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Last Updated: March 28, 2024

Claims for Patent: 9,364,553


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Summary for Patent: 9,364,553
Title:Synergistic biomolecule-polymer conjugates
Abstract: The synergistic biomolecule-polymer conjugates are the long-acting, in vivo controlled continuous-release and hybrid synergy systems of biomolecules that provide increased biological activities and enhanced pharmacological properties for achieving greater therapeutic efficacies.
Inventor(s): Lee; Chyi (Princeton Junction, NJ)
Assignee: PEG Biosciences, Inc. (Monmouth Junction, NJ)
Application Number:14/444,555
Patent Claims:1. A synergistic biomolecule-polymer conjugate comprising the formula: [(P-L).sub.n-R--C].sub.x-M wherein M is a biologically active biomolecule; wherein x is the number of cleavable-linkage polymers coupled to said biomolecule and x.gtoreq.1; wherein n.gtoreq.2; wherein P is a polymer or polymer lipid; wherein P.sub.n are multiple polymeric arms or pieces wherein their types and sizes may be the same or different; wherein L.sub.n is a functional linkage moiety comprising at least one cleavable linkage and at least one permanent linkage; or L.sub.n are all cleavable linkages; wherein R is a non-cleavable spacer connected between polymer and the biomolecule; and C is a coupling group attached to the biomolecule, wherein said synergistic biomolecule-polymer conjugate is cleaved in human blood plasma so that biologically active cleavage products are released.

2. The synergistic biomolecule-polymer conjugate of claim 1, wherein the permanent linkage is selected from the group consisting of amide, carbamate, imide, amine, urea, ether, sulfide, thiourea, thiocarbamate, and dithiocarbamate; and the cleavable linkage is selected from the group consisting of carboxylic ester, carbonate, sulfonic ester, phosphoric ester, acylimidazo and carbamate-imidazo.

3. The synergistic biomolecule-polymer conjugate of claim 1, wherein said coupling group C is selected from the group consisting of active ester, mixed anhydride, alkyl aldehyde, aromatic aldehyde, maleimide, haloacetyl, carboxylic acid, isocyanate, isothiocyanate, carbonyl, thiol, disulfide, amino, hydroxyl, hydrazide, and hydrazine, wherein said active ester is selected from the group consisting of N-hydroxysuccinimide ester, p-nitrophenyl ester, N-succinimidyl carbonate, p-nitrophenyl carbonate, acylimidazo and trichlorophenylcarbonate.

4. The synergistic biomolecule-polymer conjugate of claim 1, wherein R is selected from the group consisting of lysine, serine, threonine, cysteine, tyrosine, histidine, arginine, glutamic acid, aspartic acid, homocysteine, homoserine and ornithine.

5. The synergistic biomolecule-polymer conjugate of claim 1, wherein n=2, providing a cleavable-branched polymer conjugate comprising the formula: ##STR00009## wherein L.sub.1 is a permanent linkage and wherein L.sub.2 is a cleavable linkage, providing a permanent-cleavable-linkage two-arm branched polymer; or wherein L.sub.1 and L.sub.2 both are cleavable linkages providing an all-cleavable-linkage two-arm branched polymer.

6. The synergistic biomolecule-polymer conjugate of claim 1, wherein P.sub.1 and P.sub.2 are methoxy poly(ethylene glycol); wherein R is lysine, having a structure represented by: ##STR00010## wherein bond a is a permanent linkage selected from the group consisting of amide, carbamate, urea, imide, amine, thiocarbamate, thiourea, and dithiocarbamate; wherein bond a is connected to either an .alpha.- or .epsilon.-amino group; wherein bond b is a cleavable linkage selected from the group consisting of carboxylic ester, carbonate, and carboxyl-imidazo, wherein the free amino group further connects spacers comprising activated moieties selected from the group consisting of N-hydroxysuccinimide ester, p-nitrophenyl ester, N-succinimidyl carbonate, p-nitrophenyl carbonate, acylimidazo, aldehyde, maleimide, haloacetyl, carboxylic acid, hydroxyl, isocyanate, isothiocyanate, carbonyl, thiol, disulfide, amino, hydroxyl, hydrazide, and hydrazine.

7. The synergistic biomolecule-polymer conjugate of claim 6, wherein the permanent-cleavable linkages branched PEG derivative includes Lys(.alpha.-10K mPEG, carbamate; 20K mPEG Ester) .epsilon.-Succinimidyl Suberate, Compound 5.

8. The synergistic biomolecule-polymer conjugate of claim 6, wherein the permanent-cleavable linkages branched PEG derivative includes Lys(.alpha.-10K mPEG, Amide; 20K mPEG, Ester) .epsilon.-Succinimidyl Suberate, Compound 6.

9. The synergistic biomolecule-polymer conjugate of claim 6, wherein the permanent-cleavable linkages branched PEG derivative includes Lys(.epsilon.-10K mPEG, carbamate; 20K mPEG, Ester) .alpha.-Succinimidyl Suberate, Compound 7.

10. The synergistic biomolecule-polymer conjugate of claim 6, wherein the permanent-cleavable linkages branched PEG derivative is Lys(.epsilon.-10K mPEG, amide; 20K mPEG, Ester) .alpha.-Succinimidyl Suberate, Compound 8.

11. The synergistic biomolecule-polymer conjugate of claim 6, wherein the permanent-cleavable linkages branched PEG derivative is 3-Maleimidopropionyl Lys(.alpha.-10K mPEG, carbamate)-20K mPEG Ester, Compound 9.

12. The synergistic biomolecule-polymer conjugate of claim 1, wherein M is an interferon selected from the group consisting of interferon-.alpha., interferon-.beta., interferon-.gamma., interferon gamma-1b and interferon-.lamda. (interferon lambda).

