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饮食限制诱导长寿基因的转录后调控。

Dietary restriction induces posttranscriptional regulation of longevity genes.

机构信息

Mount Desert Island Biological Laboratory, Salisbury Cove, ME, USA

Mount Desert Island Biological Laboratory, Salisbury Cove, ME, USA.

出版信息

Life Sci Alliance. 2019 Jun 28;2(4). doi: 10.26508/lsa.201800281. Print 2019 Aug.

Abstract

Dietary restriction (DR) increases life span through adaptive changes in gene expression. To understand more about these changes, we analyzed the transcriptome and translatome of subjected to DR. Transcription of muscle regulatory and structural genes increased, whereas increased expression of amino acid metabolism and neuropeptide signaling genes was controlled at the level of translation. Evaluation of posttranscriptional regulation identified putative roles for RNA-binding proteins, RNA editing, miRNA, alternative splicing, and nonsense-mediated decay in response to nutrient limitation. Using RNA interference, we discovered several differentially expressed genes that regulate life span. We also found a compensatory role for translational regulation, which offsets dampened expression of a large subset of transcriptionally down-regulated genes. Furthermore, 3' UTR editing and intron retention increase under DR and correlate with diminished translation, whereas trans-spliced genes are refractory to reduced translation efficiency compared with messages with the native 5' UTR. Finally, we find that and , which are genes governing selection and turnover of nonsense-mediated decay targets, are required for increased life span under DR.

摘要

饮食限制(DR)通过基因表达的适应性变化来延长寿命。为了更深入地了解这些变化,我们分析了 进行 DR 时的转录组和翻译组。肌肉调节和结构基因的转录增加,而氨基酸代谢和神经肽信号基因的表达增加则在翻译水平上受到控制。对转录后调控的评估确定了 RNA 结合蛋白、RNA 编辑、miRNA、可变剪接和无意义介导的衰变在响应营养限制时的潜在作用。通过 RNA 干扰,我们发现了几个调节寿命的差异表达基因。我们还发现了翻译调控的补偿作用,它抵消了转录下调基因的大部分表达减弱。此外,DR 下 3' UTR 编辑和内含子保留增加,与翻译减少相关,而与具有天然 5' UTR 的消息相比,跨剪接基因对翻译效率降低的抵抗力更强。最后,我们发现, 和 ,这两个基因控制着无意义介导的衰变靶标选择和周转,是 DR 下寿命延长所必需的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/297e/6600014/dc0b7f32333c/LSA-2018-00281_Fig1.jpg

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