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环ADP-碳环核糖和-4-硫代核糖,作为环ADP-核糖(一种钙动员第二信使)的稳定类似物。

Cyclic ADP-Carbocyclic-Ribose and -4-Thioribose, as Stable Mimics of Cyclic ADP-Ribose, a Ca-Mobilizing Second Messenger.

作者信息

Shuto Satoshi

机构信息

Faculty of Pharmaceutical Sciences, Hokkaido University.

出版信息

Chem Pharm Bull (Tokyo). 2018;66(2):155-161. doi: 10.1248/cpb.c17-00668.

Abstract

Cyclic ADP-ribose (cADPR), a general mediator involved in Ca signaling, has the characteristic 18-membered ring consisting of an adenine, two riboses and a pyrophosphate, in which the two primary hydroxy groups of the riboses are linked by a pyrophosphate unit. This review focuses on chemical synthetic studies of cADPR analogues of biological importance. Although cADPR analogues can be synthesized by enzymatic and chemo-enzymatic methods using ADP-ribosyl cyclase, the analogues obtained by these methods are limited due to the substrate-specificity of the enzymes. Consequently, chemical synthetic methods providing a greater variety of cADPR analogues are required. Although early chemical synthetic studies demonstrated that construction of the large 18-membered ring structure is difficult, the construction was achieved using the phenylthiophosphate-type substrates by treating with AgNO or I. This is now a general method for synthesizing these types of biologically important cyclic nucleotides. Using this method as the key step, the chemically and biologically stable cADPR mimic, cADP-carbocyclic-ribose (cADPcR) and -4-thioribose (cADPtR), were synthesized.

摘要

环磷酸腺苷核糖(cADPR)是参与钙信号传导的一种通用介质,其特征是具有由一个腺嘌呤、两个核糖和一个焦磷酸组成的18元环,其中核糖的两个伯羟基通过一个焦磷酸单元相连。本综述聚焦于具有生物学重要性的cADPR类似物的化学合成研究。虽然cADPR类似物可以通过使用ADP - 核糖基环化酶的酶法和化学酶法合成,但由于酶的底物特异性,通过这些方法获得的类似物有限。因此,需要能提供更多种类cADPR类似物的化学合成方法。尽管早期的化学合成研究表明构建大的18元环结构很困难,但通过用硝酸银或碘处理苯基硫代磷酸酯型底物实现了该结构的构建。这现在是合成这类具有生物学重要性的环核苷酸的通用方法。以该方法为关键步骤,合成了化学和生物学性质稳定的cADPR模拟物,即环化ADP - 碳环核糖(cADPcR)和 - 4 - 硫代核糖(cADPtR)。

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