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CIN85是一种与Cbl相互作用的蛋白,是AMAP1介导的乳腺癌侵袭机制的一个组成部分。

CIN85, a Cbl-interacting protein, is a component of AMAP1-mediated breast cancer invasion machinery.

作者信息

Nam Jin-Min, Onodera Yasuhito, Mazaki Yuichi, Miyoshi Hiroyuki, Hashimoto Shigeru, Sabe Hisataka

机构信息

Department of Molecular Biology, Osaka Bioscience Institute, Suita, Osaka, Japan.

出版信息

EMBO J. 2007 Feb 7;26(3):647-56. doi: 10.1038/sj.emboj.7601534. Epub 2007 Jan 25.

DOI:10.1038/sj.emboj.7601534
PMID:17255943
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1794391/
Abstract

Expression of AMAP1 correlates well with the invasive phenotypes and malignancy of human primary breast carcinomas. AMAP1 recruits its binding proteins, such as cortactin and paxillin, to sites of Arf6 activation to form invadopodia. A mouse ortholog of AMAP1, ASAP1, is known to bind to CIN85, a binding partner of an E3 ligase, Cbl. Here, we found that CIN85 colocalizes with AMAP1 at invadopodia, and binding of AMAP1 with CIN85 is important for the invasive activities of breast cancer cells, including MDA-MB-231. siRNA-mediated silencing of CIN85, as well as Cbl, also inhibited the invasion. We moreover found that AMAP1 is monoubiquitinated, rather than polyubiquitinated, by virtue of Cbl and provide evidence that the ability of AMAP1 to be monoubiquitinated is important for its involvement in invasion. Our results indicate that CIN85, as well as Cbl, which is a well-known suppressor of growth factor receptor signaling, can be positively involved in tumor invasion, and suggest that a complex epigenetic process is involved in AMAP1 function in breast cancer cell invasion.

摘要

AMAP1的表达与人类原发性乳腺癌的侵袭表型和恶性程度密切相关。AMAP1将其结合蛋白,如皮层肌动蛋白和桩蛋白,募集到Arf6激活位点以形成侵袭性伪足。已知AMAP1的小鼠直系同源物ASAP1与E3连接酶Cbl的结合伴侣CIN85结合。在这里,我们发现CIN85与AMAP1在侵袭性伪足处共定位,并且AMAP1与CIN85的结合对于包括MDA-MB-231在内的乳腺癌细胞的侵袭活性很重要。siRNA介导的CIN85以及Cbl的沉默也抑制了侵袭。我们还发现,AMAP1通过Cbl发生单泛素化而非多泛素化,并提供证据表明AMAP1发生单泛素化的能力对其参与侵袭很重要。我们的结果表明,CIN85以及作为生长因子受体信号传导的著名抑制剂的Cbl可以积极参与肿瘤侵袭,并表明复杂的表观遗传过程参与了AMAP1在乳腺癌细胞侵袭中的功能。

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