WO2003008408A1 - Polymorph of the antihistamine norastemizole - Google Patents

Polymorph of the antihistamine norastemizole Download PDF

Info

Publication number
WO2003008408A1
WO2003008408A1 PCT/US2002/022583 US0222583W WO03008408A1 WO 2003008408 A1 WO2003008408 A1 WO 2003008408A1 US 0222583 W US0222583 W US 0222583W WO 03008408 A1 WO03008408 A1 WO 03008408A1
Authority
WO
WIPO (PCT)
Prior art keywords
norastemizole
temperature
hours
polymoφh
solvent
Prior art date
Application number
PCT/US2002/022583
Other languages
French (fr)
Inventor
Roger P. Bakale
Chris H. Senanayake
Yaping Hong
Kostas Saranteas
Martin P. Redmon
Stephen A. Wald
Original Assignee
Sepracor Inc.
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
Application filed by Sepracor Inc. filed Critical Sepracor Inc.
Publication of WO2003008408A1 publication Critical patent/WO2003008408A1/en

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D401/00Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom
    • C07D401/02Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings
    • C07D401/12Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings linked by a chain containing hetero atoms as chain links
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P37/00Drugs for immunological or allergic disorders
    • A61P37/08Antiallergic agents

Definitions

  • the invention relates to polymorphic crystalline forms of the antihistaminic drug norastemizole and to processes for the production of the preferred polymorph.
  • Norastemizole, 1 - [(4-fluorophenyl)methy 1] -N-4-piperidiny 1- 1 H- benzimidazol-2-amine, is an active metabolite of the histamine H r receptor antagonist astemizole (HISMANALTM). It is described in US patent 6,124,320 for use in the treatment of allergic disorders.
  • polymorphic behavior of drugs can be of crucial importance in pharmacy and pharmacology.
  • Polymorphs are, by definition, crystals of the same molecule having different physical properties as a result of the order of the molecules in the crystal lattice.
  • the differences in physical properties exhibited by polymorphs affect pharmaceutical parameters such as storage stability, compressibility and density (important in formulation and product manufacturing), and dissolution rates (an important factor in determining bio-availability).
  • Differences in stability can result from changes in chemical reactivity (e.g. differential oxidation, such that a dosage form discolors more rapidly when comprised of one polymorph than when comprised of another polymorph) or mechanical changes (e.g.
  • some polymorphic transitions may result in lack of potency or, at the other extreme, toxicity.
  • the physical properties of the crystal may be important in processing: for example, one polymorph might be more likely to form solvates or might be difficult to filter and wash free of impurities (i.e particle shape and size distribution might be different between one polymorph relative to the other).
  • Each pharmaceutical compound has an optimal therapeutic blood concentration and a lethal concentration.
  • the bio-availability of the compound determines the dosage strength in the drug formulation necessary to obtain the ideal blood level. If the drug can crystallize as two or more polymorphs differing in bio- availability, the optimal dose will depend on the polymorph present in the formulation. Some drugs show a narrow margin between therapeutic and lethal concentrations.
  • Chloramphenicol-3-palmitate (CAPP) for example, is a broad spectrum antibiotic known to crystallize in at least three polymorphic forms and one amorphous form. The most stable form, A, is marketed.
  • thermodynamic stability is not sufficient to ensure that the stable polymo ⁇ h will always be produced.
  • the unstable polymo ⁇ h or pseudo polymo ⁇ h in the form of a hydrate or solvate that tends to crystallize first (kinetic form). This is, in essence, Ostwald's Rule of Stages, which posits that an unstable system does not transform directly to the most stable state. Instead, it transforms to a transient state accompanied by the smallest loss of free energy.
  • the invention relates to norastemizole in the form of a crystalline solid comprising at least 95% of a first polymo ⁇ h (hereinafter referred to as polymo ⁇ h A) defined by the X-ray powder diffraction pattern (including both characteristic peaks and intensities) shown below.
  • polymo ⁇ h A a first polymo ⁇ h defined by the X-ray powder diffraction pattern (including both characteristic peaks and intensities) shown below.
  • the invention relates to a process for producing crystalline norastemizole, predominantly as polymo ⁇ h A.
  • the process comprises:
  • the process comprises: (a) dissolving norastemizole in a solvent at a temperature between 70°C and 110°C; (b) adding an amount of anti-solvent sufficient to initiate crystallization at a temperature above 70 °C; (c) stirring at a temperature above 70 °C for at least one hour; (d) adding a second portion of anti-solvent at a temperature above 70 °C and over a period of at least 2 hours, in an amount sufficient to produce crystallization of at least 85%> of dissolved norastemizole; and (e) stirring and cooling from above 70 °C to below 30 °C over the course of at least 6 hours in a non-linear fashion such that no more than a 15%) temperature drop occurs in the first 3 hours.
  • the invention relates to norastemizole (predominantly in the form of polymo ⁇ h A) produced by the process described above.
  • the invention in another aspect, relates to a method for treating allergic conditions in a mammal comprising administering a therapeutically effective amount of norastemizole in the form of polymo ⁇ h A.
  • the invention in another aspect, relates to a pharmaceutical composition
  • a pharmaceutical composition comprising a pharmaceutically acceptable carrier for a solid dosage form and norastemizole in the form of polymo ⁇ h A.
  • FIG. 1 is an Oak Ridge Thermal Ellipsoid Plot (ORTEP) drawing of the norastemizole molecule in one of the two conformations found in both polymo ⁇ hs of crystalline norastemizole.
  • ORTEP Oak Ridge Thermal Ellipsoid Plot
  • FIG. 2 is an ORTEP drawing of the norastemizole molecule in the other of the two conformations found in both polymo ⁇ hs of crystalline norastemizole.
  • FIG. 3 is a representation of the arrangement of molecules of norastemizole in polymo ⁇ h A of crystalline norastemizole.
  • FIG. 4 is a representation of the arrangement of molecules of norastemizole in polymo ⁇ h B of crystalline norastemizole.
  • FIG. 5 is a calculated powder diffraction pattern for polymo ⁇ h A of crystalline norastemizole.
  • FIG. 6 is an experimentally obtained powder diffraction pattern for polymo ⁇ h A of crystalline norastemizole.
  • FIG. 7 is a calculated powder diffraction pattern for polymo ⁇ h B of crystalline norastemizole.
  • FIG. 8 is an experimentally obtained powder diffraction pattern for polymo ⁇ h B of crystalline norastemizole.
  • FIG. 9 is a graph of the solubility of norastemizole polymo ⁇ h A as a function of temperature in three different solvent systems.
  • FIG. 10 is a graph of the solubilities of norastemizole polymo ⁇ h A and polymo ⁇ h B as a function of temperature in 17:10 water/ethanol.
  • FIG. 11 is a graphic representation of the time-course of three parameters (temperature, volume of water added and stirring rate) in a process of the invention.
  • FIG. 12 is a graphic representation of the temperature time during the claimed process.
  • Both polymo ⁇ h A and polymo ⁇ h B have unit cells made up of two molecules and differ only in that a rotation of 180 ° has occurred around the N(l )- C(7) or N(5)-C(26) axis (Fig. 1 and Fig. 2).
  • the hydrogen bonding sequence is between molecules of the same type; in polymo ⁇ h B, the hydrogen bonding sequence alternates. Therefore, the number of hydrogen bonds is the same; it is only the sequence that differs.
  • each polymo ⁇ h has two unique molecules - molecule type (1) (Fig. 1) and molecule type (2) (Fig. 2) - hydrogen bonded in a unit cell.
  • Fig. 1 molecule type (1)
  • Fig. 2 molecule type (2)
  • the hydrogen bonds are between molecules of type (1) or molecules of type (2) but not between the two types.
  • polymo ⁇ h B Fig. 4 molecules of type (1) and (2) are connected in an alternating fashion.
  • the hydrogen bonding can be described in terms of the secondary amine groups in norastemizole.
  • the respective nitrogen atoms can be described as the "linking" nitrogen and the "terminal” nitrogen.
  • the linking nitrogen atoms are designated N(3) and N(7)
  • the terminal nitrogen atoms are designated N(4) and N(8).
  • Each molecule in a unit cell contains one linking nitrogen and one terminal nitrogen.
  • molecule (1) contains N(3) and N(4)
  • molecule (2) contains N(7) and N(8).
  • the hydrogen bonding sequence in a cell is
  • Polymo ⁇ h B exhibits the following bonding sequence:
  • FIG. 5 and 6 show the XRPD patterns typical of polymo ⁇ h A; figures 7 and 8 show patterns typical of polymo ⁇ h B.
  • Figures 5 and 7 are calculated from the measured diffraction values for a single crystal.
  • the X-ray intensities, which come from the diffraction of a well-formed single crystal, and the powder pattern, which would come from the same material if ground to a fine powder, are not exactly equivalent.
  • the single crystal experiment aligns each crystal reflecting plane exactly in the reflecting position, while the powder pattern is derived from many planes, most of them slightly misaligned with respect to the perfect reflecting angle. The magnitude of this difference depends (among other things) on the diffracting angle.
  • Figures 6 and 8 are patterns measured directly from powders of the respective polymo ⁇ hs. The unique reflections are shown in Table 3 below. Reflections are considered "unique” if no reflection is observed within +0.2 ° when comparing 2 ⁇ values for the two norastemizole forms.
  • Figure 9 illustrates the solubility of norastemizole Form A as a function of co-solvent composition and temperature for an ethanol and two water/ethanol co-solvent systems. In this description, and in the descriptions of all solvent mixtures herein, the ratios of solvents are given in volume-to-volume.
  • Figure 10 illustrates the solubility of the two polymo ⁇ hs A and B as function of temperature in 17:10 water/ethanol.
  • thermodynamic stability of the two enantiotropic solid forms of norastemizole was also studied by examining the isothermal stability of mixtures of the two polymo ⁇ hs.
  • Two different solvent systems were tested (17:10 water/ethanol and DMSO) at 6 different temperatures (5, 25, 40, 60, 80 and 100 °C).
  • Samples were prepared by saturating the solvent system at the temperature of interest with pure form A, filtering, and, then, adding a 1:1 mixture of both seeds. The samples were then allowed to slurry for one week. Results summarized in Table 4 indicate that form A is the more thermodynamically stable form in the temperature region tested.
  • Some residual B reported at high temperatures is most likely due to cooling- induced crystallization during filtering.
  • the high temperature sample is filtered using a filtration system that is at room temperature (i.e. causing an initial thermal shock and, as a result, generating some product precipitation in the kinetically favorable form B).
  • the effect of temperature on the interconversion dynamic was measured by periodic sampling of a norastemizole slurry under the well-defined process conditions of controlled temperature and mixing in a 17:10 co-solvent ratio of water in denatured ethanol.
  • Table 5 illustrates the effect of operating temperature on interconversion rate. As the temperature decreases, the interconversion rate decreases. An operating temperature of 70-76 °C leads to a complete interconversion within 4 hours.
  • Table 6 illustrates the effect of mixing energy on interconversion dynamics. As the agitation rate increases (improved mass transfer) the interconversion rate also increases. Operation at a low agitation rate requires a longer mixing time for complete interconversion, while a higher agitation leads to complete interconversion in less than 4 hours of operation at 76 °C. Table 6. Effect of Agitation Mixing Energy on Interconversion Dynamics (76 °C)
  • Table 7 shows the effect of co-solvent composition on relative interconversion rates. While both co-solvent systems lead to good interconversion rates, a 2/1 co-solvent ratio leads to a faster interconversion (i.e. complete interconversion in under 3 hours) while maintaining other key factors constant (mixing energy and cooling profile).
  • Figure 12 illustrates the crystallization cooling profile adopted for controlling the polymo ⁇ h selectivity following a 2-hour water addition.
  • the ideal cooling curve is approximately described by a third order polynomial equation:
  • T -0.7788-t 3 + 4.623-t 2 - 8.7012-t + 80.87 wherein T represents batch temperature in degrees centigrade and t represents time in hours.
  • the present invention relates to polymo ⁇ hs of norastemizole, rather than particle size, but particle size is often another important variable in determining bioavailability and formulation of solid dosage forms.
  • the effects of agitation rate, cooling profile and hold time on particle size distribution appear to be interdependent.
  • increased agitation/energy dissipation increases particle size through improved mass transfer and growth rate, while, at the same time, reduces particle size during the cooling/aging profile through a secondary nucleation-particle break-up mechanism. Agitation has a different effect on different regions of the crystallization.
  • Sample had the same XRPD pattern as sample H1632-6A but could not be sufficiently fit using Rietveld analysis due to intense reflections at approximately 26 and 30 °2 ⁇ .
  • the sample does not contain polymo ⁇ h A
  • the procedure for reducing the volume is not disclosed in Hong et al. US patent 5,817,823 column 36, lines 31-34, but the person of ordinary skill would normally reduce volume on a rotary evaporator under vacuum, (the procedure used in the table).
  • a parallel experiment to the one identified as H1632-30A was run. In the parallel experiment, concentration was carried out by atmospheric pressure distillation for an extended period to reduce the solution to half-filtration volume before dilution with water. As would be predicted from the results of applicants' studies described above, this provided predominantly the A polymo ⁇ h.
  • the process for producing crystalline norastemizole of greater than 95% polymo ⁇ h A comprises:
  • Possible solvents include lower alkanols, THF, acetone and glycol ethers. DMF and DMSO are also possible, but their high boiling points make them unattractive for a number of reasons.
  • Water is the preferred anti-solvent, although one could consider alkanes.
  • the norastemizole is dissolved in ethanol at about 78 °C (the boiling point) and an amount of water just sufficient to initiate crystallization is added at or near reflux. The mixture is stirred at a temperature above 70 °C for at least one hour; and a second portion of water is added at a temperature above 70 °C and over a period of at least 2 hours.
  • the mixture is stirred and cooled from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion, such that the temperature remains above 70 °C for the first three hours.
  • the norastemizole is dissolved in about 4 parts by weight of ethanol at reflux; 6 to 7 parts by weight of water is added and the mix is stirred at a temperature above 70 °C for at least one hour. (Parts by weight are relative to norastemizole.)
  • a second portion of about 2 parts by weight of water is added over a period of at least 2 hours at a temperature above 70 °C, and the mixture is stirred and cooled from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion as shown in Figure 12.
  • the norastemizole is dissolved in 3.9 parts by weight of ethanol at reflux; 6.5 parts by weight of water is added and the mix is stirred at a temperature above 70 °C for at least one hour. A second portion of 2 parts by weight of water is added over a period of at least 2 hours at a temperature above 70 °C, and the mixture is stirred and cooled from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion as shown in Figure 12.
  • a supply of seeds of polymo ⁇ h A is available, the process is improved by seeding after the first addition of anti-solvent.
  • compositions of the present invention comprise polymo ⁇ h A of norastemizole as the active ingredient, together with one or more pharmaceutically acceptable carriers for solid dosage fonns.
  • Tablets and capsules may be prepared by methods well known in the pharmaceutical art. (See Remington: The Science and Practice of Pharmacy 19th Edition 1995, Chapter 94) .
  • US patent 6,124,320 discloses methods of treating mammals with norastemizole and compositions therfor. The disclosures of both are inco ⁇ orated herein by reference.

