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培养的诺维科夫细胞对嘌呤和嘧啶的转运。转运的特异性、机制及其与磷酸核糖基化的关系。

Purine and pyrimidine transport by cultured Novikoff cells. Specificities and mechanism of transport and relationship to phosphoribosylation.

作者信息

Zylka J M, Plagemann P G

出版信息

J Biol Chem. 1975 Aug 10;250(15):5756-67.

PMID:168203
Abstract

Adenine, guanine, and hypoxanthine were rapidly incorporated into the acid-soluble nucleotide pool and nucleic acids by wild type Novikoff cells. Incorporation followed normal Michaelis-Menten kinetics, but the following evidence indicates that specific transport processes precede the phosphoribosyltransferase reactions and are the rate-limiting step in purine incorporation by whole cells. Cells of an azaguanine-resistant subline of Novikoff cells which lacked hypoxanthine-guanine phosphoribosyltransferase activity and failed to incorporate guanine or hypoxanthine into the nucleotide pool, exhibited uptake of guanine and hypoxanthine by a saturable process. Similarly, wild type cells which had been preincubated in a glucose-free basal medium containing KCN and iodoacetate transported guanine and hypoxanthine normally, although a conversion of these purines to nucleotides did not occur in these cells. The mutant and KCN-iodoacetate treated wild type cells also exhibited countertransport of guanine and hypoxanthine when preloaded with various purines, uracil, and pyrimidine nucleosides. The cells also possess a saturable transport system for uracil although they lack phosphoribosyltransferase activity for uracil. In the absence of phosphoribosylation, none of the substrates was accumulated against a concentration gradient. Thus transport is by facilitated diffusion (nonconcentrative transport). Furthermore, the apparent Km values for purine uptake by untreated wild type and azaguanine-resistant cells were higher and the apparent Vmax values were lower than those for the corresponding phosphoribosyltransferases...

摘要

腺嘌呤、鸟嘌呤和次黄嘌呤可被野生型诺维科夫细胞迅速掺入酸溶性核苷酸库和核酸中。掺入过程遵循正常的米氏动力学,但以下证据表明,特定的转运过程先于磷酸核糖基转移酶反应,并且是全细胞嘌呤掺入的限速步骤。诺维科夫细胞的一个对氮杂鸟嘌呤耐药的亚系细胞缺乏次黄嘌呤 - 鸟嘌呤磷酸核糖基转移酶活性,无法将鸟嘌呤或次黄嘌呤掺入核苷酸库,但却能通过一个可饱和过程摄取鸟嘌呤和次黄嘌呤。同样,在含有氰化钾和碘乙酸盐的无糖基础培养基中预孵育的野生型细胞,尽管这些嘌呤在这些细胞中不会转化为核苷酸,但仍能正常转运鸟嘌呤和次黄嘌呤。当预先加载各种嘌呤、尿嘧啶和嘧啶核苷时,突变细胞以及经氰化钾 - 碘乙酸盐处理的野生型细胞也表现出鸟嘌呤和次黄嘌呤的反向转运。这些细胞虽然缺乏尿嘧啶的磷酸核糖基转移酶活性,但对尿嘧啶也具有一个可饱和的转运系统。在没有磷酸核糖化的情况下,没有一种底物能逆浓度梯度积累。因此,转运是通过易化扩散(非浓缩性转运)进行的。此外,未经处理的野生型细胞和对氮杂鸟嘌呤耐药的细胞摄取嘌呤的表观米氏常数较高,而表观最大反应速度值低于相应的磷酸核糖基转移酶的表观最大反应速度值……

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