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AICA-核苷对人B淋巴母细胞嘌呤代谢的影响。

Alteration of purine metabolism by AICA-riboside in human B lymphoblasts.

作者信息

Barankiewicz J, Jimenez R, Ronlov G, Magill M, Gruber H E

机构信息

Gensia Pharmaceuticals, Inc., Research Department, San Diego, California 92121.

出版信息

Arch Biochem Biophys. 1990 Nov 1;282(2):377-85. doi: 10.1016/0003-9861(90)90132-i.

Abstract

The effect of 5-amino-4-imidazole-carboximide (AI-CA)-riboside on different pathways of purine metabolism (biosynthesis de novo, salvage pathways, adenosine metabolism, ATP catabolism) was studied in human B lymphoblasts (WI-L2). AICA-Riboside markedly decreased intracellular levels of 5-phosphoribosyl-1-pyrophosphate and in consequence affected purine biosynthesis de novo and purine salvage pathways. AICA-riboside inhibited incorporation of glycine into purine nucleotides, but when formate was used as the precursor of purine biosynthesis de novo, a biphasic effect was observed. The incorporation of formate into purine nucleotides was increased by AICA-riboside at concentrations up to 2 mM but decreased at higher concentrations. Salvage of the purine bases adenine, hypoxanthine, and guanine was markedly inhibited and utilization of extracellular adenosine in B lymphoblasts was reduced by AICA-riboside. AICA-riboside increased ribose 1-phosphate concentrations and increased degradation of prelabeled ATP. No effect on the intracellular levels of orthophosphate was found. Proliferation of WI-L2 lymphoblasts was only slightly affected at concentrations of AICA-riboside below 500 microM but markedly inhibited by higher concentrations.

摘要

研究了5-氨基-4-咪唑甲酰胺(AICA)-核苷对人B淋巴母细胞(WI-L2)嘌呤代谢不同途径(从头合成、补救途径、腺苷代谢、ATP分解代谢)的影响。AICA-核苷显著降低了5-磷酸核糖-1-焦磷酸的细胞内水平,从而影响嘌呤的从头合成和嘌呤补救途径。AICA-核苷抑制甘氨酸掺入嘌呤核苷酸,但当甲酸用作嘌呤从头合成的前体时,观察到双相效应。在浓度高达2 mM时,AICA-核苷可增加甲酸掺入嘌呤核苷酸的量,但在更高浓度时则减少。嘌呤碱基腺嘌呤、次黄嘌呤和鸟嘌呤的补救显著受到抑制,AICA-核苷降低了B淋巴母细胞中细胞外腺苷的利用。AICA-核苷增加了1-磷酸核糖的浓度,并增加了预先标记的ATP的降解。未发现对细胞内正磷酸盐水平有影响。在AICA-核苷浓度低于500 microM时,WI-L2淋巴母细胞的增殖仅受到轻微影响,但更高浓度则显著抑制。

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