 21.0° ( ⁇ 0.1°), 21.3° ( ⁇ 0.1°), 26.2° ( ⁇ 0.1°) and 27.5° ( ⁇ 0.1°) 2 ⁇ .
  • Polymorph II when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 5.5° ( ⁇ 0.1°), 13.5° ( ⁇ 0.1°), 18.3° ( ⁇ 0.1°), 22.7° ( ⁇ 0.1°) and 24.3° ( ⁇ 0.1°) 2 ⁇ .
  • substantially pure and essentially anhydrous Polymorph II has an X-ray powder diffraction pattern containing specific peaks at 5.5° ( ⁇ 0.1°), 6.8° ( ⁇ 0.1°), 10.6° ( ⁇ 0.1°), 13.5° ( ⁇ 0.1°), 14.9° ( ⁇ 0.1°), 18.3° ( ⁇ 0.1°), 19.2° ( ⁇ 0.1°), 22.7° ( ⁇ 0.1°), 24.3° ( ⁇ 0.1°) and 27.1° ( ⁇ 0.1°) 2 ⁇ .
  • Polymorph III when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 14.0° ( ⁇ 0.1°), 17.4° ( ⁇ 0.1°), 18.4° ( ⁇ 0.1°), 21.4° ( ⁇ 0.1°) and 24.1° ( ⁇ 0.1°) 2 ⁇ .
  • substantially pure and essentially anhydrous Polymorph m has an X-ray powder diffraction pattern containing specific peaks at 5.6° ( ⁇ 0.1°), 12.5° ( ⁇ 0.1°), 14.0° ( ⁇ 0.1°), 17.4° ( ⁇ 0.1°), 18.4° ( ⁇ 0.1°), 21.4° ( ⁇ 0.1°), 22.2° ( ⁇ 0.1°), 22.9° ( ⁇ 0.1°), 24.1° ( ⁇ 0.1°) and 24.5° ( ⁇ 0.1°) 2 ⁇ .
  • Polymorph IV when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 4.9° ( ⁇ 0.1°), 9.2° ( ⁇ 0.1°), 11.6° ( ⁇ 0.1°), 15.6° ( ⁇ 0.1°) and 16.4° ( ⁇ 0.1°) 2 ⁇ .
  • substantially pure and essentially anhydrous Polymorph IV has an X-ray powder diffraction pattern containing specific peaks at 4.9° ( ⁇ 0.1°), 6.0° ( ⁇ 0.1°), 9.2° ( ⁇ 0.1°), 11.6° ( ⁇ 0.1°), 12.8° ( ⁇ 0.1°), 15.6° ( ⁇ 0.1°), 16.4° ( ⁇ 0.1°), 17.2° ( ⁇ 0.1°) and 18.1° ( ⁇ 0.1°) 2 ⁇ .
  • Form ⁇ when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing no sharp peaks.
  • a solvated form may be formed, for example, a hydrated form (a “hydrate”). Therefore in this aspect of the invention there is provided a hydrate of the compound of formula (I) in crystalline form.
  • a hydrate has 0.8 or more water molecules per compound molecule (80% or more hydrated).
  • a hemi-hydrate has between 0.4 and 0.8 water molecules per compound molecule (40-80% hydrated).
  • the mixture is of Polymorph I, Polymorph II, Polymorph III, Polymorph IV and/or Form ⁇ . More preferably, the invention provides any mixture of Polymorph II and Polymorph III.
  • a process for the production of a crystalline form of the compound of formula (I) by crystallisation of the compound of formula (I) from a suitable solvent is selected from the group: ethanol, ethyl acetate, iso-propanol, iso-octane, acetonitrile, water, or a mixture thereof. More preferably, the solvent is selected from the group: ethanol, ethyl acetate, iso-propanol, iso-octane, water, or a mixture thereof.
  • the solvent is selected from the group: a mixture of methanol and water, ethanol, ethyl acetate, a mixture of ethanol and water, a mixture of iso-propanol and water, a mixture of ethyl acetate and iso-octane, and acetonitrile.
  • the compound of formula (I) can be prepared by methods analogous to those described in WO 9905143.
  • Crystallisation of the compound of formula (I) from an appropriate solvent system may be achieved by attaining supersaturation, for example, by cooling, by solvent evaporation and or by the addition of an anti-solvent (a solvent in which the compound of formula (I) is poorly soluble; examples of suitable anti-solvents include heptane or isooctane). Crystallisation temperatures and times will vary depending upon the concentration of the compound in solution, the solvent system used and the method of crystallisation adopted.
  • the compound of formula (I) in crystalline form may be isolated from the above reaction mix using techniques well known to those skilled in the art, for example, by decanting, filtration or centrifuging. Similarly the compound of formula (I) in crystalline form may be dried in accordance with well-known procedures.
  • the crystallisation is carried out directly from the reaction solution.
  • the crystallisation is performed from a subsequent solution.
  • a process for preparing Polymorph I which comprises obtaining a few seed crystals of Polymorph I from the slow crystal growth of Polymorph I from a melt of Polymorph II, and using this to seed a reaction mixture comprising of the compound of formula (I), and a suitable mixed solvent system such as methanol/water.
  • a process for preparing Polymorph III which comprises crystallisation in a suitable solvent such as an alcohol, for example ethanol or isopropyl alcohol (IPA), in particular seeding with crystals of Polymorph m or slurrying a compound of formula (I) in a suitable solvent such as IPA.
  • a suitable solvent such as an alcohol, for example ethanol or isopropyl alcohol (IPA)
  • IPA isopropyl alcohol
  • a process for preparing Polymorph IV which comprises crystallisation from a suitable solvent such as acetonitrile, in particular seeding with crystals of Polymorph IV or a period of slurrying a compound of formula (I) in a suitable solvent such as acetonitrile.
  • a further feature of the invention provides a process for preparing Polymorph III substantially free of Polymorph II, which comprises, for example, slurrying a compound of formula (I) in C 1-6 aliphatic alcohol/water solvent system (preferably IPA/water) at a temperature of 5-65° C. for 1-10 days.
  • C 1-6 aliphatic alcohol/water solvent system preferably IPA/water
  • a process for the production of the compound of formula (I) in substantially amorphous form which comprises freeze drying or spray drying a solution of a compound of Formula (I) using a suitable solvent system, for example ethanol/water.
  • substantially free refers to less than 10% of the other polymorph, preferably less than 5%.
  • the compound of formula (I) in crystalline and/or amorphous form acts as P 2T (P2Y ADP or P2T AC ) receptor antagonists. Accordingly, the compound of formula (I) in crystalline and/or amorphous form is useful in therapy, including combination therapy.
  • the compound of formula (I) in crystalline form is indicated for use in the treatment or prophylaxis of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease.
  • Arterial thrombotic complications may include unstable angina, primary arterial thrombotic complications of atherosclerosis such as thrombotic or embolic stroke, transient ischaemic attacks, peripheral vascular disease, myocardial infarction with or without thrombolysis, arterial complications due to interventions in atherosclerotic disease such as angioplasty, including coronary angioplasty (PTCA), endarterectomy, stent placement, coronary and other vascular graft surgery, thrombotic complications of surgical or mechanical damage such as tissue salvage following accidental or surgical trauma, reconstructive surgery including ski and muscle flaps, conditions with a diffuse thrombotic/platelet consumption component such as disseminated intravascular coagulation, thrombotic thrombocytopaenic purpura, haemolytic uraemic syndrome, thrombotic complications of septicaemia, adult respiratory distress syndrome, anti-phospholipid syndrome, heparin-induced thrombocytopaenia and pre-eclampsia/eclampsia
  • platelet concentrates, or shunt occlusion such as in renal dialysis and plasmapheresis, thrombosis secondary to vascular damage/inflammation such as vasculitis, arteritis, glomerulonephritis, inflammatory bowel disease and organ graft rejection, conditions such as migraine, Raynaud's phenomenon, conditions in which platelets can contribute to the underlying inflammatory disease process in the vascular wall such as atheromatous plaque formation/progression, stenosis/restenosis and in other inflammatory conditions such as asthma, in which platelets and platelet-derived factors are implicated in the immunological disease process. Further indications include treatment of CNS disorders and prevention of the growth and spread of tumours.
  • a compound of formula (I) in crystalline and/or amorphous form for use in a method of treatment of the human or animal body by therapy.
  • the compound of formula (I) in crystalline and/or amorphous form for use as a medicament.
  • the compound of formula (I) in crystalline and/or amorphous form is used as a medicament to antagonise the P 2T (P2Y ADP or P2T AC ) receptor in a warm-blooded animal such as a human being.
  • the compound of formula (I) in crystalline and/or amorphous form is used as a medicament for treating or preventing arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease in a warm-blooded animal such as a human being.
  • the use of the compound of formula (I) in crystalline and/or amorphous form in the manufacture of a medicament for use as an antagonist of the P 2T (P2Y ADP or P2T AC ) receptor in particular there is further provided the use of the compound of formula (I) in crystalline and/or amorphous form in the manufacture of a medicament for use in the treatment or prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease.
  • the invention also provides a method of treatment or prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease, which comprises administering to a person suffering from or susceptible to such a disorder a therapeutically effective amount of the compound of formula (I) in crystalline and/or amorphous form.
  • the compound of formula (I) in crystalline and/or amorphous form may be administered on its own or as a pharmaceutical composition comprising the compound of formula (I) in crystalline and/or amorphous form in combination with a pharmaceutically acceptable diluent, adjuvant and/or carrier. Therefore there is provided as a further feature of the invention a pharmaceutical composition comprising the compound of formula (I) in crystalline and/or amorphous form in association with a pharmaceutically acceptable diluent, adjuvant and/or carrier. Particularly preferred are compositions not containing material capable of causing an adverse reaction, such as an adverse allergic reaction.
  • Dry powder formulations and pressurised HFA aerosols of the compound of formula (I) in crystalline and/or amorphous form may be administered by oral or nasal inhalation.
  • the compound of formula (I) in crystalline and/or amorphous form is desirably finely divided.
  • the compound of formula (I) in crystalline and/or amorphous form may also be administered by means of a dry powder inhaler.
  • the inhaler may be a single or a multi dose inhaler, and may be a breath actuated dry powder inhaler.
  • One possibility is to mix the finely divided compound of formula (I) in crystalline and/or amorphous form with a carrier substance, e.g. a mono-, di- or polysaccharide, a sugar alcohol or another polyol. Suitable carriers include sugars and starch.
  • a carrier substance e.g. a mono-, di- or polysaccharide, a sugar alcohol or another polyol.
  • Suitable carriers include sugars and starch.
  • the finely divided compound of formula (I) in crystalline and/or amorphous form may be coated by another substance.
  • the powder mixture may also be dispensed into hard gelatine capsules, each containing the desired dose of the active compound of formula (I) in crystalline and/or amorphous form.
  • the compound of formula (I) in crystalline and/or amorphous form may be admixed with an adjuvant or a carrier, e.g. lactose, saccharose, sorbitol, mannitol, starches such as potato starch, corn starch or amylopectin, cellulose derivatives, a binder such as gelatine or polyvinylpyrrolidone, and a lubricant such as magnesium stearate, calcium stearate, polyethylene glycol, waxes, paraffin, and the like, and then compressed into tablets.
  • a carrier e.g. lactose, saccharose, sorbitol, mannitol, starches such as potato starch, corn starch or amylopectin, cellulose derivatives, a binder such as gelatine or polyvinylpyrrolidone, and a lubricant such as magnesium stearate, calcium stearate, polyethylene glycol, waxes, par
  • the compound of formula (I) in crystalline and/or amorphous form may be admixed with e.g. a vegetable oil or polyethylene glycol.
  • Hard gelatine capsules may contain granules of the compound using either the above mentioned excipients for tablets, e.g. lactose, saccharose, sorbitol, mannitol, starches, cellulose derivatives or gelatine. Also liquid or semisolid formulations of the drug may be filled into hard gelatine capsules.
  • Liquid preparations for oral application may be in the form of syrups or suspensions, for example solutions containing the compound of formula (I) in crystalline and/or amorphous form, the balance being sugar and a mixture of ethanol, water, glycerol and propylene glycol.
  • Such liquid preparations may contain colouring agents, flavouring agents, saccharine and carboxymethylcellulose as a thickening agent or other excipients known to those skilled in art.
  • FIG. 1. 1 is an X-ray diffraction pattern for Polymorph I was obtained using a Philips X'Pert MPD machine in ⁇ - ⁇ configuration over the scan range 1° to 40° 2 ⁇ with 2 or 5 seconds exposure per 0.02° 2 ⁇ increment.
  • the X-rays were generated by a copper long-fine focus tube operated at 40 kV and 50 mA.
  • the wavelength of the X-rays was 1.5406 ⁇ .
  • FIG. 1.2 is an X-ray diffraction pattern for Polymorph II obtained using a Siemens D5000 machine in ⁇ - ⁇ configuration over the scan range 2° to 30° 2 ⁇ with 4 seconds exposure per 0.02° 2 ⁇ increment.
  • the X-rays were generated by a copper long-fine focus tube operated at 45 kV and 40 mA.
  • the wavelength of the X-rays was 1.5406 ⁇ .
  • Data were collected using a zero background on which ⁇ 10 mg of the compound was placed.
  • the holder was made from a single crystal of silicon, which had been cut along a non-diffracting plane and then polished to an optically flat finish The X-rays incident upon this surface were negated by Bragg extinction.
  • FIG. 1. 4 is an X-ray diffraction pattern for Polymorphs IV obtained using a Siemens D5000 machine as described above.
  • FIG. 1. 5 is an X-ray diffraction pattern for Form a obtained using a Siemens D5000 machine as described above.
  • a solution comprising of the compound of formula (I), 5 ml/g methanol and 7.3 ml/g water and a small quantity of seeds of Polymorph I, was crystallised at 30° C. XRPD and DSC confirmed that substantially pure Polymorph I had been formed.
  • Ethanol 200 ⁇ l was added to 10 mg of the compound of formula (I) and the mixture warmed to dissolution over a steam bath. The resulting solution was left to crystallise over night.
  • XRPD and DSC confirmed that a mixture of Polymorphs II and III had been formed. This material was used to seed a larger scale preparation: 191 mg of Polymorph II were slurried in 1 ml of a 50% aqueous solution of isopropanol. To this slurry, 15 mg of seeds of mixed Polymorph II/III were added. After 2 days complete conversion into Polymorph III had occurred as shown by XRPD.
  • the starting materials are either commercially available or are readily prepared by standard methods from known materials. For example the following reactions are illustrations but not limitations of the preparation of some of the starting materials used in the above reactions.
  • DIBAL-H® (1.0M solution in hexanes, 5.15 ml) was added to an ice-cooled solution of ⁇ 3aR-[3a ⁇ ,4 ⁇ ,6 ⁇ (1R*,2S*),6a ⁇ ] ⁇ - ⁇ [6-(7- ⁇ [2-(3,4-Difluorophenyl)cyclopropyl]amino ⁇ -5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl)-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-yl]oxy ⁇ acetic acid, methyl ester (Method B, 0.76 g) in THF (1 ml) and the solution was stirred at this temperature for 2 hours.
  • the title compound may be prepared according to the procedure described in WO 9905143.
  • Mass Spectra were measured as follows: EI spectra were obtained on a VG70-250S or Finnigan Mat Incos-XL spectrometer, FAB spectra were obtained on a VG70-250SEQ spectrometer, ESI and APCI spectra were obtained on Finnigan Mat SSQ7000 or a Micromass Platform spectrometer.

