Title of Invention

A PHARMACEUTICAL COMPOSITION FOR TREATING HEPATITIS B INFECTION

Abstract A pharmaceutical composition effective for once a day oral administration to treat Hepatitis B virus infection in a human adult patient comprising up to 1 % of entecavir, adhered to a carrier substrate of kind such as herein described, and pharmaceutically acceptable excipients such as herein described in an amount as herein described, wherein the said percentage is based on a total composition weight of 100 mg.
Full Text FORM 2
THE PATENTS ACT 1970
[39 OF 1970] 8B
THE PATENTS RULES, 2003
COMPLETE SPECIFICATION
[See Section 10; rule 13]
"A PHARMACEUTICAL COMPOSTION'
BRISTOL-MYERS SQUIBB COMPANY, a Delaware corporation of P O Box 4000, Princeton, New Jersey 08543-4000, United States of America
The following specification particularly describes the invention and the manner in which it is to be performed:

The present invention relates to a pharmaceutical composition.
Entecavir' tls~ (la' 3a, 40 H'-2-amino-1, 9-dihydro-9- [4-hydroxy-3-(hydroxymethyl)-2-methylenecyclopentyl]-6H-purin-6-one

is an antiviral agent currently undergoing clinical evaluation £or tne treatment of hepatitis B virus
infection.
Entecavlr and its use in treating hepatitis B are
disclosed by Zahler et al. in U.S. Patent 5,206,244. -This patent .disc„lp.§es that..an effective antiviral dose for oral or parenteral administration will likely be in the range oi about 1.0 to 50 mg/kg of body weight and that the derec dose may be administered several times daily at approPriate intervals.
Improved methods for the synthesis of entecavir are disclosed by Bisacchi et al. in WO 98/09964.
-1-

This invention is directed to pharmaceutical compositions containing a low dose of entecavir and the use of such low dose composition to safely and effectively treat hepatitis B virus infection.
This invention is also directed to pharmaceutical compositions -for oral administration containing low doses of a pharmaceutically active substance. This resjult is „ achieved by adhering particles of the pharmaceutically activ^sjibsiaftee to the surface of a carrier substrate. The process of depositing the active substance on the carrier substrate is controlled to minimize the agglomeration of the active substance/carrier substrate particles.
This invention is directed to pharmaceutical compositions containing a low dose of from about 0.001 mg to about 25 mg of the active antiviral agent entecavir for once daily administration to treat hepatitis B virus infection in an adult human patient. Preferred pharmaceutical compositions contain from about 0.01 mg to about 10 mg of entecavir and most preferred pharmaceutical compositions contain from about 0.01 to about 5 mg of entecavir. Such preferred and most preferred pharmaceutical compositions are also administered once daily to treat hepatitis B virus infection in an adult patient.
The term adult human patient is defined as a patient of about 16 years or more of age and a weight equal to or greater than about 50 kilograms. Pharmaceutical compositions containing entecavir at the lower end of the above ranges are suitable for administration to pediatric

patients or adult patients weighing less than about 50 kilograms.
The low dose entecavir pharmaceutical compositions described above for daily administration may also be administered to certain patients less often. For example, patients who have been treated by daily administration of the low dose entecavir pharmaceutical compositions so that their hepatitis B virus infection is low under control may be placed on. a maintenance regimen to protect against further infection. Such maintenance therapy may involve the administration of the low dose entecavir composition on a less than daily basis. For example, a single dose administered every three or four jiays or administered on a weekly basis may be sufficient.
The low dose entecavir pharmaceutical compositions of this invention can be formulated for administration by any suitable means. For example, compositions for oral administration, which are preferred, can be in the form of tablets, capsules, granules or powders or in the form of elixirs, solutions or suspensions. The low dose entecavir pharmaceutical compositions may also be formulated for parenteral, rectal, transdermal or nasal administration according to methods well known in the art. Such formulations can include pharmaceutical^ acceptable excipients including bulking agents, lubricants, disintegrants, binding agents, etc. as commonly employed in such compositions. Sustained release formulations are also within the scope of this invention.
Surprisingly, it has been found that once daily administration of the low dose entecavir pharmaceutical compositions of this invention are effective in treating hepatitis B virus infection without undesirable side effects that can result from administration of the high dose regimen described in U.S. Patent 5,206,24 4.