Abstract

Polymorphic crystalline forms of the antihistaminic drug norastemizole are disclosed. Processes for the production of the preferred polymorph are also disclosed.

Description

POLYMORPH OF THE ANTIHISTAMINE NORASTEMIZOLE
Field of the Invention
The invention relates to polymorphic crystalline forms of the antihistaminic drug norastemizole and to processes for the production of the preferred polymorph.
Background of the Invention
Norastemizole, 1 - [(4-fluorophenyl)methy 1] -N-4-piperidiny 1- 1 H- benzimidazol-2-amine, is an active metabolite of the histamine Hrreceptor antagonist astemizole (HISMANAL™). It is described in US patent 6,124,320 for use in the treatment of allergic disorders.
Figure imgf000002_0001
The polymorphic behavior of drugs can be of crucial importance in pharmacy and pharmacology. Polymorphs are, by definition, crystals of the same molecule having different physical properties as a result of the order of the molecules in the crystal lattice. The differences in physical properties exhibited by polymorphs affect pharmaceutical parameters such as storage stability, compressibility and density (important in formulation and product manufacturing), and dissolution rates (an important factor in determining bio-availability). Differences in stability can result from changes in chemical reactivity (e.g. differential oxidation, such that a dosage form discolors more rapidly when comprised of one polymorph than when comprised of another polymorph) or mechanical changes (e.g. tablets crumble on storage as a kinetically favored polymorph converts to thermodynamically more stable polymorph) or both (e.g. tablets of one polymorph are more susceptible to breakdown at high humidity). As a result of solubility/dissolution differences, in the extreme case, some polymorphic transitions may result in lack of potency or, at the other extreme, toxicity. In addition, the physical properties of the crystal may be important in processing: for example, one polymorph might be more likely to form solvates or might be difficult to filter and wash free of impurities (i.e particle shape and size distribution might be different between one polymorph relative to the other).
Each pharmaceutical compound has an optimal therapeutic blood concentration and a lethal concentration. The bio-availability of the compound determines the dosage strength in the drug formulation necessary to obtain the ideal blood level. If the drug can crystallize as two or more polymorphs differing in bio- availability, the optimal dose will depend on the polymorph present in the formulation. Some drugs show a narrow margin between therapeutic and lethal concentrations. Chloramphenicol-3-palmitate (CAPP), for example, is a broad spectrum antibiotic known to crystallize in at least three polymorphic forms and one amorphous form. The most stable form, A, is marketed. The difference in bio- activity between this polymorph and another form B, is a factor of eight - creating the possibility of fatal overdosages of the compound if unwittingly administered as form B due to alterations during processing and/or storage. Therefore, regulatory agencies, such as the US Food and Drug Administration, have begun to place tight controls on the polymoφhic content of the active component in solid dosage forms. In general, for drugs that exist in polymoφhic forms, if anything other than the pure thermodynamically preferred polymoφh is to be marketed, the regulatory agency will require batch-by-batch monitoring. Thus, it becomes important for both medical and commercial reasons to produce and market the most thermodynamically stable polymoφh, substantially free of other kinetically favored polymoφhs.
From thermodynamic considerations, only one polymoφh will be stable; the one with the lowest free energy at a given temperature and pressure. From the industrial crystallization point of view, however, thermodynamic stability is not sufficient to ensure that the stable polymoφh will always be produced. During primary nucleation, in the absence of seed crystals, it is the unstable polymoφh or pseudo polymoφh in the form of a hydrate or solvate that tends to crystallize first (kinetic form). This is, in essence, Ostwald's Rule of Stages, which posits that an unstable system does not transform directly to the most stable state. Instead, it transforms to a transient state accompanied by the smallest loss of free energy. The eventual transition(s) to the most stable phase is inevitable but the transformation can be extremely fast or extremely slow depending on the process conditions present. Most transformations occur in suspension and are solvent mediated. Some polymoφhic transformations can be reversible when the relative solubilities of the polymoφhs invert over a range of temperatures (enantiotropic). Other transformations are irreversible (monotropic) over abroad range of temperatures..
Although several syntheses of norastemizole are described in the literature, polymoφhism of the solid product is not disclosed. Applicants have now discovered that solid norastemizole exists in two polymoφhic forms. As is shown in the results of applicants' experiments below, the product produced by methods previously described in the literature of which applicants are aware is in every case composed of greater than 80% of the kinetically favored polymoφh and less than 20%) of the desired thermodynamically stable polymoφh. Those references which have been examined include:(l) Janssen et al. US patent 4,695,569, column 24, lines 22-32; (2) Hong et al. US patent 5,817,823, column 32, lines 9-18; column 33, lines 16-23; column 36, lines 31-41; and column 43, lines 19-24; and (3) Maynard et al. US patent 5,922,737, column 39, lines 20-30.
Summary of the Invention
In one aspect, the invention relates to norastemizole in the form of a crystalline solid comprising at least 95% of a first polymoφh (hereinafter referred to as polymoφh A) defined by the X-ray powder diffraction pattern (including both characteristic peaks and intensities) shown below.
Table 1
Figure imgf000005_0001
Figure imgf000006_0001
This is the more thermodynamically stable polymoφh. The kinetically favored polymoφh B exhibits an XRPD pattern as follows: Table 2
Figure imgf000007_0001
Figure imgf000008_0001
In another aspect, the invention relates to a process for producing crystalline norastemizole, predominantly as polymoφh A. In a generic sense the process comprises:
(a) dissolving norastemizole in just enough solvent to achieve dissolution at a first, elevated temperature;
(b) adding an amount of anti-solvent just sufficient to initiate crystallization at the first temperature (just sufficient means that less than 5% of the norastemizole crystallizes);
(c) stirring at the first temperature for a period of time to allow crystallization of a small amount (less than 5%) of the norastemizole; the combination of time and temperature is such as to allow equilibration of the crystallizing norastemizole to greater than 95%> of polymoφh A;
(d) adding a second portion of anti-solvent at the same elevated first temperature and over a second period of time such that norastemizole that crystallizes during the second addition of anti-solvent is greater than 95% of the polymoφh of claim 1; to accomplish this, the second portion of anti-solvent is of sufficient amount to produce ultimate crystallization of at least 85% of the norastemizole at a lower temperature, but the amount and rate of addition are kept such that the solubility curve for polymoφh B at the temperature of addition is not crossed; and
(e) stirring and cooling from the first, higher temperature to a second, lower temperature in a non-linear fashion over a third period of time such that no more than a 15% temperature drop occurs in the first half of the cooling time; in this fashion, at least 85%) of the norastemizole is crystallized and greater than 95% of it is in the form of the polymoφh A.
In a particular embodiment of the process aspect, the process comprises: (a) dissolving norastemizole in a solvent at a temperature between 70°C and 110°C; (b) adding an amount of anti-solvent sufficient to initiate crystallization at a temperature above 70 °C; (c) stirring at a temperature above 70 °C for at least one hour; (d) adding a second portion of anti-solvent at a temperature above 70 °C and over a period of at least 2 hours, in an amount sufficient to produce crystallization of at least 85%> of dissolved norastemizole; and (e) stirring and cooling from above 70 °C to below 30 °C over the course of at least 6 hours in a non-linear fashion such that no more than a 15%) temperature drop occurs in the first 3 hours.
In another aspect, the invention relates to norastemizole (predominantly in the form of polymoφh A) produced by the process described above.
In another aspect, the invention relates to a method for treating allergic conditions in a mammal comprising administering a therapeutically effective amount of norastemizole in the form of polymoφh A.
In another aspect, the invention relates to a pharmaceutical composition comprising a pharmaceutically acceptable carrier for a solid dosage form and norastemizole in the form of polymoφh A.
Brief Description of the Drawings
FIG. 1 is an Oak Ridge Thermal Ellipsoid Plot (ORTEP) drawing of the norastemizole molecule in one of the two conformations found in both polymoφhs of crystalline norastemizole.
FIG. 2 is an ORTEP drawing of the norastemizole molecule in the other of the two conformations found in both polymoφhs of crystalline norastemizole.
FIG. 3 is a representation of the arrangement of molecules of norastemizole in polymoφh A of crystalline norastemizole.
FIG. 4 is a representation of the arrangement of molecules of norastemizole in polymoφh B of crystalline norastemizole.
FIG. 5 is a calculated powder diffraction pattern for polymoφh A of crystalline norastemizole.
FIG. 6 is an experimentally obtained powder diffraction pattern for polymoφh A of crystalline norastemizole.
FIG. 7 is a calculated powder diffraction pattern for polymoφh B of crystalline norastemizole.
FIG. 8 is an experimentally obtained powder diffraction pattern for polymoφh B of crystalline norastemizole.
FIG. 9 is a graph of the solubility of norastemizole polymoφh A as a function of temperature in three different solvent systems.
FIG. 10 is a graph of the solubilities of norastemizole polymoφh A and polymoφh B as a function of temperature in 17:10 water/ethanol.
FIG. 11 is a graphic representation of the time-course of three parameters (temperature, volume of water added and stirring rate) in a process of the invention.
FIG. 12 is a graphic representation of the temperature time during the claimed process.
Detailed Description of the Invention
Applicants have investigated solid norastemizole using quantitative thermal analysis (OSC), x-ray powder diffraction (XRPD), and hot stage microscopy and have discovered two polymoφhs of norastemizole. From these crystal structures, XRPD patterns were generated that match the patterns measured for products from the process described in the invention. Based on the data, the process of the invention, described below, produces a single polymoφh (within the <5% limit of detection).
Both polymoφh A and polymoφh B have unit cells made up of two molecules and differ only in that a rotation of 180 ° has occurred around the N(l )- C(7) or N(5)-C(26) axis (Fig. 1 and Fig. 2). In polymoφh A, the hydrogen bonding sequence is between molecules of the same type; in polymoφh B, the hydrogen bonding sequence alternates. Therefore, the number of hydrogen bonds is the same; it is only the sequence that differs.
The following is a brief description of the differences between the two polymoφhs. Essentially each polymoφh has two unique molecules - molecule type (1) (Fig. 1) and molecule type (2) (Fig. 2) - hydrogen bonded in a unit cell. In Polymoφh A (Fig. 3), the hydrogen bonds are between molecules of type (1) or molecules of type (2) but not between the two types. In polymoφh B (Fig. 4) molecules of type (1) and (2) are connected in an alternating fashion.
More specifically, the hydrogen bonding can be described in terms of the secondary amine groups in norastemizole. The respective nitrogen atoms can be described as the "linking" nitrogen and the "terminal" nitrogen. The linking nitrogen atoms are designated N(3) and N(7), the terminal nitrogen atoms are designated N(4) and N(8). Each molecule in a unit cell contains one linking nitrogen and one terminal nitrogen. By definition, molecule (1) contains N(3) and N(4) and molecule (2) contains N(7) and N(8). In the polymoφh A, the hydrogen bonding sequence in a cell is
N(3)-H...N(4)-H...N(3)-H... i.e., molecule 1 linking N... molecule 1 terminal N... molecule 1 linking N or
N(7)-H...N(8)-H...N(7)-H... i.e., molecule 2 linking N... molecule 2 terminal N... molecule 2 linking N... In other words, there is a sequence of linking-nitrogen to terminal-nitrogen hydrogen bonds between molecules either all of molecule (1) or all of molecule (2).
Polymoφh B exhibits the following bonding sequence:
N(3)-H...N(8)-H...N(3)... and N(7)-H...N(4)...N(7)-H... Molecule 1 linking N... molecule 2 terminal N.... molecule 1 linking N, and molecule 2 linking N... molecule 1 terminal N... molecule 2 linking N. In this case there is still a linking-nitrogen hydrogen bonded to a terminal nitrogen, but the bonding is between a molecule type of (1) followed by a molecule of type (2).
Both space groups are non-centrosymmetric: P212121 (Polymoφh A) and Cc (Polymoφh B). The formation of the crystal presumably depends on which of the two arrangements of hydrogen bonds occur in the initial crystal nuclei which form the seed for crystal growth. Polymoφh B is kinetically favored.
Parameter Polymoφh A Polvmoφh B
Crystal Color/Habit Colourless, plates Colourless, blocks
Crystal system Orthorhombic Monoclinic
Figure imgf000013_0001
Lattice type C-centered
Lattice parameters a=10.260 (8) Δ a=14.587 (8) Δ b= 33.335(3) Δ b=14.111 (5)Δ c=10.101(3)Δ c=18.101(7)Δ β=l 11.85(3)°
Volume 3454(1)A3 3458(3)A3
Space group P212121 (#19) Cc (#9)
Z values 8 8 (molecules/cell)
pcalc 1.247 g/cc 1.246 g/cc
pmeas ND 1.221 g/cc
A distinctive XRPD pattern is characteristic of each polymoφh. Figures 5 and 6 show the XRPD patterns typical of polymoφh A; figures 7 and 8 show patterns typical of polymoφh B. Figures 5 and 7 are calculated from the measured diffraction values for a single crystal. The X-ray intensities, which come from the diffraction of a well-formed single crystal, and the powder pattern, which would come from the same material if ground to a fine powder, are not exactly equivalent. In particular, the single crystal experiment aligns each crystal reflecting plane exactly in the reflecting position, while the powder pattern is derived from many planes, most of them slightly misaligned with respect to the perfect reflecting angle. The magnitude of this difference depends (among other things) on the diffracting angle. However, the relationship between the single crystal measurement and the corresponding powder pattern is well known and can be calculated. Figures 6 and 8 are patterns measured directly from powders of the respective polymoφhs. The unique reflections are shown in Table 3 below. Reflections are considered "unique" if no reflection is observed within +0.2 ° when comparing 2θ values for the two norastemizole forms.
