The SARS-CoV-2 nucleocapsid protein is dynamic, disordered, and phase separates with RNA

Author:

Cubuk Jasmine,Alston Jhullian J.,Incicco J. Jeremías,Singh SukritORCID,Stuchell-Brereton Melissa D.,Ward Michael D.,Zimmerman Maxwell I.,Vithani Neha,Griffith DanielORCID,Wagoner Jason A.,Bowman Gregory R.ORCID,Hall Kathleen B.,Soranno AndreaORCID,Holehouse Alex S.ORCID

Abstract

AbstractThe SARS-CoV-2 nucleocapsid (N) protein is an abundant RNA binding protein critical for viral genome packaging, yet the molecular details that underlie this process are poorly understood. Here we combine single-molecule spectroscopy with all-atom simulations to uncover the molecular details that contribute to N protein function. N protein contains three dynamic disordered regions that house putative transiently-helical binding motifs. The two folded domains interact minimally such that full-length N protein is a flexible and multivalent RNA binding protein. N protein also undergoes liquid-liquid phase separation when mixed with RNA, and polymer theory predicts that the same multivalent interactions that drive phase separation also engender RNA compaction. We offer a simple symmetry-breaking model that provides a plausible route through which single-genome condensation preferentially occurs over phase separation, suggesting that phase separation offers a convenient macroscopic readout of a key nanoscopic interaction.

Publisher

Cold Spring Harbor Laboratory

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