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Transfusion begets anemia: The effect of aged blood on hematopoiesis

机译:输血引起贫血:老年血液对造血功能的影响

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BACKGROUND: Following trauma, transfusion of aged stored blood is often necessary yet associated with increased morbidity and mortality. Despite blood replacement, many patients have a prolonged anemia requiring further transfusions. The effects of aged blood on bone marrow (BM) hematopoiesis have not been studied, and we hypothesized that stored blood suppresses BM function. METHODS: Blood from Sprague-Dawley rats was stored for 1, 14, or 28 days with the industry preservative citrate-phosphate-dextrose-adenine-1 (CPDA-1). For in vitro studies, 5% supernatant was incubated with normal rat BM and cultured for erythroid (CFU-E) and granulocytemacrophage (CFU-GM) colony-forming units. Datawere compared with cultures of BMalone, 5% control plasma (negative control), and 12%CPDA-1. For in vivo studies, ratswere transfused with stored supernatants (5%estimated blood volume (EBV) over 30minutes). BM from each recipient was cultured for CFU-E and CFU-GM at 3 hours after transfusion. Data were compared with cultures of BM alone. Difference between groups determined by analysis of variance and Tukey's multiple comparison test. RESULTS: In vitro exposure to CPDA-1, control plasma, or 1-day supernatant (D1) had no effect on BM growth compared with BM alone. In vitro exposure to 14-day (D14) and 28-day (D28) supernatant significantly suppressed CFU-E by 60% and CFU-GMgrowth by 71% (both p < 0.05) comparedwithD1 ormedial alone.Therewere no differences betweenD14 andD28. Invivo exposure toD14 reducedBMCFU-Eand CFU-GM growth by 55% (both p < 0.05) compared with D1 supernatant. CONCLUSION: Plasma from aged blood adversely affects CFU-E and CFU-GMgrowth in rats. The effect is notmediated by CPDA-1. Transfusion of aged stored bloodmay contribute toBMdysfunction in critically ill patients, resulting in persistent anemia and the need for further transfusion. This BMdysfunction may also partly explain the observed increased susceptibility to infection.
机译:背景:创伤后,经常需要输注老化的血液,但会增加发病率和死亡率。尽管进行了血液置换,但许多患者的贫血时间较长,需要进一步输血。尚未研究老年血液对骨髓(BM)造血作用的影响,我们假设储存的血液会抑制BM功能。方法:将来自Sprague-Dawley大鼠的血液与工业防腐剂柠檬酸盐-磷酸-葡萄糖-腺嘌呤-1(CPDA-1)储存1、14或28天。为了进行体外研究,将5%的上清液与正常大鼠BM一起孵育,并培养出类红细胞(CFU-E)和粒细胞巨噬细胞(CFU-GM)集落形成单位。将数据与BMalone,5%对照血浆(阴性对照)和12%CPDA-1的培养物进行比较。为了进行体内研究,向大鼠输注储存的上清液(30分钟内估计血量(EBV)为5%)。在输血后3小时,将每个接受者的BM培养CFU-E和CFU-GM。将数据与单独的BM文化进行比较。通过方差分析和Tukey的多重比较检验确定的组之间差异。结果:与单独的BM相比,体外暴露于CPDA-1,对照血浆或1天的上清液(D1)对BM的生长没有影响。与单独使用D1或单独使用D1相比,在体外暴露于14天(D14)和28天(D28)的上清液可显着抑制CFU-E 60%和CFU-GM生长71%(p <0.05)。与D1上清液相比,D14的体内暴露使BMCFU-E和CFU-GM的生长降低了55%(均p <0.05)。结论:高龄血浆对大鼠CFU-E和CFU-GM的生长有不利影响。 CPDA-1不介导这种作用。在危重病人中输注老化的血液可能会导致BM功能障碍,导致持续性贫血和进一步输血的需要。这种BM功能障碍也可能部分解释了观察到的对感染的敏感性增加。

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