Epigenetic regulation of global proteostasis dynamics by RBBP5 ensures mammalian organismal health
收藏NIAID Data Ecosystem2026-05-02 收录
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https://www.ncbi.nlm.nih.gov/sra/SRP529936
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Proteostasis is vital for cellular health, with disruptions leading to pathologies including aging, neurodegeneration and metabolic disorders. Traditionally, proteotoxic stress responses were studied as acute reactions to various noxious factors; however, recent evidence reveals that many stress-response genes exhibit ~12-hour ultradian rhythms under physiological conditions in mammals. These rhythms, driven by an XBP1s-dependent 12h oscillator, are crucial for managing proteostasis. By exploring the chromatin landscape of the murine 12h hepatic oscillator, we identified RBBP5, a key subunit of the COMPASS complex, as an essential epigenetic regulator of proteostasis. RBBP5 is indispensable for regulating both the hepatic 12h oscillator and transcriptional response to acute proteotoxic stress, acting as a co-activator for master proteostasis transcription factor XBP1s. RBBP5 ablation leads to increased sensitivity to proteotoxic stress, chronic inflammation, and hepatic steatosis in mice, along with impaired autophagy and reduced cell survival in vitro. In humans, lower RBBP5 expression is associated with dampened adaptive stress-response gene expression and hepatic steatosis. Our findings establish RBBP5 as a critical regulator of proteostasis, essential for maintaining mammalian organismal health. Overall design: For acute ER stress induction experiment, male littermates WT [Rbbp5 (flox/flox); Alb-CRE (-/-)] and RBBP5 LKO [Rbbp5 (flox/flox); Alb-CRE (+/-) mice] between 5 and 7 months of age were randomly divided into two groups, and intraperitoneally injected with 0.05mg/kg body weight of tunicamycin dissolved in 500ul 3% DMSO in PBS or vehicle control (3% DMSO in PBS), respectively. Mice were injected with Tu between 9~10am in the morning and 8 hours later dissected for transcriptomic analysis for liver.
创建时间:
2024-10-11



