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一种利用NAD的酶——人类CD38的共价和非共价中间体

Covalent and noncovalent intermediates of an NAD utilizing enzyme, human CD38.

作者信息

Liu Qun, Kriksunov Irina A, Jiang Hong, Graeff Richard, Lin Hening, Lee Hon Cheung, Hao Quan

机构信息

MacCHESS, Cornell High Energy Synchrotron Source, Department of Chemistry and Chemical Biology, School of Applied & Engineering Physics, Cornell University, Ithaca, NY 14853, USA.

出版信息

Chem Biol. 2008 Oct 20;15(10):1068-78. doi: 10.1016/j.chembiol.2008.08.007.

Abstract

Enzymatic utilization of nicotinamide adenine dinucleotide (NAD) has increasingly been shown to have fundamental roles in gene regulation, signal transduction, and protein modification. Many of the processes require the cleavage of the nicotinamide moiety from the substrate and the formation of a reactive intermediate. Using X-ray crystallography, we show that human CD38, an NAD-utilizing enzyme, is capable of catalyzing the cleavage reactions through both covalent and noncovalent intermediates, depending on the substrate used. The covalent intermediate is resistant to further attack by nucleophiles, resulting in mechanism-based enzyme inactivation. The noncovalent intermediate is stabilized mainly through H-bond interactions, but appears to remain reactive. Our structural results favor the proposal of a noncovalent intermediate during normal enzymatic utilization of NAD by human CD38 and provide structural insights into the design of covalent and noncovalent inhibitors targeting NAD-utilization pathways.

摘要

烟酰胺腺嘌呤二核苷酸(NAD)的酶促利用越来越多地被证明在基因调控、信号转导和蛋白质修饰中具有重要作用。许多过程需要从底物上切割烟酰胺部分并形成反应性中间体。通过X射线晶体学,我们表明人类CD38(一种利用NAD的酶)能够根据所使用的底物,通过共价和非共价中间体催化切割反应。共价中间体对亲核试剂的进一步攻击具有抗性,导致基于机制的酶失活。非共价中间体主要通过氢键相互作用稳定,但似乎仍具有反应性。我们的结构结果支持在人类CD38正常酶促利用NAD过程中存在非共价中间体的提议,并为设计靶向NAD利用途径的共价和非共价抑制剂提供了结构见解。

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