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人胸苷激酶2:抗病毒和细胞抑制性核苷底物的酶活性分子克隆及特性分析

Human thymidine kinase 2: molecular cloning and characterisation of the enzyme activity with antiviral and cytostatic nucleoside substrates.

作者信息

Wang L, Munch-Petersen B, Herrström Sjöberg A, Hellman U, Bergman T, Jörnvall H, Eriksson S

机构信息

Department of Veterinary Medical Chemistry, Swedish University of Agricultural Sciences, Biomedical Center, Uppsala.

出版信息

FEBS Lett. 1999 Jan 25;443(2):170-4. doi: 10.1016/s0014-5793(98)01711-6.

Abstract

Based on amino acid sequence information from purified mitochondrial thymidine kinase (TK2), a cDNA of 1930 bp was cloned, containing an open reading frame encoding 232 amino acid residues starting with the N-terminal sequence determined from the native human protein preparation. Northern blot analysis with the cDNA coding region demonstrated several TK2 mRNAs, with 2 and 4 kb forms present in many tissues. We also characterised N-terminally truncated (starting at position 18) human TK2 with pharmacologically important antiviral and cytostatic nucleoside analogues. Results were highly similar to those with the native TK2 preparation. The anti-leukaemic drug arabinosyl cytosine is phosphorylated. The antitumour drug difluorodeoxycytidine and its metabolite difluorodeoxyuridine are good substrates, with K(m) values of 66 and 29 microM, respectively, and a relative Vmax of 0.6 compared to that of thymidine. Negative cooperativity was found with thymidine and the anti-HIV drug 3'-azidothymidine, but the reaction followed Michaelis-Menten kinetics with deoxycytidine, arabinosyl cytosine, and arabinosyl thymine. The results demonstrate a broad substrate specificity and complex kinetics, and suggest a role for TK2 in the activation of chemotherapeutic nucleoside analogues.

摘要

基于纯化的线粒体胸苷激酶(TK2)的氨基酸序列信息,克隆了一个1930 bp的cDNA,其包含一个开放阅读框,编码232个氨基酸残基,起始于从天然人源蛋白制品中确定的N端序列。用该cDNA编码区进行的Northern印迹分析显示了几种TK2 mRNA,在许多组织中存在2 kb和4 kb的形式。我们还用具有重要药理学意义的抗病毒和细胞抑制核苷类似物对N端截短(从第18位开始)的人TK2进行了表征。结果与天然TK2制品的结果高度相似。抗白血病药物阿糖胞苷被磷酸化。抗肿瘤药物二氟脱氧胞苷及其代谢产物二氟脱氧尿苷是良好的底物,K(m)值分别为66和29 microM,与胸苷相比相对Vmax为0.6。发现与胸苷和抗HIV药物3'-叠氮胸苷存在负协同性,但与脱氧胞苷、阿糖胞苷和阿糖胸腺嘧啶的反应遵循米氏动力学。结果表明其具有广泛的底物特异性和复杂的动力学,并提示TK2在化疗核苷类似物的激活中起作用。

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