Hepatitis B virus (HBV) chronically infects 250 - 350 million people worldwide, causing most liver cancers, the second leading cause of cancer death in men and a major cancer in women. HBV maintains these chronic infections and induces cancer by active replication through poorly understood pathways that traffic viral DNA and RNAs between the nucleus and cytoplasm, and direct successive interactions of key viral and cell factors in the cytoplasm for capsid assembly, reverse transcription, envelopment and secretion. In this project, we will build on our striking new HBV discoveries and newly developed advanced imaging and other research tools to advance key issues in HBV biology, thus providing essential foundations for critically needed new approaches to disrupt HBV chronic infections and thus block development of HBV-induced liver cancers.
Aim 1 will define the sites and transport connections of key HBV capsid assembly, maturation and budding steps in the cytoplasm, including where HBV polymerase (Pol) and pregenomic RNA (pgRNA) interact and are encapsidated, and where capsids undergo successive steps in reverse transcription, interact with viral envelope proteins, and bud into the secretory pathway. The results will integrate powerfully with parallel cryo-EM studies that we are performing with our collaborator Adam Zlotnick (Indiana Univ.) of the nano-scale structures of maturing capsids at each matched step, revealing in a multi-scale vision of HBV replication how these structural changes are translated into cell biology effects.
Aim 2 will yield the first full analysis of HBV cccDNA trafficking, maintenance, mitotic segregation and transcription in the nucleus, and the unprecedented pulsiform nuclear export of HBV pgRNA that we recently discovered. These results will provide foundations for rational development of treatments targeting cccDNA as the main genome reservoir of chronic infection, and pgRNA export as an increasingly attractive control point.
Aim 3 will define the basis and functions of our exciting new discoveries that most HBV Pol localizes to mitochondria for roles independent of reverse transcription, and that Pol stimulates production of mitochondrially active ceramides that promote apoptosis and mitophagy. The results will inform if and how this association supports Pol?s multiple emerging functions in modulating mitochondrially-linked innate immune responses, which has potential implications for HBV control and for the chronic inflammation that contributes to HBV oncogenesis.

Public Health Relevance

Hepatitis B virus (HBV) chronically infects more than 250 - 350 million people worldwide and is the leading cause of liver cancer. Few treatments exist to block infectious HBV virion production or spread, reflecting our limited knowledge of the HBV functions and host interactions governing HBV replication and persistent infection. This project will combine advanced imaging, biochemical, genetic and other approaches to provide crucial new insights into the mechanisms of HBV replication and to inform the development of novel antiviral strategies.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA022443-43
Application #
9924302
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2020-05-01
Budget End
2021-04-30
Support Year
43
Fiscal Year
2020
Total Cost
Indirect Cost
Name
University of Wisconsin Madison
Department
Type
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715
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