Role of Zinc in Isoform-Selective Inhibitor Binding to Neuronal Nitric Oxide Synthase,

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Role of Zinc in Isoform-Selective Inhibitor Binding to Neuronal Nitric Oxide Synthase,

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作者：Silvia L. Delker ; Fengtian Xue ; Huiying Li ; Joumana Jamal ; Richard B. Silverman ; Thomas L. Poulos
刊名：Biochemistry
出版年：2010
出版时间：December 28, 2010
年：2010
卷：49
期：51
页码：10803-10810
全文大小：1058K
年卷期：v.49,no.51(December 28, 2010)
ISSN：1520-4995

文摘

In previous studies [Delker, S. L., et al. (2010), J. Am. Chem. Soc. 132, 5437−5442], we determined the crystal structures of neuronal nitric oxide synthase (nNOS) in complex with nNOS-selective chiral pyrrolidine inhibitors, designed to have an aminopyridine group bound over the heme where it can electrostatically interact with the conserved active site Glu residue. However, in addition to the expected binding mode with the (S,S)-cis inhibitors, an unexpected “flipped” orientation was observed for the (R,R)-cis enantiomers. In the flipped mode, the aminopyridine extends out of the active site where it interacts with one heme propionate. This prompted us to design and synthesize symmetric “double-headed” inhibitors with an aminopyridine at each end of a bridging ring structure [Xue, F., Delker, S. L., Li, H., Fang, J., Jamal, J., Martsek, P., Roman, L. J., Poulos, T. L., and Silverman, R. B. Symmetric double-headed aminopyridines, a novel strategy for potent and membrane-permeable inhibitors of neuronal nitric oxide synthase. J. Med. Chem. (submitted for publication)]. One aminopyridine should interact with the active site Glu and the other with the heme propionate. Crystal structures of these double-headed aminopyridine inhibitors in complexes with nNOS show unexpected and significant protein and heme conformational changes induced by inhibitor binding that result in removal of the tetrahydrobiopterin (H₄B) cofactor and creation of a new Zn²⁺ site. These changes are due to binding of a second inhibitor molecule that results in the displacement of H₄B and the placement of the inhibitor pyridine group in position to serve as a Zn²⁺ ligand together with Asp, His, and a chloride ion. Binding of the second inhibitor molecule and generation of the Zn²⁺ site do not occur in eNOS. Structural requirements for creation of the new Zn²⁺ site in nNOS were analyzed in detail. These observations open the way for the potential design of novel inhibitors selective for nNOS.