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多聚磷酸盐在凝血过程中生理作用研究的注意事项。

Caveats in studies of the physiological role of polyphosphates in coagulation.

作者信息

Lindahl Tomas L, Ramström Sofia, Boknäs Niklas, Faxälv Lars

机构信息

Department of Clinical and Experimental Medicine, Linköping University, SE-581 85 Linköping, Sweden

Department of Clinical and Experimental Medicine, Linköping University, SE-581 85 Linköping, Sweden.

出版信息

Biochem Soc Trans. 2016 Feb;44(1):35-9. doi: 10.1042/BST20150220.

Abstract

Platelet-derived polyphosphates (polyP), stored in dense granule and released upon platelet activation, have been claimed to enhance thrombin activation of coagulation factor XI (FXI) and to activate FXII directly. The latter claim is controversial and principal results leading to these conclusions are probably influenced by methodological problems. It is important to consider that low-grade contact activation is initiated by all surfaces and is greatly amplified by the presence of phospholipids simulating the procoagulant membranes of activated platelets. Thus, proper use of inhibitors of the contact pathway and a careful choice of materials for plates and tubes is important to avoid artefacts. The use of phosphatases used to degrade polyP has an important drawback as it also degrades the secondary activators ADP and ATP, which are released from activated platelets. In addition, the use of positively charged inhibitors, such as polymyxin B, to inhibit polyP in platelet-rich plasma and blood is problematic, as polymyxin B also slows coagulation in the absence of polyP. In conclusion we hope awareness of the above caveats may improve research on the physiological roles of polyP in coagulation.

摘要

血小板衍生的多聚磷酸盐(polyP)储存于致密颗粒中,并在血小板激活时释放,据称可增强凝血因子XI(FXI)的凝血酶激活作用,并直接激活FXII。后一种说法存在争议,得出这些结论的主要结果可能受到方法学问题的影响。需要考虑的是,低级别接触激活由所有表面引发,并因模拟活化血小板促凝膜的磷脂的存在而大大放大。因此,正确使用接触途径抑制剂并谨慎选择板和管的材料对于避免假象很重要。用于降解多聚磷酸盐的磷酸酶的使用有一个重要缺点,因为它也会降解从活化血小板释放的二级激活剂ADP和ATP。此外,使用带正电荷的抑制剂(如多粘菌素B)来抑制富含血小板血浆和血液中的多聚磷酸盐存在问题,因为多粘菌素B在没有多聚磷酸盐的情况下也会减缓凝血。总之,我们希望对上述注意事项的认识可能会改善对多聚磷酸盐在凝血中的生理作用的研究。

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