肌球蛋白IIa收缩性是血小板在胶原蛋白上铺展时维持其结构所必需的，并有助于血栓稳定性。

MyosinIIa contractility is required for maintenance of platelet structure during spreading on collagen and contributes to thrombus stability.

作者信息

Calaminus S D J, Auger J M, McCarty O J T, Wakelam M J O, Machesky L M, Watson S P

机构信息

Centre for Cardiovascular Sciences, Institute of Biomedical Research, The Medical School, University of Birmingham, Birmingham, UK.

出版信息

J Thromb Haemost. 2007 Oct;5(10):2136-45. doi: 10.1111/j.1538-7836.2007.02696.x. Epub 2007 Jul 23.

DOI:10.1111/j.1538-7836.2007.02696.x

PMID:17645784

Abstract

BACKGROUND

MyosinIIs are adenosine triphosphate-driven molecular motors that form part of a cell's contractile machinery. They are activated by phosphorylation of their light chains, by either activation of myosin light chain (MLC) kinase or inhibition of MLC phosphatase via Rho kinase (ROCK). MyosinIIa phosphorylation underlies platelet rounding and stress fiber formation.

OBJECTIVE

To identify the functional significance of myosinIIa in platelet spreading and thrombus formation on collagen using inhibitors of ROCK (Y27632) and myosinII (blebbistatin).

RESULTS

Stress fiber formation on collagen is inhibited by both Y27632 and blebbistatin. A substantial proportion of spread platelets generate internal holes or splits on collagen, presumably because of a reduction in contractile strength. Platelet integrity, however, is maintained. In an in vitro model, thrombus embolization on collagen is increased in the presence of Y27632 and blebbistatin at intermediate shear, leading to a reduction in platelet aggregate growth. Moreover, Y27632 causes a marked reduction in thrombus formation in an in vivo laser-injury model.

CONCLUSIONS

MyosinIIa contractility is required for maintenance of platelet structure during spreading on collagen and contributes to thrombus stability.

摘要

背景

肌球蛋白II是由三磷酸腺苷驱动的分子马达，是细胞收缩机制的一部分。它们通过轻链磷酸化被激活，可通过肌球蛋白轻链（MLC）激酶的激活或经由Rho激酶（ROCK）对MLC磷酸酶的抑制来实现。肌球蛋白IIa磷酸化是血小板变圆和应力纤维形成的基础。

目的

使用ROCK抑制剂（Y27632）和肌球蛋白II抑制剂（blebbistatin）来确定肌球蛋白IIa在血小板在胶原蛋白上的铺展和血栓形成中的功能意义。

结果

Y27632和blebbistatin均抑制胶原蛋白上应力纤维的形成。相当一部分铺展的血小板在胶原蛋白上产生内部孔洞或裂缝，推测是由于收缩强度降低所致。然而，血小板的完整性得以维持。在体外模型中，在中等剪切力条件下，Y27632和blebbistatin存在时，胶原蛋白上的血栓栓塞增加，导致血小板聚集体生长减少。此外，在体内激光损伤模型中，Y27632可导致血栓形成显著减少。

结论

肌球蛋白IIa的收缩性是血小板在胶原蛋白上铺展过程中维持血小板结构所必需的，并有助于血栓稳定性。

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肌球蛋白IIa收缩性是血小板在胶原蛋白上铺展时维持其结构所必需的，并有助于血栓稳定性。

MyosinIIa contractility is required for maintenance of platelet structure during spreading on collagen and contributes to thrombus stability.

作者信息

机构信息

出版信息

BACKGROUND

OBJECTIVE

RESULTS

CONCLUSIONS

背景

目的

结果

结论

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