Transient Non-local Interactions Dominate the Dynamics of Measles Virus NTAIL

Author:

Otteson Lillian,Nagy GaborORCID,Kunkel John,Kodis Gerdenis,Zheng WenweiORCID,Bignon Christophe,Longhi Sonia,Grubmüller Helmut,Vaiana Andrea C.ORCID,Vaiana Sara M.ORCID

Abstract

AbstractThe RNA genome of measles virus is encapsidated by the nucleoprotein within a helical nucleocapsid that serves as template for both transcription and replication. The intrinsically disordered domain of the nucleoprotein (NTAIL), partly protruding outward from the nucleocapsid, is essential for binding the polymerase complex responsible for viral transcription and replication. As for many IDPs, binding of NTAILoccurs through a short molecular recognition element (MoRE) that folds upon binding, with the majority of NTAILremaining disordered. Though NTAILregions far from the MoRE influence the binding affinity, interactions between them and the MoRE have not been investigated in depth. Using an integrated approach, relying on photo-induced electron transfer (PET) experiments between tryptophan and cysteine pairs placed at different positions in the protein under varying salt and pH conditions, combined with simulations and analytical models, we identified transient interactions between two disordered regions distant in sequence, which dominate NTAILdynamics, and regulate the conformational preferences of both the MoRE and the entire NTAILdomain. Co-evolutionary analysis corroborates our findings, and suggests an important functional role for the same intramolecular interactions. We propose mechanisms by which these non-local interactions may regulate binding to the phosphoprotein, polymerase recruitment, and ultimately viral transcription and replication. Our findings may be extended to other IDPs, where non-local intra-protein interactions affect the conformational preferences of intermolecular binding sites.

Publisher

Cold Spring Harbor Laboratory

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