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氘化对小鼠造血作用的影响。

Effects of deuteration on hematopoiesis in the mouse.

作者信息

Adams W H, Adams D G

机构信息

Medical Department, Brookhaven National Laboratory, Upton, New York.

出版信息

J Pharmacol Exp Ther. 1988 Feb;244(2):633-9.

PMID:2831349
Abstract

Mice ingesting 30 to 50% D2O (heavy water, deuterium oxide) developed a dose-dependent depression of formed peripheral blood elements in 4 to 9 days. The principal mechanism of anemia and thrombocytopenia is impaired hematopoiesis. Despite pancytopenia in the peripheral blood, bone marrow cellularity and morphology remained normal. Upon replacement of D2O with tap water, platelet and neutrophil concentrations returned to normal within 48 to 72 hr. In contrast, blood lymphocyte concentrations remained low for several weeks. B-lymphocytes may be more affected by deuteration than other lymphocyte subsets. In vivo reticuloendothelial cell function, as assessed by 51Cr-labeled sheep erythrocyte clearance, was unaffected by D2O. Although a dose-dependent decrease in fluid intake occurred during deuteration, hematocytopenia was not a consequence of dehydration. In view of the known kinetics of D2O in biological systems, the rapid response of myeloid elements to deuteration must be due primarily to the solvent (nonmetabolic) isotope effect. Prolonged deuteration has proven toxic when included in regimens for treatment of neoplasia, including leukemia, in animal models. The present study shows that modulation of hematopoiesis by D2O is possible without invoking the toxicities associated with prolonged deuteration.

摘要

摄入30%至50%重水(氧化氘)的小鼠在4至9天内出现了外周血有形成分剂量依赖性减少。贫血和血小板减少的主要机制是造血功能受损。尽管外周血全血细胞减少,但骨髓细胞密度和形态仍保持正常。用自来水替代重水后,血小板和中性粒细胞浓度在48至72小时内恢复正常。相比之下,血液淋巴细胞浓度在数周内一直较低。B淋巴细胞可能比重其他淋巴细胞亚群更容易受到氘化的影响。通过51Cr标记的绵羊红细胞清除率评估的体内网状内皮细胞功能不受重水影响。虽然在氘化过程中出现了剂量依赖性的液体摄入量减少,但血细胞减少并非脱水所致。鉴于重水在生物系统中的已知动力学,髓系成分对氘化的快速反应主要必定是由于溶剂(非代谢)同位素效应。在动物模型中,当重水被纳入包括白血病在内的肿瘤治疗方案时,长期氘化已被证明具有毒性。本研究表明,重水有可能调节造血功能,而不会引发与长期氘化相关的毒性。

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