Monika Dzieciatkowska, Ariel Hay, Aaron Issaian, Gregory R Keele, Shaun Bevers, Travis Nemkov, Julie A Reisz, Mark Maslanka, Daniel Stephenson, Amy L Moore, Xutao Deng, Mars Stone, Kirk C Hansen, Steve Kleinman, Philip J Norris, Michael P Busch, Grier P Page, Nareg Roubinian, Yang Xia, James C Zimring, Angelo D'Alessandro
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These human findings were mechanistically validated using a murine model deficient in ADORA2b, which demonstrated impaired glycolytic flux, compromised antioxidant defenses - including caffeine-dependent direct inhibition of recombinantly-expressed glucose 6-phosphate dehydrogenase, and decreased transfusion efficacy (lower hemoglobin increments, higher bilirubin posttransfusion), effects further exacerbated by caffeine exposure during storage. 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引用次数: 0
摘要
咖啡因是全球消费最广泛的精神活性物质,但其外周生理效应仍不完全清楚。利用red红细胞组学研究中13091名献血者的综合数据,我们确定咖啡因是红细胞(RBC)储存质量和输血结果的重要调节剂。从643名被召回的献血者中,根据他们溶血倾向的极端程度进行选择,在多次捐赠中,咖啡因水平的升高是可重复的。在筛选和召回队列中,较高的咖啡因水平与红细胞代谢紊乱有关,其特征是糖酵解减少,腺苷酸池或2,3-双磷酸甘油耗竭,氧化应激和渗透脆弱性标志物增加,包括犬尿氨酸积累。这些观察结果在8名志愿者的血浆和红细胞中进行了重述,他们分别喝了一杯咖啡(Chemex vs espresso)。在临床上,咖啡因升高与溶血增加和输血后血红蛋白增加降低相关,特别是在输注来自携带常见多态性的捐赠者的红细胞的受体中,ADORA2b基因是缺氧时红细胞代谢的关键调节因子。这些人类研究结果通过缺乏ADORA2b的小鼠模型得到了机制验证,该模型显示糖酵解流量受损,抗氧化防御受损,包括咖啡因依赖的重组表达的葡萄糖6-磷酸脱氢酶的直接抑制,以及输血效果降低(输血后血红蛋白增量降低,胆红素升高),这些影响在储存期间暴露于咖啡因进一步加剧。我们的研究将咖啡因摄入定位为输血实践中的一个可改变因素,倡导整合遗传和暴露因素的精确策略,并确定代谢干预措施以提高血液质量和临床结果。
Caffeine impairs red blood cell storage quality by dual inhibition of ADORA2b signaling and G6PD activity.
Caffeine is the most widely consumed psychoactive substance globally, yet its peripheral physiological effects remain incompletely understood. Leveraging comprehensive data from 13,091 blood donors in the REDS RBC-Omics study, we identify caffeine as a significant modulator of red blood cell (RBC) storage quality and transfusion outcomes. Elevated caffeine levels were reproducible across multiple donations from 643 recalled donors, selected based on their extremes in hemolytic propensity. Both in the screening and recalled cohorts, higher caffeine levels were associated with disrupted RBC metabolism, characterized by reduced glycolysis, depletion of adenylate pools or 2,3-bisphosphoglycerate, and increased markers of oxidative stress and osmotic fragility, including kynurenine accumulation. These observations were recapitulated in plasma and RBCs of eight volunteers upon consumption of a cup of coffee independently of brewing method (Chemex vs espresso). Clinically, elevated caffeine correlated with increased hemolysis and lower post-transfusion hemoglobin increments, especially pronounced in recipients transfused with RBCs from donors carrying common polymorphisms in the ADORA2b gene, a key regulator of RBC metabolism in hypoxia. These human findings were mechanistically validated using a murine model deficient in ADORA2b, which demonstrated impaired glycolytic flux, compromised antioxidant defenses - including caffeine-dependent direct inhibition of recombinantly-expressed glucose 6-phosphate dehydrogenase, and decreased transfusion efficacy (lower hemoglobin increments, higher bilirubin posttransfusion), effects further exacerbated by caffeine exposure during storage. Our study positions caffeine consumption as a modifiable factor in blood transfusion practice, advocating for precision strategies that integrate genetic and exposome factors, and identifies metabolic interventions to enhance blood quality and clinical outcomes.
期刊介绍:
Haematologica is a journal that publishes articles within the broad field of hematology. It reports on novel findings in basic, clinical, and translational research.
Scope:
The scope of the journal includes reporting novel research results that:
Have a significant impact on understanding normal hematology or the development of hematological diseases.
Are likely to bring important changes to the diagnosis or treatment of hematological diseases.
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