首页> 外文期刊>The journals of gerontology.Series A. Biological sciences and medical sciences >A Heart That Beats for 500 Years: Age-Related Changes in Cardiac Proteasome Activity, Oxidative Protein Damage and Expression of Heat Shock Proteins, Inflammatory Factors, and Mitochondrial Complexes in Arctica islandica, the Longest-Living Noncolonial Animal
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A Heart That Beats for 500 Years: Age-Related Changes in Cardiac Proteasome Activity, Oxidative Protein Damage and Expression of Heat Shock Proteins, Inflammatory Factors, and Mitochondrial Complexes in Arctica islandica, the Longest-Living Noncolonial Animal

机译:跳动了500年的心脏:寿命最长的非殖民地动物Arctica islandica的心脏蛋白酶体活性,氧化性蛋白损伤和热休克蛋白,炎性因子和线粒体复合物的表达与年龄相关的变化

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Study of negligibly senescent animals may provide clues that lead to better understanding of the cardiac aging process. To elucidate mechanisms of successful cardiac aging, we investigated age-related changes in proteasome activity, oxidative protein damage and expression of heat shock proteins, inflammatory factors, and mitochondrial complexes in the heart of the ocean quahog Arctica islandica, the longest-lived noncolonial animal (maximum life span potential: 508 years). We found that in the heart of A. islandica the level of oxidatively damaged proteins did not change significantly up to 120 years of age. No significant aging-induced changes were observed in caspase-like and trypsin-like proteasome activity. Chymotrypsin-like proteasome activity showed a significant early-life decline, then it remained stable for up to 182 years. No significant relationship was observed between the extent of protein ubiquitination and age. In the heart of A. islandica, an early-life decline in expression of HSP90 and five mitochondrial electron transport chain complexes was observed. We found significant age-related increases in the expression of three cytokine-like mediators (interleukin-6, interleukin-1, and tumor necrosis factor-alpha) in the heart of A. islandica. Collectively, in extremely long-lived molluscs, maintenance of protein homeostasis likely contributes to the preservation of cardiac function. Our data also support the concept that low-grade chronic inflammation in the cardiovascular system is a universal feature of the aging process, which is also manifest in invertebrates.
机译:对衰老性微不足道的动物的研究可能会提供一些线索,有助于更好地了解心脏衰老过程。为了阐明成功的心脏衰老的机制,我们调查了寿命最长的非殖民地动物洋Arctica islandica心脏中蛋白酶体活性,氧化蛋白损伤以及热休克蛋白,炎性因子和线粒体复合体表达的年龄相关变化。 (最大寿命潜力:508年)。我们发现在岛island曲霉的心脏中,氧化损伤蛋白的水平直到120岁都没有显着变化。在胱天蛋白酶样和胰蛋白酶样蛋白酶体活性中未观察到明显的衰老引起的变化。胰凝乳蛋白酶样蛋白酶体活性显示出明显的早期寿命下降,然后保持稳定长达182年。蛋白质泛素化程度和年龄之间未发现显着关系。在A. islandica的心脏,观察到HSP90和五个线粒体电子传输链复合物的早期表达下降。我们发现岛曲霉心脏中三种细胞因子样介质(白介素-6,白介素-1和肿瘤坏死因子-α)的表达与年龄显着相关。总的来说,在极长寿命的软体动物中,蛋白质稳态的维持可能有助于维持心脏功能。我们的数据也支持这样的概念,即心血管系统中的低度慢性炎症是衰老过程的普遍特征,这也体现在无脊椎动物中。

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