The impact of aging on enzyme proteins of rat liver peroxisomes: quantitative analysis by immunoblotting and immunoelectron microscopy.

K Beier, A Völkl, H D Fahimi
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引用次数: 52

Abstract

The alterations of hepatic peroxisomes and their enzymes during aging were investigated in male rats. Peroxisomes in the livers of young (2 months) and old (39 months) male Wistar rats were analyzed by morphometry and quantitative immunocytochemistry, as well as by immunoblotting of highly purified peroxisomal fractions. Immunoblots showed that catalase and acyl-CoA oxidase were decreased in peroxisomes of old animals but the trifunctional enzyme, thiolase, and urate oxidase were increased. The morphometrical analysis revealed a heterogeneous distribution of peroxisomes in the liver lobule of the old animals, with a significant elevation of peroxisomal volume density in pericentral over periportal hepatocytes, in contrast to the uniform pattern in the young rats. Furthermore, age-related lobular gradients were also observed by quantitative immunocytochemistry in the peroxisomal concentrations of trifunctional enzyme (central > portal) and, inversely, for catalase (portal > central). Whereas acyl-CoA oxidase was diminished across the liver lobule, the enzyme 3-ketoacyl-CoA thiolase was elevated. These observations show that peroxisomes are significantly altered in aged animals and suggest that these alterations may contribute to the disturbance of lipid metabolism in aged animals. Moreover, the diminution in catalase and the elevation of urate oxidase could contribute to the oxidative stress which is considered to be of fundamental importance in the aging process.

衰老对大鼠肝脏过氧化物酶体酶蛋白的影响:免疫印迹和免疫电镜定量分析。
研究了雄性大鼠肝脏过氧化物酶体及其酶在衰老过程中的变化。采用形态测定法、定量免疫细胞化学和免疫印迹法对幼龄(2月龄)和高龄(39月龄)雄性Wistar大鼠肝脏中的过氧化物酶体进行了分析。免疫印迹结果显示,老龄动物过氧化物酶体过氧化氢酶和酰基辅酶a氧化酶降低,三功能酶、硫酶和尿酸氧化酶升高。形态计量学分析显示,老年大鼠肝小叶中过氧化物酶体分布不均,中心周围和门静脉周围肝细胞的过氧化物酶体体积密度显著升高,而年轻大鼠则是均匀分布。此外,定量免疫细胞化学还观察到三功能酶的过氧化物酶体浓度(中央>门脉)和过氧化氢酶(门脉>中央)与年龄相关的小叶梯度。肝小叶酰基辅酶a氧化酶降低,3-酮酰基辅酶a硫酶升高。这些观察结果表明,过氧化物酶体在老年动物中发生了显著改变,并提示这些改变可能导致老年动物脂质代谢紊乱。过氧化氢酶的降低和尿酸氧化酶的升高可能导致氧化应激,这被认为是衰老过程中至关重要的因素。
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