Table 3. Unique Reflections for Norastemizole Forms A and B
Figure imgf000014_0001
Early bulk drug lots of norastemizole prepared by applicants were found to be mixtures of the two polymoφhs, A and B. The x-ray patterns of the two forms showed significant overlap. A Rietveld analysis was developed that allowed quantitative determination of Form B in Form A down to a detection limit at 5%. Upon analysis, it became apparent that the desired polymoφh, in any reasonable degree of purity, could not be produced by the known procedures, and indeed, even a specific ratio of polymoφhs was not consistently produced by the known procedures. As discussed above, such a situation is highly undesirable from both a medical and a regulatory standpoint. A comprehensive study was undertaken to identify critical process parameters that affect polymoφh selectivity, to develop a fundamental model that explains all experimental observations, and to derive a crystallization process that reproducibly provides norastemizole in which greater than 95%o of the total solid is in the form of the desired polymoφh, Form A.
The solubility of norastemizole in various ratios of co-solvent mixtures was determined in order to facilitate the recovery of material and to determine the level of supersaturation during crystallization. Figure 9 illustrates the solubility of norastemizole Form A as a function of co-solvent composition and temperature for an ethanol and two water/ethanol co-solvent systems. In this description, and in the descriptions of all solvent mixtures herein, the ratios of solvents are given in volume-to-volume. Figure 10 illustrates the solubility of the two polymoφhs A and B as function of temperature in 17:10 water/ethanol. The results indicate that denatured ethanol with an anti-solvent addition (water) in excess of 13 to 10 by volume can give reasonable recovery yields, and that the solubility difference between Form A and Form B decreases as the temperature decreases with an enantiotropic transition temperature around 0-10 °C.
The thermodynamic stability of the two enantiotropic solid forms of norastemizole was also studied by examining the isothermal stability of mixtures of the two polymoφhs. Two different solvent systems were tested (17:10 water/ethanol and DMSO) at 6 different temperatures (5, 25, 40, 60, 80 and 100 °C). Samples were prepared by saturating the solvent system at the temperature of interest with pure form A, filtering, and, then, adding a 1:1 mixture of both seeds. The samples were then allowed to slurry for one week. Results summarized in Table 4 indicate that form A is the more thermodynamically stable form in the temperature region tested. Some residual B reported at high temperatures is most likely due to cooling- induced crystallization during filtering. The high temperature sample is filtered using a filtration system that is at room temperature (i.e. causing an initial thermal shock and, as a result, generating some product precipitation in the kinetically favorable form B).
Table 4. Thermodynamic stability of Norastemizole Polymorphs as a function of Temperature
Figure imgf000016_0001
The effect of temperature on the interconversion dynamic was measured by periodic sampling of a norastemizole slurry under the well-defined process conditions of controlled temperature and mixing in a 17:10 co-solvent ratio of water in denatured ethanol. Table 5 illustrates the effect of operating temperature on interconversion rate. As the temperature decreases, the interconversion rate decreases. An operating temperature of 70-76 °C leads to a complete interconversion within 4 hours.
Figure imgf000017_0001
Table 6 below illustrates the effect of mixing energy on interconversion dynamics. As the agitation rate increases (improved mass transfer) the interconversion rate also increases. Operation at a low agitation rate requires a longer mixing time for complete interconversion, while a higher agitation leads to complete interconversion in less than 4 hours of operation at 76 °C. Table 6. Effect of Agitation Mixing Energy on Interconversion Dynamics (76 °C)
Figure imgf000017_0002
Table 7 below shows the effect of co-solvent composition on relative interconversion rates. While both co-solvent systems lead to good interconversion rates, a 2/1 co-solvent ratio leads to a faster interconversion (i.e. complete interconversion in under 3 hours) while maintaining other key factors constant (mixing energy and cooling profile).
Table 7. Effect of Co-solvent Composition on Inter-conversion Dynamics (76 °C/550 RPM)
Figure imgf000018_0001
As might be expected, as the relative amount of form A present increases, the inter-conversion rate also dramatically increases. A 50/50 mixture as the initial composition leads to a complete interconversion in less than 0.3 hours while a 3% form A initial composition shows a small interconversion (from 97%o form B to 16% form B) in 2 hours. This effect is consistent with fundamental crystallization principles: as the relative concentration of the stable crystal increases, the available surface area for crystal growth also increases, and the rate of growth of the less soluble (form A) dramatically increases at the expense of the more soluble (form B). Interconversion to the thermodynamically more stable polymoφh A results.
Four parameters that were initially considered possible result-effective variables in norastemizole moφhology were the following: 1) amount of second water addition after seeding; 2) rate of second water addition; 3) agitation rate during second water addition; and 4) cooling profile after end of second water addition. An eight-trial, four-factor, orthogonal array experimental design was used to screen these parameters, and it was found that only two of those four actually had a significant effect on interconversion to the more thermodynamically stable polymoφh A: 2) rate of second water addition and 4) cooling profile. The cooling curve, the addition profile of the anti-solvent (water) and the stirring rate, are shown in Figure 11. The effect of the cooling curve on the polymoφh obtained was examined. As the cooling type was changed from a 4- hour linear cooling profile to a non-linear 12 hour cooling profile, the mean polymoφh form value dropped from 39% form B to a value of <5%> form B. The effect of anti-solvent addition time on polymoφh ratio was also examined. As the addition time was increased from 15 minutes to 3 hours, the mean level of polymoφh B dropped from 37% to <5%. Significant interaction between cooling profile and addition time was observed, as illustrated in Table 8. The effect of addition time on polymoφh form is different as the cooling profile is changed from a 4-hour linear to a 12-hour non-linear cooling. A single non-linear 12-hour profile produces the desired polymoφh A with minimal contribution from addition time.
Table 8. Interaction of Cooling Type and Addition Time
Cooling Type Addition Time, min Mean Value of form B, %
4-hr Linear 15 70.0%
4-hr Linear 180 7.7%
12-hr Non-Linear 15 4.65%
12-hr Non-linear 180 2.23%
Figure 12 illustrates the crystallization cooling profile adopted for controlling the polymoφh selectivity following a 2-hour water addition. The ideal cooling curve is approximately described by a third order polynomial equation:
T = -0.7788-t3 + 4.623-t2 - 8.7012-t + 80.87 wherein T represents batch temperature in degrees centigrade and t represents time in hours.
This is an adequate description of the curve to produce highly satisfactory results, although it can be further refined by adjustment for the expected variability of solute initial concentration and for temperature measurement errors. This cooling regime allows control of constant small supersaturation during cooling to ensure that the thermodynamically stable polymoφh A exclusively grows. Any significant increase in supersaturation, due to either natural cooling or linear cooling, generates a significant amount of the metastable polymoφh B that may not have a chance to inter-convert back to A before isolation. Control of constant supersaturation through slow cooling is important at the higher temperatures during the early stages of cooling because that is where the solubility difference between the two polymoφhs is the highest and that is also where most of the product comes out of solution. Experiments were carried out on 2 liter, 50 liter and 1200 liter scales using the above cooling profile. All resulted in >95%> of polymoφh A. The time and temperature coordinates of the typical profile (Fig 12) are shown in Table 9.
Table 9
Figure imgf000020_0001
Figure imgf000021_0001
Figure imgf000022_0001
In the foregoing experiments, mixing energy proved not to be a critical factor for polymoφh control, but it was important for particle size distribution control. The present invention relates to polymoφhs of norastemizole, rather than particle size, but particle size is often another important variable in determining bioavailability and formulation of solid dosage forms. The effects of agitation rate, cooling profile and hold time on particle size distribution appear to be interdependent. During crystallization, for instance, increased agitation/energy dissipation increases particle size through improved mass transfer and growth rate, while, at the same time, reduces particle size during the cooling/aging profile through a secondary nucleation-particle break-up mechanism. Agitation has a different effect on different regions of the crystallization. Most of the significant effect is during the final cool-down period, during which polymoφh A predominates. This suggests a high agitation rate during initial stages of crystallization until interconversion to form A is completed. During the final cooling down stage, lowering the agitation favors a larger particle size distribution. We have found that, as the agitation rate increases, (initial agitation dominates PSD) the mean size also increases from 41.2 to 76.5 microns. Additionally, as the hold time following the water addition (high temperature region) is extended from 15 minutes to 225 minutes, the mean particle size increases from 65.6 microns to 113.9 microns (favors fewer primary nuclei and more crystal growth). Significant interaction between the two factors is also observed, with maximum mean size obtained (151.2 microns) at the low agitation level and 225 minute post addition hold time, while the smallest mean particle size is observed during the low agitation level and short post addition hold time (60.6 microns). Applicants have found that the critical process parameters are interdependent, and without controlling both the cooling curve and the rate of anti- solvent addition, either form B or a mixture of polymoφhic forms will be produced. All prior processes for producing norastemizole free base, described in art known to the applicants, were examined. The results are summarized below. The samples were generated following the referenced procedures and were tested using the validated XRPD method. Table 10 summarizes the results, which clearly show that the procedures described in all the references produce predominantly or exclusively the undesirable, kinetically favored polymoφh B.
Table 10. Comparison of Processes in Literature
Figure imgf000023_0001
Sample had the same XRPD pattern as sample H1632-6A but could not be sufficiently fit using Rietveld analysis due to intense reflections at approximately 26 and 30 °2Θ. The sample does not contain polymoφh A The procedure for reducing the volume is not disclosed in Hong et al. US patent 5,817,823 column 36, lines 31-34, but the person of ordinary skill would normally reduce volume on a rotary evaporator under vacuum, (the procedure used in the table). As a check on applicants' discovery of the result-effective variables, a parallel experiment to the one identified as H1632-30A was run. In the parallel experiment, concentration was carried out by atmospheric pressure distillation for an extended period to reduce the solution to half-filtration volume before dilution with water. As would be predicted from the results of applicants' studies described above, this provided predominantly the A polymoφh.
The process for producing crystalline norastemizole of greater than 95% polymoφh A comprises:
(a) dissolving norastemizole in a solvent at a temperature between 70 °C and 110°C;
(b) adding an amount of anti-solvent sufficient to initiate crystallization at a temperature above 70 °C;
(c) stirring at a temperature above 70 °C for at least one hour;
(d) adding a second portion of anti-solvent at a temperature above 70 °C and over a period of at least 2 hours, said second portion of anti-solvent being of sufficient amount to produce ultimate crystallization of at least 85% of said norastemizole; and
(e) stirring and cooling from above 70 °C to below 30 °C over the course of at least 6 hours in a non-linear fashion such that no more than a 15%> temperature drop occurs in the first 3 hours.
Possible solvents include lower alkanols, THF, acetone and glycol ethers. DMF and DMSO are also possible, but their high boiling points make them unattractive for a number of reasons. Water is the preferred anti-solvent, although one could consider alkanes. Preferably the norastemizole is dissolved in ethanol at about 78 °C (the boiling point) and an amount of water just sufficient to initiate crystallization is added at or near reflux. The mixture is stirred at a temperature above 70 °C for at least one hour; and a second portion of water is added at a temperature above 70 °C and over a period of at least 2 hours. The mixture is stirred and cooled from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion, such that the temperature remains above 70 °C for the first three hours. More preferably, the norastemizole is dissolved in about 4 parts by weight of ethanol at reflux; 6 to 7 parts by weight of water is added and the mix is stirred at a temperature above 70 °C for at least one hour. (Parts by weight are relative to norastemizole.) A second portion of about 2 parts by weight of water is added over a period of at least 2 hours at a temperature above 70 °C, and the mixture is stirred and cooled from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion as shown in Figure 12. Most preferably, the norastemizole is dissolved in 3.9 parts by weight of ethanol at reflux; 6.5 parts by weight of water is added and the mix is stirred at a temperature above 70 °C for at least one hour. A second portion of 2 parts by weight of water is added over a period of at least 2 hours at a temperature above 70 °C, and the mixture is stirred and cooled from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion as shown in Figure 12. When a supply of seeds of polymoφh A is available, the process is improved by seeding after the first addition of anti-solvent.
The pharmaceutical compositions of the present invention comprise polymoφh A of norastemizole as the active ingredient, together with one or more pharmaceutically acceptable carriers for solid dosage fonns. Tablets and capsules may be prepared by methods well known in the pharmaceutical art. (See Remington: The Science and Practice of Pharmacy 19th Edition 1995, Chapter 94) . US patent 6,124,320 discloses methods of treating mammals with norastemizole and compositions therfor. The disclosures of both are incoφorated herein by reference.

