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VEGF 165 b, an antiangiogenic VEGF-A isoform, binds and inhibits bevacizumab treatment in experimental colorectal carcinoma: balance of pro- and antiangiogenic VEGF-A isoforms has implications for therapy.

机译：VEGF 165 b是一种抗血管生成的VEGF-A亚型，可结合并抑制贝伐单抗在实验性结直肠癌中的治疗：促血管生成和抗血管生成的VEGF-A亚型的平衡对治疗具有重要意义。

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Bevacizumab, an anti-vascular endothelial growth factor (VEGF-A) antibody, is used in metastatic colorectal carcinoma (CRC) treatment, but responses are unpredictable. Vascular endothelial growth factor is alternatively spliced to form proangiogenic VEGF(165) and antiangiogenic VEGF(165)b. Using isoform-specific enzyme-linked immunosorbent assay and quantitative polymerase chain reaction, we found that over 90% of the VEGF in normal colonic tissue was VEGF(xxx)b, but there was a variable upregulation of VEGF(xxx) and downregulation of VEGF(xxx)b in paired human CRC samples. Furthermore, cultured colonic adenoma cells expressed predominantly VEGF(xxx)b, whereas colonic carcinoma cells expressed predominantly VEGF(xxx). However, adenoma cells exposed to hypoxia switched their expression from predominantly VEGF(xxx)b to predominantly VEGF(xxx). VEGF(165)b overexpression in LS174t colon cancer cells inhibited colon carcinoma growth in mouse xenograft models. Western blotting and surface plasmon resonance showed that VEGF(165)b bound to bevacizumab with similar affinity as VEGF(165). However, although bevacizumab effectively inhibited the rapid growth of colon carcinomas expressing VEGF(165), it did not affect the slower growth of tumours from colonic carcinoma cells expressing VEGF(165)b. Both bevacizumab and anti-VEGF(165)b-specific antibodies were cytotoxic to colonic epithelial cells, but less so to colonic carcinoma cells. These results show that the balance of antiangiogenic to proangiogenic isoforms switches to a variable extent in CRC, regulates tumour growth rates and affects the sensitivity of tumours to bevacizumab by competitive binding. Together with the identification of an autocrine cytoprotective role for VEGF(165)b in colonic epithelial cells, these results indicate that bevacizumab treatment of human CRC may depend upon this balance of VEGF isoforms.

机译：贝伐单抗是一种抗血管内皮生长因子（VEGF-A）抗体，用于转移性结直肠癌（CRC）治疗，但反应是不可预测的。将血管内皮生长因子剪接形成促血管生成VEGF（165）和抗血管生成VEGF（165）b。使用同工型特异性酶联免疫吸附试验和定量聚合酶链反应，我们发现正常结肠组织中90％以上的VEGF是VEGF（xxx）b，但VEGF（xxx）的上调和VEGF的下调各不相同（xxx）b在配对的人类CRC样本中。此外，培养的结肠腺瘤细胞主要表达VEGF（xxx）b，而结肠癌细胞主要表达VEGF（xxx）。然而，暴露于低氧状态的腺瘤细胞将其表达从主要的VEGF（xxx）b切换到主要的VEGF（xxx）。 LS174t结肠癌细胞中的VEGF（165）b过表达抑制了小鼠异种移植模型中结肠癌的生长。 Western印迹和表面等离振子共振表明VEGF（165）b以与VEGF（165）相似的亲和力结合贝伐单抗。但是，尽管贝伐单抗有效抑制表达VEGF（165）b的结肠癌的快速生长，但它不影响表达VEGF（165）b的结肠癌细胞的肿瘤的缓慢生长。贝伐单抗和抗VEGF（165）b特异性抗体对结肠上皮细胞均具有细胞毒性，但对结肠癌细胞则无细胞毒性。这些结果表明，抗血管生成同促血管生成同种型的平衡在CRC中变化到不同的程度，调节肿瘤的生长速率，并通过竞争性结合影响肿瘤对贝伐单抗的敏感性。这些结果与对结肠上皮细胞中VEGF（165）b的自分泌细胞保护作用的鉴定一起，表明了贝伐单抗对人CRC的治疗可能取决于VEGF同工型的这种平衡。