Abstract

The invention provides new forms of a chemical compound of formula (I). The invention relates to forms fo a chemical compound (I), in particular to crystalline and amorphous forms, more particularly four crystalline forms and an amorphous form. The invention further relates to processes for the preparation of such forms, to pharmaceutical compositions comprising the compound in crystalline and/or amorphous form and to therapeutic use of such forms.
Figure US20030181469A1-20030925-C00001

Description

  • The present invention relates to forms of a chemical compound, in particular to crystalline and amorphous forms, more particularly four crystalline forms and an amorphous form. The invention further relates to processes for the preparation of such forms, to pharmaceutical compositions comprising the compound in crystalline and/or amorphous form and to the therapeutic use of such forms. [0001]
  • In the formulation of drug compositions, it is important for the drug substance to be in a form in which it can be conveniently handled and processed. This is of importance, not only from the point of view of obtaining a commercially viable manufacturing process, but also from the point of subsequent manufacture of pharmaceutical formulations comprising the active compound. Chemical stability, solid state stability, and shelf life of the active ingredients are also very important factors. The drug substance, and compositions containing it, should be capable of being effectively stored over appreciable periods of time, without exhibiting a significant change in the active component's physico-chemical characteristics (e.g. its chemical composition, density, hygroscopicity and solubility). Moreover, it is also important to be able to provide drug in a form which is as pure as possible. Amorphous materials may present significant problems in this regard. For example, such materials are typically more difficult to handle and to formulate than crystalline material, provide for unreliable solubility, and are often found to be unstable and chemically impure. The skilled person will appreciate that, if a drug can be readily obtained in a stable crystalline form, the above problems may be solved. Thus, in the manufacture of commercially viable and pharmaceutically acceptable, drug compositions, it is desirable, wherever possible, to provide drug in a substantially crystalline, and stable. form. It is to be noted, however, that this goal is not always achievable. Indeed, typically, it is not possible to predict, from molecular structure alone, what the crystallisation behaviour of a compound will be, and this can usually only be determined empirically. [0002]
  • Platelet adhesion and aggregation arc initiating events in arterial thrombosis. Although the process of platelet adhesion to the sub-endothelial surface may have an important role to play in the repair of damaged vessel walls, the platelet aggregation that this initiates can precipitate acute thrombotic occlusion of vital vascular beds, leading to events with high morbidity such as myocardial infarction and unstable angina The success of interventions used to prevent or alleviate these conditions, such as thrombolysis and angioplasty are also compromised by platelet-mediated occlusion or re-occlusion. [0003]
  • It has been found that [0004] adenosine 5′-diphosphate (ADP) acts as a key mediator of thrombosis. ADP-induced platelet aggregation is mediated by the P2T receptor subtype located on the platelet membrane. The P2T receptor (also known as P2YADP or P2TAC) is to primarily involved in mediating platelet aggregation/activation and is a G-protein coupled receptor which is as yet uncloned. The pharmacological characteristics of this receptor have been described, for example, in the references by Humphries et al., Br. J. Pharmacology (1994), 113, 1057-1063, and Fagura et al., Br. J. Pharmacology (1998) 124, 157-164. Recently it has been shown that antagonists at this receptor offer significant improvements over other anti-thrombotic agents (see J. Med. Chem. (1999) 42, 213). International Patent Application WO 9905143 discloses generically a series of triazolo [4,5-d]pyrimidine compounds having activity as P2T (P2YADP or P2TAC) antagonists. The compound of formula (I) (as depicted below) is embraced by the generic scope of International Patent Application WO 9905143 but is not specifically disclosed therein. This compound exhibits high potency as a P2T (P2YADP or P2TAC) antagonist. It also has a surprisingly high metabolic stability and bioavailibility.
  • Accordingly the present invention relates to the compound of formula (I): [0005]
    Figure US20030181469A1-20030925-C00002
  • in a substantially crystalline form. [0006]
  • The compound of formula (I) is conventionally named: {1S-[1α, 2α, 3β (1S*,2R*),5β]}-3-(7-{[2-(3,4difluorophenyl)cyclopropyl[amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol. [0007]
  • The compound of formula (I) may exist in four different substantially crystalline forms referred to hereafter as Polymorph I, Polymorph II, Polymorph III and Polymorph IV. A polymorph is a particular crystalline form of a compound. [0008]
  • The different physical properties of polymorphic forms with respect to each other and with respect to the amorphous state may influence markedly the chemical and pharmaceutical processing of a compound, particularly when the compound is prepared or used on an industrial scale. [0009]
  • In one aspect of the invention, the preferred crystalline form of the compound of formula (I) is in the form of Polymorph I, Polymorph II, Polymorph m and/or Polymorph IV. [0010]
  • In an alternative aspect of the invention, a preferred crystalline form of the compound of formula (I) is Polymorph I. [0011]
  • In another aspect of the invention, a preferred crystalline form of the compound of formula (I) is Polymorph II. [0012]
  • In a further aspect of the invention, a preferred crystalline form of the compound of formula (I) is Polymorph III. [0013]
  • In an additional aspect of the invention, a preferred crystalline form of the compound of formula (I) is Polymorph IV. [0014]
  • In a further aspect of the invention, the compound of formula (I) is in a substantially amorphous form. In an amorphous form, the three dimensional long range order that normally exists in a crystalline form (for example in a polymorph) does not exist, and the positions of the molecules relative to one another in the amorphous form are essentially random (see B. C. Hancock and G. Zografi, J. Pharm. Sci. (1997) 86 1). The amorphous form of the compound of formula (I) is referred to as Form α. [0015]
  • We have isolated the compound of formula (I) in crystalline and amorphous forms. These forms may exist substantially or essentially free of water (“anhydrous” forms). Therefore in one aspect of the invention there is provided an anhydrous form of the compound of formula (I) in a crystalline form or an amorphous form. By the use of the term “substantially pure and essentially in the anhydrous form”, we do not exclude the presence of some solvent, including water, within the crystal lattice structure or outside the crystal lattice structure. An anhydrous form has less than 0.4 water molecules per compound molecule (less than 40% hydrated). Preferably, the anhydrous form contains less than 0.1 water molecules per compound molecule. [0016]
  • Polymorphs I, II, III and IV can be distinguished by reference to their onset of melting, powder X-ray diffraction patterns and/or single crystal X-ray data, [0017]
  • Polymorph I has an onset of melting which is in the range 146-152° C., for example about 151° C., when it is substantially pure and essentially in the anhydrous form. [0018]
  • Polymorph II has an onset of melting that is in the range 136-139° C., for example about 137.5° C., when it is substantially pure and essentially in the anhydrous form. [0019]
  • Polymorph III has an onset of melting that is in the range 127-132° C., for example about 132° C., when it is substantially pure and essentially in the anhydrous form. [0020]
  • Polymorph IV has an onset of melting which is typically about 139° C., when it is substantially pure and essentially in the anhydrous form. [0021]
  • Form α typically undergoes a glass transition followed by crystallisation into one of the above Polymorph forms, for example Polymorph II, prior to melting. [0022]
  • The melting points were determined using differential scanning calorimetry (DSC) using Perkin Elmer DSC7 instrumentation. The onset of melting is defined as the point at which a significant change from the baseline occurs and was measured by Perkin Elmer Pyris software. It will be appreciated that alternative readings of melting point may be given by other types of equipment or by using conditions different to those described here. Hence the figures quoted are not to be taken as absolute values. The skilled person will realise that the precise value of the melting point will be influenced by the purity of the compound, the sample weight, the heating rate and the particle size. [0023]
  • Polymorph I, when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 5.3° (±0.1°), 20.1° (±0.1), 20.7° (±0.1°), 21.0° (±0.1°) and 21.3° (±0.1°) 2θ. More preferably, substantially pure and essentially anhydrous Polymorph I has an X-ray powder diffraction pattern containing specific peaks at 5.3° (±0.1°), 8.0° (±0.1°), 9.6° (±0.1°), 13.9° (±0.1°), 15.3° (±0.1°), 20.1° (±0.1° ), 20.7° (±0.1°), 21.0° (±0.1°), 21.3° (±0.1°), 26.2° (±0.1°) and 27.5° (±0.1°) 2θ. [0024]
  • Polymorph II, when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 5.5° (±0.1°), 13.5° (±0.1°), 18.3° (±0.1°), 22.7° (±0.1°) and 24.3° (±0.1°) 2θ. More preferably, substantially pure and essentially anhydrous Polymorph II has an X-ray powder diffraction pattern containing specific peaks at 5.5° (±0.1°), 6.8° (±0.1°), 10.6° (±0.1°), 13.5° (±0.1°), 14.9° (±0.1°), 18.3° (±0.1°), 19.2° (±0.1°), 22.7° (±0.1°), 24.3° (±0.1°) and 27.1° (±0.1°) 2θ. [0025]
  • Polymorph III, when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 14.0° (±0.1°), 17.4° (±0.1°), 18.4° (±0.1°), 21.4° (±0.1°) and 24.1° (±0.1°) 2θ. More preferably, substantially pure and essentially anhydrous Polymorph m has an X-ray powder diffraction pattern containing specific peaks at 5.6° (±0.1°), 12.5° (±0.1°), 14.0° (±0.1°), 17.4° (±0.1°), 18.4° (±0.1°), 21.4° (±0.1°), 22.2° (±0.1°), 22.9° (±0.1°), 24.1° (±0.1°) and 24.5° (±0.1°) 2θ. [0026]
  • Polymorph IV, when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing specific peaks of high intensity at 4.9° (±0.1°), 9.2° (±0.1°), 11.6° (±0.1°), 15.6° (±0.1°) and 16.4° (±0.1°) 2θ. More preferably, substantially pure and essentially anhydrous Polymorph IV has an X-ray powder diffraction pattern containing specific peaks at 4.9° (±0.1°), 6.0° (±0.1°), 9.2° (±0.1°), 11.6° (±0.1°), 12.8° (±0.1°), 15.6° (±0.1°), 16.4° (±0.1°), 17.2° (±0.1°) and 18.1° (±0.1°) 2θ. [0027]