This invention is also directed to the treatment of hepatitis B virus infection with low dose entecavir compositions as described above in combination with one or more other pharmaceutically active agents. Suitable pharmaceutically active agents for this purpose include one or more antiviral agents, for example, didanosine, lamivudine, abacavir, adefovir, adefovir dipivoxil, famciclovir, (2R,4R)-4-(2,6-diamino-9H-purin-9-yl)-2-hydroxymethyl-1,3-dioxolane (DAPD), hepatitis B immunomodulating proteins (EHT 899 from Enzo Biochem),
emtricitabine, 1- (2-deoxy-2-fluoro-|3-D-arabinofuranosyl)thymine(FMAU), GLQ-223 (Compound A, alpha-trichosanthin), epavudine (L-dT), epcitabine (L~ dC), ribavirin, tenofovir (PMPA), 2',3'-dideoxy-2',3'-didehydro-beta-L(-)-5-fluorocytidine[L
(-)Fd4C], as well as other fluoro L- and D- nucleosides. Suitable pharmaceutically active agents for this purpose also include one or more immuhomodulators, for example, alpha interferon, beta interferon, pegylated interferon, thymosin alpha, and hepatitis B vaccines such as HBV/MF59, Hepagene and Theradigm-HBV.
When the other pharmaceutically active agent or agents are suitable for oral administration, they can be combined with the low dose of entecavir into a single tablet or capsule. If the other pharmaceutically active agent or agents are not compatable with entecavir for co¬administration from a single dosage form, for example, if the mode of administration is different or if the frequency of administration is different, then the other pharmaceutically active agent or agents will be administered separately. The amount of the other agent or agents administered is that conventionally employed in mono therapy or a reduced amount as determined by the treating physician. The separate dose forms can be

administered at the same time or sequentially according to a prescribed schedule.
This invention also includes the treatment of co-infected patients with the low dose entecavir compositions described above. A co-infected patient is one infected with other viral or non-viral diseases in addition to hepatitis B. In particular, such treatment is possible for hepatitis B patients co-infected with hepatitis C or HIV. Such co-infected patients are preferably treated with the low dose entecavir compositions as described above in combination with one or more other pharmaceutically active agents as described above. For example, a patient co-infected with hepatitis B and hepatitis C can be.treated with the low dose entecavir composition in addition to being treated with a regimen of ribavirin and an interferon.
Another aspect of this invention is the preparation of pharmaceutical compositions, particularly tablets and capsules, containing entecavir in an amount of less than or equal to about 10 mg. Such compositions cannot be prepared with good content uniformity by simply mixing the active substance and the excipients. The traditional methods of granulation are also not suitable for products active at such low doses.
TableT-a7ioT^alpsule formulations containing from about 0.001 mg to about 10 mg of entecavir are prepared according to the following procedures that ensure high potency and good uniformity of the product. The compositions are prepared by first carefully depositing the entecavir on the surface of carrier substrate particles. This step is accomplished by forming a solution of the entecavir in a solvent along with an adhesive substance at temperatures ranging from about 25°C to about 80°C and applying the solution as a spray or a stream while the carrier substrate particles are in