Claims

1. Norastemizole in the form of a crystalline solid comprising at least 95%> of a first polymoφh having peaks at the diffraction degrees with the intensity shown below in an X-ray powder diffraction pattern:
Figure imgf000026_0001
Figure imgf000027_0001
2. A process for producing crystalline norastemizole as defined in claim 1 comprising:
(a) dissolving norastemizole in a solvent, said solvent being in an amount sufficient to achieve dissolution of said norastemizole at a first temperature;
(b) adding an amount of anti-solvent just sufficient to initiate crystallization at said first temperature, whereby less than 5%> of said norastemizole crystallizes;
(c) stirring at said first temperature for a first period of time to allow crystallization of less than 5% of said norastemizole and equilibration of said norastemizole to greater than 95% of the polymoφh of claim 1;
(d) adding a second portion of anti-solvent at said first temperature and over a second period of time such that norastemizole that crystallizes during said adding said second portion of anti-solvent is greater than 95% of the polymoφh of claim 1, said second portion of anti-solvent being of sufficient amount to produce ultimate crystallization of at least 85% of said norastemizole at a second temperature, said second temperature being lower than said first temperature; and
(e) stirring and cooling from said first temperature to said second temperature in a non-linear fashion over a third period of time such that no more than a 15% temperature drop occurs in the first half of said third period of time, whereby at least 85% of said norastemizole is crystallized and greater than 95% of said norastemizole is in the form of the polymoφh of claim 1 .
3. A process for producing crystalline norastemizole as defined in claim 1 comprising:
(a) dissolving norastemizole in a solvent at a temperature between 70 °C and 110°C;
(b) adding an amount of anti-solvent sufficient to initiate crystallization at a temperature above 70 °C;
(c) stirring at a temperature above 70 °C for at least one hour;
(d) adding a second portion of anti-solvent at a temperature above 70 °C and over a period of at least 2 hours, said second portion of anti-solvent being of sufficient amount to produce ultimate crystallization of at least 85% of said norastemizole; and
(e) stirring and cooling from above 70 °C to below 30 °C over the course of at least 6 hours in a non-linear fashion such that no more than a 15% temperature drop occurs in the first 3 hours.
4. A process for producing crystalline norastemizole comprising:
(a) dissolving norastemizole in ethanol at about 78 °C; (b) adding an amount of water sufficient to initiate crystallization at reflux;
(c) stirring at a temperature above 70 °C for at least one hour;
(d) adding a second portion of water at a temperature above 70 °C and over a period of at least 2 hours;
(e) stirring and cooling from above 70 ° C to room temperature over the course of at least 6 hours in a non-linear fashion such that the temperature remains above 70 °C for the first three hours.
5. A process for producing crystalline norastemizole comprising:
(a) dissolving norastemizole in about 4 parts by weight of ethanol at reflux;
(b) adding from 6 to 7 parts by weight of water;
(c) stirring at a temperature above 70 °C for at least one hour;
(d) adding a second portion of about 2 parts by weight of water at a temperature above 70 °C and over a period of at least 2 hours;
(e) stirring and cooling from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fasliion, such that the temperature remains between 78 °C and 70 °C for the first three hours.
6. A process for producing crystalline norastemizole comprising:
(a) dissolving norastemizole in about 4 parts by weight of ethanol at reflux;
(b) adding about 6.5 parts by weight of water; (c) seeding with crystals comprising greater than 95% by weight of a polymoφh of norastemizole having peaks at the diffraction degrees with the intensity shown below in an X-ray powder diffraction pattern:
Figure imgf000030_0001
Figure imgf000031_0001
(d) stirring at a temperature above 70 °C for at least one hour;
(e) adding a second portion of about 2 parts by weight of water at a temperature above 70 °C and over a period of at least 2 hours;
(f) stirring and cooling from above 70 °C to room temperature over the course of at least 6 hours in a non-linear fashion, such that the temperature remains between 78 °C and 70 °C for the first three hours.
7. Crystalline norastemizole produced by the process of claim 2.
8. Crystalline norastemizole produced by the process of claim 3.
9. Crystalline norastemizole produced by the process of claim 4.
10. Crystalline norastemizole produced by the process of claim 5.
11. Crystalline norastemizole produced by the process of claim 6.
12. A method for treating allergic conditions in a mammal comprising administering to said mammal a therapeutically effective amount of the solid norastemizole of claim 1.
13. A pharmaceutical composition comprising a pharmaceutically acceptable carrier for a solid dosage form and the solid norastemizole of claim 1.
PCT/US2002/022583 2001-07-17 2002-07-16 Polymorph of the antihistamine norastemizole WO2003008408A1 (en)

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US09/907,556 2001-07-17
US09/907,556 US6627646B2 (en) 2001-07-17 2001-07-17 Norastemizole polymorphs

Publications (1)

Publication Number Publication Date
WO2003008408A1 true WO2003008408A1 (en) 2003-01-30

Family

ID=25424302

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/US2002/022583 WO2003008408A1 (en) 2001-07-17 2002-07-16 Polymorph of the antihistamine norastemizole

Country Status (2)

Country Link
US (1) US6627646B2 (en)
WO (1) WO2003008408A1 (en)