13. The synergistic biomolecule-polymer conjugate of claim 1, wherein M is an interferon-a selected from the group consisting of interferon-.alpha.-2a, interferon-.alpha.-2b, interferon-.alpha.-1, interferon alfacon-1 and consensus interferon.

14. A synergistic biomolecule-polymer conjugate of claim 1, wherein M is interferon-.alpha.-2b; wherein R is lysine, aspartic acid or glutamic acid; wherein P.sub.1 and P.sub.2 are mPEG and each one has a molecular weight ranging from about 50 to 40,000; wherein L.sub.1 is an amide, carbamate or amine linkage and L.sub.2 is a carboxylic ester or carbonate linkage.

15. A synergistic biomolecule-polymer conjugate of claim 1, wherein M is an interleukin or cytokine; wherein R is lysine, aspartic acid or glutamic acid; wherein P.sub.1 and P.sub.2 are mPEG and each one has a molecular weight ranging from about 50 to 40,000; wherein L.sub.1 is an amide, carbamate or amine linkage and L.sub.2 is a carboxylic ester or carbonate linkage.

16. A synergistic interferon .alpha.-30kPEG (10k mPEG carbamate, 20k mPEG ester) .epsilon.-Suberate conjugate comprising one single component, x=1, wherein the synergistic interferon conjugate is cleaved in human blood plasma so that biologically active cleavage products are released.

17. A synergistic interferon .alpha.-30kPEG (10k mPEG carbamate, 20k mPEG ester) .epsilon.-Suberate conjugate, wherein the conjugate comprises a mixture having composition x=1 to 2 or x=1 to 3, wherein the synergistic interferon conjugate is cleaved in human blood plasma so that biologically active cleavage products are released.

18. The synergistic interferon .alpha.-30kPEG (10k mPEG carbamate, 20k mPEG ester) conjugate of claim 16, wherein the interferon a is interferon .alpha.-2b.

19. A synergistic biomolecule-polymer conjugate of claim 1, wherein M is selected from the group of blood clotting factors consisting of clotting factors VII, VIIa, VIII and IX, and wherein the synergistic biomolecule-polymer conjugate is effective in prophylactic treatment for hemophilia.

20. The synergistic biomolecule-polymer conjugate of claim 1, wherein P.sub.1 and P.sub.2 are methoxy poly(ethylene glycol); wherein R is aspartic acid connected with said methoxy poly(ethylene glycol) having a structure represented by: ##STR00011## wherein the permanent linkage is selected from the group consisting of amide, carbamate, urea, imide, amine, thiocarbamate, thiourea, and dithiocarbamate; wherein the cleavable linkage is selected from the group consisting of carboxylic ester, carbonate, and carboxyl-imidazo; wherein X is an activated ester selected from the group consisting of N-hydroxysuccinimide ester, p-nitrophenyl ester, N-succinimidyl carbonate, p-nitrophenyl carbonate, and acylimidazo; or X is an aldehyde, maleimide, haloacetyl, carboxylic acid, hydroxyl, isocyanate, isothiocyanate, carbonyl, thiol, disulfide, amino, hydroxyl, hydrazide, or hydrazine group.

21. The synergistic biomolecule-polymer conjugate of claim 1, wherein P.sub.1 and P.sub.2 are methoxy poly(ethylene glycol); wherein R is glutamic acid connected with methoxy poly(ethylene glycol) having a structure represented by: ##STR00012## wherein the permanent linkage selected from the group consisting of amide, carbamate, urea, imide, amine, thiocarbamate, thiourea, and dithiocarbamate; wherein the cleavable linkage selected from the group consisting of carboxylic ester, carbonate, and carboxyl-imidazo; wherein X is an activated ester selected from the group consisting of N-hydroxysuccinimide ester, p-nitrophenyl ester, N-succinimidyl carbonate, p-nitrophenyl carbonate, and acylimidazo; or X is an aldehyde, maleimide, haloacetyl, carboxylic acid, hydroxyl, isocyanate, isothiocyanate, carbonyl, thiol, disulfide, amino, hydroxyl, hydrazide, or hydrazine group.

22. The synergistic biomolecule-polymer conjugate of claim 1, wherein the plasma cleavage provides controlled release of the biomolecule.

23. The synergistic biomolecule-polymer conjugate of claim 1, wherein the biologically active cleavage products are as active as, or more active than said synergistic biomolecule-polymer conjugate.

24. A method of treating hepatitis C, hepatitis B, hairy-cell leukemia, non-Hodgkin's lymphoma, malignant melanoma, or chronic myelogenous leukemia, comprising administering to a subject in need thereof an effective amount of the synergistic interferon .alpha.-30kPEG (10k mPEG carbamate, 20k mPEG ester) .epsilon.-Suberate conjugate of claim 16.

25. A method of treating hepatitis C, hepatitis B, hairy-cell leukemia, non-Hodgkin's lymphoma, malignant melanoma, or chronic myelogenous leukemia, comprising administering to a subject in need thereof an effective amount of the synergistic interferon .alpha.-30kPEG (10k mPEG carbamate, 20k mPEG ester) .epsilon.-Suberate conjugate of claim 17.

Details for Patent 9,364,553

Applicant Tradename Biologic Ingredient Dosage Form BLA Approval Date Patent No. Expiredate
Kadmon Pharmaceuticals Llc INFERGEN interferon alfacon-1 Injection 103663 10/06/1997 ⤷  Try a Trial 2026-05-24
Horizon Therapeutics Ireland Dac ACTIMMUNE interferon gamma-1b Injection 103836 02/25/1999 ⤷  Try a Trial 2026-05-24
>Applicant >Tradename >Biologic Ingredient >Dosage Form >BLA >Approval Date >Patent No. >Expiredate

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