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The three-way switch operation of Rac1/RhoA GTPase-based circuit controlling amoeboid-hybrid-mesenchymal transition

机译:基于Rac1 / RhoA GTPase的电路的三向开关操作控制了变形虫-混合-间充质过渡

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摘要

Metastatic carcinoma cells exhibit at least two different phenotypes of motility and invasion - amoeboid and mesenchymal. This plasticity poses a major clinical challenge for treating metastasis, while its underlying mechanisms remain enigmatic. Transitions between these phenotypes are mediated by the Rac1/RhoA circuit that responds to external signals such as HGF/SF via c-MET pathway. Using detailed modeling of GTPase-based regulation to study the Rac1/RhoA circuit's dynamics, we found that it can operate as a three-way switch. We propose to associate the circuit's three possible states to the amoeboid, mesenchymal and amoeboid/mesenchymal hybrid phenotype. In particular, we investigated the range of existence of, and the transition between, the three states (phenotypes) in response to Grb2 and Gab1 - two downstream adaptors of c-MET. The results help to explain the regulation of metastatic cells by c-MET pathway and hence can contribute to the assessment of possible clinical interventions.
机译:转移性癌细胞表现出至少两种不同的运动和侵袭表型-变形虫和间充质。这种可塑性对治疗转移提出了重大的临床挑战,而其潜在机制仍然是个谜。这些表型之间的转换是由Rac1 / RhoA电路介导的,该电路通过c-MET途径响应外部信号(例如HGF / SF)。使用基于GTPa​​se的调节的详细模型来研究Rac1 / RhoA电路的动力学,我们发现它可以作为三向开关工作。我们建议将电路的三个可能状态与变形虫,间充质和变形虫/间充质混合表型相关联。特别地,我们研究了响应于Grb2和Gab1-c-MET的两个下游衔接子的三种状态(表型)的存在范围和它们之间的过渡。该结果有助于解释c-MET途径对转移细胞的调控,因此可有助于评估可能的临床干预措施。

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