A cell‐surface β‐hydroxylase is a biomarker and therapeutic target for hepatocellular carcinoma

Hepatocellular carcinoma (HCC) has a poor prognosis as a result of widespread intra‐ and extrahepatic metastases. There is an urgent need to understand signaling cascades that promote disease progression. Aspartyl‐(asparaginyl)‐β‐hydroxylase (ASPH) is a cell‐surface enzyme that generates enhanced ce...

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Published in:	Hepatology (Baltimore, Md.) Vol. 60; no. 4; pp. 1302 - 1313
Main Authors:	Aihara, Arihiro, Huang, Chiung‐Kuei, Olsen, Mark J., Lin, Qiushi, Chung, Waihong, Tang, Qi, Dong, Xiaoqun, Wands, Jack R.
Format:	Journal Article
Language:	English
Published:	United States 01-10-2014
Subjects:	Animals Biomarkers, Tumor - antagonists & inhibitors Biomarkers, Tumor - metabolism Carcinoma, Hepatocellular - drug therapy Carcinoma, Hepatocellular - metabolism Carcinoma, Hepatocellular - pathology Cell Line, Tumor Cell Movement - drug effects Cell Movement - physiology Cell Proliferation - drug effects Cell Proliferation - physiology Disease Models, Animal Enzyme Inhibitors - pharmacology Female Furans - pharmacology Heterografts Humans In Vitro Techniques Liver Neoplasms - drug therapy Liver Neoplasms - metabolism Liver Neoplasms - pathology Membrane Proteins - antagonists & inhibitors Membrane Proteins - drug effects Membrane Proteins - metabolism Mice Mice, Nude Mixed Function Oxygenases - antagonists & inhibitors Mixed Function Oxygenases - drug effects Mixed Function Oxygenases - metabolism Neoplasm Metastasis - drug therapy Neoplasm Metastasis - physiopathology Receptors, Notch - antagonists & inhibitors Receptors, Notch - drug effects Signal Transduction - drug effects Sulfonic Acids - pharmacology
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Summary:	Hepatocellular carcinoma (HCC) has a poor prognosis as a result of widespread intra‐ and extrahepatic metastases. There is an urgent need to understand signaling cascades that promote disease progression. Aspartyl‐(asparaginyl)‐β‐hydroxylase (ASPH) is a cell‐surface enzyme that generates enhanced cell motility, migration, invasion, and metastatic spread in HCC. We hypothesize that inhibition of its enzymatic activity could have antitumor effects. Small molecule inhibitors (SMIs) were developed based on the crystal structure of the ASPH catalytic site followed by computer‐assisted drug design. Candidate compounds were tested for inhibition of β‐hydroxylase activity and selected for their capability to modulate cell proliferation, migration, invasion, and colony formation in vitro and to inhibit HCC tumor growth in vivo using orthotopic and subcutaneous murine models. The biological effects of SMIs on the Notch signaling cascade were evaluated. The SMI inhibitor, MO‐I‐1100, was selected because it reduced ASPH enzymatic activity by 80% and suppressed HCC cell migration, invasion, and anchorage‐independent growth. Furthermore, substantial inhibition of HCC tumor growth and progression was observed in both animal models. The mechanism(s) for this antitumor effect was associated with reduced activation of Notch signaling both in vitro and in vivo. Conclusions: These studies suggest that the enzymatic activity of ASPH is important for hepatic oncogenesis. Reduced β‐hydroxylase activity generated by the SMI MO‐I‐1100 leads to antitumor effects through inhibiting Notch signaling cascade in HCC. ASPH promotes the generation of an HCC malignant phenotype and represents an attractive molecular target for therapy of this fatal disease. (Hepatology 2014;60:1302–1313)
Bibliography:	Potential conflict of interest: Nothing to report. This work was supported by grants from the Ruth L. Kirschstein National Research Service Award (NRSA) Institutional Research Training (IT‐32 DK60415), the National Institutes of Health/National Cancer Institute (NIH)/NCI (R01CA123544), the National Institute for General Medical Sciences (NIGMS), an NIH RI‐INBRE Faculty Development Research Project Grant (8P20GM103430‐12), 2012 URI Division of Research & Economic Development and URI Council for Research Proposal Development Grants, and 2011 AACR‐FNAB Fellows Grant for Translational Pancreatic Cancer Research (11‐30‐14‐DONG). ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23
ISSN:	0270-9139 1527-3350
DOI:	10.1002/hep.27275