Families Citing this family (139)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
GB0021865D0 (en) * 2000-09-06 2000-10-18 Smithkline Beecham Plc Novel pharmaceutical
SI20875A (en) * 2001-04-25 2002-10-31 LEK, tovarna farmacevtskih in kemi�nih izdelkov, d.d. Crystal form of omeprazole
US7183410B2 (en) * 2001-08-02 2007-02-27 Bidachem S.P.A. Stable polymorph of flibanserin
US20030060475A1 (en) * 2001-08-10 2003-03-27 Boehringer Ingelheim Pharma Kg Method of using flibanserin for neuroprotection
US10675280B2 (en) 2001-10-20 2020-06-09 Sprout Pharmaceuticals, Inc. Treating sexual desire disorders with flibanserin
UA78974C2 (en) * 2001-10-20 2007-05-10 Boehringer Ingelheim Pharma Use of flibanserin for treating disorders of sexual desire
TW200303304A (en) * 2002-02-18 2003-09-01 Astrazeneca Ab Chemical compounds
AU2003224781A1 (en) * 2002-03-26 2003-10-13 Dr. Reddy's Laboratories Limited Crystalline forms of rabeprazole sodium
AU2002253425B2 (en) * 2002-04-04 2008-09-25 Dr. Reddy's Laboratories Ltd. Novel pharmaceutical compositions for antihistaminic-decongenstant combination and method of making such compositions
US20040048877A1 (en) * 2002-05-22 2004-03-11 Boehringer Ingelheim Pharma Gmbh & Co. Kg Pharmaceutical compositions containing flibanserin
CN1777598A (en) * 2003-02-28 2006-05-24 兰贝克赛实验室有限公司 Polymorphs of s-omeprazole.
ES2245277T1 (en) * 2003-03-12 2006-01-01 Teva Pharmaceutical Industries Limited SOLIDOS CRYSTALS AND AMORPHES OF PANTOPRAZOL AND PROCEDURES FOR THEIR PREPARATION.
DE10339862A1 (en) * 2003-08-29 2005-03-24 Boehringer Ingelheim Pharma Gmbh & Co. Kg New crystalline forms of ethyl 3-(N-(2-(4-(hexyloxycarbonylamidino)phenylaminomethyl)-1-methyl-1H-benzimidazole-5-carbonyl)-N-(2-pyridyl)amino)propionate methanesulfonate used for post-operative prophylaxis of deep vein thrombosis
ITMI20032259A1 (en) * 2003-11-20 2005-05-21 Chemi Spa NEW POLYMORPHOUS OF ACID 1-CYCLOPROPYL-7- (S, S-2,8-DIAZABICLO-4.3.0-NON-8-IL) -6-FLUORO-1,4-DIIDRO-8-METOSSI-4-OXO -CHINOLIN CARBOSXYL CHLORIDRATE AND METHODS FOR ITS PREPARATION
KR100854211B1 (en) 2003-12-18 2008-08-26 동아제약주식회사 Novel oxazolidinone derivatives, a process for the preparation thereof and pharmaceutical composition comprising the same for antibiotics
GB0329319D0 (en) * 2003-12-18 2004-01-21 Alizyme Therapeutics Ltd Synthesis
US7629465B2 (en) * 2004-03-05 2009-12-08 Ipca Laboratories Ltd. Industrial process for preparation of Clopidogrel hydrogen sulphate
DE102004015981A1 (en) * 2004-04-01 2005-10-20 Bayer Healthcare Ag New kirstalline form of 8-cyano-1-cyclopropyl-7- (1S, 6S-2,8-diazabicyclo [4.3.0] nonan-8-yl) -6-fluoro-1,4-dihydro-4-oxo 3-quinolinecarboxylic
MY134672A (en) * 2004-05-20 2007-12-31 Japan Tobacco Inc Stable crystal of 4-oxoquinoline compound
US20080249134A1 (en) * 2004-06-24 2008-10-09 Ursula Hohlneicher New Esomeprazole Sodium Salt Crystal Modification
ES2349798T3 (en) * 2004-07-22 2011-01-11 Eli Lilly And Company CRYSTAL VARIABLE HYDRATION OF SALT HEMISUCCINATE FROM (S) -6- (4- (2 - ((3- (9H-CARBAZOL-4-ILOXI) -2-HYDROXIPROPIL) AMINO) -2-METHYLPROPIL) PHENOXY) -3- PYRIDINOCARBOXAMIDE.
ITMI20041568A1 (en) * 2004-07-30 2004-10-30 Dipharma Spa "BASE FEXOFENADINA POLYMORPHS"
MX2007001506A (en) * 2004-08-05 2007-03-27 Wyeth Corp Crystalline polymorph of pipindoxifene hydrochloride monohydrate.
BRPI0517924A (en) * 2004-11-02 2008-10-21 Pfizer polymorphic forms of 6- [2 (methylcarbamoyl) phenylsufanyl] -3-e- [2- (pyridin-2-yl) ethenyl] indazole
EP1848420A4 (en) 2005-01-28 2008-01-23 Merck & Co Inc Polymorphic forms of a gabaa agonist
CN101119986B (en) * 2005-02-07 2011-07-06 田边三菱制药株式会社 Optically active tetrahydronaphthalene derivative
CA2607583A1 (en) * 2005-05-06 2007-04-05 Medichem, S.A. Pantoprazole free acid form iii
DE102005025728A1 (en) * 2005-06-04 2006-12-07 Boehringer Ingelheim Pharma Gmbh & Co. Kg Polymorphs of 3 - [(2 - {[4- (hexyloxycarbonylamino-imino-methyl) -phenyl-amino] -methyl} -1-methyl-1H-benzimidazole-5-carbonyl) -pyridin-2-yl-amino] -propionic acid ethyl ester
JP2008545768A (en) * 2005-06-08 2008-12-18 レツク・フアーマシユーテイカルズ・デー・デー Crystalline solvate of omeprazole sodium
ES2646326T3 (en) 2005-08-03 2017-12-13 Sprout Pharmaceuticals, Inc. Use of flibanserin in the treatment of obesity
US7576219B2 (en) * 2005-10-26 2009-08-18 Hanmi Pharm. Co., Ltd Crystalline S-omeprazole strontium hydrate, method for preparing same, and pharmaceutical composition containing same
US7923449B2 (en) 2005-10-29 2011-04-12 Boehringer Ingelheim International Gmbh Benzimidazolone derivatives for the treatment of premenstrual and other female sexual disorders
US7977359B2 (en) 2005-11-04 2011-07-12 Amira Pharmaceuticals, Inc. 5-lipdxygenase-activating protein (FLAP) inhibitors
US8399666B2 (en) * 2005-11-04 2013-03-19 Panmira Pharmaceuticals, Llc 5-lipoxygenase-activating protein (FLAP) inhibitors
ATE549317T1 (en) 2005-11-08 2012-03-15 Millennium Pharm Inc PHARMACEUTICAL SALTS AND POLYMORPHOS OF N-(5-CHLORO-2-PYRIDINYL)-2-ÄÄ4-Ä(DIMETHYLAMINO)IMINOMETHYLÜBENZOYLÜAMINOÜ-5-METHOXY-BENZAMIDE, A FACTOR XA INHIBITOR
US20070105869A1 (en) * 2005-11-08 2007-05-10 Stephane Pollentier Use of flibanserin for the treatment of pre-menopausal sexual desire disorders
EP2395002B1 (en) 2005-11-08 2014-06-18 Vertex Pharmaceuticals Inc. Pharmaceutical composition containing a heterocyclic modulator of atp-binding cassette transporters.
US9108962B2 (en) 2005-12-19 2015-08-18 Sicor, Inc. Forms of tiotropium bromide and processes for preparation thereof
WO2007075858A2 (en) * 2005-12-19 2007-07-05 Sicor Inc. Novel forms of tiotropium bromide and processes for preparation thereof
WO2007072868A1 (en) * 2005-12-21 2007-06-28 Eisai R & D Management Co., Ltd. Crystal of 1,2-dihydropyridine compound (type iv)
ES2353482T3 (en) * 2006-02-10 2011-03-02 Amgen, Inc HYGRATE FORMS OF AMG706.
TWI394753B (en) 2006-03-17 2013-05-01 Otsuka Pharma Co Ltd Novel tetomilast crystal
TW200812582A (en) * 2006-04-06 2008-03-16 Astrazeneca Ab Medicaments
US8063074B2 (en) * 2006-05-04 2011-11-22 Dr. Reddy's Laboratories Limited Polymorphic forms of esomeprazole sodium
CA2649938A1 (en) * 2006-05-09 2007-11-15 Boehringer Ingelheim International Gmbh Use of flibanserin for the treatment of post-menopausal sexual desire disorders
GB0612422D0 (en) * 2006-06-23 2006-08-02 Generics Uk Ltd Novel hydrate form
EP2037927B1 (en) * 2006-06-30 2010-01-27 Boehringer Ingelheim International GmbH Flibanserin for the treatment of urinary incontinence and related diseases
