Phosphorylation-dependent Binding of Hepatitis B Virus Core Particles to the Nuclear Pore Complex

doi:10.1083/jcb.145.1.45

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J. Cell Biol., Volume 145, Number 1, April 5, 1999 45-55

Phosphorylation-dependent Binding of Hepatitis B Virus Core Particles to the Nuclear Pore Complex

Michael Kann,^* Beate Sodeik, Angelika Vlachou,^* Wolfram H. Gerlich,^* and Ari Helenius

^* Institute of Medical Virology, Justus Liebig University, D-35392 Giessen, Germany; and Yale University School of Medicine, Department of Cell Biology, New Haven, Connecticut 06520-8002

Although many viruses replicate in the nucleus, little is known about the processes involved in the nuclear import of viralgenomes. We show here that in vitro generated core particles ofhuman hepatitis B virus bind to nuclear pore complexes (NPCs)in digitonin-permeabilized mammalian cells. This only occurredif the cores contained phosphorylated core proteins. Binding wasinhibited by wheat germ agglutinin, by antinuclear pore complexantibodies, and by peptides corresponding either to classicalnuclear localization signals (NLS) or to COOH-terminal sequencesof the core protein. Binding was dependent on the nuclear transportfactors importins (karyopherins) $alpha$ and $beta$ . The results suggestedthat phosphorylation induces exposure of NLS in the COOH-terminalportion of the core protein that allows core binding to the NPCsby the importin- (karyopherin-) mediated pathway. Thus, phosphorylationof the core protein emerged as an important step in the viralreplication cycle necessary for transport of the viral genometo thenucleus.

Key words: core; hepatitis B virus; nuclear pore; nucleocapsid; phosphorylation

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