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VEGF抗體說明書

2012-5-7  閱讀(11112)

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VEGF單克隆抗體    100ul    2000元

VEGF,即vascular endothelial growth factor,也稱VEGFA或VEGF-A,中文名為血管內(nèi)皮生長因子,是一種可以強烈誘導血管生長的因子,在血管過程中起重要作用。腫瘤細胞在低氧(hypoxia)情況下可以分泌VEGF。VEGF的7種isoform是VEGF mRNA可變剪接(alternative splicing)的結果。zui常見的VEGF的isoform包括VEGF 121,VEGF 165,VEGF 189(相當于VEGF f、VEGF d和VEGF b)。VEGF的表達水平和腫瘤內(nèi)的血管生長情況呈正相關,并且和腫瘤的轉移風險呈正相關。VEGF可以促進內(nèi)皮細胞增殖,促進細胞遷移,并抑制細胞凋亡。抑制VEGF信號轉導可以抑制多種腫瘤的發(fā)生和發(fā)展。VEGF可以形成同源二聚體,可以和其受體VEGFR1/Flt-1和VEGFR2/Kdr,以及heparan sulfate和肝素相結合。VEGF-165和VEGF-145可以和Neuropilin-1相結合。
 

 

 
 


BACKGROUND
The onset of angiogenesis is believed to be an early event in tumorigenesis and may facilitate tumor progression and metastasis. Several growth factors with angiogenic activity have been described. These include fibroblast growth factors (FGFs), plaet derived growth factor (PDGF) and vascular endothelial growth factor (VEGF). VEGF is a dimeric glycoprotein with structural homology to PDGF. Several variants of VEGF have been described that arise by alter­native mRNA splicing. It has been speculated that VEGF may function as a tumor angiogenesis factor in vivo because the expression pattern of VEGF is consistent with a role in embryonic angiogenesis. VEGF mRNA is formed in some primary tumors, VEGF is produced by tumor cell lines in vitro and VEGF mitogenic activity appears to be restricted to endothelial cells. A member of the PDGF receptor family, Flt, has been identified as a high-affinity receptor for VEGF.
 
 
REFERENCES
1. Folkman, J., et al. 1989. Induction of angiogenesis during the transition from hyperplasia to neoplasia. Nature 339: 58-61.
2. Conn, G., et al. 1990. Purification of a glycoprotein vascular endothelial cell mitogen from a rat glioma-derived cell line. Proc. Natl. Acad. Sci. USA
87: 1323-1327.
3. Tischer, E., et al. 1991. The human gene for vascular endothelial growth factor. Multiple protein forms are encoded through alternative exon splicing.
J. Biol. Chem. 266: 11947-11954.
4. Ferrara, N., et al. 1991. The vascular endothelial growth factor family of polypeptides. J. Cell. Biochem. 47: 211-218.
5. Breier, G., et al. 1992. Expression of vascular endothelial growth factor during embryonic angiogenesis and endothelial cell differentiation. Development 114: 521-532.
6. Berse, B., et al. 1992. Vascular permeability factor (vascular endothelial growth factor) gene is expressed differentially in normal tissues, macro-phages and tumors. Mol. Biol. Cell 3: 211-220.
7. Plate, K.H., et al. 1992. Vascular endothelial growth factor is a potential tumour angiogenesis factor in human gliomas in vivo. Nature 359: 845-848.
 
 
 
CHROMOSOMAL LOCATION
Genetic locus: VEGFA (human) mapping to 6p21.1; Vegfa (mouse) mapping to 17 C.
 
 
SOURCE
VEGF (VG-1) is a mouse monoclonal antibody raised against recombinant VEGF189 protein.
 
 
PRODUCT
Each vial contains 200 μg IgG1 in 1.0 ml of PBS with < 0.1% sodium azide and 0.1% gelatin.
 
 
RESEARCH USE
For research use only, not for use in diagnostic procedures.
 
 
APPLICATIONS
VEGF (VG-1) is recommended for detection of the 189, 165 and 121 amino acid splice variants of VEGF of mouse, rat, human and dog origin by Western Blotting (starting dilution 1:200, dilution range 1:100-1:1000), immunoprecipi­tation [1-2 μg per 100-500 μg of total protein (1 ml of cell lysate)], immuno­fluorescence (starting dilution 1:50, dilution range 1:50-1:500) and immuno­histochemistry (including paraffin-embedded sections) (starting dilution 1:50, dilution range 1:50-1:500).
Suitable for use as control antibody for VEGF siRNA (h): sc-29520, VEGF siRNA (m): sc-36815, VEGF shRNA Plasmid (h): sc-29520-SH, VEGF shRNA Plasmid (m): sc-36815-SH, VEGF shRNA (h) Lentiviral Particles: sc-29520-V and VEGF shRNA (m) Lentiviral Particles: sc-36815-V.
Molecular Weight of VEGF: 15 kDa.
Molecular Weight of GST-tagged VEGF: 40 kDa.
 
 
DATA
AB 97 K ­65 K ­48 K ­
< VEGF fusion 31 K ­
protein
22 K ­
VEGF (VG-1): sc-53462. Western blot analysis of biologically active human recombinant VEGF (A) and mouse recombinant VEGF (B).
 
 
SELECT PRODUCT CITATIONS
1. Economou, M.A. 2008. Uveal melanoma and macular degeneration: molecular biology and potential therapeutic applications. Acta Ophthalmol.
86: 930-931.
1           Economou, M.A., et al. 2008. Inhibition of VEGF secretion and experimen­tal choroidal neovascularization by picropodophyllin (PPP), an inhibitor of the insulin-like growth factor-1 receptor. Acta Ophthalmol. 86 Thesis 4: 42-49.
2           Economou, M.A., et al. 2008. Inhibition of VEGF secretion and experimental choroidal neovascularization by picropodophyllin (PPP), an inhibitor of the Insulin-like growth factor-1 receptor. Invest. Ophthalmol. Vis. Sci. 49: 2620-2626.
3           Ma, J., et al. 2009. PTEN regulate angiogenesis through PI3K/Akt/VEGF signaling pathway in human pancreatic cancer cells. Mol. Cell. Biochem. E-Published.
 
 
 
STORAGE
Store at 4° C, **DO NOT FREEZE**. Stable for one year from the date of shipment. Non-hazardous. No MSDS required.
Santa Cruz Biotechnology, Inc. 1.800.457.3801 831.457.3800 831.457.3801 Europe +00800 4573 8000 49 6221 4503 0

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