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次氯酸对血小板的抑制作用涉及环磷酸腺苷信号传导。

Platelet inhibition by hypochlorous acid involves cAMP signalling.

作者信息

O'Donoghue Lorna, Hiebner Dishon, Krishnankutty Roopesh, Schoen Ingmar, von Kriegsheim Alex, Smolenski Albert

机构信息

UCD School of Medicine, UCD Conway Institute, University College Dublin, Dublin 4, Belfield, Ireland; Irish Centre for Vascular Biology, Royal College of Surgeons in Ireland, 123 St Stephen's Green, Dublin D02 YN77, Ireland.

Irish Centre for Vascular Biology, Royal College of Surgeons in Ireland, 123 St Stephen's Green, Dublin D02 YN77, Ireland; UCD School of Chemical & Bioprocess Engineering, Engineering & Materials Science Centre University College Dublin, Dublin 4, Belfield, Ireland.

出版信息

Cell Signal. 2025 Mar;127:111568. doi: 10.1016/j.cellsig.2024.111568. Epub 2024 Dec 16.

DOI:10.1016/j.cellsig.2024.111568
PMID:39689749
Abstract

Hypochlorous acid (HOCl), made by neutrophil-derived myeloperoxidase, has been suggested to inhibit platelets, however, the mechanisms involved have not been described. Here we confirm that HOCl exposure changes platelet morphology and inhibits platelet spreading and aggregation. HOCl effects could be reversed by glutathione suggesting a role for cysteine oxidation. Mass spectrometry-based proteomics of HOCl-exposed platelets revealed oxidised cysteine residues in 37 proteins including adenylate cyclase 6 and Rap1B. Adenylate cyclase is involved in the inhibitory cAMP pathway triggered by endothelium-derived prostacyclin and Rap1 is a small G protein required for integrin αIIbβ3 activation and platelet aggregation. We show that HOCl exposure stimulates cAMP production and phosphorylation of the cAMP-dependent protein kinase substrate VASP in platelets and transfected HEK293T cells. In addition, HOCl inhibited Rap1-GTP formation. These data suggest that HOCl inhibits platelets at least in part through the cAMP pathway and by regulating Rap1. Thus, this study provides new insights into HOCl mediated crosstalk between neutrophils and platelets.

摘要

由中性粒细胞衍生的髓过氧化物酶产生的次氯酸(HOCl)被认为可抑制血小板,然而,其中涉及的机制尚未被描述。在此,我们证实HOCl暴露会改变血小板形态并抑制血小板铺展和聚集。谷胱甘肽可逆转HOCl的作用,提示半胱氨酸氧化起作用。基于质谱的HOCl暴露血小板蛋白质组学揭示了37种蛋白质中的氧化半胱氨酸残基,包括腺苷酸环化酶6和Rap1B。腺苷酸环化酶参与由内皮衍生的前列环素触发的抑制性cAMP途径,而Rap1是整合素αIIbβ3激活和血小板聚集所需的小G蛋白。我们表明,HOCl暴露会刺激血小板和转染的HEK293T细胞中cAMP的产生以及cAMP依赖性蛋白激酶底物VASP的磷酸化。此外,HOCl抑制Rap1-GTP的形成。这些数据表明,HOCl至少部分通过cAMP途径并通过调节Rap1来抑制血小板。因此,本研究为HOCl介导的中性粒细胞与血小板之间的串扰提供了新的见解。

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