CA2657043A1 (en) * 2006-07-14 2008-01-17 Boehringer Ingelheim International Gmbh Use of flibanserin for the treatment of sexual disorders in females
TW200811160A (en) * 2006-07-14 2008-03-01 Astellas Pharma Inc Crystal of benzoxadiazole derivative
MX2009001551A (en) 2006-08-14 2009-02-20 Boehringer Ingelheim Int Formulations of flibanserin and method for manufacturing the same.
CL2007002214A1 (en) 2006-08-14 2008-03-07 Boehringer Ingelheim Int PHARMACEUTICAL COMPOSITION IN THE FORM OF COMPRESSED, WHERE AT LEAST THE LENGTH OF THE COMPRESSED IN THE PREVIOUS STATE OF THE APPLICATION IS AT LEAST 7/12 OF THE PILOR DIAMETER OF THE PATIENT AND AFTER INGERING IT IN THE FOOD STATE, THE LENGTH OF THE COMP
MX2009002031A (en) * 2006-08-25 2009-03-06 Boehringer Ingelheim Int Controlled release system and method for manufacturing the same.
ATE544749T1 (en) * 2006-11-02 2012-02-15 Millennium Pharm Inc METHOD FOR SYNTHESIZING PHARMACEUTICAL SALTS FROM A FACTOR XA INHIBITOR
DE102006054005A1 (en) * 2006-11-16 2008-05-21 Boehringer Ingelheim Pharma Gmbh & Co. Kg New polymorphs of 3 - [(2 - {[4- (hexyloxycarbonylamino-imino-methyl) -phenyl-amino] -methyl} -1-methyl-1H-benzimidazole-5-carbonyl) -pyridin-2-yl-amino] -propionic acid ethyl
ITMI20062449A1 (en) * 2006-12-19 2008-06-20 Dipharma Spa CRYSTALLINE FORM OF RABEPRAZOLO SODICO
JP2010514685A (en) * 2006-12-20 2010-05-06 ブリストル−マイヤーズ スクイブ カンパニー Crystal forms of aryl-substituted pyrazole amide compounds
RS54853B1 (en) * 2006-12-21 2016-10-31 Hoffmann La Roche Polymorphs of a mglur5 receptor antagonist
CA2674358C (en) * 2006-12-29 2013-10-08 Il Yang Pharmaceutical Company, Ltd. Crystalline forms of solvated ilaprazole
WO2008090742A1 (en) * 2007-01-23 2008-07-31 National University Corporation Hokkaido University Non-human animal for eye disease model
MX2009009344A (en) * 2007-03-02 2009-09-11 Novartis Ag Solid forms of a raf kinase inhibitor.
US8258161B2 (en) * 2007-03-02 2012-09-04 Merck Sharp & Dohme Corp. Crystalline salt form of an antidiabetic compound
SI2134702T2 (en) * 2007-04-05 2023-12-29 Pfizer Products Inc. Crystalline forms of 6-(2-(methylcarbamoyl)phenylsulfanyl)-3-e-(2-(pyridin-2-yl)ethenyl)indazole suitable for the treatment of abnormal cell growth in mammals
CN104447716A (en) 2007-05-09 2015-03-25 沃泰克斯药物股份有限公司 Modulators of CFTR
WO2008138754A2 (en) * 2007-05-10 2008-11-20 F. Hoffmann-La Roche Ag New solid forms of fxa inhibitors
UY31335A1 (en) 2007-09-12 2009-04-30 VASOMOTOR SYMPTOMS TREATMENT
TW200920369A (en) * 2007-10-26 2009-05-16 Amira Pharmaceuticals Inc 5-lipoxygenase activating protein (flap) inhibitor
AU2008335440B2 (en) 2007-12-07 2013-11-07 Vertex Pharmaceuticals Incorporated Processes for producing cycloalkylcarboxamido-pyridine benzoic acids
NZ614151A (en) 2007-12-07 2015-04-24 Vertex Pharma Solid forms of 3-(6-(1-(2,2-difluorobenzo[d][1,3]dioxol-5-yl) cyclopropanecarboxamido)-3-methylpyridin-2-yl)benzoic acid
JP2011507977A (en) * 2007-12-31 2011-03-10 武田薬品工業株式会社 Solvated crystal form of (R) -2-[[[3-Methyl-4- (2,2,2-trifluoroethoxy) -2-pyridinyl] methyl] sulfinyl] -1H-benzimidazole
NZ602030A (en) 2008-02-28 2014-02-28 Vertex Pharma Heteroaryl derivatives as cftr modulators
KR20110002462A (en) 2008-03-17 2011-01-07 바이알 - 포르텔라 앤드 씨에이 에스에이 Crystal forms of 5-[3-(2,5-dichloro-4,6-dimethyl-1-oxy-pyridine-3-yl) [1,2,3]oxadiazol-5-yl]-3-nitrobenzene-1,2-diol
CA2724726C (en) * 2008-05-23 2018-02-27 Amira Pharmaceuticals, Inc. 5-lipoxygenase-activating protein inhibitor
EP2143722A1 (en) * 2008-07-09 2010-01-13 Lek Pharmaceuticals D.D. Process for preparation of esomeprazole sodium of high chemical purity and new forms of esomeprazole sodium
CA2733922A1 (en) * 2008-08-12 2010-02-18 Astrazeneca Ab A crystalline form of 4-(5-{(1r)-1-[5-(3-chlorophenyl)isoxazol-3-yl]ethoxy}-4-methyl-4h-1,2,4-triazol-3-yl)pyridine
US8546431B2 (en) 2008-10-01 2013-10-01 Panmira Pharmaceuticals, Llc 5-lipoxygenase-activating protein (FLAP) inhibitors
US8604209B2 (en) * 2008-10-10 2013-12-10 Trius Therapeutics, Inc. Methods for preparing oxazolidinones and compositions containing them
CA2686480A1 (en) 2008-12-15 2010-06-15 Boehringer Ingelheim International Gmbh New salts
EP2376452A4 (en) * 2009-01-12 2012-08-29 Hetero Research Foundation Novel polymorph of atazanavir sulfate
KR101739923B1 (en) 2009-02-03 2017-05-25 머크 샤프 앤드 돔 코포레이션 Crystalline form of R)-3-(4-(2-(2-methyltetrazol-5-yl)pyridin-5-yl)-3-fluorophenyl)-5-hydroxymethyl oxazolidin-2-one dihydrogen phosphate
TW201036957A (en) * 2009-02-20 2010-10-16 Astrazeneca Ab Novel salt 628
JP5864409B2 (en) 2009-04-01 2016-02-17 ノヴィファーマ ソシエテ アノニム Pharmaceutical preparation containing nitrocatechol derivative and method for producing the same
EP2263672A1 (en) * 2009-05-19 2010-12-22 Bioprojet Novel pharmaceutically acceptable salts of 4-(1H-imidazol-4-ylmethyl)pyridine and their therapeutical uses
US8580767B2 (en) 2009-05-28 2013-11-12 Trius Therapeutics, Inc. Oxazolidinone containing dimer compounds, compositions and methods to make and use
CA2784921A1 (en) * 2009-12-17 2011-07-14 Millennium Pharmaceuticals, Inc. Salts and crystalline forms of a factor xa inhibitor
TWI549950B (en) * 2010-04-07 2016-09-21 維泰克斯製藥公司 Solid forms of 3-(6-(1-(2,2-difluorobenzo[d][1,3]dioxol-5-yl)cyclopropa necarboxamido)-3-methylpyridin-2-yl)benzoic acid
US8552034B2 (en) 2010-04-07 2013-10-08 Vertex Pharmaceuticals Incorporated Pharmaceutical compositions of 3-(6-(1-(2,2-difluorobenzo[d][1,3]dioxol-5-yl) cyclopropanecarboxamido)-3-methylpyridin-2-yl)benzoic acid and administration thereof
AR082804A1 (en) 2010-09-01 2013-01-09 Portola Pharm Inc CRYSTAL FORMS OF AN XA FACTOR INHIBITOR
PL2797416T3 (en) 2011-12-28 2017-12-29 Global Blood Therapeutics, Inc. Substituted benzaldehyde compounds and methods for their use in increasing tissue oxygenation
EP2797597B1 (en) 2011-12-28 2020-02-26 Global Blood Therapeutics, Inc. Substituted heteroaryl aldehyde compounds and methods for their use in increasing tissue oxygenation
NZ703638A (en) * 2012-07-25 2017-02-24 Fujiyakuhin Co Ltd 4-[5-(pyridine-4-yl)-1h-1,2,4-triazole-3-yl]pyridine-2-carbonitrile crystalline polymorph and production method therefor
US10266551B2 (en) 2013-03-15 2019-04-23 Global Blood Therapeutics, Inc. Compounds and uses thereof for the modulation of hemoglobin
US8952171B2 (en) 2013-03-15 2015-02-10 Global Blood Therapeutics, Inc. Compounds and uses thereof for the modulation of hemoglobin
US9458139B2 (en) 2013-03-15 2016-10-04 Global Blood Therapeutics, Inc. Compounds and uses thereof for the modulation of hemoglobin
