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AS-1红细胞保存的代谢组学研究

Metabolomics of ADSOL (AS-1) red blood cell storage.

作者信息

Roback John D, Josephson Cassandra D, Waller Edmund K, Newman James L, Karatela Sulaiman, Uppal Karan, Jones Dean P, Zimring James C, Dumont Larry J

机构信息

Center for Transfusion and Cellular Therapies, Department of Pathology and Laboratory Medicine, Emory University School of Medicine, Atlanta, GA.

Center for Transfusion and Cellular Therapies, Department of Pathology and Laboratory Medicine, Emory University School of Medicine, Atlanta, GA.

出版信息

Transfus Med Rev. 2014 Apr;28(2):41-55. doi: 10.1016/j.tmrv.2014.01.003. Epub 2014 Feb 5.

Abstract

Population-based investigations suggest that red blood cells (RBCs) are therapeutically effective when collected, processed, and stored for up to 42 days under validated conditions before transfusion. However, some retrospective clinical studies have shown worse patient outcomes when transfused RBCs have been stored for the longest times. Furthermore, studies of RBC persistence in the circulation after transfusion have suggested that considerable donor-to-donor variability exists and may affect transfusion efficacy. To understand the limitations of current blood storage technologies and to develop approaches to improve RBC storage and transfusion efficacy, we investigated the global metabolic alterations that occur when RBCs are stored in AS-1 (AS1-RBC). Leukoreduced AS1-RBC units prepared from 9 volunteer research donors (12 total donated units) were serially sampled for metabolomics analysis over 42 days of refrigerated storage. Samples were tested by gas chromatography/mass spectrometry and liquid chromatography/tandem mass spectrometry, and specific biochemical compounds were identified by comparison to a library of purified standards. Over 3 experiments, 185 to 264 defined metabolites were quantified in stored RBC samples. Kinetic changes in these biochemicals confirmed known alterations in glycolysis and other pathways previously identified in RBCs stored in saline, adenine, glucose and mannitol solution (SAGM-RBC). Furthermore, we identified additional alterations not previously seen in SAGM-RBCs (eg, stable pentose phosphate pathway flux, progressive decreases in oxidized glutathione), and we delineated changes occurring in other metabolic pathways not previously studied (eg, S-adenosyl methionine cycle). These data are presented in the context of a detailed comparison with previous studies of SAGM-RBCs from human donors and murine AS1-RBCs. Global metabolic profiling of AS1-RBCs revealed a number of biochemical alterations in stored blood that may affect RBC viability during storage as well as therapeutic effectiveness of stored RBCs in transfusion recipients. These results provide future opportunities to more clearly pinpoint the metabolic defects during RBC storage, to identify biomarkers for donor screening and prerelease RBC testing, and to develop improved RBC storage solutions and methodologies.

摘要

基于人群的调查表明,红细胞(RBCs)在经过验证的条件下采集、处理并储存长达42天,然后进行输血时具有治疗效果。然而,一些回顾性临床研究表明,输注储存时间最长的红细胞时患者预后较差。此外,对输血后红细胞在循环中的持久性研究表明,供体之间存在相当大的变异性,这可能会影响输血效果。为了了解当前血液储存技术的局限性,并开发改善红细胞储存和输血效果的方法,我们研究了红细胞储存在AS-1(AS1-RBC)中时发生的全球代谢变化。从9名志愿者研究供体(共捐献12个单位)制备的白细胞滤除AS1-RBC单位在冷藏储存42天期间进行连续采样以进行代谢组学分析。样品通过气相色谱/质谱和液相色谱/串联质谱进行测试,并通过与纯化标准品库进行比较来鉴定特定的生化化合物。在3次实验中,对储存的红细胞样品中的185至264种确定的代谢物进行了定量。这些生化物质的动力学变化证实了先前在储存在盐水、腺嘌呤、葡萄糖和甘露醇溶液(SAGM-RBC)中的红细胞中发现的糖酵解和其他途径的已知变化。此外,我们还发现了SAGM-RBC中以前未见的其他变化(例如,稳定的磷酸戊糖途径通量,氧化型谷胱甘肽逐渐减少),并且我们描绘了以前未研究过的其他代谢途径中发生的变化(例如,S-腺苷甲硫氨酸循环)。这些数据是在与先前对人类供体的SAGM-RBC和小鼠AS1-RBC的研究进行详细比较的背景下呈现的。AS1-RBC的全球代谢谱分析揭示了储存血液中的一些生化变化,这些变化可能会影响储存期间红细胞的活力以及储存红细胞在输血受者中的治疗效果。这些结果为更清楚地确定红细胞储存期间的代谢缺陷、识别用于供体筛选和红细胞预发放检测的生物标志物以及开发改进的红细胞储存溶液和方法提供了未来的机会。

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Metabolomics of ADSOL (AS-1) red blood cell storage.AS-1红细胞保存的代谢组学研究
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