血小板与多形核白细胞相互作用的最新进展。

Haemostasis Pub Date : 1999-09-01 DOI:10.1159/000022459
G de Gaetano, C Cerletti, V Evangelista
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引用次数: 105

摘要

流行病学证据表明,PMN的数量与缺血性血管疾病的风险呈正相关。活化的PMN诱导血小板活化的观察为PMN在血栓形成中的作用提供了一些生物学上的合理性。在其他PMN产物中,组织蛋白酶G是PMN激活过程中释放的一种蛋白酶,是一种有效的血小板激动剂。然而,血浆中存在的抗蛋白酶实际上可以消除其活性。事实上,研究表明,当PMN与混合细胞群中的血小板相互作用后受到刺激时,p选择素介导的血小板-PMN粘附可能导致形成一个隔离的微环境,在这个微环境中,组织蛋白酶G的活性受到抗蛋白酶的保护。p选择素介导的粘附也被证明促进花生四烯酸的跨细胞代谢,导致血栓素B2和白三烯C4的产生增加。在高剪切速率的混合细胞悬浮液中,PMN与活化血小板的粘附可以建模为粘附级联反应,包括p选择素依赖的识别步骤,然后是β(2)-整合素Mac-1介导的粘附强化相互作用。此外,还需要一种调节β(2)-整合素粘附性的酪氨酸激酶依赖的中间信号。事实上,活化的血小板不仅表达p -选择素,还表达不同的β(2)-整合素配体,包括纤维蛋白原和ICAM-2。p -选择素在PMN上引起的一些功能反应可以被p -选择素糖蛋白配体-1的特异性抗体所阻止,这表明这种粘附受体在配体参与时能够转导“由外向内”信号。通过活化血小板、表达p -选择素的CHO细胞和可溶性重组p -选择素,p -选择素可触发PMN蛋白酪氨酸磷酸化和Mac-1酪氨酸激酶依赖功能。总之,活化血小板粘附在PMN上可能是血栓形成过程中的一个关键事件。除p -选择素外,PMN β(2)-整合素在血小板-PMN粘附中的重要作用的认识为PMN整合素参与的广泛功能和机制提供了额外的证据,并可能成为药物干预的潜在靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Recent advances in platelet-polymorphonuclear leukocyte interaction.

Epidemiological evidence suggests a positive correlation between the number of PMN and the risk of ischemic vascular disease. The observation that activated PMN induce platelet activation my provide some biological plausibility to the role of PMN in thrombogenesis. Between other PMN products, cathepsin G, a protease released during PMN activation, is a potent platelet agonist. However, the antiproteinases present in plasma could virtually abolish its activity. Indeed it was shown that, when PMN were stimulated after interaction with platelets in mixed cell population, P-selectin-mediated platelet-PMN adhesion may result in the formation of a sequestered microenvironment in which cathepsin G activity is protected by antiproteases. P-selectin-mediated adhesion was also shown to facilitate the transcellular metabolism of arachidonic acid, resulting in increased production of both thromboxane B2 and leukotriene C4. PMN adhesion to activated platelets in mixed cell suspensions subjected to high shear rate can be modeled as an adhesion cascade involving a P-selectin-dependent recognition step followed by an adhesion-strengthening interaction mediated by the beta(2)-integrin Mac-1. Moreover, an intermediate tyrosine-kinase-dependent signal regulating beta(2)-integrin adhesiveness is required. Indeeed activated platelets express not only P-selectin but also different beta(2)-integrin ligands including fibrinogen and ICAM-2. Some of the functional responses elicited by P-selectin on PMN could be prevented by specific antibody to the P-selectin glycoprotein ligand-1, indicating that this adhesive receptor is able to transduce an 'outside-in' signal when engaged by the ligand. By using activated platelets, P-selectin-expressing CHO cells and soluble recombinant P-selectin, P-selectin was shown to trigger protein tyrosine phosphorylation in PMN and the tyrosine kinase-dependent function of Mac-1. In conclusion, adherence of activated platelets to PMN may be a key event in the sequence of thrombus formation. The recognition of the essential contribution of PMN beta(2)-integrins in addition to P-selectin in platelet-PMN adhesion provides an additional evidence to the broad range of function and mechanisms in which PMN integrins are involved and may be potential targets for pharmacological intervention.

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