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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Mapping the ribonucleolytic active site of bovine seminal ribonuclease. The binding of pyrimidinyl phosphonucleotide inhibitors.
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Mapping the ribonucleolytic active site of bovine seminal ribonuclease. The binding of pyrimidinyl phosphonucleotide inhibitors.

机译:映射牛精原核糖核酸酶的核糖核酸水解活性位点。嘧啶基磷酸核苷酸抑制剂的结合。

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摘要

Bovine seminal ribonuclease (BS-RNase) is a 27kDa homodimeric enzyme and a member of the pancreatic RNase A superfamily. It is the only RNase with a quaternary structure and it is a mixture of two dimeric forms. In the most abundant form the active site is formed by the swapping of the N-terminal segments. BS-RNase is a potent antitumor agent with severe side effects such as aspermatogenicity, and immunosuppression. As a first step towards the design of potent inhibitors of this enzyme we mapped its active site through the study of the binding of uridine 2'-phosphate (U2'p), uridine 3'-phosphate (U3'p), uridine 5'-diphosphate (UDP), cytidine 3'-phosphate (C3'p), and cytidine 5-phosphate (C5'p), by kinetics, and X-ray crystallography. These phosphonucleotides are potent inhibitors with C3'p being the most potent with a K(i) value of 22 microM. Absorption, distribution, metabolism, and excretion pharmacokinetic property predictions reveal U2'p, U3'p, and C5'p as the most promising with respect to oral bioavailability. In vivo studies on the aspermatogenic effect have shown that C3'p and C5'p inhibit significantly this biological action of BS-RNase.
机译:牛精原核糖核酸酶(BS-RNase)是一种27kDa的同型二聚酶,是胰腺RNase A超家族的成员。它是唯一具有四级结构的RNase,并且是两种二聚体形式的混合物。活性部位以最丰富的形式通过N末端片段的交换形成。 BS-RNase是一种有效的抗肿瘤药物,具有严重的副作用,例如生精和免疫抑制。作为设计该酶有效抑制剂的第一步,我们通过研究尿苷2'-磷酸(U2'p),尿苷3'-磷酸(U3'p),尿苷5'的结合来绘制其活性位点-二磷酸(UDP),胞苷3'-磷酸(C3'p)和胞苷5-磷酸(C5'p),通过动力学和X射线晶体学分析。这些磷酸核苷酸是有效的抑制剂,其中C3'p最有效,其K(i)值为22 microM。吸收,分布,代谢和排泄的药代动力学特性预测表明,就口服生物利用度而言,U2'p,U3'p和C5'p是最有希望的。体内对生精作用的研究表明,C3'p和C5'p显着抑制BS-RNase的这种生物学作用。

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