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膜蛋白的周转:大鼠肝脏微粒体细胞色素P-450七种形式、NADPH-细胞色素P-450还原酶和环氧水解酶的诱导和降解动力学。

Turnover of membrane proteins: kinetics of induction and degradation of seven forms of rat liver microsomal cytochrome P-450, NADPH-cytochrome P-450 reductase, and epoxide hydrolase.

作者信息

Shiraki H, Guengerich F P

出版信息

Arch Biochem Biophys. 1984 Nov 15;235(1):86-96. doi: 10.1016/0003-9861(84)90257-1.

Abstract

The in vivo turnover of several rat liver microsomal proteins was studied using techniques designed to maximize antibody recognition specificity and minimize reutilization of radioactive labels. The kinetics of degradation of seven cytochrome P-450 isozymes, NADPH-cytochrome P-450 reductase, and epoxide hydrolase were determined in untreated rats and rats treated with phenobarbital or beta-naphthoflavone. In the cases where induction of these enzymes occurred with the above chemicals, rates of synthesis of the proteins were also estimated. In general, the degradation rates of the different proteins were rather similar to each other, and the effects of phenobarbital and beta-naphthoflavone on these rates were not very great. However, in the case of cytochromes P-450, a general trend was observed in which the heme moiety was degraded more rapidly than the apoprotein. Changes in the rates of synthesis of the individual proteins appear to contribute more to the altered steady-state levels which are expressed than do the rates of degradation, and profiles of steady-state enzyme concentrations predicted by the kinetic constants approximate those observed in vivo.

摘要

利用旨在最大化抗体识别特异性并最小化放射性标记再利用的技术,研究了几种大鼠肝脏微粒体蛋白的体内周转率。在未处理的大鼠以及用苯巴比妥或β-萘黄酮处理的大鼠中,测定了七种细胞色素P-450同工酶、NADPH-细胞色素P-450还原酶和环氧水解酶的降解动力学。在这些酶被上述化学物质诱导的情况下,还估计了蛋白质的合成速率。一般来说,不同蛋白质的降解速率彼此相当相似,苯巴比妥和β-萘黄酮对这些速率的影响不是很大。然而,在细胞色素P-450的情况下,观察到一个普遍趋势,即血红素部分比脱辅基蛋白降解得更快。各个蛋白质合成速率的变化似乎比降解速率对所表达的稳态水平变化的贡献更大,并且由动力学常数预测的稳态酶浓度曲线与体内观察到的曲线近似。

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