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The kinetic dissection of transport from metabolic trapping during substrate uptake by intact cells. Uridine uptake by quiescent and serum-activated Nil 8 hamster cells and their murine sarcoma virus-transformed counterparts.

作者信息

Heichal O, Ish-Shalom D, Koren R, Stein W D

出版信息

Biochim Biophys Acta. 1979 Feb 20;551(1):169-86. doi: 10.1016/0005-2736(79)90363-8.

DOI:10.1016/0005-2736(79)90363-8
PMID:218628
Abstract
  1. We present a theoretical analysis of the tandem processes of transport and metabolic trapping which together constitute uptake of a substrate by intact cells. 2. Transport is assumed to occur by means of a simple carrier here analysed in its general form. Trapping is assumed to occur by a simple enzymic reaction. 3. We show how to obtain the separate parameters of the steps by analysing uptake data over a range of uptake times and substrate concentrations. 4. We present uptake data for uridine and cytosine-beta-D-arabinoside entering Nil 8 hamster fibroblasts, normal and murine sarcoma virus transformed, in the quiescent condition and after stimulation by added serum. We analyse the data in terms of the theory for tandem processes. 5. Transport is characterised by a system having a high Km and a high V for entry. The data for cytosine-beta-D-arabinoside suggest that the cytosine-beta-D-arabinoside system is not far from a symmetric one. The data for uridine transport do not differ when quiescent and serum-activated cells are compared. Transformed cells transport uridine at half the maximum velocity of normal cells, with or without added serum. 6. Trapping of cytosine-beta-D-arabinoside is insignificant. Trapping of uridine occurs by a system with both V and Km at least an order of magnitude smaller than are these parameters for transport. Trapping of uridine by non-transformed cells activated by serum, has twice the V of such cells in the quiescent state. 7. In the virus-transformed cells, the control of uridine trapping by added serum is lost, along with control of growth by this stimulant.
摘要

相似文献

1
The kinetic dissection of transport from metabolic trapping during substrate uptake by intact cells. Uridine uptake by quiescent and serum-activated Nil 8 hamster cells and their murine sarcoma virus-transformed counterparts.
Biochim Biophys Acta. 1979 Feb 20;551(1):169-86. doi: 10.1016/0005-2736(79)90363-8.
2
S-substituted derivatives of 6-mercaptopurine ribosides interact both with the transport and metabolic phosphorylation of uridine by virus-transformed hamster fibroblasts.
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A kinetic analysis of the uptake of cytosine-beta-D-arabinoside by rat-B77 cells. Differentiation between transport and phosphorylation.大鼠B77细胞对胞嘧啶-β-D-阿拉伯糖苷摄取的动力学分析。转运与磷酸化的区分。
Eur J Biochem. 1979 Apr 2;95(2):333-9. doi: 10.1111/j.1432-1033.1979.tb12970.x.
4
Distinct properties of uridine transport systems in growing, quiescent and serum-stimulated hamster embryo cells.
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Nucleoside transport in mammalian cell membranes. III. Kinetic and chemical modification studies of cytosine-arabinoside and uridine transport in hamster cells in culture.哺乳动物细胞膜中的核苷转运。III. 培养的仓鼠细胞中阿糖胞苷和尿苷转运的动力学及化学修饰研究。
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Temperature dependence of uridine transport in quiescent and serum-stimulated 3T3 cells.静止和血清刺激的3T3细胞中尿苷转运的温度依赖性
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Investigations on the mechanism of induction of the alkaline phosphatase by bromodesoxyuridine in herpes simplex virus transformed cells and the transport of uridine.对溴脱氧尿苷在单纯疱疹病毒转化细胞中诱导碱性磷酸酶的机制及尿苷转运的研究。
Z Naturforsch C Biosci. 1980 Nov-Dec;35(11-12):1036-45. doi: 10.1515/znc-1980-11-1230.
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The kinetics of dissociation of the inhibitor of nucleoside transport, nitrobenzylthioinosine, from the high-affinity binding sites of cultured hamster cells.核苷转运抑制剂硝基苄硫基肌苷从培养的仓鼠细胞高亲和力结合位点解离的动力学。
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10
Magnesium ions and serum activation of uridine uptake by quiescent hamster fibroblasts.
FEBS Lett. 1979 Oct 1;106(1):149-52. doi: 10.1016/0014-5793(79)80715-2.

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