motion. The. conditions are controlled to minimize particle agglomeration. Subsequently, the solvent is removed from the carrier surface leaving the entecavir
particlesadhered to the surface of the carrier
substrate. This prevents the separation of the enteca-vir fr"6m"the substrate and minimizes the loss of entecavir during subsequent processing.
Following drying, the entecavir coated carrier substrate particles are mixed with any other ingredients to be included in the composition such as'a disintegrant and/or lubricant. The resulting powder is then compressed into tablets or filled into capsules.
The carrier substrate particles are kept in motion during the spraying step by means of mechanical or air stream agitation. In the mechanical agitation procedure, the carrier substrate is placed in a mechanical (high shear) mixer and agitated. A solution containing the entecavir and adhesive substance maintained at a
temperature of from about 25°C to about 80°C is sprayed onto the carrier substrate particles at a controlled rate and atomizing pressure (0 to 2 bar). To maximize the amount of entecavir deposited on the carrier, the position of the spray assembly is adjusted to make certain that the spray pattern only encompasses the carrier. The rate of deposition and the spray pattern are controlled to minimize particle agglomeration. Once the entecavir containing solution is deposited, the wet entecavir/carrier substrate particles are transferred to a drier, either a tray drier or fluidbed drier is suitable. The solvent is removed at an elevated temperature. When the solvent is water or pH adjusted water, a temperature of from about 50° to about 80°C is suitable.

In the air stream agitation procedure, the carrier substrate is placed in a bowl with a fine mesh screen at the bottom. The incoming air stream is adjusted so that the substrate particle motion is constant and fluid. The carrier material is equilibrated to a temperature of from
about 25°C to about 80°C. A solution containing the entecavir and adhesive substance maintained at a temperature of from about 25°C to about 80°C is sprayed onto the carrier substrate particles at a controlled rate and atomizing pressure as described above. Again, the position of the spray assembly is adjusted to make certain that the spray pattern only encompasses the carrier and the rate of deposition is controlled to minimize particle agglomeration. Once the entecavir solution is deposited, the temperature is elevated to remove the solvent. When the solvent is water or pH adjusted water, a temperature of from about 50°C to about 80°C is suitable. In the air stream agitation procedure, both the deposition of the entecavir onto the carrier substrate and the removal of the solvent are carried out in a single unit whereas the mechanical agitation procedure requires a two-unit operation.
The above procedures have the additional advantage of reducing exposure of the manufacturing personnel to entecavir in the atmosphere of the facility.
While the above procedures are described for preparing pharmaceutical compositions containing from about 0.005 mg to about 10 mg of entecavir, they can also be employed to prepare pharmaceutical compositions containing low doses of any soluble pharmaceutically active substance.
Preferred solvents in the above procedures are water and pH adjusted water. The solubility of entecavir in water can be increased by lowering the pH of water by the

addition of an acid such as hydrochloric acid or by raising the pH of water by the addition of a base such as ammonium hydroxide.
The adhesive substance is preferably a polymeric material possessing a high degree of tackiness. Suitable materials include povidone, methylcellulose, hydroxymethylcellulose, hydroxypropylmethylcellulose, hydroxypropylcellulose, hydroxyethylcellulose, gelatin, guar gum, and xanthan gum and mixtures thereof with povidone being preferred. The adhesive substance is preferably present in the final composition at from about 0.01% to about 10% by weight of the total composition.
The carrier substrate is a pharmaceutically acceptable substance that can be readily spray coated and yet will not easily agglomerate. Suitable materials include lactose, microcrystalline cellulose, calcium phosphate, dextrin, dextrose, dextrates, mannitol, sorbitol, and sucrose and mixtures thereof with lactose and microcrystalline cellulose and mixtures thereof being preferred. The carrier substrate is preferably present in the final composition at from about 80% to about 95% by weight of the total composition.
A disintegrant is preferably included in the final composition at from about 1% to about 7% by weight of the total composition. Suitable disintegrants include crospovidone, croscarmellose, sodium starch glycolate, pregelatinized starch, and corn starch and mixtures thereof with crospovidone being preferred.
A lubricant is preferably included in the final composition at from about 0.1% to about 5% by weight of the total composition. Suitable lubricants include magnesium stearate, stearic acid, sodium stearyl fumarate, and sodium lauryl sulfate with magnesium stearate being preferred.

