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Receptor-cytoskeletal unbinding in detachment of P-selectin from PSGL-1 on leukocytes

机译:P-选择素从PSGL-1脱离白细胞时的受体-细胞骨架解离

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Using a biomembrane force probe decorated with P-selectin, discrete bonds were formed to PSGL-1 receptors on PMN surfaces and detached at speeds from /spl sim/1 - 100 /spl mu/m/sec. High resolution tracking of the distance between probe tip and PMN revealed an initial elastic deformation that was either terminated by abrupt detachment or interrupted by yield and fluid-like extrusion of a macroscale tether plus subsequent detachment. Selecting tests that exhibited first yield then a single detachment step, we were able to quantify cohesive strengths between single PSGL-1 receptors and the PMN cytoskeleton. Prior to yield, the constant force rate was set by elastic stiffness (/spl sim/0.25 pNm) of the cytostructure and the pulling speed. Collected at rates over a span from 265 pN/sec to 38000 pN/sec, distributions of yield forces were found to agree precisely with probability densities for rupture of a single bond defined by a spontaneous dissociation rate of /spl sim/0.5/sec and an energy barrier projected at /spl sim/0.25 nm along the direction of force. By comparison, single P-selectin bonds to PSGL-1 covalently attached to microspheres were slightly stronger at all loading rates as characterized by a spontaneous dissociation rate of /spl sim/0.15/sec and an energy barrier projected at /spl sim/0.22 nm. Weaker anchoring to the cytoskeleton implies frequent tether formation that can reduce the hydrodynamic load applied to selectin bonds and prolog PMN attachments to vessel walls under conditions of flow.
机译:使用装饰有P-选择素的生物膜力探针,在PMN表面上与PSGL-1受体形成离散键,并以/ spl sim / 1-100 / spl mu / m / sec的速度脱离。对探针尖端和PMN之间距离的高分辨率跟踪显示出初始弹性变形,该弹性变形要么通过突然脱离而终止,要么由于屈服和大尺度系绳的流体状挤出以及随后的脱离而中断。选择显示出第一个产量然后一个分离步骤的测试,我们能够量化单个PSGL-1受体和PMN细胞骨架之间的内聚强度。在屈服之前,通过细胞结构的弹性刚度(/ spl sim / 0.25 pN / nm)和拉动速度设置恒定的力率。以从265 pN / sec到38000 pN / sec的速率收集,发现屈服力的分布与/ spl sim / 0.5 / sec的自发解离速率定义的单键断裂的概率密度精确一致。沿力方向投射在/ spl sim / 0.25 nm处的能垒。相比之下,共价连接至微球的PSGL-1的单个P-选择素键在所有加载速率下均稍强,其自发解离速率为/ spl sim / 0.15 / sec,能量垒为/ spl sim / 0.22 nm。 。较弱的锚定在细胞骨架上意味着频繁的系链形成,这可以减少施加在选择素键上的流体动力负荷以及在流动条件下将PMN附着在血管壁上的过程。

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