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α3β1 整合素调节三维环境中癌细胞中 CD151 复合物的组装和膜动态。

α3β1 integrins regulate CD151 complex assembly and membrane dynamics in carcinoma cells within 3D environments.

机构信息

Randall Division of Cell and Molecular Biophysics, King's College London, New Hunts House, Guys Campus, London, UK.

出版信息

Oncogene. 2013 Aug 22;32(34):3965-79. doi: 10.1038/onc.2012.415. Epub 2012 Sep 17.

DOI:10.1038/onc.2012.415
PMID:22986527
Abstract

Integrins are extracellular matrix (ECM) receptors that are key players in the regulation of tumour cell invasion. The laminin-binding integrin α3β1 has previously been shown to regulate adhesion and migration of carcinoma cells in part through co-operative signalling with the tetraspanin family of transmembrane proteins. However, the spatial and temporal regulation of crosstalk between these families of transmembrane proteins in intact cells remains poorly understood. Here we have used fluorescence resonance energy transfer (FRET) to demonstrate for the first time that α3β1 and the tetraspanin CD151 directly associate at the front and retracting rear of polarised migrating breast carcinoma cells in both two-dimentional (2D) and three-dimentional (3D)matrices. Furthermore, localised α3β1-CD151 binding correlates with lower CD151 homodimerisation in cells migrating on laminin or within matrigel. Loss of α3β1 integrin leads to increased CD151 homodimer formation, increased activation of Rho GTPase, loss of cell polarity and decreased invasion in 3D ECM. As a result, α3-silenced cells show decreased actin-based membrane protrusion and retraction in both 2D and 3D environments. These data demonstrate that associations between α3β1 and CD151 occur dynamically within discrete subcellular compartments and act to establish local GTPase signalling to promote tumour cell invasion. These novel findings shed light on the complex crosstalk and switching between receptor complexes in response to different extracellular cues during cell invasion in 3D environments.

摘要

整合素是细胞外基质 (ECM) 的受体,是调节肿瘤细胞侵袭的关键因素。先前已经表明,层粘连蛋白结合的整合素 α3β1 通过与跨膜蛋白四旋蛋白家族的合作信号传导,部分调节癌细胞的粘附和迁移。然而,完整细胞中这些跨膜蛋白家族之间串扰的时空调节仍然知之甚少。在这里,我们首次使用荧光共振能量转移 (FRET) 证明,α3β1 和四旋蛋白 CD151 在前部和缩回的极性迁移的乳腺癌细胞的前部和缩回的后部直接相关,无论是在二维 (2D) 和三维 (3D) 基质中。此外,局部 α3β1-CD151 结合与在层粘连蛋白或基质胶上迁移的细胞中 CD151 同源二聚体形成的减少相关。α3β1 整合素的缺失导致 Rho GTPase 的激活增加,细胞极性丧失,在 3D ECM 中的侵袭性降低。结果,α3 沉默的细胞在 2D 和 3D 环境中均显示出 actin 基膜突和缩回的减少。这些数据表明,α3β1 和 CD151 之间的关联在离散的细胞内隔室中动态发生,并作用于建立局部 GTPase 信号传导,以促进肿瘤细胞侵袭。这些新发现揭示了在三维环境中细胞侵袭过程中,不同细胞外线索对受体复合物的复杂串扰和切换。

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