  • Form α, when it is substantially pure and essentially in the anhydrous form, has an X-ray powder diffraction pattern containing no sharp peaks. [0028]
  • The X-ray diffraction data for Polymorph II, Polymorph III, Polymorph IV and Form α. were obtained using Siemens D5000 equipment. The X-ray diffraction data for Polymorph I was obtained using a Philips X'Pert MPD machine. It will be appreciated that different equipment and/or conditions may result in slightly different data being generated. Hence the figures quoted are not to be taken as absolute values. [0029]
  • In an alternative aspect of the invention, a solvated form may be formed, for example, a hydrated form (a “hydrate”). Therefore in this aspect of the invention there is provided a hydrate of the compound of formula (I) in crystalline form. A hydrate has 0.8 or more water molecules per compound molecule (80% or more hydrated). A hemi-hydrate has between 0.4 and 0.8 water molecules per compound molecule (40-80% hydrated). [0030]
  • In a further feature of the invention there is provided any mixture of crystalline and/or amorphous forms of the compound of formula (I). Preferably, the mixture is of Polymorph I, Polymorph II, Polymorph III, Polymorph IV and/or Form α. More preferably, the invention provides any mixture of Polymorph II and Polymorph III. [0031]
  • In a further feature of the invention there is provided a process for the production of a crystalline form of the compound of formula (I) by crystallisation of the compound of formula (I) from a suitable solvent. Preferably the solvent is selected from the group: ethanol, ethyl acetate, iso-propanol, iso-octane, acetonitrile, water, or a mixture thereof. More preferably, the solvent is selected from the group: ethanol, ethyl acetate, iso-propanol, iso-octane, water, or a mixture thereof. Suitably, the solvent is selected from the group: a mixture of methanol and water, ethanol, ethyl acetate, a mixture of ethanol and water, a mixture of iso-propanol and water, a mixture of ethyl acetate and iso-octane, and acetonitrile. [0032]
  • The compound of formula (I) can be prepared by methods analogous to those described in WO 9905143. [0033]
  • To initiate crystallisation, seeding with crystal(s) of the compound of formula (I) may be required. Seeding with the required polymorph may be necessary to obtain the polymorph of choice. Crystallisation of the compound of formula (I) from an appropriate solvent system may be achieved by attaining supersaturation, for example, by cooling, by solvent evaporation and or by the addition of an anti-solvent (a solvent in which the compound of formula (I) is poorly soluble; examples of suitable anti-solvents include heptane or isooctane). Crystallisation temperatures and times will vary depending upon the concentration of the compound in solution, the solvent system used and the method of crystallisation adopted. [0034]
  • The compound of formula (I) in crystalline form may be isolated from the above reaction mix using techniques well known to those skilled in the art, for example, by decanting, filtration or centrifuging. Similarly the compound of formula (I) in crystalline form may be dried in accordance with well-known procedures. [0035]
  • Optional recrystallisation step(s) may be performed using the same or different solvent systems to reduce flier impurities, such as amorphous material, chemical impurities or to convert the crystalline form from one polymorph into another polymorph or into a hydrate or an anhydrous form. In addition a conditioning step may be performed, exposing the solid to high humidity, in order to remove amorphous material. [0036]
  • Preferably the crystallisation is carried out directly from the reaction solution. Alternatively the crystallisation is performed from a subsequent solution. [0037]
  • In a further feature of the invention, there is provided a process for preparing Polymorph I, which comprises obtaining a few seed crystals of Polymorph I from the slow crystal growth of Polymorph I from a melt of Polymorph II, and using this to seed a reaction mixture comprising of the compound of formula (I), and a suitable mixed solvent system such as methanol/water. [0038]
  • In a further feature of the invention, there is provided a process for preparing Polymorph II, which comprises crystallisation in a suitable solvent such as ethyl acetate. [0039]
  • In a further feature of the invention, there is provided a process for preparing Polymorph III, which comprises crystallisation in a suitable solvent such as an alcohol, for example ethanol or isopropyl alcohol (IPA), in particular seeding with crystals of Polymorph m or slurrying a compound of formula (I) in a suitable solvent such as IPA. [0040]
  • In a further feature of die invention, there is provided a process for preparing Polymorph IV, which comprises crystallisation from a suitable solvent such as acetonitrile, in particular seeding with crystals of Polymorph IV or a period of slurrying a compound of formula (I) in a suitable solvent such as acetonitrile. [0041]
  • A further feature of the invention provides a process for preparing Polymorph III substantially free of Polymorph II, which comprises, for example, slurrying a compound of formula (I) in C[0042] 1-6 aliphatic alcohol/water solvent system (preferably IPA/water) at a temperature of 5-65° C. for 1-10 days.
  • In a further feature of the invention, there is provided a process for the production of the compound of formula (I) in substantially amorphous form which comprises freeze drying or spray drying a solution of a compound of Formula (I) using a suitable solvent system, for example ethanol/water. [0043]
  • The term “substantially free” refers to less than 10% of the other polymorph, preferably less than 5%. [0044]
  • In a further aspect of the invention, there is provided a compound obtainable by any of the above-mentioned processes. [0045]
  • The compound of formula (I) in crystalline and/or amorphous form acts as P[0046] 2T (P2YADP or P2TAC) receptor antagonists. Accordingly, the compound of formula (I) in crystalline and/or amorphous form is useful in therapy, including combination therapy. In particular, the compound of formula (I) in crystalline form is indicated for use in the treatment or prophylaxis of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease. Arterial thrombotic complications may include unstable angina, primary arterial thrombotic complications of atherosclerosis such as thrombotic or embolic stroke, transient ischaemic attacks, peripheral vascular disease, myocardial infarction with or without thrombolysis, arterial complications due to interventions in atherosclerotic disease such as angioplasty, including coronary angioplasty (PTCA), endarterectomy, stent placement, coronary and other vascular graft surgery, thrombotic complications of surgical or mechanical damage such as tissue salvage following accidental or surgical trauma, reconstructive surgery including ski and muscle flaps, conditions with a diffuse thrombotic/platelet consumption component such as disseminated intravascular coagulation, thrombotic thrombocytopaenic purpura, haemolytic uraemic syndrome, thrombotic complications of septicaemia, adult respiratory distress syndrome, anti-phospholipid syndrome, heparin-induced thrombocytopaenia and pre-eclampsia/eclampsia, or venous thrombosis such as deep vein thrombosis, venoocclusive disease, haematological conditions such as myeloproliferative disease, including thrombocythaemia, sickle cell disease; or in the prevention of mechanically-induced platelet activation in vivo, such as cardiopulmonary bypass and extracorporeal membrane oxygenation (prevention of microthromboembolism), mechanically-induced platelet activation in vitro, such as use in the preservation of blood products, e.g. platelet concentrates, or shunt occlusion such as in renal dialysis and plasmapheresis, thrombosis secondary to vascular damage/inflammation such as vasculitis, arteritis, glomerulonephritis, inflammatory bowel disease and organ graft rejection, conditions such as migraine, Raynaud's phenomenon, conditions in which platelets can contribute to the underlying inflammatory disease process in the vascular wall such as atheromatous plaque formation/progression, stenosis/restenosis and in other inflammatory conditions such as asthma, in which platelets and platelet-derived factors are implicated in the immunological disease process. Further indications include treatment of CNS disorders and prevention of the growth and spread of tumours.
  • According to a further aspect of the present invention there is provided a compound of formula (I) in crystalline and/or amorphous form for use in a method of treatment of the human or animal body by therapy. [0047]
  • According to an additional feature of the present invention there is provided the compound of formula (I) in crystalline and/or amorphous form for use as a medicament. Preferably, the compound of formula (I) in crystalline and/or amorphous form is used as a medicament to antagonise the P[0048] 2T (P2YADP or P2TAC) receptor in a warm-blooded animal such as a human being. More preferably, the compound of formula (I) in crystalline and/or amorphous form is used as a medicament for treating or preventing arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease in a warm-blooded animal such as a human being.
  • According to the invention there is further provided the use of the compound of formula (I) in crystalline and/or amorphous form in the manufacture of a medicament for use as an antagonist of the P[0049] 2T (P2YADP or P2TAC) receptor. In particular there is further provided the use of the compound of formula (I) in crystalline and/or amorphous form in the manufacture of a medicament for use in the treatment or prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease.
  • The invention also provides a method of treatment or prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease, which comprises administering to a person suffering from or susceptible to such a disorder a therapeutically effective amount of the compound of formula (I) in crystalline and/or amorphous form. [0050]
  • The compound of formula (I) in crystalline and/or amorphous form may be administered topically, e.g. to the lung and/or the airways, in the form of solutions, suspensions, HFA aerosols and dry powder formulations; or systemically, e.g. by oral administration in the form of tablets, pills, capsules, syrups, powders or granules, or by parenteral administration in the form of sterile parenteral solutions or suspensions, by subcutaneous administration, or by rectal administration in the form of suppositories or transdermally. [0051]
  • The compound of formula (I) in crystalline and/or amorphous form may be administered on its own or as a pharmaceutical composition comprising the compound of formula (I) in crystalline and/or amorphous form in combination with a pharmaceutically acceptable diluent, adjuvant and/or carrier. Therefore there is provided as a further feature of the invention a pharmaceutical composition comprising the compound of formula (I) in crystalline and/or amorphous form in association with a pharmaceutically acceptable diluent, adjuvant and/or carrier. Particularly preferred are compositions not containing material capable of causing an adverse reaction, such as an adverse allergic reaction. [0052]
