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内皮抑素:酵母生产、突变体及在肾细胞癌中的抗肿瘤作用

Endostatin: yeast production, mutants, and antitumor effect in renal cell carcinoma.

作者信息

Dhanabal M, Ramchandran R, Volk R, Stillman I E, Lombardo M, Iruela-Arispe M L, Simons M, Sukhatme V P

机构信息

Renal Division, Beth Israel Deaconess Medical Center and Harvard Medical School, Boston, Massachusetts 02215, USA.

出版信息

Cancer Res. 1999 Jan 1;59(1):189-97.

PMID:9892206
Abstract

Endostatin is a Mr 20,000 COOH-terminal fragment of collagen XVIII that inhibits the growth of several primary tumors. We report here the cloning and expression of mouse endostatin in both prokaryotic and eukaryotic expression systems. Soluble recombinant protein expressed in yeast (15-20 mg/L) inhibited the proliferation and migration of endothelial cells in response to stimulation by basic fibroblast growth factor. A rabbit polyclonal antibody was raised that showed positive immunoreactivity to the recombinant protein expressed from both systems. Importantly, the biological activity of the mouse recombinant protein could be neutralized by this antiserum in both endothelial proliferation and chorioallantoic membrane assays. Systemic administration of endostatin at 10 mg/kg suppressed the growth of renal cell cancer in a nude mouse model. The inhibition of tumor growth with soluble yeast-produced protein was comparable to that obtained with non-refolded precipitated protein expressed from bacteria. In addition, two closely related COOH-terminal deletion mutants of endostatin were also tested and showed strikingly differing activity. Collectively, these findings demonstrate the expression of a biologically active form of mouse endostatin in yeast, define a role for the molecule in inhibiting endothelial cell migration, extend its antitumor effects to renal cell carcinoma, and provide a formal proof (via the neutralizing antiserum experiments and the mutant data) that endostatin (and not a possible contaminant) acts as an antiangiogenic agent. Finally, the high level expression of mouse endostatin in yeast serves as an endotoxin free, soluble source of protein for fundamental studies on the mechanisms of tumor growth suppression by angiogenesis inhibitors.

摘要

内皮抑素是胶原蛋白XVIII的一个分子量为20,000的羧基末端片段,可抑制多种原发性肿瘤的生长。我们在此报告小鼠内皮抑素在原核和真核表达系统中的克隆与表达。酵母中表达的可溶性重组蛋白(15 - 20 mg/L)可抑制碱性成纤维细胞生长因子刺激下内皮细胞的增殖和迁移。制备了一种兔多克隆抗体,该抗体对两个系统中表达的重组蛋白均显示出阳性免疫反应性。重要的是,在内皮细胞增殖和绒毛尿囊膜试验中,该抗血清均可中和小鼠重组蛋白的生物活性。在裸鼠模型中,以10 mg/kg的剂量全身给予内皮抑素可抑制肾细胞癌的生长。可溶性酵母产生的蛋白对肿瘤生长的抑制作用与细菌表达的未重折叠沉淀蛋白相当。此外,还测试了两种紧密相关的内皮抑素羧基末端缺失突变体,其活性表现出显著差异。总体而言,这些发现证明了具有生物活性形式的小鼠内皮抑素在酵母中的表达,确定了该分子在抑制内皮细胞迁移中的作用,将其抗肿瘤作用扩展至肾细胞癌,并通过中和抗血清实验和突变体数据提供了正式证据,证明内皮抑素(而非可能的污染物)作为一种抗血管生成剂发挥作用。最后,小鼠内皮抑素在酵母中的高水平表达为研究血管生成抑制剂抑制肿瘤生长机制的基础研究提供了一种无内毒素的可溶性蛋白来源。

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