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首页> 外文期刊>Antioxidants and redox signalling >May serum levels of advanced oxidized protein products serve as a prognostic marker of disease duration in patients with idiopathic parkinson's disease?
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May serum levels of advanced oxidized protein products serve as a prognostic marker of disease duration in patients with idiopathic parkinson's disease?

机译:特发性帕金森氏病患者的血清高级氧化蛋白产物水平可以作为疾病持续时间的预后标志吗?

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摘要

Protein and amine halogenation is a type of oxidative stress induced by phagocytic overstimulation, and its role in Parkinson's disease (PD) has not been discerned. We have detected that advanced oxidized protein products, markers of protein halogenation, are reliably enhanced in serum of patients with PD (n=60) relative to control subjects (n=45, p0.012), and to a lesser extent in the cerebrospinal fluid. Amine halogenation, as evaluated through 3-chlorotyrosine, is not affected. Mieloperoxidase and hydrogen peroxide levels, halogenative factors of phagocytes, are devoid of changes. Levels of advanced oxidized protein products are progressively reduced over time, and the duration of PD is larger in the Hoehn-Yahr-stage-2/3 patients (n=34) with low serum levels (R2=0.0145, p0.003). Levodopa treatment contributes to this reduction (R2=0.259, p0.001). These protein products are not cytotoxic, unlike 3-chlorotyrosine, but they are known to form inflammatory mediators after conjugation with serum albumin. Our observations lead to the hypothesis that the serum level of advanced oxidized protein products is a prognostic marker of PD duration, and these oxidized proteins could participate in the development of parkinsonian neurodegeneration. Antioxid. Redox Signal. 18, 1296-1302. ?
机译:蛋白质和胺的卤化是吞噬细胞过度刺激引起的一种氧化应激,尚不清楚其在帕金森氏病(PD)中的作用。我们已经检测到,相对于对照组(n = 45,p <0.012),PD患者(n = 60)的血清中可靠地增强了高级氧化蛋白质产物(蛋白质卤化的标志物),在脑脊髓中的程度较小体液。通过3-氯酪氨酸评估的胺卤化不受影响。吞噬细胞的卤化因子微过氧化物酶和过氧化氢水平没有变化。血清水平低的Hoehn-Yahr-2 / 3期患者(n = 34)(R2 = 0.0145,p <0.003),随着时间的推移,高级氧化蛋白产物的水平逐渐降低,PD的持续时间更长。左旋多巴治疗有助于减少(R2 = 0.259,p <0.001)。与3-氯酪氨酸不同,这些蛋白质产物无细胞毒性,但已知它们与血清白蛋白结合后会形成炎症介质。我们的观察结果得出这样的假设:高级氧化蛋白产物的血清水平是PD持续时间的预后标志物,这些氧化蛋白可能参与帕金森氏神经变性的发展。抗氧化。氧化还原信号。 18,1296-1302。 ?

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