The resulting tablet or capsule can be film coated for ease of administration. Suitable materials for use in the film coating are polymeric coating agents, pigments, plasticizers, solubilizing agents, etc. Suitable coating agents include hydroxypropyl methylcellulose, hydroxyethyl cellulose, hydroxypropyl cellulose, hydroxypropyl methylcellulose phthalate, etc. Polyethylene glycol can be included in the film coating composition as a plasticizer. Additional plasticizers such as diethyl citrate and trietyl citrate may also be included in the film coating composition. Suitable solubilizing agents include polyoxyethylene sorbitan fatty acid esters particularly polysorbate 80. Suitable pigments include titanium dioxide and various iron oxides.
The ingredients of the' coating compositions are dispersed in a suitable solvent, preferably water. The coating composition can be applied to the tablets or capsules using conventional pan coating or spray coating techniques.
The following examples describe low dose entecavir compositions within the scope of this invention.

Example 1
Employing the above procedures a tablet of 0.5 milligram strength entecavir was prepared.

Ingredient Amount % weight/weight Amount . per tablet
Entecavir 0.5 0.50 mg
'Lactose monohydrate, NF 60.00 60.00 mg
Microcrystalline cellulose, NF 32.50 32.50 mg
TTrospovidone, NF 4.00 4.00 mg
Povidone, USP 2.50 • 2.50 mg
Magnesium Stearate,NF 0.50 0.50 mg
Purified Water, USP* q.s. —
Total 100.00 100.00 mg^f*
*removed by drying

Example 2
Employing the above procedures a tablet of 0.1 milligram strength entecavir was prepared.

Ingredient Amount % weight/weight Amount per capsule
Entecavir
. 0.1 0.1 mg
Lactose monohydrate, NF 60,00 60.00
Microcrystalline cellulose, NF 35.39 35.39 mg
Crospovidone, NF 4.0 4.00 mg
Povidone, USP 0.01 0.01 mg
Magnesium Stearate,NF 0.5 0.5 mg
Purified Water, USP* .q.s
Total 100.00 100.00 mg
*removed by drying

Example 3
Employing the above procedures a tablet of 0.01 milligram strength entecavir was prepared.

Ingredient Amount % weight/weight Amount per tablet
Entecavir 0.01 0.01 mg
Macrocrystalline cellulose, NF 93.24 93.24 mg
Crospovidone, NF 4.00 4.00 mg
Povidone, USP 2.50 2.50 mg
Magnesium Stearate,NF 0.25 0.25 mg
Purified Water, USP* q.s.
Total 100.00 100.00 mg
*removed by drying

Example 4
Employing the above procedures a 10 milligram strength entecavir capsule was prepared.

Ingredient Amount % weight/weight Amount per capsule
Entecavir 10.00 10.00 mg
Microcrystalline cellulose, NF 82.03 82.03 mg
Crospovidone, NF 4.00 4.00 mg
Povidone, USP 2.50 2.50 mg
Magnesium Stearate,NF 0.25 0.25 mg
Hydrochloric acid 1.22 1.22 mg
Purified Water, USP* g.s. — —.—
Total 100.00 100.00 mg
Capsule shell
*removed by drying

Example 5
Employing the above procedures a 0.05 milligram strength entecavir capsule was prepared.

Ingredient Amount % weight/weight Amount per capsule
Entecavir 0.05 0.05 mg
Dicalcium phosphate, NF 93.20 93.20 mg
Crospovidone, NF 4.00 4.00 mg
Hydroxypropyl cellulose, NF 2.50 2.50 mg
Magnesium Stearate,NF 0.25 0.25 mg
Purified Water, USP*' q.s. — __
Total 100.00 100.00 mg
Capsule shell
*removed by drying

Example 6
Employing the above procedures a tablet of 1 milligram strength entecavir was prepared.

