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首页> 外文期刊>Cell biology international. >Annexin V relocates to the periphery of activated platelets following thrombin activation: an ultrastructural immunohistochemical approach.
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Annexin V relocates to the periphery of activated platelets following thrombin activation: an ultrastructural immunohistochemical approach.

机译:凝血酶活化后,膜联蛋白V会重新定位到活化血小板的周围:一种超微结构免疫组织化学方法。

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摘要

We have previously shown biochemically that the physiological agonist thrombin can cause translocation of endogenous annexin V to a fraction containing all platelet membranes. This paper reports ultrastructural immunohistochemical data revealing that annexin V molecules localize with plasma membranes of blood platelets following thrombin activation. When ultrathin sections of resting platelets were examined by immunogold staining, annexin V was found to be cytosolic, having a generalized distribution throughout the platelet. After thrombin activation, annexin V became peripheral in location and plasmalemma association increased. Morphometric analysis of gold particles shows that annexin V relocates specifically to the plasma membrane and its underlying cytoskeleton following treatment with thrombin. In control platelets 6.1% +/- 0.78 of annexin V is present at the plasma membrane and 15.0% +/- 0.82 in the region corresponding to the membrane cytoskeleton (10-80 nm); after stimulation with 0.5 unit/ml thrombin for 2 min this increased to 16.7% +/- 0.22 and 40.4% +/- 0.53, respectively.
机译:先前我们已经从生物化学上证明了生理激动剂凝血酶可以引起内源性膜联蛋白V移位到包含所有血小板膜的部分。本文报道了超结构免疫组织化学数据,揭示了凝血酶激活后膜联蛋白V分子定位在血小板的质膜上。当通过免疫金染色检查静息血小板的超薄切片时,发现膜联蛋白V是胞质的,在整个血小板中具有普遍分布。凝血酶激活后,膜联蛋白V的位置变得外围,血浆膜结合增加。金颗粒的形态分析表明,在用凝血酶处理后,膜联蛋白V特异地重定位到质膜及其下层的细胞骨架。在对照血小板中,质膜上存在膜联蛋白V的6.1%+ /-0.78,而在对应于膜细胞骨架(10-80nm)的区域中存在15.0%+ /-0.82。用0.5单位/毫升的凝血酶刺激2分钟后,分别增加到16.7%+ /-0.22和40.4%+ /-0.53。

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