  • Dry powder formulations and pressurised HFA aerosols of the compound of formula (I) in crystalline and/or amorphous form may be administered by oral or nasal inhalation. For inhalation the compound of formula (I) in crystalline and/or amorphous form is desirably finely divided. The compound of formula (I) in crystalline and/or amorphous form may also be administered by means of a dry powder inhaler. The inhaler may be a single or a multi dose inhaler, and may be a breath actuated dry powder inhaler. [0053]
  • One possibility is to mix the finely divided compound of formula (I) in crystalline and/or amorphous form with a carrier substance, e.g. a mono-, di- or polysaccharide, a sugar alcohol or another polyol. Suitable carriers include sugars and starch. Alternatively the finely divided compound of formula (I) in crystalline and/or amorphous form may be coated by another substance. The powder mixture may also be dispensed into hard gelatine capsules, each containing the desired dose of the active compound of formula (I) in crystalline and/or amorphous form. [0054]
  • Another possibility is to process the finely divided powder into spheres which break up during the inhalation procedure. This spheronized powder may be filled into the drug reservoir of a multidose inhaler, e.g. that known as the Turbuhaler® in which a dosing unit meters the desired dose which is then inhaled by the patient. With this system the active compound of formula (I) with or without a carrier substance is delivered to the patient. The pharmaceutical composition comprising the compound of formula (I) in crystalline and/or amorphous form may conveniently be tablets, pills, capsules, syrups, powders or granules for oral administration; sterile parenteral or subcutaneous solutions, suspensions for parenteral administration or suppositories for rectal administration. [0055]
  • For oral administration the compound of formula (I) in crystalline and/or amorphous form may be admixed with an adjuvant or a carrier, e.g. lactose, saccharose, sorbitol, mannitol, starches such as potato starch, corn starch or amylopectin, cellulose derivatives, a binder such as gelatine or polyvinylpyrrolidone, and a lubricant such as magnesium stearate, calcium stearate, polyethylene glycol, waxes, paraffin, and the like, and then compressed into tablets. If coated tablets are required, the cores, prepared as described above, may be coated with a concentrated sugar solution which may contain e.g. gum arabic, gelatine, talcum, titanium dioxide, and the like. Alternatively, the tablet may be coated with a suitable polymer dissolved either in a readily volatile organic solvent or an aqueous solvent. [0056]
  • For the preparation of soft gelatine capsules, the compound of formula (I) in crystalline and/or amorphous form may be admixed with e.g. a vegetable oil or polyethylene glycol. Hard gelatine capsules may contain granules of the compound using either the above mentioned excipients for tablets, e.g. lactose, saccharose, sorbitol, mannitol, starches, cellulose derivatives or gelatine. Also liquid or semisolid formulations of the drug may be filled into hard gelatine capsules. [0057]
  • Liquid preparations for oral application may be in the form of syrups or suspensions, for example solutions containing the compound of formula (I) in crystalline and/or amorphous form, the balance being sugar and a mixture of ethanol, water, glycerol and propylene glycol. Optionally such liquid preparations may contain colouring agents, flavouring agents, saccharine and carboxymethylcellulose as a thickening agent or other excipients known to those skilled in art.[0058]
  • FIG. 1.[0059] 1 is an X-ray diffraction pattern for Polymorph I was obtained using a Philips X'Pert MPD machine in θ-θ configuration over the scan range 1° to 40° 2θ with 2 or 5 seconds exposure per 0.02° 2θ increment. The X-rays were generated by a copper long-fine focus tube operated at 40 kV and 50 mA. The wavelength of the X-rays was 1.5406 Å.
  • FIG. 1.2 is an X-ray diffraction pattern for Polymorph II obtained using a Siemens D5000 machine in θ-θ configuration over the [0060] scan range 2° to 30° 2θ with 4 seconds exposure per 0.02° 2θ increment. The X-rays were generated by a copper long-fine focus tube operated at 45 kV and 40 mA. The wavelength of the X-rays was 1.5406 Å. Data were collected using a zero background on which˜10 mg of the compound was placed. The holder was made from a single crystal of silicon, which had been cut along a non-diffracting plane and then polished to an optically flat finish The X-rays incident upon this surface were negated by Bragg extinction.
  • FIG. 1.[0061] 3 is an X-ray diffraction pattern for Polymorphs m obtained using a Siemens D5000 machine as described above.
  • FIG. 1.[0062] 4 is an X-ray diffraction pattern for Polymorphs IV obtained using a Siemens D5000 machine as described above.
  • FIG. 1.[0063] 5 is an X-ray diffraction pattern for Form a obtained using a Siemens D5000 machine as described above.
  • FIG. 2 shows DSC graphs for Polymorph I, II, III and IV and Form a obtained using a Perkin Elmer DSC 7 instrument. The pan type was aluminium with a pierced lid. The sample weight was 1 to 3 mg. The procedure was carried out under a flow of nitrogen gas (30 ml/min) and the temperature range studied was 30° C. to 325° C. at a constant rate of temperature increase of 10° C. per minute.[0064]
  • It should be realised that analysis of samples with grains above 30 microns in size and non-unitary aspect ratios may affect the relative intensity of peaks. The skilled person will also realise that the position of reflections is affected by the precise height at which the sample sits in the diffractometer and the zero calibration of the diffractometer. The surface planarity of the sample may also have a small effect. Hence the diffraction pattern data presented are not to be taken as absolute values. [0065]
  • The invention may be illustrated by the following non-limiting Examples. [0066]
    • EXAMPLE 1 {1S-[1α,2α,3β(1S*,2R*),5β]}-3-(7-{[2-(3,4-difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol in the Form of Polymorph I
  • [0067] Part 1
  • The compound of formula (I) in the form of Polymorph II (2 mg) was heated and cooled in a DSC in the following way: 35 to 143 to 35 to 148 to 35 to 148 to 35° C. This annealing process resulted in the crystallisation of pure Polymorph I as indicated by DSC. [0068]
  • [0069] Part 2
  • A solution comprising of the compound of formula (I), 5 ml/g methanol and 7.3 ml/g water and a small quantity of seeds of Polymorph I, was crystallised at 30° C. XRPD and DSC confirmed that substantially pure Polymorph I had been formed. [0070]
    • EXAMPLE 2 {1S-1α,2α,3β(1S*,2R*),5β]}-3-(7-{[2-(3,4-difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol in the form of Polymorph II
  • Chloroform (150 μl) was added to 45 mg of the compound of formula (I) and the mixture was warmed to dissolution over a steam bath. The resulting solution was left to crystallise over night and dried under flowing nitrogen. XRPD and DSC confirmed that substantially pure Polymorph II had been formed. [0071]
    • EXAMPLE 3 {1S-[1α,2α,3β(1S*,2R*),5β]}-3-(7-{[2-(3,4-difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol in the Form of Polymorph III
  • Ethanol (200 μl) was added to 10 mg of the compound of formula (I) and the mixture warmed to dissolution over a steam bath. The resulting solution was left to crystallise over night. XRPD and DSC confirmed that a mixture of Polymorphs II and III had been formed. This material was used to seed a larger scale preparation: 191 mg of Polymorph II were slurried in 1 ml of a 50% aqueous solution of isopropanol. To this slurry, 15 mg of seeds of mixed Polymorph II/III were added. After 2 days complete conversion into Polymorph III had occurred as shown by XRPD. [0072]
    • EXAMPLE 4 {1S-[1α,2α,3β(1S* ,2R*),5β]}-3-(7-{[2-(3,4-difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol in the Form of Polymorph IV
  • Acetonitrile (0.12 ml) was added to 10mg of the compound of formula (I) and the mixture warmed to dissolution over a steam bath. The warm solution was allowed to cool slowly in a water jacket of hot water. The resulting crystals were dried under nitrogen. XRPD indicated that this was a distinct polymorph. [0073]
    • EXAMPLE 5 {1S-[1α,2α,3β(1S*,2R*),5β]}-3-(7-{[2-(3,4-difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol Predominently in the Form of Form α.
  • The compound of formula (I) (218 mg) was dissolved in a 50% aqueous solution of ethanol (24 ml). To this solution, a further 14.5 ml of water were added dropwise. The resulting saturated solution was then freeze dried using Virtis instrumentation under the following conditions (vacuum 2170 mT, run time 20.2 hours, condensed temperature −52° C., ambient temperature 20.3° C.). [0074]
    • REFERENCE EXAMPLE 1 {1S-[1α,2α,3β(1S*,2R*),5β]}-3-(7-{[2-(3 4-difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl)-5-(2-hydroxyethoxy)cyclopentane-1,2-diol
  • A solution of {3aR-[3aα,4α,6α(1R*,2S*),6aα]}-2-[6-({7-[2-(3,4-difluorophenyl) cyclopropyl]amino-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl}tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4yl)oxy]ethanol (Method A, 0.59 g) in trifluoroacetic acid (15 ml) and water(15 ml) was stirred at room temperature for 30 minutes. The reaction mixture was carefully added to a solution of sodium bicarbonate (21 g) in water (150 ml) and stirred for 30 minutes. The mixture was extracted with ethyl acetate, which was dried and evaporated. The residue was purified (SiO[0075] 2, ethyl acetate as eluent) to afford the title compound (0.44 g). MS (APCI) 523 M+W+, 100%); NMR: 8.95 (1H, d, J=3.3), 7.39-7.21 (2H, m), 7.10-7.00 (1H, m), 5.12 (1H, d, J=6.4), 5.05 (1H, d, J=3.6), 4.96 (1H, q, J=9.0), 4.62-4.54 (2H, m), 3.95 (1H, br s), 3.79-3.73 (1H, m), 3.55-3.47 (4H, m), 3.20-3.13 (1H, m), 2.98-2.81 (2H, m), 2.63 (1H, dt, J=13.6, 8.5), 2.29-2.21 and 2.16-2.09 (1H, m), 2.07-2.00 (1H, m), 1.73-1.33 (4H, m), 0.99 (3H, t, J=7.4).
  • Preparation of Starting Materials [0076]
  • The starting materials are either commercially available or are readily prepared by standard methods from known materials. For example the following reactions are illustrations but not limitations of the preparation of some of the starting materials used in the above reactions. [0077]
  • Method A [0078]
    • {3aR-[3aα,4α,6α(1R*,2S*),6aα]}-2-[6-({7-[2-(3,4Difluorophenyl) cyclopropyl]amino-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]pyrimidin-3-yl}tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-yl)oxy]ethanol
