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白细胞介素-6 受体通过上调卵巢癌细胞中甘露糖家族受体 LY75 增强对鼠大网膜的早期定植。

Interleukin-6 receptor enhances early colonization of the murine omentum by upregulation of a mannose family receptor, LY75, in ovarian tumor cells.

机构信息

Department of Cancer and Cell Biology, Vontz Center for Molecular Studies, University of Cincinnati, 3125 Eden Avenue, Cincinnati, OH 45267-0521, USA.

出版信息

Clin Exp Metastasis. 2011 Dec;28(8):887-97. doi: 10.1007/s10585-011-9420-x. Epub 2011 Sep 2.

Abstract

One of the earliest metastatic events in human ovarian cancer, tumor spread to the omentum, may be influenced by expression of interleukin 6 (IL6) and its cognate receptor (IL6Rα). Previous reports have shown that IL6 and IL6Rα expression is elevated in the serum and ascites of patients with ovarian cancer and that this can influence in vitro processes such as cell survival, proliferation and migration. In this study, overexpression of IL6Rα, and to a lesser extent IL6, enhanced tumor growth on the omentum. Moreover, adherence to plastic and to peritoneal extracellular matrix components was enhanced in tumor cells overexpressing IL6 or IL6Rα. Host production of IL6 and IL6Rα was also sufficient to influence tumor adherence to the omentum. Expression of LY75/CD205/DEC205, a collagen-binding mannose family receptor, was directly influenced by IL6Rα expression. Blocking LY75 with antibody reduced the adherence of tumor cells overexpressing IL6Rα to matrices in vitro and to the omentum. The association between IL6Rα expression and LY75 expression has not been previously reported, and the promotion of cellular adherence is a novel role for LY75. These studies indicate that overexpression of LY75 may be an additional mechanism by which IL6 signaling influences the progression of ovarian cancer, and suggests that blocking LY75 could be a valuable clinical strategy for reducing the early metastasis of ovarian cancer.

摘要

人类卵巢癌最早的转移事件之一,肿瘤扩散到网膜,可能受到白细胞介素 6 (IL6)及其同源受体 (IL6Rα)的表达影响。先前的报告表明,卵巢癌患者的血清和腹水中 IL6 和 IL6Rα 的表达升高,这可以影响体外过程,如细胞存活、增殖和迁移。在这项研究中,IL6Rα 的过表达,在较小程度上还有 IL6 的过表达,增强了肿瘤在网膜上的生长。此外,过表达 IL6 或 IL6Rα 的肿瘤细胞对塑料和腹膜细胞外基质成分的黏附性增强。宿主产生的 IL6 和 IL6Rα 也足以影响肿瘤对网膜的黏附。LY75/CD205/DEC205 的表达(一种胶原结合的甘露糖家族受体)直接受到 IL6Rα 表达的影响。用抗体阻断 LY75 减少了过表达 IL6Rα 的肿瘤细胞在体外和在网膜上与基质的黏附。IL6Rα 表达与 LY75 表达之间的关联以前没有报道过,而细胞黏附的促进是 LY75 的一个新作用。这些研究表明,LY75 的过表达可能是 IL6 信号影响卵巢癌进展的另一种机制,并表明阻断 LY75 可能是减少卵巢癌早期转移的有价值的临床策略。

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