81 / 2024-10-20 11:36:45
CTCFL Maintains Liver Metabolic Homeostasis by Regulating Chromatin Accessibility and 3D Genome Topology
CTCF,CTCFL,transcription regulation,genome topology,metabolism homeostasis
摘要录用
卞迁 / 上海交通大学医学院
左武 / 上海交通大学医学院
Mammals experience regular cycles of fasting and feeding, leading to dynamic transcriptional changes in metabolic tissues under fluctuating nutritional conditions. However, the transcriptional regulatory mechanisms employed by the liver, the primary metabolic organ, in response to metabolic stress remain unclear. In this study, we identify CTCFL, a testis-specific paralog of chromatin architecture protein CTCF, as a key transcriptional regulator that responds to metabolic stresses. Although CTCFL is typically expressed at low levels in somatic tissues, its expression in the liver increases significantly during starvation. The elevated genome occupancy of CTCFL at genes involved in fatty acid metabolism is associated with increased chromatin accessibility and transcriptional activity of these genes. We further found that mice lacking CTCFL exhibit dysregulation of metabolic genes and prominent lipid droplet accumulation at a young age, even on a regular diet. Interestingly, the loss of CTCFL also leads to a redistribution of CTCF and cohesin and the alteration in enhancer-promoter loops, thereby affecting the expression of loop-associated genes. Collectively, our study suggests that the liver modulates chromatin accessibility and higher-order chromatin structure in response to nutritional status by regulating CTCFL expression. This highlights a previously unappreciated, pleiotropic role of CTCFL in maintaining fatty acid metabolic homeostasis.
重要日期
  • 会议日期

    10月31日

    2024

    11月03日

    2024

  • 11月03日 2024

    注册截止日期

主办单位
崖州湾国家实验室
华中农业大学
浙江大学
中国遗传学会
中国遗传学会三维基因组学专委会
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中国生物信息学基因组信息学专委会
中国遗传学会表观遗传分会
中国细胞生物学学会染色质生物学分会
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