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被抗坏血酸还原的醌类的氧化还原循环。

Redox cycling of quinones reduced by ascorbic acid.

作者信息

Njus David, Asmaro Karam, Li Guoliang, Palomino Eduardo

机构信息

Department of Biological Sciences, Wayne State University, Detroit, MI, 48202, USA.

Department of Biological Sciences, Wayne State University, Detroit, MI, 48202, USA.

出版信息

Chem Biol Interact. 2023 Mar 1;373:110397. doi: 10.1016/j.cbi.2023.110397. Epub 2023 Feb 9.

Abstract

In aqueous solutions containing ascorbic acid and O, many quinones undergo reduction to the semiquinone followed by reoxidation. This redox cycling mediates the oxidation of ascorbic acid and the reduction of O to superoxide and ultimately hydrogen peroxide. For that reason, redox cycling has attracted attention as a source of reactive oxygen species. This redox cycling is paradoxical, however, because the one-equivalent reduction potentials of the reactants are unfavorable, so the concentrations of the products, monodehydroascorbate and superoxide, must be kept extremely low. Disproportionation is not fast enough to eliminate these products. We have investigated the mechanism of ascorbate-driven redox cycling by monitoring the redox status of the quinone and the rate of redox cycling in parallel. Evidence is presented for a mechanism in which monodehydroascorbate is oxidized by the semiquinone. The result is that cycling of the semiquinone and hydroquinone mediates a rapid disproportionation of monodehydroascorbate. This mechanism accounts for the dependence of the redox cycling rate on quinone and ascorbate concentrations as well as on the reduction potential of the quinone. Therefore, it predicts how fast ascorbate-driven redox cycling will generate hydrogen peroxide under a variety of conditions and with different quinones.

摘要

在含有抗坏血酸和氧的水溶液中,许多醌会先还原为半醌,然后再重新氧化。这种氧化还原循环介导了抗坏血酸的氧化以及氧还原为超氧化物,最终生成过氧化氢。因此,氧化还原循环作为活性氧的一个来源已引起关注。然而,这种氧化还原循环是自相矛盾的,因为反应物的单电子还原电位不利,所以产物单脱氢抗坏血酸和超氧化物的浓度必须保持极低。歧化反应不够快,无法消除这些产物。我们通过同时监测醌的氧化还原状态和氧化还原循环速率,研究了抗坏血酸驱动的氧化还原循环机制。有证据表明存在一种机制,即单脱氢抗坏血酸被半醌氧化。结果是半醌和对苯二酚的循环介导了单脱氢抗坏血酸的快速歧化。该机制解释了氧化还原循环速率对醌和抗坏血酸浓度以及醌还原电位的依赖性。因此,它预测了在各种条件下以及使用不同醌时,抗坏血酸驱动的氧化还原循环生成过氧化氢的速度有多快。

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