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血液捐献者外显子组与常见药物对红细胞代谢的影响。

Blood donor exposome and impact of common drugs on red blood cell metabolism.

机构信息

Department of Biochemistry and Molecular Genetics, University of Colorado Denver - Anschutz Medical Campus, Aurora, Colorado, USA.

Omix Technologies Inc., Aurora, Colorado, USA.

出版信息

JCI Insight. 2021 Feb 8;6(3):146175. doi: 10.1172/jci.insight.146175.

Abstract

Computational models based on recent maps of the RBC proteome suggest that mature erythrocytes may harbor targets for common drugs. This prediction is relevant to RBC storage in the blood bank, in which the impact of small molecule drugs or other xenometabolites deriving from dietary, iatrogenic, or environmental exposures ("exposome") may alter erythrocyte energy and redox metabolism and, in so doing, affect red cell storage quality and posttransfusion efficacy. To test this prediction, here we provide a comprehensive characterization of the blood donor exposome, including the detection of common prescription and over-the-counter drugs in blood units donated by 250 healthy volunteers in the Recipient Epidemiology and Donor Evaluation Study III Red Blood Cell-Omics (REDS-III RBC-Omics) Study. Based on high-throughput drug screenings of 1366 FDA-approved drugs, we report that approximately 65% of the tested drugs had an impact on erythrocyte metabolism. Machine learning models built using metabolites as predictors were able to accurately predict drugs for several drug classes/targets (bisphosphonates, anticholinergics, calcium channel blockers, adrenergics, proton pump inhibitors, antimetabolites, selective serotonin reuptake inhibitors, and mTOR), suggesting that these drugs have a direct, conserved, and substantial impact on erythrocyte metabolism. As a proof of principle, here we show that the antacid ranitidine - though rarely detected in the blood donor population - has a strong effect on RBC markers of storage quality in vitro. We thus show that supplementation of blood units stored in bags with ranitidine could - through mechanisms involving sphingosine 1-phosphate-dependent modulation of erythrocyte glycolysis and/or direct binding to hemoglobin - improve erythrocyte metabolism and storage quality.

摘要

基于最近 RBC 蛋白质组图谱的计算模型表明,成熟红细胞可能存在常见药物的靶点。这一预测与血库中的 RBC 储存有关,其中小分子药物或其他源自饮食、医源性或环境暴露的 xenometabolites(“暴露组”)的影响可能改变红细胞的能量和氧化还原代谢,从而影响红细胞储存质量和输血后疗效。为了验证这一预测,我们在这里全面描述了献血者的暴露组,包括在 Recipient Epidemiology and Donor Evaluation Study III Red Blood Cell-Omics (REDS-III RBC-Omics) Study 中检测了 250 名健康志愿者捐献的血液单位中的常见处方药和非处方药。基于对 1366 种 FDA 批准药物的高通量药物筛选,我们报告约 65%的测试药物对红细胞代谢有影响。使用代谢物作为预测因子构建的机器学习模型能够准确预测几种药物类别/靶点(双膦酸盐、抗胆碱能药、钙通道阻滞剂、肾上腺素能药、质子泵抑制剂、抗代谢物、选择性 5-羟色胺再摄取抑制剂和 mTOR)的药物,这表明这些药物对红细胞代谢有直接、保守且显著的影响。作为原理验证,我们在这里表明抗酸剂雷尼替丁 - 尽管在献血者人群中很少检测到 - 对 RBC 储存质量标志物具有强烈的体外作用。因此,我们表明在袋子中储存的血液单位中补充雷尼替丁可以通过涉及鞘氨醇 1-磷酸依赖性调节红细胞糖酵解和/或直接与血红蛋白结合的机制 - 改善红细胞代谢和储存质量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0fbf/7934844/1125239c4d20/jciinsight-6-146175-g076.jpg

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