Chauhan A K, Goerge T, Schneider S W, Wagner D D
CBR Institute for Biomedical Research and Department of Pathology, Harvard Medical School, Boston, MA 02115, USA.
J Thromb Haemost. 2007 Mar;5(3):583-9. doi: 10.1111/j.1538-7836.2007.02361.x. Epub 2006 Dec 13.
Ultra-large von Willebrand factor (ULVWF) and the receptor P-selectin are released from endothelial Weibel-Palade bodies during injury or inflammation. VWF mediates platelet adhesion and P-selectin promotes leukocyte rolling. ADAMTS-13 limits the duration of platelet adhesion by cleaving the ULVWF. In the absence of ADAMTS-13, long VWF filaments decorated with platelets form. Recent in vitro studies suggested that P-selectin might anchor these platelet strings to endothelium, but whether the same mechanism exists in vivo remains to be elucidated.
We address the role of P-selectin and beta(3) integrin in platelet string formation in vivo using intravital microscopy by infusing inhibitory ADAMTS-13 antibody in P-selectin-/- and beta(3)-deficient mice and activating the endothelium by injecting histamine.
We show that inhibition of ADAMTS-13 combined with endothelial activation leads to similar extents of platelet string formation in wild-type, P-selectin- and integrin beta(3)-deficient mice. Further, in venules the platelet strings can coalesce into VWF-platelet aggregates. This process utilizes neither the platelet beta(3) integrin nor P-selectin. We also show in vitro that platelets can act as a bridge between the VWF fibers and that VWF can self-associate even in areas devoid of platelets.
The formation or retention of the platelet strings does not require P-selectin or the endothelial VWF receptor alpha(v)beta(3). Furthermore, in the presence of low ADAMTS-13 activity, VWF-dependent and alpha(IIb)beta(3)-independent platelet clustering occurs in veins, as has been shown at high arterial shear rates. Our study further supports the importance of regulation of VWF multimer size upon secretion from Weibel-Palade bodies.
在损伤或炎症过程中,超大血管性血友病因子(ULVWF)和受体P-选择素从内皮细胞的Weibel-Palade小体中释放出来。血管性血友病因子(VWF)介导血小板黏附,P-选择素促进白细胞滚动。ADAMTS-13通过切割ULVWF来限制血小板黏附的持续时间。在缺乏ADAMTS-13的情况下,会形成由血小板装饰的长VWF细丝。最近的体外研究表明,P-选择素可能将这些血小板链锚定在内皮细胞上,但体内是否存在相同机制仍有待阐明。
我们通过在P-选择素基因敲除小鼠和β3缺陷小鼠中注入抑制性ADAMTS-13抗体,并通过注射组胺激活内皮细胞,利用活体显微镜研究P-选择素和β3整合素在体内血小板链形成中的作用。
我们发现,抑制ADAMTS-13并结合内皮细胞激活,在野生型、P-选择素和整合素β3缺陷小鼠中导致相似程度的血小板链形成。此外,在小静脉中,血小板链可聚集成VWF-血小板聚集体。这个过程既不利用血小板β3整合素也不利用P-选择素。我们还在体外表明,血小板可以作为VWF纤维之间的桥梁,并且VWF即使在没有血小板的区域也能自我结合。
血小板链的形成或保留不需要P-选择素或内皮VWF受体αvβ3。此外,在ADAMTS-13活性较低的情况下,静脉中会发生VWF依赖性和α(IIb)β3非依赖性血小板聚集,正如在高动脉剪切速率下所显示的那样。我们的研究进一步支持了在Weibel-Palade小体分泌时调节VWF多聚体大小的重要性。
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