Functional study of two flexible regions of the hepatitis E virus ORF1 replicase
Léa Mézière, Sonia Fieulaine, Claire Montpellier, Martin Ferrié, Thibault Tubiana, Gabriel Vanegas Arias, Stéphane Bressanelli, Laurence Cocquerel, Cécile-Marie Aliouat-Denis

TL;DR
This paper studies two flexible regions of the hepatitis E virus ORF1 protein to understand their role in virus replication.
Contribution
The study reveals that two disordered regions in HEV ORF1 are functionally important for replication despite not being cleavage sites.
Findings
Mutations in the Hel/RdRp linker strongly impair HEV replication.
The RdRp C-terminal tail's conformational flexibility is critical for polymerase activity.
ORF1 is predominantly expressed as a full-length protein with some truncated products.
Abstract
Hepatitis E virus (HEV), like other positive-sense RNA viruses, encodes a multidomain protein essential for replication, termed ORF1. However, the number, organization, and functions of its domains remain debated. Using AlphaFold2-based structural modeling, we investigated two structurally disordered regions with potential regulatory functions: (i) a 16-residue linker between the Helicase (Hel) and RNA-dependent RNA polymerase (RdRp) domains, proposed as a cleavage site and/or a flexible hinge, and (ii) the RdRp C-terminal tail, suggested to modulate polymerase activity through conformational plasticity. We performed mutagenesis of the Hel/RdRp linker and analyzed the impact of mutations on ORF1 maturation, subcellular localization, and replication efficiency. Using an extensive antibody panel combined with precise protein sizing, we found that ORF1 is predominantly expressed as a…
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Taxonomy
TopicsHepatitis Viruses Studies and Epidemiology · Viral gastroenteritis research and epidemiology · Viral Infections and Immunology Research
