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Direct interaction of focal adhesion kinase (FAK) with Met is required for FAK to promote hepatocyte growth factor-induced cell invasion

机译：FaK需要粘着斑激酶（FaK）与met的直接相互作用以促进肝细胞生长因子诱导的细胞侵袭

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Focal adhesion kinase (FAK) has been implicated to be a point of convergence of integrin and growth factor signaling pathways. Here we report that FAK directly interacts with the hepatocyte growth factor receptor c-Met. Phosphorylation of c-Met at Tyr-1349 and, to a lesser extent, Tyr-1356 is required for its interaction with the band 4.1 and ezrin/radixin/moesin homology domain (FERM domain) of FAK. The F2 subdomain of the FAK FERM domain alone is sufficient for Met binding, in which a patch of basic residues ((216)KAKTLRK(222)) are critical for the interaction. Met-FAK interaction leads to FAK activation and subsequent contribution to hepatocyte growth factor-induced cell motility and cell invasion. Our results provide evidence that constitutive Met-FAK interaction may be a critical determinant for tumor cells to acquire invasive potential.

机译：局灶性粘附激酶（FAK）已被认为是整合素和生长因子信号通路的汇合点。在这里，我们报道FAK直接与肝细胞生长因子受体c-Met相互作用。 c-Met在Tyr-1349和较小程度上需要Tyr-1356的磷酸化是其与FAK的4.1带和ezrin / radixin / moesin同源结构域（FERM域）相互作用所必需的。单独的FAK FERM域的F2子域足以满足Met结合，其中碱性残基的补丁（（216）KAKTLRK（222））对于相互作用至关重要。 Met-FAK相互作用导致FAK活化并随后对肝细胞生长因子诱导的细胞运动和细胞侵袭做出贡献。我们的结果提供了证据，表明本构Met-FAK相互作用可能是决定肿瘤细胞获得侵袭潜能的关键因素。

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Chen, S.Y.; Chen, H.C.; 陳鴻震;
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年度 2014
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1. Direct Interaction of Focal Adhesion Kinase (FAK) with Met Is Required for FAK To Promote Hepatocyte Growth Factor-Induced Cell Invasion [J] . Shu-Yi Chen, Hong-Chen Chen Molecular and Cellular Biology . 2006,第13期

机译：黏着斑激酶（FAK）与蛋氨酸的直接相互作用是FAK促进肝细胞生长因子诱导的细胞侵袭所必需的
2. Grb2 Promotes Integrin-Induced Focal Adhesion Kinase (FAK) Autophosphorylation and Directs the Phosphorylation of Protein Tyrosine Phosphatase α by the Src-FAK Kinase Complex [J] . Suzanne Y. S. Cheng, Guobin Sun, David D. Schlaepfer, Molecular and Cellular Biology . 2014,第3期

机译：Grb2促进整合素诱导的局灶性粘附激酶（FAK）自磷酸化，并通过Src-FAK激酶复合体指导蛋白酪氨酸磷酸酶α的磷酸化。
3. Identification of sequences required for the efficient localization of the focal adhesion kinase, pp125FAK, to cellular focal adhesions. [J] . J D Hildebrand, M D Schaller, J T Parsons Journal of cell biology . 1993,第4期

机译：鉴定将粘着斑激酶pp125FAK有效定位到细胞粘着斑所需的序列。
4. Establishment of Stable Focal adhesion kinase(FAK) RNA Interference Cell Line [C] . Lan Yan, Tang Bo, Hua Zi-Chun International Symposium on Medical and Pharmaceutical Biotechnology(医药生物技术国际研讨会) . 2009

机译：稳定的黏着斑激酶（FAK）RNA干扰细胞系的建立
5. Necroptosis and Its Interactions with Focal Adhesion Kinase (FAK) and Extracellular Receptor Kinase (ERK1/2) Following Optic Nerve Injury [D] . D'Onofrio, Philippe Matteo. 2019

机译：椎间盘神经损伤后骨髓凋亡及其与局灶性粘附激酶（FAK）和细胞外受体激酶（ERK1 / 2）的相互作用
6. Direct Interaction of Focal Adhesion Kinase (FAK) with Met Is Required for FAK To Promote Hepatocyte Growth Factor-Induced Cell Invasion [O] . Shu-Yi Chen, Hong-Chen Chen 2006

机译：黏着斑激酶（FAK）与蛋氨酸的直接相互作用是FAK促进肝细胞生长因子诱导的细胞侵袭所必需的
7. Direct Interaction of Focal Adhesion Kinase (FAK) with Met Is Required for FAK To Promote Hepatocyte Growth Factor-Induced Cell Invasion† [O] . Chen, Shu-Yi, Chen, Hong-Chen 2006

机译：黏着斑激酶（FAK）与Met的直接相互作用是FAK促进肝细胞生长因子诱导的细胞侵袭所必需的†

Direct interaction of focal adhesion kinase (FAK) with Met is required for FAK to promote hepatocyte growth factor-induced cell invasion

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