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昼夜转录途径图谱突出了间歇性禁食中的蛋白酶体开关。

Circadian transcriptional pathway atlas highlights a proteasome switch in intermittent fasting.

机构信息

Center for Biomedical Aging, National & Local Joint Engineering Laboratory of Animal Peptide Drug Development, College of Life Sciences, Hunan Normal University, Changsha, Hunan 410081, China.

Department of Cell Biology, School of Life Sciences, Central South University, Changsha, Hunan 41001, China.

出版信息

Cell Rep. 2022 Oct 25;41(4):111547. doi: 10.1016/j.celrep.2022.111547.

Abstract

While intermittent fasting is a safe strategy to benefit health, it remains unclear whether a "timer" exists in vivo to record fasting duration and trigger a transcriptional switch. Here, we map a circadian transcriptional pathway atlas from 600 samples across four metabolic tissues of mice under five feeding regimens. Results show that 95.6% of detected canonical pathways are rhythmic in a tissue-specific and feeding-regimen-specific manner, while only less than 25% of them induce changes in transcriptional function. Fasting for 16 h initiates a circadian resonance of 43 pathways in the liver, and the resonance punctually switches following refeeding. The hepatic proteasome coordinates the resonance, and most genes encoding proteasome subunits display a 16-h fasting-dependent transcriptional switch. These findings indicate that the hepatic proteasome may serve as a fasting timer and a coordinator of pathway transcriptional resonance, which provide a target for revealing the underlying mechanism of intermittent fasting.

摘要

虽然间歇性禁食是一种有益于健康的安全策略,但目前尚不清楚体内是否存在“计时器”来记录禁食时间并触发转录开关。在这里,我们绘制了来自 4 种代谢组织的 600 个样本的昼夜转录途径图谱,这些样本来自于小鼠的 5 种喂养方案。结果表明,95.6%的检测到的经典途径以组织特异性和喂养方案特异性的方式呈节律性,而只有不到 25%的途径诱导转录功能发生变化。禁食 16 小时会引发肝脏中 43 种途径的昼夜共振,而重新进食后,这种共振会准时切换。肝脏蛋白酶体协调共振,并且编码蛋白酶体亚基的大多数基因显示出 16 小时禁食依赖性的转录开关。这些发现表明,肝脏蛋白酶体可能作为禁食计时器和途径转录共振的协调者,为揭示间歇性禁食的潜在机制提供了一个目标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/45b6/9671760/ad64ff3b9c65/nihms-1847029-f0002.jpg

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