Literature DB >> 22357885

Human hepatocellular carcinoma in a mouse model: assessment of tumor response to percutaneous ablation by using glyceraldehyde-3-phosphate dehydrogenase antagonists.

Shanmugasundaram Ganapathy-Kanniappan1, Rani Kunjithapatham, Michael S Torbenson, Pramod P Rao, Kathryn A Carson, Manon Buijs, Mustafa Vali, Jean-François H Geschwind.   

Abstract

PURPOSE: To characterize tumor response to percutaneous injection of glyceraldehyde-3-phosphate dehydrogenase (GAPDH) antagonists in a mouse model of human hepatocellular carcinoma (HCC).
MATERIALS AND METHODS: Animal experiments were approved by the Johns Hopkins University Animal Care and Use Committee. Luciferase (luc) gene-expressing Hep3B tumor-bearing athymic nude mice were randomly divided into four groups of six mice each. Tumor-specific GAPDH inhibition was achieved by using percutaneous injection of GAPDH antagonists-3-bromopyruvate (3-BrPA) or GAPDH-specific short hairpin RNA (shRNA). Tumor response to treatment was assessed by using bioluminescence imaging and analysis of GAPDH function and apoptotic markers (caspase-3, caspase-9, and positive staining for terminal deoxynucleotidyl transferase-mediated deoxyuridine 5-triphospate nick end labeling). HCC samples from 34 patients were obtained from the Johns Hopkins tumor bank, as approved by the Institutional Review Board, for GAPDH expression analysis. Statistical analysis was performed by using a two-sample t test or Spearman rank correlation coefficient.
RESULTS: In vitro, 3-BrPA affected Hep3B cell viability (half maximal inhibitory concentration = 0.15 mmol/L), and GAPDH shRNA suppressed (45.5%) colony formation. In vivo, percutaneous injection of GAPDH antagonists into luc-Hep3B tumors decreased bioluminescence imaging signal and viability (3-BrPA, P < .0001; GAPDH shRNA, P = .03). The 3-BrPA treatment primarily inhibited GAPDH activity (74.5%) compared with its expression (34.3%), whereas GAPDH shRNA inhibited both activity (60.6%) and expression (44.4%). Targeted inhibition of GAPDH by using 3-BrPA or shRNA induced apoptosis. HCC samples from patients demonstrated a strong correlation between GAPDH upregulation and the proto-oncogene c-jun expression (r = 0.543, P = .003).
CONCLUSION: Percutaneous injection of GAPDH antagonists induces apoptosis and blocks Hep3B tumor progression, which demonstrates the therapeutic potential of targeting GAPDH in human HCC. © RSNA, 2012.

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Year:  2012        PMID: 22357885      PMCID: PMC3285229          DOI: 10.1148/radiol.11111569

Source DB:  PubMed          Journal:  Radiology        ISSN: 0033-8419            Impact factor:   11.105


  33 in total

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Authors:  Muneeb Ahmed; Christopher L Brace; Fred T Lee; S Nahum Goldberg
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Authors:  Eleni Liapi; Jean-Francois H Geschwind
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Authors:  Riccardo Lencioni
Journal:  Hepatology       Date:  2010-08       Impact factor: 17.425

Review 4.  Hepatocellular carcinoma: A global view.

Authors:  Ju Dong Yang; Lewis R Roberts
Journal:  Nat Rev Gastroenterol Hepatol       Date:  2010-07-13       Impact factor: 46.802

Review 5.  RNA interference as therapeutics for hepatocellular carcinoma.

Authors:  Chuanrui Xu; Susie A Lee; Xin Chen
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6.  Intratumoral therapy of glioblastoma multiforme using genetically engineered transferrin for drug delivery.

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Journal:  Cancer Res       Date:  2010-05-11       Impact factor: 12.701

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Review 9.  Molecular bases of liver cancer refractoriness to pharmacological treatment.

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  22 in total

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2.  Metabolic perturbation sensitizes human breast cancer to NK cell-mediated cytotoxicity by increasing the expression of MHC class I chain-related A/B.

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Journal:  Oncoimmunology       Date:  2015-01-14       Impact factor: 8.110

3.  Targeting glucose metabolism in cancer: new class of agents for loco-regional and systemic therapy of liver cancer and beyond?

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4.  Occurrence of a multimeric high-molecular-weight glyceraldehyde-3-phosphate dehydrogenase in human serum.

Authors:  Rani Kunjithapatham; Jean-Francois Geschwind; Lauren Devine; Tatiana N Boronina; Robert N O'Meally; Robert N Cole; Michael S Torbenson; Shanmugasundaram Ganapathy-Kanniappan
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Review 5.  The anticancer agent 3-bromopyruvate: a simple but powerful molecule taken from the lab to the bedside.

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Review 6.  Metabolic interplay between glycolysis and mitochondrial oxidation: The reverse Warburg effect and its therapeutic implication.

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Journal:  World J Biol Chem       Date:  2015-08-26

7.  The transmembrane transporter ABCC3 participates in liver cancer progression and is a potential biomarker.

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8.  AS30D model of hepatocellular carcinoma: tumorigenicity and preliminary characterization by imaging, histopathology, and immunohistochemistry.

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Journal:  Cardiovasc Intervent Radiol       Date:  2012-08-25       Impact factor: 2.740

9.  Effect of methyl jasmonate and 3-bromopyruvate combination therapy on mice bearing the 4 T1 breast cancer cell line.

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Journal:  J Bioenerg Biomembr       Date:  2020-01-20       Impact factor: 2.945

10.  Deregulation of energy metabolism promotes antifibrotic effects in human hepatic stellate cells and prevents liver fibrosis in a mouse model.

Authors:  Swathi Karthikeyan; James J Potter; Jean-Francois Geschwind; Surojit Sur; James P Hamilton; Bert Vogelstein; Kenneth W Kinzler; Esteban Mezey; Shanmugasundaram Ganapathy-Kanniappan
Journal:  Biochem Biophys Res Commun       Date:  2015-10-23       Impact factor: 3.575

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