US2010028256A1PendingUtilityA1

Differential gene expression in physiological and pathological angiogenesis

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Assignee: ST CROIX BRADPriority: Nov 9, 2006Filed: Jun 28, 2007Published: Feb 4, 2010
Est. expiryNov 9, 2026(~0.3 yrs left)· nominal 20-yr term from priority
A61P 35/00C12Q 1/6886A61K 45/06C12Q 2600/16C12N 15/1072A61K 39/39558C12Q 2600/158A61P 35/04G01N 33/6893G01N 33/57595G01N 33/57557G01N 33/5759G01N 33/575
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Claims

Abstract

Methods of inhibiting pathological angiogenesis in a subject are disclosed. In particular examples, the method includes administering a therapeutically effective amount of a composition to a subject wherein the composition includes a specific binding agent that preferentially binds to one or more pathological angiogenesis marker proteins including Vscp, CD276, ETSvg4 (Pea3), CD137(4-1BB), MiRP2, Ubiquitin D (Fat10), Doppel (prion-PLP), Apelin, Plgf, Ptprn (IA-2), CD109, Ankylosis, and collagen VIIIα1. In additional examples, methods to deliver a therapeutic agent to a brain or liver endothelial cell are also disclosed.

Claims

exact text as granted — not AI-modified
1 . A method of inhibiting pathological angiogenesis in a subject, comprising:
 administering to the subject a therapeutically effective amount of a composition, wherein the composition comprises a specific binding agent that preferentially binds to one or more pathological angiogenesis marker proteins comprising Vscp, CD276, ETSvg4 (Pea3), CD137(4-1BB), MiRP2, Ubiquitin D (Fat10), Doppel (prion-PLP), Apelin, Plgf, Ptprn (IA-2), CD109, Ankylosis, and collagen VIIIα1, thereby inhibiting pathological angiogenesis in the subject.   
     
     
         2 . The method of  claim 1 , wherein the one or more pathological angiogenesis marker proteins is Vscp, CD276, MiRP2, Ptprn (IA-2), or ankylosis. 
     
     
         3 . The method of  claim 1 , wherein the specific binding agent significantly reduces the biological activity of the one or more pathological angiogenesis marker proteins. 
     
     
         4 . The method of  claim 1 , wherein the specific binding agent further comprises a therapeutic molecule. 
     
     
         5 . The method of  claim 4 , wherein the specific binding agent is an antibody to one or more of the pathological angiogenesis marker proteins conjugated to the therapeutic molecule, and wherein the therapeutic molecule comprises a cytotoxin, chemotherapeutic reagent, radionucleotide, or combination thereof. 
     
     
         6 . (canceled) 
     
     
         7 . The method of  claim 1 , wherein inhibiting pathological angiogenesis treats a tumor, and the composition includes a specific binding agent that preferentially binds to one or more of: Vscp, CD276, ETSvg4 (Pea3), MiRP2, Ubiquitin D (Fat10), Doppel (prion-PLP), Apelin, Plgf, Ptprn (IA-2), CD109, Ankylosis, or collagen VIII. 
     
     
         8 . The method of  claim 7 , wherein the specific binding agent is an antibody to one or more of: Vscp, CD276, ETSvg4 (Pea3), MiRP2, Ubiquitin D (Fat10), Doppel (prion-PLP), Apelin, Plgf, Ptprn (IA-2), CD109, Ankylosis, or collagen VIII conjugated to a therapeutic molecule comprising a cytotoxin, chemotherapeutic reagent, radionucleotide, or combination thereof. 
     
     
         9 . (canceled) 
     
     
         10 . The method of  claim 8 , wherein the composition includes a specific binding agent that preferentially binds to one or more of Vscp, CD276, MiRP2, Ptprn (IA-2), or ankylosis. 
     
     
         11 . A method of screening for pathological angiogenesis in a subject, comprising:
 detecting at least one expression product comprising one or more of: Vscp, CD276, ETSvg4 (Pea3), CD137(4-1BB), MiRP2, Ubiquitin D (Fat10), Doppel (prion-PLP), Apelin, Plgf, Ptprn (IA-2), CD109, Ankylosis, and collagen VIII, 1, in a sample obtained from the subject,   wherein detection of the at least one expression product indicates pathological angiogenesis in the subject.   
     