  • DIBAL-H® (1.0M solution in hexanes, 5.15 ml) was added to an ice-cooled solution of {3aR-[3aα,4α,6α(1R*,2S*),6aα]}- {[6-(7-{[2-(3,4-Difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl)-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-yl]oxy} acetic acid, methyl ester (Method B, 0.76 g) in THF (1 ml) and the solution was stirred at this temperature for 2 hours. The reaction mixture was concentrated in vacuo and the residue was dissolved in ethyl acetate (75 ml). A saturated aqueous solution of sodium potassium tartrate (75 ml) was added and the mixture stirred vigorously for 16 hours. The organics were collected and the aqueous re-extracted with ethyl acetate (2×50 ml). The combined organics were dried and concentrated and the residue purified (SiO[0079] 2, isohexane:ethylacetate 1:1 as eluant) to give the title compound (0.63 g). MS (APCI) 563 (M+H30 ,100%).
  • Method B [0080]
    • {3aR-[3aα,4α,6α(1R*,2S*),6aα]}-{[6-(7-{[2-(3,4-Difluorophenyl)cyclopropyl]amino}-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl)-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4yl]oxy}acetic acid, methyl ester
  • To a mixture of [3aR-(3aα,4α,6α,6aα)]-({6-[7-bromo-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol}oxy)acetic acid, methyl ester (Method D, 0.80 g) and (1R-trans)-2-(3,4-difluorophenyl) cyclopropanamine,[R-(R*,R*)]-2,3-dihydroxybutanedioate (1:1) (Method C, 0.61 g) in dichloromethane (25 ml) was added N,N-diisopropylethylamine (0.85 ml). The resulting solution was stirred at room temperature for 16 hours then concentrated in vacuo. Purification (SiO[0081] 2, isohexane:ethylacetate 3:1 as eluant) gave the title compound as a colourless foam (0.77 g). MS (APCI) 591 (M+H+, 100%).
  • Method C [0082]
    • (1R-trans)-2-(3,4-Difluorophenyl)cyclopropananine,[R-(R*,R*)]-2,3- dihydroxybutanedioate (1:1)
  • The title compound may be prepared according to the procedure described in WO 9905143. [0083]
  • Method D [0084]
    • [3aR-(3aα,4α, 6α,6aα)]-({6-[7-Bromo-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol}oxy)acetic acid, Methyl Ester
  • [3aR-(3aα,4α,6α,6aα)]-({6-[7-Amino-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol}oxy)acetic acid, methyl ester (Method E, 1.1 g) and isoamylnitrite (2.4 ml) in bromoform (30 ml) was heated at 80° C. for 30 minutes. The cooled reaction mixture was purified (SiO[0085] 2, ethyl acetate:isohexane 1:4 as eluent) to afford the title compound (0.44 g). MS (APCI) 502/4 (M+H+), 504 (100%).
  • Method E [0086]
    • [3a,R-(3aα,4α,6α,6aα)]-({6-[7-Amino-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol}oxy)acetic acid, Methyl Ester
  • To a solution of [3aR(3aα,4α,6α,6aα)]-6-(7-Amino-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol (Method F, 0.50 g) in TBF (25 ml) at 0° C., was added butyllithium (0.62 ml of 2.5N in hexanes). After 20 minutes, the suspension was treated with a solution of trifluoromethanesulfonyloxy-acetic acid methyl ester (0.34 g) (prepared according to the method of Biton, Tetrahedron, 1995, 51, 10513) in THF (10 ml). The resulting solution was allowed to warm to room temperature then concentrated and purified (SiO[0087] 2, ethyl acetate: hexane 4:6 as eluant) to afford the title compound (0.25 g). MS (APCI) 439 (M+H+, 100%).
  • Method F [0088]
    • [3aR-(3aα,4α,6α,6aα)]-6-[7-Amino-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol
  • [3aR-(3aα,4α,6α,6aα)]-6-[7-Chloro-5-(propylthio)-3H-1,2,3-triazolo[4,5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol (Method G, 13.2 g) in THF (200 ml) containing 0.88 ammonia (5 ml) was stirred for 2 hours then concentrated to dryness and the residue partitioned between water and ethyl acetate. The organics were dried and then concentrated to afford the title compound (12.5 g). MS (APCI) 367 (M+H[0089] +, 100%).
  • Method G [0090]
    • [3aR-(3aα,4α,6α,6aα)]-6-[7-Chloro-5-(propylthio)-3H-1,2,3-triazolo[4.5-d]-pyrimidin-3-yl]-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol
  • Isoamyl nitrite (1.1 ml) was added to a solution of [3aR-(3aα,4α, ,6α,6aα)]-6-{[5-amino-6-Chloro-2-(propylthio)pyrimidin-4-yl]amino}-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol (Method H, 2.0 g) in acetonitrile (100 ml) and the solution was heated at 70° C. for 1 hour. The cooled reaction mixture was concentrated and purified (SiO[0091] 2, ethyl acetate:isohexane 1:3 as eluant) to afford the title compound (1.9 g). MS (APCI) 386 (M+H+, 100%).
  • Method H [0092]
    • [3aR-(3aα,4α,6α,6aα)]-6-{[5-Amino-6-Chloro-2-(propylthio)pyrimidin-4-yl]amino}-tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol
  • Iron powder (3.0 g) was added to a stirred solution of [3aR-(3aα,4α,6α,6aα)]-6-{[6-chloro-5-nitro-2-(propylthio)pyrimidin-4-yl]amino}tetrahydro-2,2- dimethyl-4H-cyclopenta-1,3-dioxol-4-ol (Method I, 2.7 g) in acetic acid (100 ml). The reaction mixture was stirred at room temperature for 2 hours, concentrated to half volume, diluted with ethyl acetate and washed with water. The organic phase was dried and concentrated to afford the title compound (2.0 g). MS (APCI) 375 (M+H[0093] +, 100%).
  • Method I [0094]
    • [3aR-(3aα,4α,6α,6aα)]-6-{[6-Choro-5-nitro-2-(propylthio)pyrimidin-4-yl]amino}tetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol
  • A solution of [3aR-(3aα,4α,6α,6aα)]-6-aminotetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol, hydrochloride (Method J, 10.0 g) and N,N-diisopropylethylamine (35 ml) in THF (600 ml) was stirred for 1 hour. The mixture was filtered and the solution was added over 1 hour to a solution of 4,6-dichloro-5-nitro-2-(propylthio)pyrimidine (WO 9703084, 25 .6 g) in THF (1000 ml) and stirred for a further 2 hours. The solvent volume was reduced in vacuo and ethyl acetate was added (1000 ml). The mixture was washed with water and the organic layers were dried, evaporated and purified (SiO[0095] 2, isohexane-ethyl acetate as eluant) to afford the title compound (14.2 g). MS (APCI) 405 (M+H+, 100%).
  • Method J [0096]
    • [3aR-(3aα,4α,6α,6aα)]-6-Aminotetrahydro-2,2-dimethyl-4H-cyclopenta-1,3-dioxol-4-ol, Hydrochloride [1R-(1α,2β,3β,4α)]-2,3,4-Trihydroxycyclopentenylimidodicarbonic acid, bis(1,1-dimethylethyl) ester (Method K, 17.4 g) in 6M HCl (100 ml)/methanol (500 ml) was stirred for 18 hours. The mixture was evaporated and then azeotroped with toluene (4×200 ml) to give a colourless powder (8.7 g). This solid was suspended in acetone (250 ml) containing 2,2-dimethoxypropane (25 ml) and conc. HCl (0.2 ml) then heated under reflex for 2 hours. The mixture was cooled, evaporated and azeotroped with toluene (3×200 ml). The residue was dissolved in 20% aqueous acetic acid and stirred for 2 hours. The mixture was evaporated and azeotroped with toluene (4×200 ml) to afford the title compound (10.1 g). MS (APCI) 174 (M+H+, 100%)
  • Method K [0097]
    • [1R-(1α,2β,3β,4α]-2,3,4-Trihydroxycyclopentenylimidodicarbonic acid, bis(1,1-dimethylethyl) ester
  • To a solution of (1R-cis)-Bis(1,1-dimethylethyl)-4hydroxy-2-cyclopentenylimido-dicarbonate (Method L, 17.1 g) in THF (500 ml)/water (50 ml) was added N-methylmorpholine-N-oxide (9.4 g) followed by osmium tetroxide (10 ml, 2.5% solution in t-butanol). The mixture was stirred at room temperature for 4 days then treated with sodium hydrosulphite (6.0 g). The suspension was filtered through diatomaceous earth and the product purified (SiO[0098] 2, ethyl acetate: hexane 1:1 as eluant) to afford the title compound (19.1 g). NMR: 1.44 (18H, s), 1.46-1.60 (1H, m), 1.97-2.05 (1H, m), 3.55-3.58 (1H, m), 3.66-3.73 (1H, m), 4.11-4.21 (2H, m), 4.54 (1H, d,J=4.8), 4.56 (1H, d,J=5.9), 4.82 (1H, d, J=4.6).
  • Method L [0099]
    • (1R-cis)-Bis(1,1-dimethylethyl)-4-hydroxy-2-cyclopentenylimidodicarbonate
  • To a suspension of ether washed sodium hydride (60% dispersion in oil; 0.31 g) in THF (30 ml) was added imidodicarbonic acid bis-(1,1-dimethylethyl)ester (1.84 g). The mixture was stirred at 40° C. for 1 hour. To the mixture, at ambient temperature, was then added (1S-cis)-4-acetoxy-2-cyclopenten-1-ol (0.5 g) and tetrakis(triphenylphosphine)palladium(0) (0.18 g). The reaction mixture was stirred for 24 hours then purified (SiO[0100] 2, ethyl acetate: hexane 1:9 as eluant) to give the title compound as a colourless solid (0.90 g). NMR: 1.43 (18H, s), 1.61 (1H, ddd, J=12.3, 7.7, 6.4), 2.54 (1H, dt, J=12.6, 7.4), 4.51-4.57 (1H, m), 4.86 (1H, tq, J=8.0, 1.8), 4.91 (1H, d, J=5.4), 5.71-5.77 (2H, m).
    • EXAMPLE 2
  • The following illustrate representative pharmaceutical dosage forms containing the compound of formula (I) in crystalline and/or amorphous form (hereafter compound X), for therapeutic or prophylactic use in humans: [0101]
    (a) Tablet I mg/tablet
    Compound X 100
    Lactose Ph.Eur 182.75
    Croscarmellose sodium  12.0
    Maize starch paste (5% w/v paste)  2.25
    Magnesium stearate  3.0
    (b) Tablet II mg/tablet
    Compound X  50
    Lactose Ph.Eur 223.75
    Croscarmellose sodium  6.0
    Maize starch  15.0
    Polyvinylpyrrolidone (5% w/v paste)  2.25
    Magnesium stearate  3.0
    (c) Tablet III mg/tablet
    Compound X  1.0
    Lactose Ph.Eur  93.25
    Croscarmellose sodium  4.0
    Maize starch paste (5% w/v paste)  0.75
    Magnesium stearate  1.0
    (d) Capsule mg/capsule
    Compound X  10
    Lactose Ph.Eur 488.5
    Magnesium stearate  1.5
    (e) Injection I (50 mg/ml)
    Compound X  5.0% w/v
    1N Sodium hydroxide solution 15.0% v/v
    0.1N Hydrochloric acid (to adjust pH to 7.6)
    Polyethylene glycol 400  4.5% w/v
    Water for injection to 100%
    (f) Injection II (10 mg/ml)
    Compound X  1.0% w/v
    Sodium phosphate BP  3.6% w/v
    0.1N Sodium hydroxide solution 15.0% v/v
    Water for injection to 100%
    (g) Injection III (1 mg/ml, buffered to pH6)
    Compound X  0.1% w/v
    Sodium phosphate BP 2.26% w/v
    Citric acid 0.38% w/v
    Polyethylene glycol 400  3.5% w/v
    Water for injection to 100%
  • NMR spectra were measured on a [0102] Varian Unity Inova 300 or 400 spectrometer; NMR data is quoted in the form of delta values for major diagnostic protons, given in parts per million (ppm) relative to tetramethylsilane (TMS) as an internal standard using perdeuterio dimethyl sulphoxide (DMSO-δ6) as solvent unless otherwise indicated; for examples which showed the presence of rotamers in the proton NMR spectra only the chemical shifts of the major rotamer are quoted; coupling constants (J) are given in Hz.
  • Mass Spectra (MS) were measured as follows: EI spectra were obtained on a VG70-250S or Finnigan Mat Incos-XL spectrometer, FAB spectra were obtained on a VG70-250SEQ spectrometer, ESI and APCI spectra were obtained on Finnigan Mat SSQ7000 or a Micromass Platform spectrometer. [0103]
  • Preparative RPLC separadoizs were generally performed using a Novapak®, Bondapak® or Hypersil® column packed with BDSC-18 reverse phase silica [0104]
  • Flash chromatography (indicated in the Examples as (SiO[0105] 2)) was carried out using Fisher Matrix silica, 35-70 μm.
  • Abbreviations [0106]
    THF tetrahydrofuran
    XRPD X-ray Powder Diffraction
    DSC Differential scanning calorimetry

