首页> 外文期刊>Mechanisms of Ageing and Development >Age-related changes in the 20S and 26S proteasome activities in the liver of male F344 rats.
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Age-related changes in the 20S and 26S proteasome activities in the liver of male F344 rats.

机译:雄性F344大鼠肝脏中20S和26S蛋白酶体活性的年龄相关变化。

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Accumulation of altered proteins in old animals has been ascribed to slower turnover of proteins. Since proteasomes can be regarded as the major proteolytic enzymes responsible for the degradation of the majority of cellular proteins, we examined age-related changes of 20S and 26S proteasomes in the liver of young (8-10-month-old), middle-aged (15-18-month-old) and old (25-28-month-old) Fischer 344 male rats. The two forms of proteasomes were separated by glycerol gradient centrifugation. Fluorogenic peptides were used as substrates to evaluate three types of peptidase activities. The ratio of peptidase activities in the 20S proteasome vs. those in the 26S form did not appear to change with age. Unstimulated chymotrypsin-like activity found only in the 26S form decreased by 30% in the old rats as compared with that in the young ones, while no change in the activity was observed during aging when stimulated by sodium dodecyl sulfate. The trypsin-like activity declined significantly by 17% to an apparently similar extent in both 20S and 26S forms. The peptidylglutamyl peptide hydrolyzing activity exhibited gradual decrease with age, resulting in 60% lower value in the old rats as compared with the young animals. These changes are considered to account for the age-related extension of half-life of proteins. Since the amount of total proteasomes measured by immunoblot did not appear to change with age, posttranslational modifications or subunit replacement is possibly responsible for the decrease in the activities.
机译:老年动物体内蛋白质变化的积累被归因于蛋白质更新速度减慢。由于蛋白酶体可以被认为是导致大多数细胞蛋白降解的主要蛋白水解酶,因此我们检查了中青年(8-10个月大)的肝脏中与年龄相关的20S和26S蛋白酶体的变化。 (15-18个月大)和老(25-28个月大)Fischer 344雄性大鼠。通过甘油梯度离心分离两种形式的蛋白酶体。荧光肽用作底物以评估三种类型的肽酶活性。 20S蛋白酶体中的肽酶活性与26S形式中的酶活性之比似乎并未随年龄变化。在老年大鼠中,仅以26S形式发现的未刺激的胰凝乳蛋白酶样活性比年轻大鼠降低了30%,而在十二烷基硫酸钠刺激下,衰老过程中未观察到活性的变化。在20S和26S形式中,类胰蛋白酶的活性均显着下降了17%,至相似的程度。肽基谷氨酰胺肽的水解活性随着年龄的增长而逐渐降低,与年幼动物相比,老年大鼠的水解值降低了60%。这些变化被认为是蛋白质半衰期与年龄相关的延长。由于通过免疫印迹测得的总蛋白酶体的量似乎并未随年龄而变化,因此翻译后修饰或亚基置换可能是导致活性降低的原因。

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