Department of Cell Biology, Microbiology and Molecular Biology, University of South Florida, Tampa, FL, 33620, USA.
BMC Genet. 2015 Feb 3;16(1):8. doi: 10.1186/s12863-015-0167-2.
Little is known about the role of amino acids in cellular signaling pathways, especially as it pertains to pathways that regulate the rate of aging. However, it has been shown that methionine or tryptophan restriction extends lifespan in higher eukaryotes and increased proline or tryptophan levels increase longevity in C. elegans. In addition, leucine strongly activates the TOR signaling pathway, which when inhibited increases lifespan.
Therefore each of the 20 proteogenic amino acids was individually supplemented to C. elegans and the effects on lifespan were determined. All amino acids except phenylalanine and aspartate extended lifespan at least to a small extent at one or more of the 3 concentrations tested with serine and proline showing the largest effects. 11 of the amino acids were less potent at higher doses, while 5 even decreased lifespan. Serine, proline, or histidine-mediated lifespan extension was greatly inhibited in eat-2 worms, a model of dietary restriction, in daf-16/FOXO, sir-2.1, rsks-1 (ribosomal S6 kinase), gcn-2, and aak-2 (AMPK) longevity pathway mutants, and in bec-1 autophagy-defective knockdown worms. 8 of 10 longevity-promoting amino acids tested activated a SKN-1/Nrf2 reporter strain, while serine and histidine were the only amino acids from those to activate a hypoxia-inducible factor (HIF-1) reporter strain. Thermotolerance was increased by proline or tryptophan supplementation, while tryptophan-mediated lifespan extension was independent of DAF-16/FOXO and SKN-1/Nrf2 signaling, but tryptophan and several related pyridine-containing compounds induced the mitochondrial unfolded protein response and an ER stress response. High glucose levels or mutations affecting electron transport chain (ETC) function inhibited amino acid-mediated lifespan extension suggesting that metabolism plays an important role. Providing many other cellular metabolites to C. elegans also increased longevity suggesting that anaplerosis of tricarboxylic acid (TCA) cycle substrates likely plays a role in lifespan extension.
Supplementation of C. elegans with 18 of the 20 individual amino acids extended lifespan, but lifespan often decreased with increasing concentration suggesting hormesis. Lifespan extension appears to be caused by altered mitochondrial TCA cycle metabolism and respiratory substrate utilization resulting in the activation of the DAF-16/FOXO and SKN-1/Nrf2 stress response pathways.
关于氨基酸在细胞信号通路中的作用知之甚少,尤其是在调节衰老速度的通路方面。然而,已经表明甲硫氨酸或色氨酸限制可延长高等真核生物的寿命,并且脯氨酸或色氨酸水平的增加可延长秀丽隐杆线虫的寿命。此外,亮氨酸强烈激活 TOR 信号通路,当该通路受到抑制时,寿命会延长。
因此,将 20 种蛋白质氨基酸中的每一种单独补充到秀丽隐杆线虫中,并确定对寿命的影响。除苯丙氨酸和天冬氨酸外,所有氨基酸在 3 种测试浓度中的一种或多种浓度下至少在一定程度上延长了寿命,其中丝氨酸和脯氨酸的效果最大。11 种氨基酸在较高剂量时效果较弱,而 5 种氨基酸甚至降低了寿命。在饮食限制模型 eat-2 蠕虫、daf-16/FOXO、sir-2.1、rsks-1(核糖体 S6 激酶)、gcn-2 和 aak-2(AMPK)长寿途径突变体以及 bec-1 自噬缺陷型敲低蠕虫中,丝氨酸、脯氨酸或组氨酸介导的寿命延长受到严重抑制。在 10 种测试的促进长寿的氨基酸中有 8 种激活了 SKN-1/Nrf2 报告株,而丝氨酸和组氨酸是唯一从那些激活缺氧诱导因子 (HIF-1) 报告株的氨基酸。脯氨酸或色氨酸的补充增加了热耐受性,而色氨酸介导的寿命延长与 DAF-16/FOXO 和 SKN-1/Nrf2 信号无关,但色氨酸和几种相关的吡啶类化合物诱导了线粒体未折叠蛋白反应和内质网应激反应。高葡萄糖水平或影响电子传递链 (ETC) 功能的突变抑制了氨基酸介导的寿命延长,这表明代谢起重要作用。向秀丽隐杆线虫提供许多其他细胞代谢物也增加了寿命,这表明三羧酸 (TCA) 循环底物的回补可能在延长寿命中起作用。
向秀丽隐杆线虫补充 20 种氨基酸中的 18 种可延长寿命,但随着浓度的增加,寿命往往会降低,表明存在兴奋效应。寿命的延长似乎是由线粒体 TCA 循环代谢和呼吸底物利用的改变引起的,导致 DAF-16/FOXO 和 SKN-1/Nrf2 应激反应途径的激活。
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