首页> 外文期刊>Journal of Inorganic Biochemistry: An Interdisciplinary Journal >Anaerobic iron deposition into horse spleen, recombinant human heavy and light and bacteria ferritins by large oxidants
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Anaerobic iron deposition into horse spleen, recombinant human heavy and light and bacteria ferritins by large oxidants

机译:厌氧铁沉积在马脾,重组人的体重和体重中以及铁蛋白被大氧化剂氧化

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Large-molecule oxidants oxidize Fe(II) to form Fe(III) cores in the interior of ferritins at rates comparable to or faster than the iron deposition reaction using O(2) as oxidant. Iron deposition into horse spleen ferritin (HoSF) occurs using ferricyanide ion, 2,6-dichlorophenol-indophenol, and several redox proteins: cytochrome c, stellacyanin, and ceruloplasmin. Cytochrome c also loads iron into recombinant human H-chain (rHF), human L-chain (rLF), and A. vinelandii bacterioferritin (AvBF). The enzymatic activities of ferritins were monitored anaerobically using stopped-flow kinetic spectrophotometry. The reactions exhibit saturation kinetics with respect to the large oxidant concentrations, giving apparent Michaelis constants for cytochrome c as oxidant: K(m)=39.6 microM for HoSF and 6.9 microM for AvBF. Comparison of the kinetic parameters with that of iron deposition by O(2) shows that large oxidants load iron into HoSF and AvBF more effectively than O(2) and may use a mechanism different than the ferroxidase center. Large oxidants did not deposit iron as efficiently with rHF and rLF. The results suggest that the heme groups in AvBF and the protein redox centers present in heteropolymers may assist in anaerobic iron deposition by large oxidants. The physiological relevance of iron deposition by large molecules, including protein oxidants is discussed.
机译:大分子氧化剂在铁蛋白内部氧化Fe(II)形成Fe(III)核,其速率与使用O(2)作为氧化剂的铁沉积反应相当或更快。铁沉积在马脾铁蛋白(HoSF)中是通过使用铁氰化物离子,2,6-二氯苯酚-吲哚酚和几种氧化还原蛋白进行的:细胞色素c,恒星蓝蛋白和铜蓝蛋白。细胞色素c还将铁加载到重组人H链(rHF),人L链(rLF)和藤蔓曲霉细菌铁蛋白(AvBF)中。使用停止流动力学分光光度法厌氧监测铁蛋白的酶活性。该反应相对于较大的氧化剂浓度表现出饱和动力学,从而给出了作为氧化剂的细胞色素c的表观米氏常数:对于HoSF,K(m)= 39.6 microM,对于AvBF,6.9 microM。动力学参数与O(2)沉积铁的动力学参数的比较表明,大氧化剂比O(2)更有效地将铁加载到HoSF和AvBF中,并且可能使用的机制不同于亚铁氧化酶中心。大型氧化剂不能通过rHF和rLF高效地沉积铁。结果表明,AvBF中的血红素基团和杂聚物中存在的蛋白质氧化还原中心可能有助于大型氧化剂对厌氧铁的沉积。讨论了由大分子(包括蛋白质氧化剂)沉积铁的生理相关性。

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