Abstract

Infection of humans with hepatitis B viruses cause acute and persistent infections of worldwide significance. Persistent infections, in particular, are associated with a very high risk of hepatocellular carcinoma (HCC). HCCs arise in HBV carriers after long periods of immunologically driven liver disease that is characterized by periods of inflammation, regeneration, cirrhosis and finally HCC. One of the hallmarks of HCCs arising in I-IBV carriers is the presence of clonally amplified viral DNA integrations. Our laboratory has carried out studies to understand the mechanisms by which viral DNA integrations may act as mutagenic agents during hepatocarcinogenesis. Our approach has been to study the natural history and frequency of integrations in clonal populations of cells. These studies have implicated a minor form of hepadnavirus DNA, specifically, double strand linear (DSL) viral DNA molecules as the precursors for integration and have also shown that DSL DNAs integrate at a higher frequency than wild type DNAs. Furthermmore, we have shown that integrations can be lost from the cells along with cellular DNA in a """"""""hit and run"""""""" mutagenesis mechanism. In the current proposal we will utilize a new assay system that can detect single integrations to study integration frequencies of DSL versus WT viral DNA and follow the dynamic flux of integrations in cell culture. We will pursue integration studies during infection of primary hepatocytes under conditions that cause DNA damage and we will also utilize mutational analysis to test the hypothesis that topoisomerase I (top 1) acts as a regulator of viral replication and integration. These studies will increase our understanding of the genetic and physiologic controls of integration and their mutagenic impact on the host cell. Finally, in a new area of research, we will utilize cDNA microarrays to investigate the effects of the HBV X regualtory protein on the transcriptome of murine liver stem cells in both the liver progenitor and hepatocytic differentiation states. These studies will begin to help us understand the impact ofHBx on transcriptional regulation from a global perspective.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA037232-18
Application #
6335489
Study Section
Virology Study Section (VR)
Program Officer
Read-Connole, Elizabeth Lee
Project Start
1984-04-01
Project End
2006-04-30
Budget Start
2001-05-09
Budget End
2002-04-30
Support Year
18
Fiscal Year
2001
Total Cost
$434,799
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
009095365
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Rogler, Charles E; Bebawee, Remon; Matarlo, Joe et al. (2017) Triple Staining Including FOXA2 Identifies Stem Cell Lineages Undergoing Hepatic and Biliary Differentiation in Cirrhotic Human Liver. J Histochem Cytochem 65:33-46
Rogler, Leslie E; Kosmyna, Brian; Moskowitz, David et al. (2014) Small RNAs derived from lncRNA RNase MRP have gene-silencing activity relevant to human cartilage-hair hypoplasia. Hum Mol Genet 23:368-82
Connolly, Erin C; Van Doorslaer, Koenraad; Rogler, Leslie E et al. (2010) Overexpression of miR-21 promotes an in vitro metastatic phenotype by targeting the tumor suppressor RHOB. Mol Cancer Res 8:691-700
Rogler, Charles E; Levoci, Lauretta; Ader, Tammy et al. (2009) MicroRNA-23b cluster microRNAs regulate transforming growth factor-beta/bone morphogenetic protein signaling and liver stem cell differentiation by targeting Smads. Hepatology 50:575-84
Connolly, Erin; Melegari, Margherita; Landgraf, Pablo et al. (2008) Elevated expression of the miR-17-92 polycistron and miR-21 in hepadnavirus-associated hepatocellular carcinoma contributes to the malignant phenotype. Am J Pathol 173:856-64
Rogler, Charles E; Zhou, Hong Chou; LeVoci, Lauretta et al. (2007) Clonal, cultured, murine fetal liver hepatoblasts maintain liver specification in chimeric mice. Hepatology 46:1971-8
Hajjou, Mustapha; Norel, Raquel; Carver, Robert et al. (2005) cDNA microarray analysis of HBV transgenic mouse liver identifies genes in lipid biosynthetic and growth control pathways affected by HBV. J Med Virol 77:57-65
Rogler, Charles E; Tchaikovskaya, Tatyana; Norel, Raquel et al. (2004) RNA expression microarrays (REMs), a high-throughput method to measure differences in gene expression in diverse biological samples. Nucleic Acids Res 32:e120
Plescia, C; Rogler, C; Rogler, L (2001) Genomic expression analysis implicates Wnt signaling pathway and extracellular matrix alterations in hepatic specification and differentiation of murine hepatic stem cells. Differentiation 68:254-69
Pourquier, P; Jensen, A D; Gong, S S et al. (1999) Human DNA topoisomerase I-mediated cleavage and recombination of duck hepatitis B virus DNA in vitro. Nucleic Acids Res 27:1919-25

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