[慢性肾脏疾病中脂质过氧化和蛋白质激活的体外途径建模]。

L. Korol
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引用次数: 2

摘要

在不影响肾脏排泄功能的情况下,对86例慢性肾盂肾炎(cPN)和64例慢性肾小球肾炎(cGN)患者的脂质过氧化和血液蛋白在丙二醛(MDA)和蛋白羰基(PCG)形成中的自发氧化和金属诱导的脂质和蛋白质氧化进行了体外模型研究。cPN患者血中MDAs升高2倍,MDAe- 14%, PCG升高1.5倍;cGN- MDAs为2.3倍,MDAe为29%,PCG为2倍。发现cPN患者血液中丙二醛和PCG含量升高,且cGN时表达更明显。与基线相比,刺激体外过氧化过程显著增加了MDA的产生。在体外模拟抗坏血酸依赖和nadph依赖的脂质过氧化方式以及两组患者MDA和PCG蛋白生成的增加,特别是nadph依赖的方式,这在纠正氧化过程和抗氧化治疗的确定中必须考虑。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[MODELING IN VITRO PATHWAYS OF ACTIVATION OF LIPID PEROXIDATION AND PROTEIN IN CHRONIC KIDNEY DISEASE].
We studied the spontaneous and metal induced oxidation of lipids and proteins in in vitro modeling ways of lipid peroxidation and blood proteins in the formation of malondialdehyde (MDA) and protein carbonyl groups (PCG) in 86 patients with chronic pyelonephritis (cPN) and 64 patients chronic glomerulonephritis(cGN) without prejudice excretory function of the kidneys. Installed the increase in the blood of patients with cPN MDAs 2 times, MDAe--14%, PCG 1.5 times; and cGN--MDAs 2.3 times, MDAe--29%, PCG--2 times. Found increased MDA content and PCG in the blood of patients with cPN and more expressive when cGN. Stimulation of in vitro peroxidation processes contributed significantly increased of production of MDA comparedwith baseline. In the modeling in vitro ascorbate-dependent and NADPH-dependent lipid peroxidation ways and the increase in protein production of MDA and PCG in both groups of patients, especially in the NADPH-dependent way, which must be considered in the correction of oxidative processes and antioxidant therapy appointment.
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