WO2014145040A1 (en) 2013-03-15 2014-09-18 Global Blood Therapeutics, Inc. Substituted aldehyde compounds and methods for their use in increasing tissue oxygenation
PE20160078A1 (en) 2013-03-15 2016-03-02 Global Blood Therapeutics Inc COMPOUNDS AND THEIR USES TO MODULATE HEMOGLOBIN
US9422279B2 (en) 2013-03-15 2016-08-23 Global Blood Therapeutics, Inc. Compounds and uses thereof for the modulation of hemoglobin
MX2015011445A (en) 2013-03-15 2016-04-20 Global Blood Therapeutics Inc Compounds and uses thereof for the modulation of hemoglobin.
MX2015011448A (en) 2013-03-15 2016-06-06 Global Blood Therapeutics Inc Compounds and uses thereof for the modulation of hemoglobin.
BR112016010403A2 (en) 2013-11-12 2017-08-08 Vertex Pharma PROCESS OF PREPARING PHARMACEUTICAL COMPOSITIONS FOR THE TREATMENT OF CFTR-MEDIATED DISEASES
EA202092627A1 (en) 2013-11-18 2021-09-30 Глобал Блад Терапьютикс, Инк. COMPOUNDS AND THEIR APPLICATIONS FOR HEMOGLOBIN MODULATION
PL3102576T3 (en) 2014-02-03 2019-12-31 Vitae Pharmaceuticals, Llc Dihydropyrrolopyridine inhibitors of ror-gamma
AP2016009261A0 (en) 2014-02-07 2016-06-30 Global Blood Therapeutics Inc Crystalline polymorphs of the free base of 2-hydroxy-6-((2-(1-isopropyl-1h-pyrazol-5-yl)pyridin-3-yl)methoxy)benzaldehyde
WO2015158202A1 (en) * 2014-04-18 2015-10-22 杭州普晒医药科技有限公司 Crystal form of oxazolidinone antibiotics and preparation method, composition and use thereof
CN105646451A (en) * 2014-11-12 2016-06-08 江苏豪森药业集团有限公司 Potassium ion competitive acid blocker crystal form and preparation method thereof
BR112017010406B1 (en) 2014-11-18 2021-03-09 Vertex Pharmaceuticals Incorporated process of carrying out high-throughput testing of high-performance liquid chromatography
KR20170095972A (en) * 2014-12-18 2017-08-23 머크 샤프 앤드 돔 코포레이션 (s)-n-(3-(6-isopropoxypyridin-3-yl)-1h-indazol-5-yl)-1-(2-(4-(4-(1-methyl-1h-1,2,4-triazol-3-yl)phenyl)-3,6-dihydropyridin-1(2h)-yl)-2-oxoethyl)-3-(methylthio)pyrrolidine-3-carboxamide compositions for pharmaceutical preparations
MX2017014799A (en) * 2015-05-21 2023-02-23 Crystal Pharmatech Co Ltd New crystal form of lenvatinib methanesulfonate salt and preparation method thereof.
CN111848603B (en) 2015-08-14 2022-08-09 上海海雁医药科技有限公司 Preparation method of orexin receptor antagonist receptor compound and intermediate and crystal form thereof
CA3005658A1 (en) 2015-11-20 2017-05-26 Vitae Pharmaceuticals, Inc. Modulators of ror-gamma
SG10201912511WA (en) 2015-12-04 2020-02-27 Global Blood Therapeutics Inc Dosing regimens for 2-hydroxy-6-((2-(1-isopropyl-1h-pyrazol-5-yl)pyridin-3-yl)methoxy)benzaldehyde
US10189808B2 (en) 2016-01-08 2019-01-29 Celgene Corporation Solid forms of 2-(4-chlorophenyl)-N-((2-(2,6-dioxopiperidin-3-yl)-1-oxoisoindolin-5-yl)methyl)-2,2-difluoroacetamide, and their pharmaceutical compositions and uses
CN108779129A (en) * 2016-03-09 2018-11-09 赛比亚斯药业股份公司 Vinorelbine list tartrate and its medicinal usage
TWI825524B (en) 2016-05-12 2023-12-11 美商全球血液治療公司 Process for synthesizing 2-hydroxy-6-((2-(1-isopropyl-1hpyrazol-5-yl)-pyridin-3-yl)methoxy)benzaldehyde
AU2017277002B2 (en) * 2016-06-07 2021-01-21 Jiangsu Hengrui Medicine Co., Ltd. Pharmaceutically acceptable salt as renal outer medullary potassium channel inhibitor
US10562855B2 (en) * 2016-06-08 2020-02-18 Crystal Pharmatech Co., Ltd. Crystalline form of lenvantinib mesylate and process of preparation thereof
US10604521B2 (en) * 2016-06-17 2020-03-31 Crystal Pharmaceuticals (Suzhou) Co., Ltd. Crystalline forms of PLX3397 hydrochloride, processes for preparation and use thereof
WO2018006870A1 (en) * 2016-07-07 2018-01-11 苏州科睿思制药有限公司 Galunisertib crystal form and preparation method therefor and use thereof
TW201811326A (en) * 2016-07-18 2018-04-01 比利時商健生藥品公司 Salt forms of 4-cyano-N-(2-(4,4-dimethylcyclohex-1-en-1-yl)-6-(2,2,6,6-tetramethyltetrahydro-2H-pyran-4-yl)pyridin-3-yl)-1H-imidazole-2-carboxamide
CN109563072B (en) * 2016-08-26 2021-05-11 东丽株式会社 Crystal of cyclic amine derivative and medical use thereof
EP3299360A1 (en) * 2016-09-21 2018-03-28 INDENA S.p.A. Crystal forms of lenvatinib
TWI735652B (en) * 2016-09-29 2021-08-11 心悅生醫股份有限公司 Co-crystal and/or eutectic crystal of kojic acid, compositions comprising the same, and uses thereof
TW202332423A (en) 2016-10-12 2023-08-16 美商全球血液治療公司 Tablets comprising 2-hydroxy-6-((2-(1-isopropyl-1h-pyrazol-5-yl)pyridin-3-yl)methoxy)benzaldehyde
GB201622007D0 (en) * 2016-12-22 2017-02-08 And See Cambridge Display Tech Ltd Syngenta Participations Ag Polymorphs
WO2018117267A1 (en) * 2016-12-22 2018-06-28 大鵬薬品工業株式会社 Salt of substituted piperidine compound
US10093647B1 (en) * 2017-05-26 2018-10-09 Celgene Corporation Crystalline 4-amino-2-(2,6-dioxopiperidine-3-yl)isoindoline-1,3-dione dihydrate, compositions and methods of use thereof
AU2018294314A1 (en) * 2017-06-30 2020-02-06 Bristol-Myers Squibb Company Amorphous and crystalline forms of IDO inhibitors
WO2019018975A1 (en) * 2017-07-24 2019-01-31 Vitae Pharmaceuticals, Inc. Inhibitors of ror gamma
US10093648B1 (en) 2017-09-22 2018-10-09 Celgene Corporation Crystalline 4-amino-2-(2,6-dioxopiperidine-3-yl)isoindoline-1,3-dione hemihydrate, compositions and methods of use thereof
US10093649B1 (en) * 2017-09-22 2018-10-09 Celgene Corporation Crystalline 4-amino-2-(2,6-dioxopiperidine-3-yl)isoindoline-1,3-dione monohydrate, compositions and methods of use thereof
US11465974B2 (en) * 2017-12-19 2022-10-11 Assia Chemical Industries Ltd. Crystalline polymorphs of Pracinostat and Pracinostat salts
CA3086535A1 (en) * 2017-12-22 2019-06-27 Elysium Health, Inc. Crystalline forms of nicotinamide riboside chloride
EP3732168A1 (en) * 2017-12-27 2020-11-04 Teva Pharmaceuticals International GmbH Solid state forms of pemafibrate
CN110869351B (en) * 2018-06-27 2022-03-18 深圳仁泰医药科技有限公司 Crystalline forms of (R) -N- (4-chlorophenyl) -2- (cis-4- (6-fluoroquinolin-4-yl) cyclohexyl) propionamide
ES2961765T3 (en) * 2018-07-04 2024-03-13 Cstone Pharmaceuticals Suzhou Co Ltd HDAC6 selective inhibitor polymorph and its application
US11434202B2 (en) * 2018-09-05 2022-09-06 Assia Chemical Industries Ltd. Crystalline polymorphs of Rivoceranib and Rivoceranib mesylate
EP3860975B1 (en) 2018-10-01 2023-10-18 Global Blood Therapeutics, Inc. Modulators of hemoglobin for the treatment of sickle cell disease
KR20210137159A (en) * 2019-03-12 2021-11-17 아릭사 파마슈티컬스 인코포레이티드 Crystalline Forms of Abibactam Derivatives
WO2021007189A1 (en) * 2019-07-08 2021-01-14 Rezolute, Inc. Crystalline forms of plasma kallikrein inhibitors
MX2022013304A (en) * 2020-04-21 2022-12-15 Idience Co Ltd Crystalline forms of phthacaz1nonf compound.

Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4695569A (en) * 1983-11-30 1987-09-22 Janssen Pharmaceutica N.V. Bicyclic heterocyclyl containing N-(bicyclic heterocyclyl)-4-piperidinamines
US5817823A (en) * 1997-04-17 1998-10-06 Sepracor Inc. Method for synthesizing 2-substituted imidazoles
US5922737A (en) * 1996-02-21 1999-07-13 Hoechst Marion Roussel, Inc. Substituted N-methyl-N-(4-(4-(1H-Benzimidazol-2-YL-amino) piperidin-1-YL)-2-(arlyl) butyl) benzamides useful for the treatment of allergic diseases

Family Cites Families (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4835161A (en) * 1986-02-03 1989-05-30 Janssen Pharmaceutica N.V. Anti-histaminic compositions containing n-heterocyclyl-4-piperidinamines
EP0658110B1 (en) 1992-09-03 1999-12-15 Sepracor, Inc. Use of norastemizole for the treatment of allergic rhinitis

Patent Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4695569A (en) * 1983-11-30 1987-09-22 Janssen Pharmaceutica N.V. Bicyclic heterocyclyl containing N-(bicyclic heterocyclyl)-4-piperidinamines
US5922737A (en) * 1996-02-21 1999-07-13 Hoechst Marion Roussel, Inc. Substituted N-methyl-N-(4-(4-(1H-Benzimidazol-2-YL-amino) piperidin-1-YL)-2-(arlyl) butyl) benzamides useful for the treatment of allergic diseases
US5817823A (en) * 1997-04-17 1998-10-06 Sepracor Inc. Method for synthesizing 2-substituted imidazoles

Also Published As

Publication number Publication date
US6627646B2 (en) 2003-09-30
US20030100581A1 (en) 2003-05-29

Similar Documents

Publication Publication Date Title
US6627646B2 (en) Norastemizole polymorphs
EP2535339A1 (en) Polymorphs of dasatinib, preparation methods and pharmaceutical compositions thereof
TW201313703A (en) Novel crystalline forms of Azilsartan and preparation thereof
EP3243824A1 (en) Solid forms of ibrutinib free base
EP3636640B1 (en) Crystal of heterocyclidene acetamide derivative
RU2627702C2 (en) Crystalline forms of 1-(3-tret-butyl-1-p-tolyl-1h-pyrazol-5-yl)-3-(5-fluoro-2-(1-(2-hydroxyetil)-1h-indasol-5-yloxy)benzyl) hydrochloride urea
KR20210105931A (en) Novel crystalline form of NRTTI compound
WO2007128561A1 (en) Crystalline forms of letrozole and processes for making them
CN111205290B (en) Crystal form of JAK kinase inhibitor and preparation method thereof
US20040063782A1 (en) Bicalutamide forms
BRPI0602206B1 (en) polymorphic form of dexketoprofen trometamol and compositions containing it
JP2024500665A (en) 2-Hydroxy-5-[2-(4-(trifluoromethylphenyl)ethylamino)]benzoic acid crystal form and its production method
Caplette et al. Characterization of new crystalline forms of hydroxyprogesterone caproate
JP2006160766A (en) CRYSTAL OF (±)2-(DIMETHYLAMINO)-1-{[O-(m-METHOXYPHENETHYL)PHENOXY]METHYL}ETHYL HYDROGEN SUCCINATE HYDROCHLORIDE
JP2022508864A (en) Crystal form of maleate, a tyrosine kinase inhibitor, and its preparation method
KR20140072323A (en) New crystalline form of (S)-bepotastine p-toluenesulfonic acid salt and the process for preparing thereof
US20040038985A1 (en) Crystal forms of 1- [6-chloro-5-(trifluoromethly) -2-pyridinyl] piperazine hydrochloride
EP3800175A1 (en) Hexadecyl treprostinil crystals and methods for preparation thereof
EP3656768A1 (en) Beraprost-314d crystals and methods for preparation thereof
JP2010077155A (en) CRYSTAL OF (±)2-(DIMETHYLAMINO)-1-{[O-(m-METHOXYPHENETYL)PHENOXY]METHYL}ETHYL HYDROGEN SUCCINATE HYDROCHLORIDE
US20100113831A1 (en) Highly Pure Crystalline Benzphetamine Hydrochloride and Processes for Preparing
TW202342470A (en) Crystalline (+)-tetrabenazine
EP4313945A1 (en) Crastalline hydrobromide salt of 5-meo-dmt
WO2015170827A1 (en) Method for producing gamma-form crystal of silodosin
EP1768961A1 (en) Novel form of celecoxib

Legal Events

Date Code Title Description
AK Designated states

Kind code of ref document: A1

Designated state(s): AE AG AL AM AT AU AZ BA BB BG BR BY BZ CA CH CN CO CR CU CZ DE DK DM DZ EC EE ES FI GB GD GE GH GM HR HU ID IL IN IS JP KE KG KP KR KZ LC LK LR LS LT LU LV MA MD MG MK MN MW MX MZ NO NZ OM PH PL PT RO RU SD SE SG SI SK SL TJ TM TN TR TT TZ UA UG UZ VN YU ZA ZM ZW

AL Designated countries for regional patents

Kind code of ref document: A1

Designated state(s): GH GM KE LS MW MZ SD SL SZ TZ UG ZM ZW AM AZ BY KG KZ MD RU TJ TM AT BE BG CH CY CZ DE DK EE ES FI FR GB GR IE IT LU MC NL PT SE SK TR BF BJ CF CG CI CM GA GN GQ GW ML MR NE SN TD TG

121 Ep: the epo has been informed by wipo that ep was designated in this application
DFPE Request for preliminary examination filed prior to expiration of 19th month from priority date (pct application filed before 20040101)
REG Reference to national code

Ref country code: DE

Ref legal event code: 8642

122 Ep: pct application non-entry in european phase
NENP Non-entry into the national phase

Ref country code: JP

WWW Wipo information: withdrawn in national office

Country of ref document: JP