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Structural basis for dipeptide amide isoform-selective inhibition of neuronal nitric oxide synthase
- Authors
- Flinspach, Mack L.; Li, Huiying; Jamal, Joumana; Yang, Weiping; Huang, Hui; Hah, Jung-Mi; Gómez-Vidal, José Antonio; Litzinger, Elizabeth A.; Silverman, Richard B.; Poulos, Thomas L.
- Issue Date
- Jan-2004
- Publisher
- NATURE PUBLISHING GROUP
- Citation
- NATURE STRUCTURAL & MOLECULAR BIOLOGY, v.11, no.1, pp 54 - 59
- Pages
- 6
- Indexed
- SCIE
SCOPUS
- Journal Title
- NATURE STRUCTURAL & MOLECULAR BIOLOGY
- Volume
- 11
- Number
- 1
- Start Page
- 54
- End Page
- 59
- ISSN
- 1545-9993
1545-9985
- Abstract
- Three nitric oxide synthase (NOS) isoforms, eNOS, nNOS and iNOS, generate nitric oxide (NO) crucial to the cardiovascular, nervous and host defense systems, respectively. Development of isoform-selective NOS inhibitors is of considerable therapeutic importance. Crystal structures of nNOS-selective dipeptide inhibitors in complex with both nNOS and eNOS were solved and the inhibitors were found to adopt a curled conformation in nNOS but an extended conformation in eNOS. We hypothesized that a single-residue difference in the active site, Asp597 (nNOS) versus Asn368 (eNOS), is responsible for the favored binding in nNOS. In the D597N nNOS mutant crystal structure, a bound inhibitor switches to the extended conformation and its inhibition of nNOS decreases >200-fold. Therefore, a single-residue difference is responsible for more than two orders of magnitude selectivity in inhibition of nNOS over eNOS by L-N-omega-nitroarginine-containing dipeptide inhibitors.
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Related Researcher
- Hah, Jung Mi
- COLLEGE OF PHARMACY (DEPARTMENT OF PHARMACY)