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CD73和AMPD3缺乏通过降低血红蛋白氧亲和力的红细胞ATP增强代谢性能。

CD73 and AMPD3 deficiency enhance metabolic performance via erythrocyte ATP that decreases hemoglobin oxygen affinity.

作者信息

O'Brien William G, Berka Vladimir, Tsai Ah-Lim, Zhao Zhaoyang, Lee Cheng Chi

机构信息

Department of Biochemistry and Molecular Biology, University of Texas Health Science Center, Houston, Texas, USA 77030.

Division of Hematology, Department of Internal Medicine, University of Texas Health Science Center, Houston, Texas, USA 77030.

出版信息

Sci Rep. 2015 Aug 7;5:13147. doi: 10.1038/srep13147.

Abstract

Erythrocytes are the key target in 5'-AMP induced hypometabolism. To understand how regulation of endogenous erythrocyte AMP levels modulates systemic metabolism, we generated mice deficient in both CD73 and AMPD3, the key catabolic enzymes for extracellular and intra-erythrocyte AMP, respectively. Under physiological conditions, these mice displayed enhanced capacity for physical activity accompanied by significantly higher food and oxygen consumption, compared to wild type mice. Erythrocytes from Ampd3(-/-) mice exhibited higher half-saturation pressure of oxygen (p50) and about 3-fold higher levels of ATP and ADP, while they maintained normal 2,3-bisphosphoglycerate (2,3-BPG), methemoglobin levels and intracellular pH. The affinity of mammalian hemoglobin for oxygen is thought to be regulated primarily by 2,3-BPG levels and pH (the Bohr effect). However, our results show that increased endogenous levels of ATP and ADP, but not AMP, directly increase the p50 value of hemoglobin. Additionally, the rise in erythrocyte p50 directly correlates with an enhanced capability of systemic metabolism.

摘要

红细胞是5'-AMP诱导的代谢减退的关键靶点。为了了解内源性红细胞AMP水平的调节如何影响全身代谢,我们培育了分别缺乏细胞外和红细胞内AMP关键分解代谢酶CD73和AMPD3的小鼠。在生理条件下,与野生型小鼠相比,这些小鼠表现出更强的体力活动能力,同时食物和氧气消耗量显著更高。Ampd3(-/-)小鼠的红细胞表现出更高的氧半饱和压力(p50)以及约3倍高的ATP和ADP水平,而它们的2,3-二磷酸甘油酸(2,3-BPG)、高铁血红蛋白水平和细胞内pH值保持正常。哺乳动物血红蛋白对氧的亲和力被认为主要受2,3-BPG水平和pH值(波尔效应)调节。然而,我们的结果表明,内源性ATP和ADP水平升高,而不是AMP,直接增加了血红蛋白的p50值。此外,红细胞p50的升高与全身代谢能力增强直接相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a6bb/4650700/a4b8f9d46cd7/srep13147-f1.jpg

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