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Varey, AH; Rennel, ES; Qiu, Y; Bevan, HS; Perrin, RM; Raffy, S; Dixon, AR; Paraskeva, C; Zaccheo, O; Hassan, AB; Harper, SJ; Bates, DO;
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年度 2008
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1. VEGF165b, an antiangiogenic VEGF-A isoform, binds and inhibits bevacizumab treatment in experimental colorectal carcinoma: balance of pro- and antiangiogenic VEGF-A isoforms has implications for therapy [J] . A H R Varey, E S Rennel, Y Qiu, British Journal of Cancer . 2008,第8期

机译：VEGF165b，一种抗血管生成的VEGF-A亚型，结合并抑制贝伐单抗在实验性结直肠癌中的治疗：促血管生成素和抗血管生成的VEGF-A亚型的平衡对治疗具有重要意义
2. VEGF-A isoforms program differential VEGFR2 signal transduction, trafficking and proteolysis VEGF-A isoforms program differential VEGFR2 signal transduction, trafficking and proteolysis VEGF-A isoforms program differential VEGFR2 signal transduction, trafficking and proteolysis [J] . Shervanthi Homer-Vanniasinkam, Mark T. Kearney, Michael A. Harrison, Biology Open . 2016,第5期

机译：VEGF-A同工型程序差异VEGFR2信号转导，运输和蛋白水解VEGF-A同工型程序差异VEGFR2信号转导，运输和蛋白水解VEGF-A同工型程序差异VEGFR2信号转导，运输和蛋白质水解
3. VEGF-A isoform-specific regulation of calcium ion flux, transcriptional activation and endothelial cell migration VEGF-A isoform-specific regulation of calcium ion flux, transcriptional activation and endothelial cell migration VEGF-A isoform-specific regulation of calcium ion flux, transcriptional activation and endothelial cell migration [J] . Alexander F. Bruns, Stephen B. Wheatcroft, Gareth W. Fearnley, Biology Open . 2015,第6期

机译：VEGF-A亚型特异性调节钙离子通量，转录激活和内皮细胞迁移VEGF-A亚型特异性调节钙离子通量，转录激活和内皮细胞迁移VEGF-A亚型特异性调节钙离子通量，转录激活和内皮细胞迁移
4. Evaluation of rVEGF164b, a novel antiangiogenic VEGF-A isoform, in inflammatory bowel disease: Implications on VEGF-A regulation and potental therapeutic options. [D] . Cromer, Walter. 2011

机译：炎性肠病中新型抗血管生成VEGF-A亚型rVEGF164b的评估：对VEGF-A调节和潜在治疗选择的影响。
5. VEGF165b an antiangiogenic VEGF-A isoform binds and inhibits bevacizumab treatment in experimental colorectal carcinoma: balance of pro- and antiangiogenic VEGF-A isoforms has implications for therapy [O] . A H R Varey, E S Rennel, Y Qiu, 2008

机译：VEGF165b是一种抗血管生成的VEGF-A亚型可结合并抑制贝伐单抗在实验性结直肠癌中的治疗：前血管生成和抗血管生成的VEGF-A亚型的平衡对治疗具有重要意义
6. VEGF165b, an antiangiogenic VEGF-A isoform, binds and inhibits bevacizumab treatment in experimental colorectal carcinoma: balance of pro- and antiangiogenic VEGF-A isoforms has implications for therapy [O] . Varey, A H R, Rennel, E S, Qiu, Y, 2008

机译：VEGF165b是一种抗血管生成的VEGF-A亚型，可结合并抑制贝伐单抗在实验性结直肠癌中的治疗：前血管生成和抗血管生成的VEGF-A亚型的平衡对治疗具有重要意义

VEGF 165 b, an antiangiogenic VEGF-A isoform, binds and inhibits bevacizumab treatment in experimental colorectal carcinoma: balance of pro- and antiangiogenic VEGF-A isoforms has implications for therapy.

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