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Cell culture-based profiling across mammals reveals DNA repair and metabolism as determinants of species longevity

机译:跨哺乳动物的基于细胞培养的分析揭示了DNA修复和代谢是决定物种长寿的因素

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摘要

Mammalian lifespan differs by >100 fold, but the mechanisms associated with such longevity differences are not understood. Here, we conducted a study on primary skin fibroblasts isolated from 16 species of mammals and maintained under identical cell culture conditions. We developed a pipeline for obtaining species-specific ortholog sequences, profiled gene expression by RNA-seq and small molecules by metabolite profiling, and identified genes and metabolites correlating with species longevity. Cells from longer lived species up-regulated genes involved in DNA repair and glucose metabolism, down-regulated proteolysis and protein transport, and showed high levels of amino acids but low levels of lysophosphatidylcholine and lysophosphatidylethanolamine. The amino acid patterns were recapitulated by further analyses of primate and bird fibroblasts. The study suggests that fibroblast profiling captures differences in longevity across mammals at the level of global gene expression and metabolite levels and reveals pathways that define these differences.>DOI:
机译:哺乳动物的寿命相差> 100倍,但与这种寿命差异相关的机制尚不清楚。在这里,我们对从16种哺乳动物中分离并维持在相同细胞培养条件下的原代皮肤成纤维细胞进行了研究。我们开发了一个管道,用于获取物种特异性直系同源序列,通过RNA-seq进行基因表达分析以及通过代谢物谱分析来鉴定小分子,并鉴定与物种寿命相关的基因和代谢物。寿命更长的物种的细胞上调基因,参与DNA修复和葡萄糖代谢,下调蛋白水解和蛋白质运输,并显示出高水平的氨基酸,而低水平的溶血磷脂酰胆碱和溶血磷脂酰乙醇胺。通过对灵长类和鸟类成纤维细胞的进一步分析概括了氨基酸模式。该研究表明,成纤维细胞谱分析在全球基因表达和代谢产物水平上捕获了哺乳动物寿命的差异,并揭示了定义这些差异的途径。> DOI:

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