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Discrete spatial organization of TGFβ receptors couples receptor multimerization and signaling to cellular tension

机译:TGFβ受体的离散空间组织将受体多聚化和信号传导耦合到细胞张力

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摘要

Cell surface receptors are central to the cell's ability to generate coordinated responses to the multitude of biochemical and physical cues in the microenvironment. However, the mechanisms by which receptors enable this concerted cellular response remain unclear. To investigate the effect of cellular tension on cell surface receptors, we combined novel high-resolution imaging and single particle tracking with established biochemical assays to examine TGFβ signaling. We find that TGFβ receptors are discretely organized to segregated spatial domains at the cell surface. Integrin-rich focal adhesions organize TβRII around TβRI, limiting the integration of TβRII while sequestering TβRI at these sites. Disruption of cellular tension leads to a collapse of this spatial organization and drives formation of heteromeric TβRI/TβRII complexes and Smad activation. This work details a novel mechanism by which cellular tension regulates TGFβ receptor organization, multimerization, and function, providing new insight into the mechanisms that integrate biochemical and physical cues.>DOI:
机译:细胞表面受体对于细胞对微环境中多种生化和物理线索产生协调响应的能力至关重要。但是,受体使这种协调的细胞应答的机制尚不清楚。为了研究细胞张力对细胞表面受体的影响,我们将新型高分辨率成像和单颗粒跟踪与已建立的生化分析相结合,以检查TGFβ信号传导。我们发现TGFβ受体被离散地组织到细胞表面的空间区域。富含整联蛋白的粘着斑将TβRII组织在TβRI周围,从而限制了TβRII的整合,同时将TβRI隔离在这些位点。细胞张力的破坏导致该空间组织的崩溃并驱动异聚TβRI/TβRII复合物的形成和Smad活化。这项工作详述了一种新的机制,通过该机制,细胞张力可调节TGFβ受体的组织,多聚化和功能,从而为整合生化和物理线索的机制提供新见解。> DOI:

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