Ingredient Amount % weight/weight Amount per tablet
Entecavir 1.00 1.00 mg
Mannitol, NF 90.00 90.00 mg
Croscarmellose sodium, NF 4.00 4.00 mg
Methyl Cellulose, NF 2.50 2.50 mg
Stearic Acid, NF 2.50 0.25 mg
Purified Water, USP* q. s. — — —
Total 100.00 100.00 mg
♦removed by drying

Example 7
The 100 mg tablet of Example 1 containing 0.5 mg of entecavir, the 100'mg tablet of Example 2 containing 0.1 mg of entecavir, the 100 mg tablet of Example 3 containing 0.01 mg of entecavir and the 100 mg tablet of Example 6 containing 1.0 mg of 'entecavir can be film coated with the composition set forth below using conventional pan coating or spray coating techniques.

Ingredient Amount % weight/weight Amount per tablet1
Opadry® 1 to 10 1 to 10 mg
Plasticizer'4 0 to 10 0 to 10 mg
Purified Water, USP* q.s. » — — —
removed by drying
Opadry® is commercially available and contains hydroxypropylmethylcellulose, titanium dioxide, polyethylene glycol, polysorbate 80, synthetic yellow iron oxide and synthetic red iron oxide.
1 The calculations are done assuming a tablet weight of
100 mg.
2 Suitable plasticizers are diethyl citrate and triethyl
citrate.

Example 8
The safety and antiviral activity of entecavir given for 28 days to human subjects with chronic hepatitis B virus infection was studied in a randomized, double-blind, placebo-controlled, dose-escalating trial. Entecavir demonstrated potent antiviral activity at all doses tested. The mean log reduction in hepatitis B virus DNA viral levels in the blood at day 28 were 2.21, 2,25, 2.81, and 2.42 for the 0.05, 0.1, 0.5 and 1.0 mg once daily doses of entecavir, respectively. Entecavir was well tolerated.
Example 9
The safety and antiviral activity of three doses of entecavir (0.01 mg, 0.1 mg and 0.5 mg) given once daily for 24 weeks were studies in adults with chronic hepatitis B in a randomized, double-blind, lamivudine (100 mg QD) controlled trial. All three doses of entecavir demonstrated potent antiviral activity. The two higher doses of entecavir produced significantly greater reductions in hepatitis B virus DNA viral levels in blood compared to lamivudine. Entecavir at all doses was well tolerated.

CLAIM;
1. A pharmaceutical composition effective for once a day oral administration to treat Hepatitis B virus infection in a human adult patient comprising up to 1 % of entecavir, adhered to a carrier substrate of kind such as herein described, and pharmaceutically acceptable excipients such as herein described in an amount as herein described, wherein the said percentage is based on a total composition weight of 100 mg.
2. A composition as claimed in claim 1 wherein the said entecavir is present at 0.01% to 1% based on the total weight of composition.
3. A composition as claimed in claim 1 wherein the said entecavir is present at 0.01% to 0.1% mg based on the total weight of composition.
4. A composition as claimed in claim 1 wherein the composition is in the form of a tablet or capsule optionally film coated.
5. A composition as claimed in claim 1 wherein the carrier substrate employed is lactose, microcrystalline cellulose, calcium phosphate, dextrine, dextrose, dextrates, mannitol, sorbitol, sucrose or mixture thereof and entecavir is adhered to carrier substrate by an adhesive substance, which is a polymeric material selected from povidone, methylcellulose, hydroxymethylcellulose, hydroxypropylmethyl-cellulose, hydroxypropylcellulose, hydroxyethylcellulose, gelatin, guar gum, and xanthan gum and mixtures thereof and the pharmaceutically acceptable excipients comprising lubricant, and disintegrant.
6. A composition as claimed in claim 5 wherein the lubricant used is selected from
magnesium stearate, stearic acid, sodium stearyl fumarate, and sodium lauryl
sulfate, and mixtures thereof and said disintegrant is selected from crospovidone,
croscarmellose sodium, sodium starch glycolate, pregelatinized starch, and corn
starch and mixtures thereof.

