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P-选择素与血小板清除

P-Selectin and platelet clearance.

作者信息

Berger G, Hartwell D W, Wagner D D

机构信息

The Center for Blood Research, Harvard Medical School, Boston, MA, USA.

出版信息

Blood. 1998 Dec 1;92(11):4446-52.

PMID:9834252
Abstract

P-selectin is an adhesion receptor for leukocytes expressed by activated platelets and endothelial cells. To assess a possible role of P-selectin in platelet clearance, we adapted an in vivo biotinylation technique in mice. Wild-type and P-selectin-deficient mice were infused with N-hydroxysuccinimido biotin. The survival of biotinylated platelets was followed by flow cytometry after labeling with fluorescent streptavidin. Both wild-type and P-selectin-deficient platelets presented identical life spans of about 4.7 days, suggesting that P-selectin does not play a role in platelet turnover. When biotinylated platelets were isolated, activated with thrombin, and reinjected into mice, the rate of platelet clearance was unchanged. In contrast, storage of platelets at 4 degreesC caused a significant reduction in their life span in vivo but again no significant differences were observed between the two genotypes. The infused thrombin-activated platelets rapidly lost their surface P-selectin in circulation, and this loss was accompanied by the simultaneous appearance of a 100-kD P-selectin fragment in the plasma. This observation suggests that the platelet membrane P-selectin was shed by cleavage. In conclusion, this study shows that P-selectin, despite its binding to leukocytes, does not mediate platelet clearance. However, the generation of a soluble form of P-selectin on platelet activation may have biological implications in modulating leukocyte recruitment or thrombus growth.

摘要

P-选择素是一种由活化血小板和内皮细胞表达的白细胞粘附受体。为了评估P-选择素在血小板清除中的可能作用,我们在小鼠中采用了一种体内生物素化技术。给野生型和P-选择素缺陷型小鼠注射N-羟基琥珀酰亚胺生物素。用荧光链霉亲和素标记后,通过流式细胞术追踪生物素化血小板的存活情况。野生型和P-选择素缺陷型血小板的寿命均约为4.7天,表明P-选择素在血小板更新中不起作用。当分离生物素化血小板、用凝血酶激活并重新注入小鼠体内时,血小板清除率没有变化。相反,在4℃储存血小板会导致其在体内的寿命显著缩短,但两种基因型之间再次未观察到显著差异。注入的凝血酶激活血小板在循环中迅速失去其表面的P-选择素,这种损失伴随着血浆中同时出现一个100-kD的P-选择素片段。这一观察结果表明血小板膜P-选择素是通过裂解而脱落的。总之,本研究表明,P-选择素尽管能与白细胞结合,但并不介导血小板清除。然而,血小板活化时产生的可溶性P-选择素形式可能在调节白细胞募集或血栓生长方面具有生物学意义。

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