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红细胞中腺嘌呤核苷酸的分解代谢途径。

Pathways of adenine nucleotide catabolism in erythrocytes.

作者信息

Bontemps F, Van den Berghe G, Hers H G

出版信息

J Clin Invest. 1986 Mar;77(3):824-30. doi: 10.1172/JCI112379.

Abstract

The exact pathway whereby the initial catabolism of the adenine nucleotides proceeds from AMP and the possibility of a recycling of adenosine were investigated in human erythrocytes. Adenine nucleotide catabolism, reflected by the production of hypoxanthine, is very slow under physiologic conditions and can be greatly increased by suppression of glucose or alkalinization of the medium. Experiments with inhibitors of adenosine deaminase and adenosine kinase demonstrated that under physiologic conditions the initial catabolism of AMP proceeds by way of a deamination of AMP, followed by dephosphorylation of inosine monophosphate, and that no recycling occurs between AMP and adenosine. Under glucose deprivation, approximately 75% of the 20-fold increase of the catabolism of the adenine nucleotides proceeded by way of a dephosphorylation of AMP followed by deamination of adenosine, and a small recycling of this nucleoside could be evidenced. Inhibition of adenosine transport showed that the dephosphorylation of AMP occurred intracellularly. When the incubation medium was alkalinized in the presence of glucose, the 15-fold increase in the conversion of AMP to hypoxanthine proceeded exclusively by way of AMP deaminase but a small recycling of adenosine could also be evidenced. The threefold elevation of intraerythrocytic inorganic phosphate (Pi) during glucose deprivation and its 50% decrease during alkalinization as well as experiments in which extracellular Pi was modified, indicate that the dephosphorylation of red blood cell AMP is mainly responsive to variations of AMP, whereas its deamination is more sensitive to Pi.

摘要

在人体红细胞中研究了腺嘌呤核苷酸从AMP开始的初始分解代谢的确切途径以及腺苷再循环的可能性。次黄嘌呤的产生反映了腺嘌呤核苷酸的分解代谢,在生理条件下非常缓慢,并且可以通过抑制葡萄糖或使培养基碱化而大大增加。使用腺苷脱氨酶和腺苷激酶抑制剂的实验表明,在生理条件下,AMP的初始分解代谢通过AMP脱氨,随后是肌苷单磷酸的去磷酸化进行,并且在AMP和腺苷之间没有再循环发生。在葡萄糖缺乏的情况下,腺嘌呤核苷酸分解代谢增加20倍,其中约75%是通过AMP去磷酸化,随后是腺苷脱氨进行的,并且可以证明这种核苷有少量再循环。腺苷转运的抑制表明AMP的去磷酸化发生在细胞内。当在葡萄糖存在下将孵育培养基碱化时,AMP向次黄嘌呤转化增加15倍完全是通过AMP脱氨酶进行的,但也可以证明有少量腺苷再循环。葡萄糖缺乏期间红细胞内无机磷酸盐(Pi)增加三倍,碱化期间减少50%,以及改变细胞外Pi的实验表明,红细胞AMP的去磷酸化主要对AMP的变化有反应,而其脱氨对Pi更敏感。

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