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The hemerythrin-like diiron protein from Mycobacterium kansasii is a nitric oxide peroxidase
Authors:Zhongxin Ma  Ashley A. Holland  Ilana Szlamkowicz  Vasileios Anagnostopoulos  Maria Luiza Caldas Nogueira  Jonathan D. Caranto  Victor L. Davidson
Affiliation:1.Burnett School of Biomedical Sciences, College of Medicine, University of Central Florida, Orlando, Florida, USA;2.Department of Chemistry, University of Central Florida, Orlando, Florida, USA
Abstract:The hemerythrin-like protein from Mycobacterium kansasii (Mka HLP) is a member of a distinct class of oxo-bridged diiron proteins that are found only in mycobacterial species that cause respiratory disorders in humans. Because it had been shown to exhibit weak catalase activity and a change in absorbance on exposure to nitric oxide (NO), the reactivity of Mka HLP toward NO was examined under a variety of conditions. Under anaerobic conditions, we found that NO was converted to nitrite (NO2) via an intermediate, which absorbed light at 520 nm. Under aerobic conditions NO was converted to nitrate (NO3). In each of these two cases, the maximum amount of nitrite or nitrate formed was at best stoichiometric with the concentration of Mka HLP. When incubated with NO and H2O2, we observed NO peroxidase activity yielding nitrite and water as reaction products. Steady-state kinetic analysis of NO consumption during this reaction yielded a Km for NO of 0.44 μM and a kcat/Km of 2.3 × 105 M−1s−1. This high affinity for NO is consistent with a physiological role for Mka HLP in deterring nitrosative stress. This is the first example of a peroxidase that uses an oxo-bridged diiron center and a rare example of a peroxidase utilizing NO as an electron donor and cosubstrate. This activity provides a mechanism by which the infectious Mycobacterium may combat against the cocktail of NO and superoxide (O2•−) generated by macrophages to defend against bacteria, as well as to produce NO2 to adapt to hypoxic conditions.
Keywords:catalase   mycobacteria   nonheme iron   nitric oxide oxidase   nitric oxide dioxygenase   nitrosylation   tuberculosis
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