首页> 美国卫生研究院文献>British Journal of Cancer >Selective toxicity of TGF-alpha-PE40 to EGFR-positive cell lines: selective protection of low EGFR-expressing cell lines by EGF.
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Selective toxicity of TGF-alpha-PE40 to EGFR-positive cell lines: selective protection of low EGFR-expressing cell lines by EGF.

机译:TGF-α-PE40对EGFR阳性细胞系的选择性毒性:EGF对低EGFR表达细胞系的选择性保护。

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摘要

The sensitivity of human breast and lung cancer cell lines to TGF-alpha-PE40, a novel chimeric recombinant cytotoxin composed of two independent domains, (i) TGF-alpha and (ii) a 40 kDa segment of the Pseudomonas exotoxin protein, PE-40, was investigated. Toxicity varied widely, correlated with epidermal growth factor receptor (EGFR) levels (P = 0.01) and was greatly reduced by EGF, indicating that binding of TGF-alpha-PE40 to EGFR is important in mediating toxicity. Cell lines expressing low EGFR levels were most highly protected by EGF, indicating that normal (low EGFR-expressing) tissue may be selectively protected by EGF in vivo. P-glycoprotein did not confer resistance to TGF-alpha-PE40, and toxicity was unaffected by multidrug resistance-modulating agents (cyclosporin A, tamoxifen, verapamil), indicating a role for TGF-alpha-PE40 in the clinical management of drug-resistant tumours.
机译:人乳腺癌和肺癌细胞系对TGF-alpha-PE40(一种由两个独立域组成的新型嵌合重组细胞毒素)的敏感性:(i)TGF-alpha和(ii)假单胞菌外毒素蛋白PE-40 kDa片段40,进行了调查。毒性变化很大,与表皮生长因子受体(EGFR)水平相关(P = 0.01),并且被EGF大大降低,表明TGF-α-PE40与EGFR的结合在介导毒性中很重要。表达低EGFR水平的细胞系受到EGF的保护程度最高,表明正常(低EGFR表达)组织可以在体内被EGF选择性保护。 P-糖蛋白不赋予对TGF-α-PE40的抗性,并且毒性不受多药抗性调节剂(环孢菌素A,他莫昔芬,维拉帕米)的影响,表明TGF-α-PE40在耐药性的临床管理中具有作用肿瘤。

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