eLife (Jan 2018)

Hepatitis B virus core protein allosteric modulators can distort and disrupt intact capsids

  • Christopher John Schlicksup,
  • Joseph Che-Yen Wang,
  • Samson Francis,
  • Balasubramanian Venkatakrishnan,
  • William W Turner,
  • Michael VanNieuwenhze,
  • Adam Zlotnick

DOI
https://doi.org/10.7554/eLife.31473
Journal volume & issue
Vol. 7

Abstract

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Defining mechanisms of direct-acting antivirals facilitates drug development and our understanding of virus function. Heteroaryldihydropyrimidines (HAPs) inappropriately activate assembly of hepatitis B virus (HBV) core protein (Cp), suppressing formation of virions. We examined a fluorophore-labeled HAP, HAP-TAMRA. HAP-TAMRA induced Cp assembly and also bound pre-assembled capsids. Kinetic and spectroscopic studies imply that HAP-binding sites are usually not available but are bound cooperatively. Using cryo-EM, we observed that HAP-TAMRA asymmetrically deformed capsids, creating a heterogeneous array of sharp angles, flat regions, and outright breaks. To achieve high resolution reconstruction (<4 Å), we introduced a disulfide crosslink that rescued particle symmetry. We deduced that HAP-TAMRA caused quasi-sixfold vertices to become flatter and fivefold more angular. This transition led to asymmetric faceting. That a disordered crosslink could rescue symmetry implies that capsids have tensegrity properties. Capsid distortion and disruption is a new mechanism by which molecules like the HAPs can block HBV infection.

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