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凝血酶-血小板相互作用:对血小板活化中可饱和与不可饱和结合作用的评估。

Thrombin-platelet interactions: an assessment of the roles of saturable and nonsaturable binding in platelet activation.

作者信息

Alexander R J, Fenton J W, Detwiler T C

出版信息

Arch Biochem Biophys. 1983 Apr 1;222(1):266-75. doi: 10.1016/0003-9861(83)90524-6.

Abstract

Thrombin binds to platelets and induces platelet activation, but the relationship of binding to activation is not clear. To better define this relationship, we have analyzed parameters of binding and activation by alpha-thrombin and by three analogous proteases that activate platelets somewhat differently. The proteases were nitro-alpha-thrombin, a derivative with nitrated tyrosine, gamma-thrombin, a product of partial proteolysis of alpha-thrombin, and trypsin, a homologous protease. Nitro-alpha-thrombin and native alpha-thrombin activated platelets similarly, whereas gamma-thrombin and trypsin activated to a slightly lesser extent than alpha-thrombin and only after a distinctive delay. alpha-Thrombin and nitro-alpha-thrombin bound to platelets to about the same extent, but only alpha-thrombin showed evidence of saturable binding. Hirudin, a thrombin inhibitor, blocked both platelet activation and saturable binding by alpha-thrombin. With nitro-alpha-thrombin, hirudin blocked platelet activation, but it had no effect on binding. gamma-Thrombin and trypsin bound less than alpha-thrombin and with no evidence of saturable binding. There were identical relationships between the total amount bound and the extent of platelet activation for the four proteases (some show no saturable binding) but distinct differences in the relationships of total amount bound and the rate of activation; similar rates of activation required the binding of three to five times more gamma-thrombin or trypsin than alpha-thrombin. That is, without saturable binding, activation was slower. These data thus show a correlation between total amount bound and extent of activation but no correlation between amount saturably bound and the extent of platelet activation. Conversely, the rate of activation is more closely correlated with saturable binding than with total binding. We conclude that high-affinity saturable binding is not essential for thrombin-induced platelet activation but that it may accelerate the reaction.

摘要

凝血酶与血小板结合并诱导血小板活化,但其结合与活化之间的关系尚不清楚。为了更好地界定这种关系,我们分析了α-凝血酶以及三种激活血小板方式略有不同的类似蛋白酶的结合和活化参数。这些蛋白酶分别是硝基-α-凝血酶(一种酪氨酸硝化衍生物)、γ-凝血酶(α-凝血酶部分蛋白水解产物)和胰蛋白酶(一种同源蛋白酶)。硝基-α-凝血酶和天然α-凝血酶对血小板的活化作用相似,而γ-凝血酶和胰蛋白酶的活化程度略低于α-凝血酶,且有明显延迟。α-凝血酶和硝基-α-凝血酶与血小板的结合程度大致相同,但只有α-凝血酶表现出饱和结合的迹象。水蛭素是一种凝血酶抑制剂,可阻断α-凝血酶引起的血小板活化和饱和结合。对于硝基-α-凝血酶,水蛭素可阻断血小板活化,但对结合无影响。γ-凝血酶和胰蛋白酶的结合量少于α-凝血酶,且无饱和结合的迹象。四种蛋白酶的总结合量与血小板活化程度之间存在相同的关系(有些无饱和结合),但总结合量与活化速率之间存在明显差异;γ-凝血酶或胰蛋白酶要达到与α-凝血酶相似的活化速率,其结合量需要多三到五倍。也就是说,在没有饱和结合的情况下,活化较慢。因此,这些数据表明总结合量与活化程度之间存在相关性,但饱和结合量与血小板活化程度之间无相关性。相反,活化速率与饱和结合的相关性比与总结合的相关性更密切。我们得出结论,高亲和力的饱和结合对于凝血酶诱导的血小板活化并非必不可少,但可能会加速反应。

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