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源自C反应蛋白(CRP)的类促吞噬肽合成肽对血小板行为的影响。

Influence of tuftsin-like synthetic peptides derived from C-reactive protein (CRP) on platelet behaviour.

作者信息

Fiedel B A

机构信息

Division of Immunology, James N. Gamble Institute of Medical Research, Cincinnati, Ohio 45219.

出版信息

Immunology. 1988 Jul;64(3):487-93.

Abstract

C-reactive protein (CRP) is an acute-phase reactant that modifies platelet function differently, depending upon its physiochemical state. Aggregated and ligand-complexed forms of CRP initiate the activation of platelets, whereas naturally occurring CRP peptides inhibit platelet activation. The present study documents neutral proteases of the polymorphonuclear leucocyte (PMN) to cleave CRP into reaction products with the potential to inhibit platelet activation, and explore the structure-function relationships involved in the regulation of platelet activation by CRP using synthetic CRP peptides. Evidence was obtained that (i) a minimum of two linear functional domains exist within CRP that influence platelet activation; (ii) they reside in the mid-portion and at the C-terminus of the CRP molecule; (iii) the mid-portion domain inhibits platelet activation stimulated by adenosine diphosphate (ADP) or acid-soluble collagen, whereas the C-terminal domain initiates platelet activation; (iv) the functional expression of the C-terminal domain is maximized when the linear peptide is immobilized on latex; and (v) both CRP domains contain a homologue of the immunoregulatory signal peptide, tuftsin. These data suggest that the molecular mechanisms by which platelet processes are modulated by CRP may be related to the presence of tuftsin homologues in CRP.

摘要

C反应蛋白(CRP)是一种急性期反应物,根据其物理化学状态,它对血小板功能的影响有所不同。聚集的和与配体结合的CRP形式可引发血小板的激活,而天然存在的CRP肽则抑制血小板激活。本研究记录了多形核白细胞(PMN)的中性蛋白酶将CRP切割成具有抑制血小板激活潜力的反应产物,并使用合成CRP肽探索CRP调节血小板激活过程中涉及的结构-功能关系。获得的证据表明:(i)CRP中至少存在两个影响血小板激活的线性功能结构域;(ii)它们位于CRP分子的中部和C末端;(iii)中部结构域抑制由二磷酸腺苷(ADP)或酸溶性胶原刺激的血小板激活,而C末端结构域引发血小板激活;(iv)当线性肽固定在乳胶上时,C末端结构域的功能表达最大化;(v)两个CRP结构域均包含免疫调节信号肽tuftsin的同源物。这些数据表明,CRP调节血小板过程的分子机制可能与CRP中tuftsin同源物的存在有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1a75/1385063/3cc34f14d987/immunology00155-0120-a.jpg

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