Cell-free Formation of RNA Granules: Low Complexity Sequence Domains Form Dynamic Fibers within Hydrogels
Author(s) -
Masato Kato,
Tina W. Han,
Shanhai Xie,
Kevin Shi,
Xinlin Du,
Leeju C. Wu,
Hamid Mirzaei,
Elizabeth J. Goldsmith,
Jamie Longgood,
Jimin Pei,
Nick V. Grishin,
Douglas E. Frantz,
Jay W. Schneider,
She Chen,
Lin Li,
M.R. Sawaya,
David Eisenberg,
Robert Tycko,
Steven L. McKnight
Publication year - 2012
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2012.04.017
Subject(s) - rna , biology , biophysics , self healing hydrogels , polymerization , rna binding protein , biotinylation , sequence (biology) , microbiology and biotechnology , polymer , biochemistry , chemistry , gene , organic chemistry
Eukaryotic cells contain assemblies of RNAs and proteins termed RNA granules. Many proteins within these bodies contain KH or RRM RNA-binding domains as well as low complexity (LC) sequences of unknown function. We discovered that exposure of cell or tissue lysates to a biotinylated isoxazole (b-isox) chemical precipitated hundreds of RNA-binding proteins with significant overlap to the constituents of RNA granules. The LC sequences within these proteins are both necessary and sufficient for b-isox-mediated aggregation, and these domains can undergo a concentration-dependent phase transition to a hydrogel-like state in the absence of the chemical. X-ray diffraction and EM studies revealed the hydrogels to be composed of uniformly polymerized amyloid-like fibers. Unlike pathogenic fibers, the LC sequence-based polymers described here are dynamic and accommodate heterotypic polymerization. These observations offer a framework for understanding the function of LC sequences as well as an organizing principle for cellular structures that are not membrane bound.
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