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氧化还原蛋白质组学与血小板活化:通过了解氧化还原蛋白质组来提高输血用血小板质量

Redox Proteomics and Platelet Activation: Understanding the Redox Proteome to Improve Platelet Quality for Transfusion.

作者信息

Sonego Giona, Abonnenc Mélanie, Tissot Jean-Daniel, Prudent Michel, Lion Niels

机构信息

Transfusion Interrégionale Croix Rouge Suisse SA, Laboratoire de Recherche sur les Produits Sanguins, Route de la Corniche 2, 1066 Epalinges, Switzerland.

Faculté de Biologie et de Médecine, Université de Lausanne, CH-1011 Lausanne, Switzerland.

出版信息

Int J Mol Sci. 2017 Feb 11;18(2):387. doi: 10.3390/ijms18020387.

Abstract

Blood banks use pathogen inactivation (PI) technologies to increase the safety of platelet concentrates (PCs). The characteristics of PI-treated PCs slightly differ from those of untreated PCs, but the underlying reasons are not well understood. One possible cause is the generation of oxidative stress during the PI process. This is of great interest since reactive oxygen species (ROS) act as second messengers in platelet functions. Furthermore, there are links between protein oxidation and phosphorylation, another mechanism that is critical for cell regulation. Current research efforts focus on understanding the underlying mechanisms and identifying new target proteins. Proteomics technologies represent powerful tools for investigating signaling pathways involving ROS and post-translational modifications such as phosphorylation, while quantitative techniques enable the comparison of the platelet resting state versus the stimulated state. In particular, redox cysteine is a key player in platelet activation upon stimulation by different agonists. This review highlights the experiments that have provided insights into the roles of ROS in platelet function and the implications for platelet transfusion, and potentially in diseases such as inflammation and platelet hyperactivity. The review also describes the implication of redox mechanism in platelet storage considerations.

摘要

血库采用病原体灭活(PI)技术来提高血小板浓缩物(PCs)的安全性。经PI处理的PCs的特性与未经处理的PCs略有不同,但其根本原因尚未完全明确。一个可能的原因是PI过程中产生了氧化应激。这一点备受关注,因为活性氧(ROS)在血小板功能中充当第二信使。此外,蛋白质氧化与磷酸化之间存在联系,而磷酸化是细胞调节的另一个关键机制。目前的研究工作集中在理解潜在机制并识别新的靶蛋白。蛋白质组学技术是研究涉及ROS和磷酸化等翻译后修饰的信号通路的有力工具,而定量技术能够比较血小板的静息状态与激活状态。特别是,氧化还原半胱氨酸在不同激动剂刺激血小板激活过程中起着关键作用。本综述重点介绍了一些实验,这些实验为ROS在血小板功能中的作用以及对血小板输血的影响提供了见解,并且可能对炎症和血小板功能亢进等疾病也有影响。该综述还描述了氧化还原机制在血小板储存考量中的意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a553/5343922/6389c6b9647b/ijms-18-00387-g001.jpg

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