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Redox Control of Platelet Function

机译:血小板功能的氧化还原控制

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摘要

There has recently been a dramatic expansion in research in the area of redox biology with systems that utilize thiols to perform redox chemistry being central to redox control. Thiol-based reactions occur in proteins involved in platelet function, including extracellular platelet proteins. The aIIb/?3 fibrinogen receptor contains free thiols that are required for the activation of this receptor to a fibrinogen-binding conformation. This process is under enzymatic control, with protein disulfide isomerase playing a central role in the activation of aIIb/?3. Other integrins, such as the oc2 beta l alpha collagen receptor on platelets, are also regulated by protein disulfide isomerase and thiol metabolism. Low molecular weight thiols that are found in blood regulate these processes by converting redox sensitive disulfide bonds to thiols and by providing the appropriate redox potential for these reactions. Additional mechanisms of redox control of platelets involve nitric oxide that inhibits platelet responses, and reactive oxygen species that potentiate platelet thrombus formation. Specific nitrosative or oxidative modifications of thiol groups in platelets may modulate platelet function. Since many biologic processes are regulated by redox reactions that involve surface thiols, the extracellular redox state can have an important influence on health and disease status and may be a target for therapeutic intervention.
机译:最近,氧化还原生物学领域的研究有了巨大的扩展,利用硫醇进行氧化还原化学的系统是氧化还原控制的核心。基于硫醇的反应发生在涉及血小板功能的蛋白质中,包括细胞外血小板蛋白质。 aIIb /β3纤维蛋白原受体含有游离硫醇,其是将该受体活化为纤维蛋白原结合构象所必需的。该过程在酶的控制下,蛋白质二硫键异构酶在aIIb /β3的激活中起着核心作用。其他整联蛋白,例如血小板上的oc2β1α胶原受体,也受蛋白质二硫键异构酶和硫醇代谢的调节。血液中发现的低分子量硫醇通过将氧化还原敏感的二硫键转化为硫醇并为这些反应提供适当的氧化还原电势来调节这些过程。血小板氧化还原控制的其他机制包括抑制血小板反应的一氧化氮和增强血小板血栓形成的活性氧。血小板中硫醇基团的特定亚硝化或氧化修饰可能会调节血小板功能。由于许多生物过程受到涉及表面硫醇的氧化还原反应的调节,因此细胞外氧化还原状态可能对健康和疾病状况产生重要影响,并且可能成为治疗干预的目标。

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