7. A composition as claimed in claim 1 contains one or more other
pharmaceutically active substances.
8. A pharmaceutical composition as claimed in claim 1 comprising entecavir coated by means of an adhesive substance adhered to a carrier substrate , a lubricant, and a disintegrant wherein said entecavir is present in the range of 0.01 to 1.0% by weight of said composition, said adhesive substance is present in the range of 0.01 to 10% by weight of said composition, said carrier substrate is present in the range of 80 to 95% by weight of said composition, said disintegrant is present in the range of 1 to 7% by weight of said composition, and said lubricant is present in the range of 0.1 to 5% by weight of said composition.
9. A composition as claimed in claim 8 wherein said adhesive substance is selected from povidone, methylcellulose, hydroxymethylcellulose, hydroxypropyl -methylcellulose, hydroxypropylcellulose, hydroxyethyl-cellulose, gelatin, guar gum, and xanthan gum and mixtures thereof, said carrier substrate is selected from lactose, microcrystalline cellulose, calcium phosphate, dextrin, dextrose, dextrates, mannitol, sorbitol, and sucrose and mixtures thereof, said disintegrant is selected from crospovidone, croscarmellose sodium, sodium starch glycolate, pregelatinized starch, and corn starch, and mixtures thereof, and said lubricant is selected from magnesium stearate, stearic acid, sodium stearyl fumarate, and sodium lauryl sulfate, and mixtures thereof.
10. A composition as claimed in preceding claim wherein said adhesive substance is povidone, carrier substrate is microcrystalline cellulose or lactose or mixtures thereof disintegrant is crospovidone, lubricant is magnesium stearate.
11. A composition as claimed in claim 1 comprising (a) 0.01% entecavir, 93.24% microcrystalline cellulose, 4.0% crospovidone, 2.50% povidone, and 0.25% magnesium stearate, (b) 1.0% entecavir, 90.0% mannitol, 4.0% croscarmellose

sodium, 2.50% methyl cellulose, and 2.50% stearic acid, (c) 0.5% entecavir, 60.00% lactose monohydrate, 32.50% microcrystalline cellulose, 4.0% crospovidone, 2.50% povidone, and 0.50% magnesium stearate, and (d) 0.1% entecavir, 60.00% lactose monohydrate, 35.39% microcrystalline cellulose, 4.0% crospovidone, 0.01% povidone, and 0.5% magnesium stearate, said percentage being on a weight/weight basis.
12. A method of preparing a pharmaceutical composition of entecavir as claimed in claim 1 comprising (a) dissolving said entecavir and an adhesive substance in a solvent wherein said solvent is water or water having an acidic or basic pH, (b) spraying said solution obtained in step (a) onto a carrier substrate while said carrier substrate is in motion, (c) drying said coated carrier substrate from step (b) to remove said solvent, and (d) combining said dried coated carrier substrate from step (c) with other excepients as claimed herein above to form said pharmaceutical composition.
13. The method as claimed in claim 12 wherein: said carrier substrate is kept in motion during spraying step (b) by air stream or by mechanical agitation, and said coated carrier substrate is dried in step (c) by means of air stream agitation in a tray drier or fluid-bed drier.
Dated this 26th day of January 2001
Applicant's Agent

Documents:

IN-PCT-2002-00891-MUM-CANCELLED PAGES(28-2-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(2-7-2002).pdf

IN-PCT-2002-00891-MUM-CLAIMS(AMENDED)-(21-2-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(AMENDED)-(27-12-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(AMENDED)-(28-2-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(AMENDED)-(4-1-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(AMENDED)-(7-2-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(AMENDED)-(9-2-2007).pdf

