4.8 Article

High-resolution mass spectrometry of viral assemblies: Molecular composition and stability of dimorphic hepatitis B virus capsids

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.0800406105

Keywords

atomic force microscopy; collision-induced dissociation; macromolecular mass spectrometry; virus assembly; viral structural biology

Funding

  1. Intramural NIH HHS [Z01 AR041117-12] Funding Source: Medline

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Hepatitis B virus (HBV) is a major human pathogen. In addition to its importance in human health, there is growing interest in adapting HBV and other viruses for drug delivery and other nanotechnological applications. In both contexts, precise biophysical characterization of these large macromolecular particles is fundamental. HBV capsids are unusual in that they exhibit two distinct icosahedral geometries, nominally composed of 90 and 120 dimers with masses of approximate to 3 and approximate to 4 MDa, respectively. Here, a mass spectrometric approach was used to determine the masses of both capsids to within 0.1 %. It follows that both lattices are complete, consisting of exactly 180 and 240 subunits. Nanoindentation experiments by atomic-force microscopy indicate that both capsids have similar stabilities. The data yielded a Young's modulus of approximate to 0.4 GPa. This experimental approach, anchored on very precise and accurate mass measurements, appears to hold considerable potential for elucidating the assembly of viruses and other macromolecular particles.

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