Abstract

The overall objective of this proposal is to define the molecular mechanisms contributing to liver carcinogenesis. The development of hepatocellular carcinoma is mediated by multiple growth signaling pathways that regulate cellular proliferation. We have shown that liver cell growth is regulated by two recently- discovered heparin-degrading endosulfatases, sulfatase 1 (SULF1) and sulfatase 2 (SULF2). These sulfatases modify the binding of heparin-binding growth factors to their receptors on the cell surface or in the extracellular matrix. We have generated striking preliminary data that show that SULF1 and SULF2 have opposing effects on proliferation and tumorigenesis of hepatocellular carcinoma cell lines. These results are particularly intriguing because SULF1 and SULF2 have both been shown to have a similar 6-O-endosulfatase action on heparan sulfate proteoglycan substrates. Our further experiments suggest that SULF1 and SULF2 exert their effects on hepatocellular carcinoma cells in part through modulation of the Wnt/?-catenin signaling pathway. Based on these extensive preliminary data, we propose the CENTRAL HYPOTHESIS that SULF1 and SULF2 differentially regulate Wnt/?-catenin signaling, leading to consequent opposing effects on cancer cell proliferation and sensitivity to apoptosis. Our proposal has three SPECIFIC AIMS. FIRST, we will test the hypothesis that SULF1 and SULF2 have opposing functional effects on Wnt/?-catenin signaling in hepatocellular carcinoma by demonstrating that i) SULF1 downregulates and ii) SULF2 upregulates Wnt/?- catenin signaling that mediates downstream effects on Wnt pathway constituents, cell growth and sensitivity to apoptosis. SECOND, we will test the hypothesis that SULF1 and SULF2 have opposing functional effects because they bind to and desulfate different subdomains of the heparan sulfate proteoglycans at the cell. In this Specific Aim we will i) examine the differences in action of SULF1 and SULF2 on subdomains of heparan sulfate on the cell surface, and ii) determine the specific protein domains on SULF1 and SULF2 responsible for the differences in functional effects of the two sulfatases. FINALLY, in the THIRD aim, we will test the hypothesis that SULF1 and SULF2 have opposing mechanistic and functional effects on liver carcinogenesis in vivo. In this aim, we will examine i) differential effects of modulation of SULF1 and SULF2 expression on Wnt signaling pathways in SULF1 and SULF2 knockout and transgenic mice, and ii) the association between SULF1 and SULF2 expression and Wnt target gene expression in human hepatocellular carcinomas. To address these questions, we have established hepatocellular carcinoma cell lines that differentially express SULF1 and SULF2 and have become adept at dissecting heparin-binding growth factor and Wnt/?-catenin signaling pathways. We are also collaborating with a structural biologist to explore SULF1 and SULF2 structure-function relationships. Finally, we have obtained SULF1 and SULF2 knockout mice and are developing SULF1 and SULF2 transgenic mouse models for the in vivo studies. The proposal is conceptually and technically innovative as it tests new concepts as to how heparin-degrading endosulfatases regulate the major cancer phenotypes of dysregulated proliferation and evasion of apoptosis. The information emanating from these studies may lead to the development of therapeutic strategies for chemoprevention and treatment of hepatocellular carcinoma.

Public Health Relevance

Liver cancer kills over 600,000 individuals worldwide each year, and over 15,000 Americans each year. The incidence of liver cancer in the United States has doubled over the past 25 years, but relatively few research projects are targeted to this disease. For most liver cancer patients, the cause of death is attributable to metastatic spread within the liver, or to the lungs or bones. The goal of this project is to understand the mechanisms that underlie initiation, growth and metastasis in human liver cancer and use this knowledge to predict, prevent and treat this condition in patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
High Priority, Short Term Project Award (R56)
Project #
3R56CA100882-06A1S1
Application #
7935583
Study Section
Hepatobiliary Pathophysiology Study Section (HBPP)
Program Officer
Ogunbiyi, Peter
Project Start
2003-04-01
Project End
2010-07-31
Budget Start
2009-08-01
Budget End
2010-07-31
Support Year
6
Fiscal Year
2009
Total Cost
$79,545
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Betesh, Lucy; Comunale, Mary Ann; Wang, Mengjun et al. (2017) Identification of fucosylated Fetuin-A as a potential biomarker for cholangiocarcinoma. Proteomics Clin Appl 11:
Yang, Ju Dong; Campion, Michael B; Liu, Minetta C et al. (2016) Circulating tumor cells are associated with poor overall survival in patients with cholangiocarcinoma. Hepatology 63:148-58
Peeraphatdit, Thoetchai; Naksuk, Niyada; Thongprayoon, Charat et al. (2015) Prognostic Value of Model for End-Stage Liver Disease Score Measurements on a Daily Basis in Critically Ill Patients With Cirrhosis. Mayo Clin Proc 90:1196-206
Chaiteerakij, Roongruedee; Zhang, Xiaodan; Addissie, Benyam D et al. (2015) Combinations of biomarkers and Milan criteria for predicting hepatocellular carcinoma recurrence after liver transplantation. Liver Transpl 21:599-606
Chaiteerakij, Roongruedee; Juran, Brian D; Aboelsoud, Mohammed M et al. (2015) Association between variants in inflammation and cancer-associated genes and risk and survival of cholangiocarcinoma. Cancer Med 4:1599-602
Shire, Abdirashid; Lomberk, Gwen; Lai, Jin-Ping et al. (2015) Restoration of epigenetically silenced SULF1 expression by 5-aza-2-deoxycytidine sensitizes hepatocellular carcinoma cells to chemotherapy-induced apoptosis. Med Epigenet 3:1-18
Dhanasekaran, Renumathy; Nakamura, Ikuo; Hu, Chunling et al. (2015) Activation of the transforming growth factor-?/SMAD transcriptional pathway underlies a novel tumor-promoting role of sulfatase 1 in hepatocellular carcinoma. Hepatology 61:1269-83
Chaiteerakij, Roongruedee; Harmsen, William S; Marrero, Carlos Romero et al. (2014) A new clinically based staging system for perihilar cholangiocarcinoma. Am J Gastroenterol 109:1881-90
Singh, Siddharth; Singh, Preet Paul; Roberts, Lewis R et al. (2014) Chemopreventive strategies in hepatocellular carcinoma. Nat Rev Gastroenterol Hepatol 11:45-54
Kisiel, John B; Li, Jia; Zou, Hongzhi et al. (2013) Methylated Bone Morphogenetic Protein 3 (BMP3) Gene: Evaluation of Tumor Suppressor Function and Biomarker Potential in Biliary Cancer. J Mol Biomark Diagn 4:1000145

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