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细胞松弛素B(CB)对凝血酶或TRAP作用后及表面激活前糖蛋白Ib(GP Ib)分布的影响。

Influence of cytochalasin B (CB) on GP Ib distribution after thrombin or TRAP and before surface activation.

作者信息

White J G, Krumwiede M D, Cocking-Johnson D J, Burris S, Rao G H

机构信息

Department of Laboratory Medicine, University of Minnesota Medical School, UMHC Box 490, 420 Delaware Street S.E., Minneapolis, Minnesota 55455, USA.

出版信息

Platelets. 1997 Jan;8(1):53-60. doi: 10.1080/09537109777546.

Abstract

The receptor for von Willebrand factor (vWF) on human platelets, glycoprotein (GP) Ib/IX, has been shown in our studies to be an immobile complex when stimulated in suspension or on surfaces. Recent investigations have revealed that GP Ib/IX remains immobile on platelets activated in suspension followed by exposure to formvar surfaces that cause the cells to spread. However, since channels of the open canalicular system (OCS) are evaginated back on to the exposed surface during spreading, it was suggested that our study missed the clearance of GP Ib/IX from the exposed surface to internal membranes. The present study has added cytochalasin B after exposure of platelets to thrombin or TRAP in suspension in order to prevent spreading and movement of GP Ib/IX during subsequent exposure to surface activation on formvar grids. Results indicate that GP Ib/IX receptors remain randomly dispersed from edge to edge on platelets activated by thrombin or TRAP in suspension 10 minutes before treatment with CB followed by surface activation. Statistical analysis of the frequency of immunogold particles binding to monoclonal antibodies attached to GP Ib/IX revealed no significant reduction in frequency, translocation from cell edges or concentration of GP Ib/IX receptors in or around channels of the OCS. Results support the concept that GP Ib/IX is not cleared from exposed surfaces to the OCS of platelets activated by thrombin or TRAP and surface activation.

摘要

在我们的研究中已表明,人血小板上血管性血友病因子(vWF)的受体糖蛋白(GP)Ib/IX在悬浮液中或表面受到刺激时是一种固定的复合物。最近的研究表明,GP Ib/IX在悬浮液中被激活然后暴露于导致细胞铺展的福尔马林中时,在血小板上仍保持固定。然而,由于在铺展过程中开放小管系统(OCS)的通道会外翻回到暴露表面,因此有人认为我们的研究忽略了GP Ib/IX从暴露表面清除到内膜的过程。本研究在血小板于悬浮液中暴露于凝血酶或TRAP后添加了细胞松弛素B,以防止在随后暴露于福尔马林网格表面激活时GP Ib/IX的铺展和移动。结果表明,在用CB处理然后进行表面激活前10分钟,在悬浮液中被凝血酶或TRAP激活的血小板上,GP Ib/IX受体从边缘到边缘仍随机分散。对结合到附着于GP Ib/IX的单克隆抗体的免疫金颗粒频率的统计分析显示,频率没有显著降低,也没有从细胞边缘移位或在OCS通道内或周围GP Ib/IX受体的聚集。结果支持这样的概念,即GP Ib/IX不会从暴露表面清除到被凝血酶或TRAP激活并经表面激活的血小板的OCS中。

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