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从血红蛋白生成 S-亚硝基硫醇:机制、构象依赖性和生理相关性。

Generating S-nitrosothiols from hemoglobin: mechanisms, conformational dependence, and physiological relevance.

机构信息

Department of Physiology and Biophysics, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

J Biol Chem. 2013 Aug 2;288(31):22408-25. doi: 10.1074/jbc.M113.482679. Epub 2013 Jun 17.

DOI:10.1074/jbc.M113.482679
PMID:23775069
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3829331/
Abstract

In vitro, ferrous deoxy-hemes in hemoglobin (Hb) react with nitrite to generate nitric oxide (NO) through a nitrite reductase reaction. In vivo studies indicate Hb with nitrite can be a source of NO bioactivity. The nitrite reductase reaction does not appear to account fully for this activity because free NO is short lived especially within the red blood cell. Thus, the exporting of NO bioactivity both out of the RBC and over a large distance requires an additional mechanism. A nitrite anhydrase (NA) reaction in which N2O3, a potent S-nitrosating agent, is produced through the reaction of NO with ferric heme-bound nitrite has been proposed (Basu, S., Grubina, R., Huang, J., Conradie, J., Huang, Z., Jeffers, A., Jiang, A., He, X., Azarov, I., Seibert, R., Mehta, A., Patel, R., King, S. B., Hogg, N., Ghosh, A., Gladwin, M. T., and Kim-Shapiro, D. B. (2007) Nat. Chem. Biol. 3, 785-794) as a possible mechanism. Legitimate concerns, including physiological relevance and the nature of the mechanism, have been raised concerning the NA reaction. This study addresses these concerns demonstrating NO and nitrite with ferric hemes under near physiological conditions yield an intermediate having the properties of the purported NA heme-bound N2O3 intermediate. The results indicate that ferric heme sites, traditionally viewed as a source of potential toxicity, can be functionally significant, especially for partially oxygenated/partially met-R state Hb that arises from the NO dioxygenation reaction. In the presence of low levels of nitrite and either NO or a suitable reductant such as L-cysteine, these ferric heme sites can function as a generator for the formation of S-nitrosothiols such as S-nitrosoglutathione and, as such, should be considered as a source of RBC-derived and exportable bioactive NO.

摘要

在体外,血红蛋白(Hb)中的亚铁脱氧血红素与亚硝酸盐通过亚硝酸盐还原酶反应生成一氧化氮(NO)。体内研究表明,含有亚硝酸盐的 Hb 可以作为 NO 生物活性的来源。亚硝酸盐还原酶反应似乎不能完全解释这种活性,因为游离的 NO 尤其是在红细胞内寿命很短。因此,NO 生物活性的输出不仅要离开 RBC,而且要经过很大的距离,这需要额外的机制。已经提出了一种亚硝酸盐脱水酶(NA)反应,其中通过 NO 与铁结合的亚硝酸盐反应生成 N2O3,这是一种有效的 S-亚硝酰化剂(Basu,S.,Grubina,R.,Huang,J.,Conradie,J.,Huang,Z.,Jeffers,A.,Jiang,A.,He,X.,Azarov,I.,Seibert,R.,Mehta,A.,Patel,R.,King,S. B.,Hogg,N.,Ghosh,A.,Gladwin,M. T.,and Kim-Shapiro,D. B.(2007)Nat. Chem. Biol. 3,785-794)作为一种可能的机制。已经提出了一些合理的担忧,包括生理学相关性和机制的性质,涉及 NA 反应。本研究解决了这些担忧,证明在接近生理条件下,带有铁血红素的 NO 和亚硝酸盐会产生具有所推测的 NA 血红素结合的 N2O3 中间体的性质的中间产物。结果表明,铁血红素位点,传统上被视为潜在毒性的来源,可以具有功能意义,特别是对于部分氧合/部分 met-R 状态的 Hb,这是由 NO 双加氧酶反应产生的。在低水平的亚硝酸盐和 NO 或合适的还原剂(如 L-半胱氨酸)存在下,这些铁血红素位点可以作为形成 S-亚硝酰硫醇(如 S-亚硝基谷胱甘肽)的生成器发挥作用,因此应被视为 RBC 衍生和可输出的生物活性 NO 的来源。

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