| Literature DB >> 31757755 |
Anupam K Chakravarty1, Tina Smejkal1, Alan K Itakura2, David M Garcia1, Daniel F Jarosz3.
Abstract
Spatiotemporal gene regulation is often driven by RNA-binding proteins that harbor long intrinsically disordered regions in addition to folded RNA-binding domains. We report that the disordered region of the evolutionarily ancient developmental regulator Vts1/Smaug drives self-assembly into gel-like condensates. These proteinaceous particles are not composed of amyloid, yet they are infectious, allowing them to act as a protein-based epigenetic element: a prion [SMAUG+]. In contrast to many amyloid prions, condensation of Vts1 enhances its function in mRNA decay, and its self-assembly properties are conserved over large evolutionary distances. Yeast cells harboring [SMAUG+] downregulate a coherent network of mRNAs and exhibit improved growth under nutrient limitation. Vts1 condensates formed from purified protein can transform naive cells to acquire [SMAUG+]. Our data establish that non-amyloid self-assembly of RNA-binding proteins can drive a form of epigenetics beyond the chromosome, instilling adaptive gene expression programs that are heritable over long biological timescales.Entities:
Keywords: IDPs; RNA-binding proteins; epigenetics; non-amyloid prions; phase separation; post-transcriptional gene regulation
Mesh:
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Year: 2019 PMID: 31757755 PMCID: PMC6980676 DOI: 10.1016/j.molcel.2019.10.028
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970