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A window into extreme longevity; the circulating metabolomic signature of the naked mole-rat a mammal that shows negligible senescence

机译:通往长寿之窗;裸mole鼠的循环代谢组学特征衰老可忽略不计

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摘要

Mouse-sized naked mole-rats (Heterocephalus glaber), unlike other mammals, do not conform to Gompertzian laws of age-related mortality; adults show no age-related change in mortality risk. Moreover, we observe negligible hallmarks of aging with well-maintained physiological and molecular functions, commonly altered with age in other species. We questioned whether naked mole-rats, living an order of magnitude longer than laboratory mice, exhibit different plasma metabolite profiles, which could then highlight novel mechanisms or targets involved in disease and longevity. Using a comprehensive, unbiased metabolomics screen, we observe striking inter-species differences in amino acid, peptide, and lipid metabolites. Low circulating levels of specific amino acids, particularly those linked to the methionine pathway, resemble those observed during the fasting period at late torpor in hibernating ground squirrels and those seen in longer-lived methionine-restricted rats. These data also concur with metabolome reports on long-lived mutant mice, including the Ames dwarf mice and calorically restricted mice, as well as fruit flies, and even show similarities to circulating metabolite differences observed in young human adults when compared to older humans. During evolution, some of these beneficial nutrient/stress response pathways may have been positively selected in the naked mole-rat. These observations suggest that interventions that modify the aging metabolomic profile to a more youthful one may enable people to lead healthier and longer lives.Electronic supplementary materialThe online version of this article (10.1007/s11357-018-0014-2) contains supplementary material, which is available to authorized users.
机译:与其他哺乳动物不同,小鼠大小的裸mole鼠(Heterocephalus glaber)不符合与年龄有关的死亡率的Gompertzian规律;成人没有显示与年龄相关的死亡风险变化。此外,我们观察到衰老的痕迹微不足道,具有良好的生理和分子功能,在其他物种中通常随着年龄而改变。我们质疑寿命比实验室小鼠长一个数量级的裸mole鼠是否表现出不同的血浆代谢产物特征,从而可以突显涉及疾病和长寿的新机制或靶标。使用全面,无偏见的代谢组学筛选,我们观察到氨基酸,肽和脂质代谢物之间的种间差异非常明显。特定氨基酸的低循环水平,特别是与蛋氨酸途径相关的氨基酸,类似于冬眠的松鼠在空腹时在玉米粉空腹时所观察到的氨基酸,以及在寿命更长的蛋氨酸限制性大鼠中所观察到的氨基酸。这些数据还与关于长寿命突变小鼠(包括艾姆斯矮人小鼠和热量受限小鼠以及果蝇)的代谢组学报告相一致,甚至还显示出与老年人相比,年轻人中循环代谢物差异的相似性。在进化过程中,其中一些有益的营养/应激反应途径可能已在裸mole鼠中被肯定选择。这些观察结果表明,将衰老的代谢组学特征改变为更年轻的干预措施可以使人们过上更健康,更长寿的生活。电子补充材料本文的在线版本(10.1007 / s11357-018-0014-2)包含补充材料,其中适用于授权用户。

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