IN-PCT-2002-00891-MUM-CLAIMS(GRANTED)-(2-1-2008).pdf

IN-PCT-2002-00891-MUM-CORRESPONDENCE 1(26-12-2007).pdf

IN-PCT-2002-00891-MUM-CORRESPONDENCE 2(11-10-2011).pdf

IN-PCT-2002-00891-MUM-CORRESPONDENCE 3(16-4-2009).pdf

IN-PCT-2002-00891-MUM-CORRESPONDENCE(10-9-2009).pdf

IN-PCT-2002-00891-MUM-CORRESPONDENCE(IPO)-(19-11-2009).pdf

IN-PCT-2002-00891-MUM-DESCRIPTION(COMPLETE)-(2-7-2002).pdf

IN-PCT-2002-00891-MUM-DESCRIPTION(GRANTED)-(2-1-2008).pdf

IN-PCT-2002-00891-MUM-FORM 1(16-8-2002).pdf

IN-PCT-2002-00891-MUM-FORM 1(17-4-2006).pdf

IN-PCT-2002-00891-MUM-FORM 1(2-7-2002).pdf

IN-PCT-2002-00891-MUM-FORM 13(21-5-2009).pdf

IN-PCT-2002-00891-MUM-FORM 13(27-9-2007).pdf

IN-PCT-2002-00891-MUM-FORM 18(22-11-2005).pdf

IN-PCT-2002-00891-MUM-FORM 2(COMPLETE)-(2-7-2002).pdf

IN-PCT-2002-00891-MUM-FORM 2(GRANTED)-(2-1-2008).pdf

IN-PCT-2002-00891-MUM-FORM 2(TITLE PAGE)-(2-7-2002).pdf

IN-PCT-2002-00891-MUM-FORM 2(TITLE PAGE)-(AMENDED)-(17-4-2006).pdf

IN-PCT-2002-00891-MUM-FORM 2(TITLE PAGE)-(GRANTED)-(2-1-2008).pdf

IN-PCT-2002-00891-MUM-FORM 3(17-4-2006).pdf

IN-PCT-2002-00891-MUM-FORM 3(2-7-2002).pdf

IN-PCT-2002-00891-MUM-FORM 4(25-6-2007).pdf

IN-PCT-2002-00891-MUM-FORM 5(17-4-2006).pdf

IN-PCT-2002-00891-MUM-FORM 5(2-7-2002).pdf

IN-PCT-2002-00891-MUM-PETITION UNDER RULE 137(17-4-2006).pdf

IN-PCT-2002-00891-MUM-PETITION UNDER RULE 138(17-4-2006).pdf

IN-PCT-2002-00891-MUM-POWER OF AUTHORITY(17-4-2006).pdf

IN-PCT-2002-00891-MUM-POWER OF AUTHORITY(2-5-2002).pdf

IN-PCT-2002-00891-MUM-SPECIFICATION(AMENDED)-(17-4-2006).pdf

IN-PCT-2002-00891-MUM-WO INTERNATIONAL PUBLICATION REPORT(2-7-2002).pdf


Patent Number 213457
Indian Patent Application Number IN/PCT/2002/00891/MUM
PG Journal Number 04/2008
Publication Date 25-Jan-2008
Grant Date 02-Jan-2008
Date of Filing 02-Jul-2002
Name of Patentee BRISTOL-MYERS SQUIBB COMPANY
Applicant Address P O BOX 4000, PRINCETON, NEW JERSEY 08543-4000, UNITED STATES OF AMERICA.
Inventors:
# Inventor's Name Inventor's Address
1 OMAR L.SPROCKEL 1250 DOGWOOD DRIVE, BRIDGEWATER, NJ 08807 USA
2 ABIZER HARIANAWALA 6103 LEXINGTON DRIVE, LEXINGTON, MA 02421
3 DIVYAKANT DESAI 19 GREENFIELD DRIVE NORTH, WEST WINDSOR, NJ 08550
4 MICHAEL G. FAKES 15 DERBY CHASE COURT, BELLE MEAD, NJ 08502, USA
5 RICHARD J COLONNO 18 SALISBURY WAY, FARMINGTON, CT 0 6032 USA
PCT International Classification Number A61K31/52
PCT International Application Number PCT/US01/02630
PCT International Filing date 2001-01-26
PCT Conventions:
# PCT Application Number Date of Convention Priority Country
1 60/185,672 2000-02-29 U.S.A.
2 60/221,313 2000-07-28 U.S.A.