Circadian regulation of macromolecular complex turnover and proteome renewal.
Estere SeinkmaneAnna EdmondsonSew Peak ChewAiwei ZengNina M RzechorzekNathan R JamesJames A WestJack MunnsDavid Chuen Soong WongAndrew D BealeJohn S O'NeillPublished in: The EMBO journal (2024)
Although costly to maintain, protein homeostasis is indispensable for normal cellular function and long-term health. In mammalian cells and tissues, daily variation in global protein synthesis has been observed, but its utility and consequences for proteome integrity are not fully understood. Using several different pulse-labelling strategies, here we gain direct insight into the relationship between protein synthesis and abundance proteome-wide. We show that protein degradation varies in-phase with protein synthesis, facilitating rhythms in turnover rather than abundance. This results in daily consolidation of proteome renewal whilst minimising changes in composition. Coupled rhythms in synthesis and turnover are especially salient to the assembly of macromolecular protein complexes, particularly the ribosome, the most abundant species of complex in the cell. Daily turnover and proteasomal degradation rhythms render cells and mice more sensitive to proteotoxic stress at specific times of day, potentially contributing to daily rhythms in the efficacy of proteasomal inhibitors against cancer. Our findings suggest that circadian rhythms function to minimise the bioenergetic cost of protein homeostasis through temporal consolidation of protein turnover.
Keyphrases
- bone mineral density
- physical activity
- protein protein
- healthcare
- amino acid
- public health
- blood pressure
- gene expression
- mental health
- induced apoptosis
- stem cells
- risk assessment
- microbial community
- metabolic syndrome
- single cell
- body composition
- bone marrow
- papillary thyroid
- young adults
- endoplasmic reticulum stress
- social media
- heat stress
- health information
- cell cycle arrest