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一种针对人血管生成素的单克隆抗体可抑制无胸腺小鼠的肿瘤生长。

A monoclonal antibody to human angiogenin suppresses tumor growth in athymic mice.

作者信息

Olson K A, French T C, Vallee B L, Fett J W

机构信息

Center for Biochemical and Biophysical Sciences and Medicine, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

Cancer Res. 1994 Sep 1;54(17):4576-9.

PMID:8062244
Abstract

Human angiogenin, a potent inducer of neovascularization, is secreted by HT-29 colon adenocarcinoma cells. microgram doses of a monoclonal antibody that neutralizes the in vitro and in vivo activities of angiogenin prevent or delay the appearance of s.c. HT-29 tumors in athymic mice in a statistically significant, dose-dependent manner. The antibody is not cytotoxic to tumor cells in vitro, which indicates that inhibition of tumor growth most likely occurs by neutralization of the activity of angiogenin in vivo and further implies a critical role for angiogenin in the early development of HT-29 tumors. The results suggest a therapeutically useful approach to the treatment of angiogenin-dependent malignancy.

摘要

人血管生成素是一种有效的新血管形成诱导剂,由HT - 29结肠腺癌细胞分泌。微克剂量的一种单克隆抗体可中和血管生成素的体外和体内活性,以具有统计学意义的剂量依赖性方式预防或延迟无胸腺小鼠皮下HT - 29肿瘤的出现。该抗体在体外对肿瘤细胞无细胞毒性,这表明肿瘤生长的抑制很可能是通过在体内中和血管生成素的活性而发生的,进一步暗示血管生成素在HT - 29肿瘤的早期发展中起关键作用。这些结果提示了一种治疗血管生成素依赖性恶性肿瘤的有用治疗方法。

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