     
         12 . The method of  claim 11 , wherein the at least one expression product is Vscp, CD276, MiRP2, Ptprn (IA-2), or ankylosis. 
     
     
         13 . The method of  claim 11 , wherein detection of the at least one expression product indicates the presence of a tumor. 
     
     
         14 . The method of  claim 13 , wherein the expression product is RNA or a protein. 
     
     
         15 .- 16 . (canceled) 
     
     
         17 . The method of  claim 13 , wherein the tumor is a cancer of the colon, liver, lung, or breast. 
     
     
         18 . (canceled) 
     
     
         19 . The method of  claim 11 , wherein the detecting the expression product is performed using serial analysis gene expression (SAGE), polymerase chain reaction, Western blot, or immunoassay. 
     
     
         20 . (canceled) 
     
     
         21 . A method of delivering a therapeutic agent to brain endothelial cells, comprising:
 administering a therapeutically effective amount of a composition, wherein the composition comprises a therapeutic agent and a binding agent that preferentially binds to one or more brain endothelial marker proteins comprising Glucose transporter GLUT-1, Organic anion transporter 2, Pleiotrophin, ATPase class V, type 10A, Peptidoglycan recognition protein 1, Organic anion transporter 14, Forkhead box Q1, Organic anion transporter 3, SN2 (Solute carrier family 38, member 5), Inter-alpha (globulin) inhibitor H5, Solute carrier 38 member 3, Zinc finger protein of the cerebellum 2, Testican-2,3-HMG-CoA synthase 2, Progestin and adipoQ receptor family member V, APC down-regulated 1 Drapc1, GDPD phosphodiesterase family Accession No. NM — 001042671, putative transmembrane protein Accession No. NM — 029001, DES2 lipid desaturase/C4-hyroxylase, Kelch repeat and BTB (POZ) domain, Lipolysis stimulated receptor, Glutathione S-transferase alpha 4, TNF receptor superfamily member 19, T-box 1 or putative secreted protein Accession No. XM — 620023, thereby evoking a therapeutic response in the brain endothelial cells or the cells underlying the brain endothelial cells.   
     
     
         22 . The method of  claim 21 , wherein the specific binding agent is an antibody to one or more of the brain endothelial markers, wherein the antibody is conjugated to the therapeutic agent and wherein the therapeutic agent comprises a cytotoxin, chemotherapeutic reagent, radionucleotide, or combination thereof. 
     
     
         23 . (canceled) 
     
     
         24 . The method of  claim 21 , wherein the brain endothelial marker protein comprises GDPD phosphodiesterase family Accession No. NM — 001042671, Forkhead box Q1 (FOXQ1), putative transmembrane protein Accession No. NM — 029001, Kelch repeat and BTB (POZ) domain, Progestin and adipoQ receptor family member V, or putative secreted protein Accession No. XM — 620023. 
     
     
         25 . A method of delivering a therapeutic agent to liver endothelial cells, comprising:
 administering a therapeutically effective amount of a composition, wherein the composition comprises a therapeutic agent and a binding agent that specifically binds to one or more liver endothelial marker proteins comprising deoxyribonuclease 1-like 3, LZP oncoprotein induced transcript 3, putative transmembrane protein Accession No. NM — 023438, CD32 15, putative G-protein coupled receptor NM — 033616, C-type lectin-like receptor 2, C-type lectin domain family 4 member g 16, Plexin C1, Wnt9B, Accession No. AK144596, GATA-binding protein 4, MBL-associated serine protease-3, Renin binding protein, putative transmembrane protein Accession No. NM — 144830, or Retinoic acid receptor, beta, thereby evoking a therapeutic response in the liver endothelial cells.   
     
     
         26 . The method of  claim 25 , wherein the specific binding agent is an antibody, wherein the antibody is conjugated to the therapeutic agent, and wherein the therapeutic agent comprises a cytotoxin, chemotherapeutic reagent, radionucleotide, or combination thereof. 
     
     
         27 . (canceled) 
     
     
         28 . The method of  claim 25 , wherein the liver endothelial marker protein comprises oncoprotein induced transcript 3, putative transmembrane protein Accession No. NM — 023438, putative G-protein coupled receptor NM — 033616, Plexin C1, MBL-associated serine protease-3, Accession No. AK144596, or putative transmembrane protein Accession No. NM — 144830.

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