Small-Molecule Effectors of Hepatitis B Virus Capsid Assembly Give Insight into Virus Life Cycle

doi:10.1128/JVI.01360-08

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Journal of Virology, October 2008, p. 10262-10270, Vol. 82, No. 20
0022-538X/08/$08.00+0 doi:10.1128/JVI.01360-08
Copyright © 2008, American Society for Microbiology. All Rights Reserved.

Small-Molecule Effectors of Hepatitis B Virus Capsid Assembly Give Insight into Virus Life Cycle

Christina Bourne,¹^, Sejin Lee,² Bollu Venkataiah,² Angela Lee,¹ Brent Korba,³ M. G. Finn,²^* and Adam Zlotnick¹^*

Department of Biochemistry and Molecular Biology, University of Oklahoma Health Sciences Center, 975 NE 10th Street, Oklahoma City, Oklahoma 73126-0901,¹ Department of Chemistry and The Skaggs Institute for Chemical Biology, The Scripps Research Institute, 10550 N. Torrey Pines Rd., La Jolla, California 92037,² Department of Microbiology and Immunology, Georgetown University Medical Center, 3900 Reservoir Rd. NW, Washington, DC 20007³

Received 29 June 2008/ Accepted 30 July 2008

The relationship between the physical chemistry and biologyof self-assembly is poorly understood, but it will be criticalto quantitatively understand infection and for the design ofantivirals that target virus genesis. Here we take advantageof heteroaryldihydropyrimidines (HAPs), which affect hepatitisB virus (HBV) assembly, to gain insight and correlate in vitroassembly with HBV replication in culture. Based on a low-resolutioncrystal structure of a capsid-HAP complex, a closely relatedseries of HAPs were designed and synthesized. These differentiallystrengthen the association between neighboring capsid proteins,alter the kinetics of assembly, and give rise to aberrant structuresincompatible with a functional capsid. The chemical nature ofthe HAP variants correlated well with the structure of the HAPbinding pocket. The thermodynamics and kinetics of in vitroassembly had strong and predictable effects on product morphology.However, only the kinetics of in vitro assembly had a strongcorrelation with inhibition of HBV replication in HepG2.2.15cells; there was at best a weak correlation between assemblythermodynamics and replication. The correlation between assemblykinetics and virus suppression implies a competition betweensuccessful assembly and misassembly, small molecule inducedor otherwise. This is a predictive and testable model for themechanism of action of assembly effectors.

* Corresponding author. Present address for Adam Zlotnick: Indiana University, Department of Biology, Simon Hall MSB, Room 220D, 212 S. Hawthorne Drive, Bloomington, IN 47405-7003. Phone: (812) 856-1925. Fax: (812) 856-5710. E-mail: azlotnic{at}indiana.edu. Mailing address for M. G. Finn: The Scripps Research Institute, Department of Chemistry, 10550 N. Torrey Pines Rd., La Jolla, CA 92037. Phone: (858) 784-8845. Fax: (858) 784-8850. E-mail: mgfinn{at}scripps.edu

Published ahead of print on 6 August 2008.

Present address: 250 McElroy Hall, Department of VeterinaryPathobiology, Oklahoma State University, Stillwater, OK 74078-2007.