Abstract

The overall goal of this proposal is to understand the molecular basis of hepatocellular carcinoma in hepadnavirus carriers. The first two specific aims of the proposal will involve and in-depth study of a new system we have developed to study the role of topoisomerase activity in viral replication and integration.
Specific Aim 1 will focus on the mechanism by which Camptothecin (CPT), a specific Topoisomerase I inhibitor, inhibits viral replication in cytoplasmic capsids in a chicken hepatoma cell line (LMH) transfected with a mutant (IS) DHBV genome which accumulates cytoplasmic capsid particles and recycles DHBV DNA into the nucleus. In addition to time course and dose response experiments, site specific mutagenesis of DHBV DNA and immune precipitation experiments will establish the nature of the topoisomerase activity and provide new genetic mapping information of the DHBV Pol gene. We will also express the spacer domain of the DHBV Pol gene and test it for topoisomerase activity """"""""in vitro."""""""" Specific Aim 2 will study the effect of CPT on the transport of DHBV DNA to the nucleus and its processing in the nucleus. We will determine whether CPT treatment induces integrated molecules using an integration assay based on inverse PCR technology. The studies in Specific Aim 3 will focus on gene expression in precancerous nodules of the woodchuck. We will attempt to understand the mechanism of N-myc activation in precancerous nodules. By studying the activity of a group of selected genes by """"""""in situ"""""""" hybridization we will gain insight into molecular mechanisms associated with precancerous lesions. In conjunction with this, we will utilize two woodchuck liver epithelial cell lines to directly test the effects of IL1, IL6, and TNF-alpha on N-myc expression.
Specific Aim 4 will directly test the effect of IGF-II in hepatocarcinogenesis using transgenic mouse mating experiments. Using the first transgenic mouse line to produce IGF-II in the adult mouse liver (developed by us) we will determine if IGF-II functions synergistically with HBV envelope proteins in inducing HCC. In a reverse approach, we will also test whether knocking out the endogeneous IGF-II gene prevents or inhibits the HBsAg lesion from progressing to HCC. Finally, we will utilize our transgenic mouse models (HBsAg line 50-4, and SV40 T Ag) to determine whether the maternally imprinted IGF-II allele can be activated during hepatocarcinogenesis. This experiment will increase our general understanding of a possible tumor suppressor, or cancer protective, role of gene imprinting.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA037232-12
Application #
2089266
Study Section
Experimental Virology Study Section (EVR)
Project Start
1984-04-01
Project End
1996-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
12
Fiscal Year
1995
Total Cost
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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