Claims (32)

1. A compound of formula (I):
Figure US20030181469A1-20030925-C00003
in a substantially crystalline form.
2. A compound of formula (I) as claimed in claim 1 that exists in a substantially anhydrous form.
3. A compound of formula (I) as claimed in claim 1, characterised by an X-ray powder diffraction pattern containing specific peaks of high intensity at 5.3° (±0.1°), 20.1° (±0.1°), 20.7° (±0.1°), 21.0° (±0.1°) and 21.3° (±0.1°) 2θ.
4. A compound of formula (I) as claimed in claim 1 or 3, characterised by an X-ray powder diffraction pattern containing specific peaks at 5.3° (±0.1°), 8.0° (±0.1°), 9.6° (±0.1°), 13.9° (±0.1°), 15.3° (±0.1°), 20.1° (±0.1), 20.7° (±0.1°), 21.0° (±0.1°), 21.3° (±0.1°), 26.2° (±0.1°) and 27.5° (±0.1°) 2θ.
5. A compound of formula (I) as claimed in any one of claims 1, 3 or 4, characterised by a differential scanning calorimetry curve to have an onset of melting which is in the range 146-152° C.
6. A compound of formula (I) as claimed in claim 1, characterised by an X-ray powder diffraction pattern containing specific peaks of high intensity at 5.5° (±0.1°), 13.5° (±0.1°), 18.3° (±0.1°), 22.7° (±0.1°) and 24.3° (±0.1°) 2θ.
7. A compound of formula (I) as claimed in claim 1 or 6, characterised by an X-ray powder diffraction pattern containing specific peaks at 5.5° (±0.1°), 6.8° (±0.1°), 10.6° (±0.1°), 13.5° (±0.1°), 14.9° (±0.1°), 18.3° (±0.1°), 19.2° (±0.1°), 22.7° (±0.1°), 24.3° (±0.1°) and 27.1° (±0.1°) 2θ.
8. A compound of formula (I) as claimed in any one of claims 1 to 6 or 7 characterised by a differential scanning calorimetry curve to have an onset of melting which is in the range 136-139° C.
9. A compound of formula (I) as claimed in claim 1, characterised by an X-ray powder diffraction pattern containing specific peaks of high intensity at 14.0° (±0.1°), 17.4° (±0.1°), 18.4° (±0.1°), 21.4° (±0.1°) and 24.1°(±0.1°) 2θ.
10. A compound of formula (I) as claimed in claims 1 or 9, characterised by an X-ray powder diffraction pattern containing specific peaks at 5.6° (±0.1°), 12.5° (±0.1°), 14.0° (±0.1°), 17.4° (±0.1°), 18.4° (±0.1°), 21.4° (±0.1°), 22.2° (±0.1°), 22.9° (±0.1°), 24.1° (±0.1°) and 24.5° (±0.1) 2θ.
11. A compound of formula (I) as claimed in any one of claims 1, 9 or 10 characterised by a differential scanning calorimetry curve to have an onset of melting which is in the range 127-132° C.
12. A compound of formula (I) as claimed in claim 1, characterised by an X-ray powder diffraction pattern containing specific peaks of high intensity at 4.9° (±0.1°), 9.2° (±0.1°), 11.6° (±0.1°), 15.6° (±0.1°) and 16.4° (±0.1°) 2θ.
13. A compound of formula (I) as claimed in claim 1 or 12 characterised by an X-ray powder diffraction pattern containing specific peaks at 4.9° (±0.1°), 6.0° (±0.1°), 9.2° (±0.1°), 11.6° (±0.1°), 12.8° (±0.1°), 15.6° (±0.1°), 16.4° (±0.1°), 17.2° (±0.1°) and 18.1°
14. A compound of formula (I) as claimed in any one of claims 1, 12 or 13 characterised by a differential scanning calorimetry curve to have an onset of melting which at approximately 139° C.
15. A compound of formula (I) in a substantially amorphous form.
16. A compound of formula (I) which is in the form of a hydrate.
17. A mixture of a compound of formula (I) as claimed in any one of claims 6 to 8 and a compound of formula (I) as claimed in any one of claims 9 to 11.
18. A process for the preparation of a compound as claimed in claim 1, wherein the compound of formula (I) is crystallised from a solvent selected from the group: lower alkyl acetates, lower alkyl alcohols, aliphatic and aromatic hydrocarbons, dialkyl ethers, dialkyl ketones, acetonitrile, water, or a mixture thereof.
19. A process as claimed in claim 18, wherein the solvent is selected from the group: ethanol, ethyl acetate, iso-propanol, iso-octane, acetonitrile, water, or a mixture thereof.
20. A process as claimed in claim 19, wherein the solvent is selected from the group: a mixture of methanol and water, ethanol, ethyl acetate, a mixture of ethanol and water, a mixture of iso-propanol and water, a mixture of ethyl acetate and iso-octane, and acetonitrile.
21. A process for the production of a compound as claimed in any one of claims 3 to 5 according to any one of claims 18 to 20 in which the solvent is a mixture of methanol and water.
22. A process for the production of a compound as claimed in any one of claims 3 to 5 using seed.
23. A process according to claim 22 in which the seed is prepared by melting a compound as claimed in any one of claims 6 to 8.
24. A process for the production of a compound as claimed in any one of claims 6 to 8 according to any one of claims 18 to 20, in which the solvent is ethyl acetate.
25. A process for the production of a compound as claimed in any one of claims 9 to 11 according to any one of claims 18 to 20, in which the solvent is an alcohol.
26. A process for the production of a compound as claimed in any one of claims 9 to 11 which comprises slurrying a compound of formula (I) in IPA/water solvent system at a temperature of 5 to 65° C.
27. A process for the production of a compound as claimed in any one of claims 12 to 14, which comprises a process according to any one of claims 18 to 20, in which the solvent is acetonitrile.
28. A compound as claimed in any one of claims 1 to 17 for use as a medicament
29. A pharmaceutical composition comprising a compound as claimed in any one of claims 1 to 17 in admixture with a pharmaceutically acceptable adjuvant, diluent or carrier.
30. A pharmaceutical composition comprising a compound as claimed in any one of claims 1 to 17 for use in the prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease.
31. The use of a compound as claimed in any one of claims 1 to 17 in the manufacture of a medicament for use in the prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease.
32. A method of treatment or prevention of arterial thrombotic complications in patients with coronary artery, cerebrovascular or peripheral vascular disease, which comprises administering to a person suffering from or susceptible to such a disorder a therapeutically effective amount of a compound as claimed in any one of claims 1 to 17.
US10/296,990 2000-06-02 2001-05-31 Crystalline and amorphous form of a triazolo(4,5-d)pyrimidine compound Abandoned US20030181469A1 (en)

Priority Applications (2)

Application Number Priority Date Filing Date Title
US11/240,801 US7265124B2 (en) 2000-06-02 2005-10-03 Cristalline and amorphous form of a triazolo (4,5-D) pyridimine compound
US11/892,597 US20070293513A1 (en) 2000-06-02 2007-08-24 Cristalline and amorphous form of a triazolo (4,5-d) pyridimine compound

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
GB0013407.2 2000-06-02
GBGB0013407.2A GB0013407D0 (en) 2000-06-02 2000-06-02 Forms of a chemical compound

Related Child Applications (1)

Application Number Title Priority Date Filing Date
US11/240,801 Continuation US7265124B2 (en) 2000-06-02 2005-10-03 Cristalline and amorphous form of a triazolo (4,5-D) pyridimine compound

Publications (1)

Publication Number Publication Date
US20030181469A1 true US20030181469A1 (en) 2003-09-25

Family

ID=9892841

Family Applications (3)

Application Number Title Priority Date Filing Date
US10/296,990 Abandoned US20030181469A1 (en) 2000-06-02 2001-05-31 Crystalline and amorphous form of a triazolo(4,5-d)pyrimidine compound
US11/240,801 Expired - Lifetime US7265124B2 (en) 2000-06-02 2005-10-03 Cristalline and amorphous form of a triazolo (4,5-D) pyridimine compound
US11/892,597 Abandoned US20070293513A1 (en) 2000-06-02 2007-08-24 Cristalline and amorphous form of a triazolo (4,5-d) pyridimine compound

Family Applications After (2)

Application Number Title Priority Date Filing Date
US11/240,801 Expired - Lifetime US7265124B2 (en) 2000-06-02 2005-10-03 Cristalline and amorphous form of a triazolo (4,5-D) pyridimine compound
US11/892,597 Abandoned US20070293513A1 (en) 2000-06-02 2007-08-24 Cristalline and amorphous form of a triazolo (4,5-d) pyridimine compound

Country Status (36)

