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蛋白质加速一氧化氮的自动氧化。

Acceleration of the autoxidation of nitric oxide by proteins.

机构信息

Laboratorio de Fisicoquímica Biológica, Instituto de Química Biológica, Facultad de Ciencias, Center for Free Radical and Biomedical Research, Universidad de la República, Igua 4225, CP11400, Montevideo, Uruguay.

出版信息

Nitric Oxide. 2019 Apr 1;85:28-34. doi: 10.1016/j.niox.2019.01.014. Epub 2019 Jan 30.

Abstract

Lipoproteins and lipid membranes accelerate NO autoxidation by increasing local concentration of NO and O. Although the idea that proteins could also accelerate this reaction was presented some time ago, it was largely criticized and dismissed. Herein the effect of proteins on NO autoxidation rates was studied following NO disappearance with a selective electrode. It was found that human serum albumin (HSA) accelerated NO autoxidation by a factor of 9 per g/mL of protein, much less than previously suggested. The acceleration by HSA was sensitive to pH and significantly decreased at pH lower than 4.5 coincident with the acid structure transition of HSA to a partially unfolded and rigid conformation. Other proteins with different surface hydrophobicity also accelerated NO autoxidation and it was found to depend mostly on the protein size and dynamics. Mathematical simulations were performed to assess the physiological importance of this acceleration. It was calculated that in plasma the autoxidation of NO is accelerated 1.38 times by HSA relative to water alone, but this becomes of little relevance when whole blood is simulated because of the rapid rate of NO consumption by red blood cells.

摘要

脂蛋白和脂质膜通过增加局部 NO 和 O 的浓度来加速 NO 的自动氧化。尽管很久以前就提出了蛋白质也可以加速这种反应的想法,但它受到了广泛的批评和否定。在此,通过选择性电极研究了蛋白质对 NO 自动氧化速率的影响。结果发现,人血清白蛋白(HSA)使 NO 自动氧化的速度提高了 9 倍/克/毫升,远低于先前的建议。HSA 的加速作用对 pH 敏感,当 pH 低于 4.5 时,HSA 的酸性结构向部分展开和刚性构象转变,加速作用显著降低。具有不同表面疏水性的其他蛋白质也加速了 NO 的自动氧化,并且发现其主要取决于蛋白质的大小和动力学。进行了数学模拟以评估这种加速的生理重要性。计算表明,与单独的水相比,在血浆中 HSA 使 NO 的自动氧化速度提高了 1.38 倍,但由于红细胞对 NO 的快速消耗,当模拟全血时,这种加速作用变得无关紧要。

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