University of North Carolina at Chapel Hill Graduate School
Doi
Abstract
Primary liver cancer, including hepatocellular carcinoma (HCC) and cholangiocarcinoma (CCA), is one of the fastest growing cancer types. Although HCCs and CCAs are anatomically co-localized, they have distinct etiologic and genomic characteristics that varies vastly in clinical outcome and response to therapy. The Cancer Genome Atlas (TCGA) identified a subset of HCC tumors with CCA genomic features, suggesting these tumors may be a separate HCC class based on their relatedness to CCA. While multiple groups have performed molecular characterization of liver tumors in an effort to identify subtypes, few have investigated beyond gene expression and/or mutations, in an integrated HCC and CCA analysis, or in association with outcomes and liver specific processes (e.g., liver regeneration). This is particularly important because DNA repair dysfunction and liver regeneration are tightly coupled processes implicated in impaired genomic integrity and hepatocarcinogenesis. Particularly, dysregulation of these pathways may be linked to chemoresistance. Given the lack of targeted therapeutic modalities for HCC and ongoing efforts to reduce recurrence, further characterizing and subdividing HCC based on multiple pathway interactions and identification of biomarkers that are associated with repair-mediated survival represents an unmet clinical need. To address this knowledge gap, the current body of work leveraged two TCGA studies, HCC and CCA, both detailed in molecular, histological, and clinical data across multiple platforms. Through a multi-omic approach, chapter 2 of this study characterized distinct HCC subclasses utilizing an integrated TCGA HCC and CCA dataset to gain insights into biology. Chapter 3 leveraged RNA expression profiling to investigate DNA repair in association with mitotic and regenerative signatures, and clinicopathologic variables in TCGA HCC study. This work identified three molecularly distinct HCC subclasses associated with viral infection and progression-free survival. In addition, RNA-based classification of DNA repair identified heterogeneity of repair pathways in HCC tumors, and a subset of tumors with substantial disrupted liver biology and poor outcomes. Collectively, this work contributes novel findings about HCC features and repair dysfunction that dictate prognosis, and highlights the importance of developing class specific biomarkers and targeted therapies.Doctor of Philosoph