Country Link
US (3) US20030181469A1 (en)
EP (3) EP1289992B1 (en)
JP (3) JP5036947B2 (en)
KR (1) KR100781864B1 (en)
CN (2) CN1817883B (en)
AR (2) AR032335A1 (en)
AT (2) ATE320430T1 (en)
AU (4) AU6287401A (en)
BG (3) BG65837B1 (en)
BR (1) BR0111328A (en)
CA (1) CA2408596C (en)
CY (1) CY1113047T1 (en)
CZ (2) CZ304347B6 (en)
DE (1) DE60117972T2 (en)
DK (2) DK1289992T3 (en)
EE (1) EE05222B1 (en)
ES (2) ES2259031T3 (en)
GB (1) GB0013407D0 (en)
HK (2) HK1052347B (en)
HU (2) HU230471B1 (en)
IL (4) IL152777A0 (en)
IS (2) IS2609B (en)
MX (1) MXPA02011795A (en)
MY (2) MY148652A (en)
NO (3) NO323780B1 (en)
NZ (1) NZ522638A (en)
PH (1) PH12011000127A1 (en)
PL (2) PL359172A1 (en)
PT (2) PT1289992E (en)
RU (3) RU2325391C2 (en)
SG (1) SG135965A1 (en)
SI (2) SI1493745T1 (en)
SK (1) SK287817B6 (en)
UA (1) UA73181C2 (en)
WO (1) WO2001092262A1 (en)
ZA (1) ZA200209324B (en)

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20060041132A1 (en) * 2000-06-02 2006-02-23 Astrazeneca Ab Novel triazolo pyrimidine compounds
US20080108635A1 (en) * 2006-10-31 2008-05-08 Han-Cheng Zhang Triazolopyrimidine derivatives as ADP P2Y12 receptor antagonists
WO2009064249A1 (en) * 2007-11-15 2009-05-22 Astrazeneca Ab A process for the preparation of (3ar,4s, 6r, 6as)-6-amino-2, 2- dimethyltetrahydro-3ah-cyclopenta[d] [1,3] dioxol-4-ol dibenzoyl-l-tartrate and to products of said process

Families Citing this family (63)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
TWI229674B (en) 1998-12-04 2005-03-21 Astra Pharma Prod Novel triazolo[4,5-d]pyrimidine compounds, pharmaceutical composition containing the same, their process for preparation and uses
GB0013407D0 (en) * 2000-06-02 2000-07-26 Astrazeneca Ab Forms of a chemical compound
JP4298212B2 (en) * 2002-03-29 2009-07-15 大日本印刷株式会社 Method for producing high melting point type epinastine hydrochloride
WO2008024044A1 (en) * 2006-08-21 2008-02-28 Astrazeneca Ab Compositions, suitable for oral administration, comprising a triazolo [4, 5] pyrimidin derivate
TWI482772B (en) * 2006-08-21 2015-05-01 Astrazeneca Ab Compositions, suitable for oral administration, comprising a triazolo(4,5-d)pyrimidin derivate
CN103071154A (en) * 2007-04-13 2013-05-01 千年药品公司 Combination anticoagulant therapy with a compound that acts as a factor XA inhibitor
UA100864C2 (en) 2007-12-03 2013-02-11 Астразенека Аб Method for the for the treatment or prevention of abdominal aortic aneurysms
US8563755B2 (en) 2008-09-09 2013-10-22 Astrazeneca Ab Process for preparing [1S-[1-α, 2-α, 3-β(1S*,2R*) 5-β]]-3-[7-[2-(3,4-difluorophenyl)-cyclopropylamino]-5-(propylthio)-3H-1,2,3-triazolo [4,5-d] pyrimidin-3-yl]-5-(2-hydroxyethoxy) cyclopentane-1,2-diol and to its intermediates
ES2605625T3 (en) 2009-07-27 2017-03-15 Auspex Pharmaceuticals, Inc. P2Y12 receptor cyclopropyl modulators
AU2010326361A1 (en) 2009-12-03 2012-06-07 Astrazeneca Ab Co - crystals of a triazolo [4,5 - D] pyrimidine platelet aggregation inhibitor
EP2633857B1 (en) 2009-12-23 2015-08-12 ratiopharm GmbH Solid pharmaceutical dosage form of ticagrelor and acetylsalicylic acid
CZ2011229A3 (en) 2011-04-19 2012-08-15 Zentiva, K.S. Optically active salts of (3aR,4S,6R,6aS)-6-amino-2,2-dimethyltetrahydro-3aH-cyclopenta-[d][1,3]dioxol-4-ole and process for their preparation
CN103764149A (en) 2011-06-01 2014-04-30 阿斯利康(瑞典)有限公司 Novel ticagrelor co-crystal
CN104039792A (en) * 2011-11-30 2014-09-10 阿特维斯集团公司 Novel crystalline form of ticagrelor and process for the preparation thereof
US9233966B2 (en) 2012-04-05 2016-01-12 Dr. Reddy's Laboratories Limited Preparation of ticagrelor
WO2014000719A1 (en) * 2012-06-29 2014-01-03 Zentiva, K.S. Novel pharmaceutical solid forms of (1s,2s,3r,5s)-3-[7-[(1r,2s)-2-(3,4difluorophenyl)cyclopropylamino]-5-(propylthio)-3h-[1,2,3]triazolo[4,5-d]pyrimidin-3yl]-5-(2-hydroxyethoxy)cyclopentane-l,2-diol
EP2870155B1 (en) 2012-07-04 2016-08-24 LEK Pharmaceuticals d.d. Ticagrelor adducts with divalent metal salts
CZ2012705A3 (en) * 2012-10-16 2014-04-23 Zentiva, K.S. Solid oral pharmaceutical formulation containing ticagrelor
CN103772393B (en) * 2012-10-18 2017-08-04 博瑞生物医药(苏州)股份有限公司 Crystal formation of Ticagrelor and preparation method thereof
WO2014083139A1 (en) * 2012-11-29 2014-06-05 Actavis Group Ptc Ehf Novel amorphous form of ticagrelor
CN103848836B (en) * 2012-12-07 2016-08-03 天津市汉康医药生物技术有限公司 Ticagrelor times semihydrate and preparation method thereof
WO2014118808A2 (en) * 2013-02-04 2014-08-07 Hetero Research Foundation Ticagrelor solid dispersion
CZ307217B6 (en) 2013-03-14 2018-04-04 Zentiva, K.S. An improved manufacturing process and new intermediates for synthesis of ticagrelor
WO2014155389A2 (en) * 2013-03-25 2014-10-02 Glenmark Pharmaceuticals Limited; Glenmark Generics Limited Process for preparation of ticagrelor
CN104098570A (en) * 2013-04-07 2014-10-15 杭州领业医药科技有限公司 Crystal form of Ticagrelor Brilinta and preparation method and purpose thereof
CN104098572A (en) * 2013-04-08 2014-10-15 博瑞生物医药技术(苏州)有限公司 Eutectic form of Ticagrelor Brilinta
CN107573333B (en) * 2013-04-10 2019-10-18 江苏恒瑞医药股份有限公司 The preparation method of intermediate of ticagrelor and preparation method thereof and ticagrelor
EP2813216A1 (en) 2013-06-10 2014-12-17 Zentiva, a.s. Stabilized amorphous ticagrelor
WO2014170026A1 (en) 2013-04-18 2014-10-23 Zentiva, K.S. Stabilized amorphous ticagrelor
BR112015029894A2 (en) 2013-05-29 2017-07-25 Ratiopharm Gmbh solid pharmaceutical dosage form
CN104211704B (en) * 2013-06-03 2017-08-25 杭州领业医药科技有限公司 Triazole [4,5 d] pyrimidine compound of crystal habit and its production and use
EP3004113A2 (en) * 2013-06-04 2016-04-13 Dr. Reddy's Laboratories Ltd. Preparation of ticagrelor
EP2816043A1 (en) 2013-06-21 2014-12-24 LEK Pharmaceuticals d.d. Spherical ticagrelor particles
WO2015001489A1 (en) * 2013-07-01 2015-01-08 Ranbaxy Laboratories Limited Pharmaceutical compositions of ticagrelor
CN104341423B (en) * 2013-08-02 2017-03-01 上海京新生物医药有限公司 Monohydrate of ticagrelor and preparation method thereof and the application in pharmacy
CN104370912A (en) * 2013-08-13 2015-02-25 开原亨泰制药股份有限公司 Ticagrelor polycrystal and preparation method thereof
IN2013CH04023A (en) * 2013-09-10 2015-08-07 Laurus Labs Pvt Ltd
CZ2013866A3 (en) 2013-11-08 2015-05-20 Zentiva, K.S. Novel crystalline form of ticagrelor synthesis intermediate and process for preparing thereof
CN104650085A (en) * 2013-11-22 2015-05-27 天津市汉康医药生物技术有限公司 Ticagrelor sesquihydrate compound
CN103601726B (en) * 2013-12-02 2016-09-28 浙江大学 Two kinds of ticagrelor pharmaceutical co-crystals and preparation method thereof
CN104710425B (en) * 2013-12-16 2019-06-14 石药集团中奇制药技术(石家庄)有限公司 A kind of ticagrelor newly crystallizes and preparation method thereof
CN104650091B (en) * 2014-01-24 2016-10-05 福州乾正药业有限公司 The micronization of ticagrelor and crystal formation thereof, and preparation method and medicinal application
CN104940204A (en) * 2014-03-27 2015-09-30 广东东阳光药业有限公司 Ticagrelor solid preparation and preparation method thereof
WO2015162537A1 (en) * 2014-04-23 2015-10-29 Glenmark Pharmaceuticals Limited; Glenmark Generics Limited Process for preparation of ticagrelor
WO2015162630A1 (en) 2014-04-25 2015-10-29 Anlon Chemical Research Organization Novel processes for preparing triazolo [4,5-d]- pyrimidines, including ticagrelor, vianew intermediates and new route of synthesis.
CN105315282B (en) * 2014-07-15 2018-09-21 博瑞生物医药(苏州)股份有限公司 It is a kind of to prepare the unformed method of Ticagrelor
WO2016016907A1 (en) * 2014-08-01 2016-02-04 Msn Laboratories Private Limited Novel polymorphs of (1s,2s,3r,5s)-3-[7-{[(1r,2s)-2-(3,4-difluorophenyl) cyclopropyl]amino}-5-(propylthio)-3h-[1,2,3]-triazolo[4,5-d]pyrimidin-3-yi]-5-(2-hydroxvethoxy) cyclopentane-1,2-diol
US10017515B2 (en) 2014-08-11 2018-07-10 Sun Pharmaceutical Industries Limited Stable amorphous ticagrelor and a process for its preparation
CN104193747B (en) * 2014-08-12 2016-05-11 许彩霞 The unbodied preparation of ADZ6140
WO2016116942A1 (en) 2015-01-20 2016-07-28 Anlon Chemical Research Organization Novel pharmaceutical compounds comprising ticagrelor with salts of aspirin
CN105968113B (en) * 2015-03-12 2019-06-07 四川海思科制药有限公司 A kind of triazolopyrimidine derivative and its application
WO2017072790A1 (en) * 2015-10-26 2017-05-04 Avra Laboratories Pvt. Ltd. An improved process for synthesis of ticagrelor
US20190002471A1 (en) * 2016-01-05 2019-01-03 Amneal Pharmaceuticals Company Gmbh Crystalline Form Of Ticagrelor
PE20190372A1 (en) 2016-04-21 2019-03-08 Astrazeneca Ab ORAL DISGREGATION TABLETS
US10905691B2 (en) 2016-09-09 2021-02-02 Université de Liège Use of triazolo(4,5-d)pyrimidine derivatives for prevention and treatment of bacterial infection
EP3292867B1 (en) * 2016-09-09 2019-05-15 Université de Liège Triazolo(4,5-d)pyrimidine derivatives for use in the prevention and treatment of bacterial infection
KR101916956B1 (en) 2016-12-13 2018-11-08 보령제약 주식회사 Novel Solid form of Ticagrelor and methods of preparing therof
WO2018178997A1 (en) 2017-03-31 2018-10-04 Natco Pharma Limited Novel crystalline form of ticagrelor
WO2019127294A1 (en) * 2017-12-29 2019-07-04 浙江天宇药业股份有限公司 Ticagrelor purification method
EP3761965A1 (en) 2018-03-08 2021-01-13 Pharmaceutical Oriented Services Ltd Ticagrelor-containing tablet formulation
EA202190328A1 (en) 2018-07-27 2021-07-01 КРКА, д.д., НОВО МЕСТО PHARMACEUTICAL COMPOSITION CONTAINING TICAGRELOR
CN110194771A (en) * 2019-05-08 2019-09-03 北京济美堂医药研究有限公司 A kind of preparation method of the medicinal II crystal form of ticagrelor
CN114634489B (en) * 2022-04-19 2023-07-04 奎马特里克斯有限公司 Crystalline forms

Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6525060B1 (en) * 1998-12-04 2003-02-25 Astrazeneca Uk Limited Triazolo(4,5-d)pyrimidine compounds
US20030148888A1 (en) * 2000-06-02 2003-08-07 Ulf Larsson Novel triazolo pyrimidine compounds
US6713483B1 (en) * 1999-11-15 2004-03-30 Astrazeneca Ab [1,2,3]-triazolo[4,5-d] pyrimidine compounds

Family Cites Families (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5561134A (en) * 1990-09-25 1996-10-01 Rhone-Poulenc Rorer Pharmaceuticals Inc. Compounds having antihypertensive, cardioprotective, anti-ischemic and antilipolytic properties
BR9609467A (en) * 1995-07-11 1999-03-02 Astra Pharma Prod Compound use of a compound Pharmaceutical composition and processes for preparing a compound and treating plank aggregation disorders
DE69710490T2 (en) * 1996-12-20 2002-10-24 Astrazeneca Ab TRIAZOLO (4,5-D) PYRIMIDINYL DERIVATIVES AND THEIR USE AS MEDICINES
TW530058B (en) * 1997-07-22 2003-05-01 Astra Pharma Prod Triazolo [4,5-d]pyrimidine compounos and their use and process for preparation
SG106656A1 (en) * 1997-07-25 2004-10-29 Gilead Sciences Inc Nucleotide analog composition and synthesis method
GB0013407D0 (en) * 2000-06-02 2000-07-26 Astrazeneca Ab Forms of a chemical compound

Patent Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6525060B1 (en) * 1998-12-04 2003-02-25 Astrazeneca Uk Limited Triazolo(4,5-d)pyrimidine compounds
US6713483B1 (en) * 1999-11-15 2004-03-30 Astrazeneca Ab [1,2,3]-triazolo[4,5-d] pyrimidine compounds
US20030148888A1 (en) * 2000-06-02 2003-08-07 Ulf Larsson Novel triazolo pyrimidine compounds

Cited By (17)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20100004444A1 (en) * 2000-06-02 2010-01-07 Astrazeneca Ab Novel Triazolo pyrimidine compounds
US20080234481A1 (en) * 2000-06-02 2008-09-25 Astrazeneca Ab Novel triazolo pyrimidine compounds
US20060041132A1 (en) * 2000-06-02 2006-02-23 Astrazeneca Ab Novel triazolo pyrimidine compounds
US7381828B2 (en) 2000-06-02 2008-06-03 AstraZēneca AB Triazolo pyrimidine compounds
US8273879B2 (en) 2000-06-02 2012-09-25 Astrazeneca Ab Triazolo pyrimidine compounds
US20070049755A1 (en) * 2000-06-02 2007-03-01 Astrazeneca Ab Novel triazolo pyrimidine compounds
US20110218330A1 (en) * 2000-06-02 2011-09-08 Astrazeneca Ab Novel triazolo pyrimidine compounds
US7566722B2 (en) 2006-10-31 2009-07-28 Janssen Pharmaceutica, N.V. Triazolopyrimidine derivatives as ADP P2Y12 receptor antagonists
US20080108635A1 (en) * 2006-10-31 2008-05-08 Han-Cheng Zhang Triazolopyrimidine derivatives as ADP P2Y12 receptor antagonists
WO2009064249A1 (en) * 2007-11-15 2009-05-22 Astrazeneca Ab A process for the preparation of (3ar,4s, 6r, 6as)-6-amino-2, 2- dimethyltetrahydro-3ah-cyclopenta[d] [1,3] dioxol-4-ol dibenzoyl-l-tartrate and to products of said process
US7816545B2 (en) 2007-11-15 2010-10-19 Astrazeneca Ab Process 054
US20110009647A1 (en) * 2007-11-15 2011-01-13 Astrazeneca Ab Process 054
US20090182157A1 (en) * 2007-11-15 2009-07-16 Rhony Aufdenblatten New Process 054
AU2008321575B2 (en) * 2007-11-15 2012-07-05 Astrazeneca Ab A process for the preparation of (3aR,4S, 6R, 6aS)-6-amino-2, 2- dimethyltetrahydro-3aH-cyclopenta[d] [1,3] dioxol-4-ol dibenzoyl-L-tartrate and to products of said process
CN101861310A (en) * 2007-11-15 2010-10-13 阿斯利康(瑞典)有限公司 A process for the preparation of (3aR,4S, 6R, 6aS)-6-amino-2, 2- dimethyltetrahydro-3aH-cyclopenta[d] [1,3] dioxol-4-ol dibenzoyl-L-tartrate and to products of said process
RU2477277C2 (en) * 2007-11-15 2013-03-10 Астразенека Аб METHOD FOR PREPARING (3aR, 4S, 6R, 6aS)-6-AMINO-2, 2-DIMETHYLTETRAHYDRO-3aNE-CYCLOPENTA[d][1,3]DIOXOL-4-OLE-DIBENZOYL-TARTRATE AND PRODUCTS OF SAID METHOD
TWI496776B (en) * 2007-11-15 2015-08-21 Astrazeneca Ab A process for preparing a diastereomerically pure dibenzoyl-l-tartrate salt of (3ar, 4s, 6r, 6as)-6-amino-2, 2-dimethyltetrahydro-3ah-cyclopenta(d)(1, 3)-dioxol-4-ol

Also Published As

Publication number Publication date
CY1113047T1 (en) 2016-04-13
AU2010257449A1 (en) 2011-01-20
EP1493745B1 (en) 2012-04-25
PL359172A1 (en) 2004-08-23
RU2325391C2 (en) 2008-05-27
US20070173518A1 (en) 2007-07-26
AU6287401A (en) 2001-12-11
MXPA02011795A (en) 2003-04-10
HUP1300386A2 (en) 2003-10-28
AU2007200958A1 (en) 2007-03-29
KR20030007829A (en) 2003-01-23
JP2012149093A (en) 2012-08-09
NO323780B1 (en) 2007-07-02
SI1493745T1 (en) 2012-08-31
BG111017A (en) 2011-12-30
HK1052347B (en) 2006-09-08
BG110440A (en) 2010-03-31
IS6623A (en) 2002-11-15
SK16852002A3 (en) 2003-08-05
HU229374B1 (en) 2013-11-28
DE60117972D1 (en) 2006-05-11
NO20071547L (en) 2003-01-24
CZ307468B6 (en) 2018-09-26
NO20120595L (en) 2003-01-24
EP1289992B1 (en) 2006-03-15
AU2007200958B2 (en) 2010-10-07
PH12011000127A1 (en) 2016-08-31
NZ522638A (en) 2004-06-25
EE200200665A (en) 2004-06-15
HU230471B1 (en) 2016-07-28
AU2001262874B2 (en) 2007-03-22
DE60117972T2 (en) 2006-11-23
EE05222B1 (en) 2009-10-15
EP1493745B2 (en) 2021-05-19
JP2014129423A (en) 2014-07-10
CN1432018A (en) 2003-07-23
SK287817B6 (en) 2011-11-04
HUP0302284A2 (en) 2003-10-28
IS2609B (en) 2010-04-15
CN1247583C (en) 2006-03-29
RU2010150799A (en) 2012-06-20
BG65837B1 (en) 2010-02-26
ATE320430T1 (en) 2006-04-15
PT1289992E (en) 2006-07-31
HUP0302284A3 (en) 2007-05-29
AR032335A1 (en) 2003-11-05
BG66332B1 (en) 2013-06-28
CZ304347B6 (en) 2014-03-19
BR0111328A (en) 2003-06-10
GB0013407D0 (en) 2000-07-26
IL187482A (en) 2010-06-16
ZA200209324B (en) 2004-02-16
DK1493745T3 (en) 2012-07-16
WO2001092262A1 (en) 2001-12-06
HK1073101A1 (en) 2005-09-23
ES2384708T3 (en) 2012-07-11
EP2292622A1 (en) 2011-03-09
AR068086A2 (en) 2009-11-04
IL152777A (en) 2008-11-26
US7265124B2 (en) 2007-09-04
IL202582A (en) 2012-12-31
IL152777A0 (en) 2003-06-24
JP5036947B2 (en) 2012-09-26
SG135965A1 (en) 2007-10-29
JP5684192B2 (en) 2015-03-11
ES2259031T3 (en) 2006-09-16
ATE555115T1 (en) 2012-05-15
AU2010257449B2 (en) 2012-03-22
MY140674A (en) 2010-01-15
SI1289992T1 (en) 2006-08-31
NO20025756L (en) 2003-01-24
JP2003535092A (en) 2003-11-25
BG107331A (en) 2003-07-31
CN1817883A (en) 2006-08-16
DK1289992T3 (en) 2006-07-03
MY148652A (en) 2013-05-15
IS8825A (en) 2009-06-02
PL392882A1 (en) 2011-03-14
US20070293513A1 (en) 2007-12-20
CZ20120293A3 (en) 2003-07-16
RU2005127356A (en) 2007-03-10
CA2408596C (en) 2010-12-21
EP1289992A1 (en) 2003-03-12
UA73181C2 (en) 2005-06-15
IS3019B (en) 2020-02-15
EP1493745A1 (en) 2005-01-05
NO20025756D0 (en) 2002-11-29
CN1817883B (en) 2011-10-05
NO333289B1 (en) 2013-04-29
HK1052347A1 (en) 2003-09-11
RU2418802C2 (en) 2011-05-20
CA2408596A1 (en) 2001-12-06
PT1493745E (en) 2012-06-28
IL202582A0 (en) 2010-06-30
NO332306B1 (en) 2012-08-20
KR100781864B1 (en) 2007-12-05

Similar Documents

Publication Publication Date Title
US7265124B2 (en) Cristalline and amorphous form of a triazolo (4,5-D) pyridimine compound
AU2001262874A1 (en) New crystalline and amorphous form of a triazolo(4,5-d)pyrimidine compound
WO2001036421A1 (en) Novel [1,2,3]-triazolo[4,5-d]pyrimidine compounds

Legal Events

Date Code Title Description
AS Assignment

Owner name: ASTRA ZENCA AB, SWEDEN

Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNORS:BOHLIN, MARTIN;COGROVE, STEVE;LASSEN, BO;REEL/FRAME:014017/0254;SIGNING DATES FROM 20021030 TO 20021210

STCB Information on status: application discontinuation

Free format text: ABANDONED -- FAILURE TO RESPOND TO AN OFFICE ACTION