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Integrin intra-heterodimer affinity inversely correlates with integrin activatability

机译:整联素异二聚体亲和力与整合素激活性相反

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Integrins are heterodimeric cell surface receptors composed of an α and β subunit that mediate cell adhesion to extracellular matrix proteins such as fibronectin. We previously studied integrin α5β1 activation during zebrafish somitogenesis, and in the present study, we characterize the integrin αV fibronectin receptors. Integrins are activated via a conformational change, and we perform single-molecule biophysical measurements of both integrin activation via fluorescence resonance energy transfer (FRET)-fluorescence lifetime imaging microscopy (FLIM) and integrin intra-heterodimer stability via fluorescence cross-correlation spectroscopy (FCCS) in living embryos. We find that integrin heterodimers that exhibit robust cell surface expression, including αVβ3, αVβ5, and αVβ6, are never activated in this in?vivo context, even in the presence of fibronectin matrix. In contrast, activatable integrins, such as integrin αVβ1, and alleles of αVβ3, αVβ5, αVβ6 that are biased to the active conformation exhibit poor cell surface expression and have a higher intra-heterodimer dissociation constant (K D ). These observations suggest that a weak integrin intra-heterodimer affinity decreases integrin cell surface stability and increases integrin activatability.
机译:整联蛋白是由α和β亚基组成的异二聚体细胞表面受体,其介导细胞粘附与细胞外基质蛋白如纤维菌蛋白。我们以前研究过Zebrafise Somitoisesis期间的整联蛋白α5β1激活,并且在本研究中,我们表征整合蛋白αv纤连蛋白受体。通过构象变化激活整联蛋白,我们通过荧光共振能量转移(FLIM) - 荧光寿命显微镜(FLIM)进行整联蛋白激活的单分子生物物理测量,并通过荧光互相关光谱整合到异二聚体稳定性(FCCS )在生物胚胎中。我们发现,即使在纤连蛋白基质存在下,也不会在该αvivo上下文中含有浓郁的细胞表面表达,包括αvβ3,αvβ5和αvβ6的整合蛋白的异二聚体。相反,可激活的整体蛋白,例如整联蛋白αvβ1和αvβ3,αvβ5,αvβ6的等位基因,其被偏置为主动构象,具有较差的细胞表面表达,并且具有更高的内杂小二聚蛋白解离常数(k d)。这些观察结果表明,弱整联蛋白异二聚体亲和力降低了整联蛋白细胞表面稳定性并增加整联素激活性。

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