A metabolic hypothesis of cell growth and death in pancreatic cancer
- PMID: 11741179
- DOI: 10.1097/00006676-200201000-00004
A metabolic hypothesis of cell growth and death in pancreatic cancer
Abstract
Introduction: Tumor cells, just as other living cells, possess the potential for proliferation, differentiation, cell cycle arrest, and apoptosis. There is a specific metabolic phenotype associated with each of these conditions, characterized by the production of both energy and special substrates necessary for the cells to function in that particular state. Unlike that of normal living cells, the metabolic phenotype of tumor cells supports the proliferative state.
Aim: To present the metabolic hypothesis that (1) cell transformation and tumor growth are associated with the activation of metabolic enzymes that increase glucose carbon utilization for nucleic acid synthesis, while enzymes of the lipid and amino acid synthesis pathways are activated in tumor growth inhibition, and (2) phosphorylation and allosteric and transcriptional regulation of intermediary metabolic enzymes and their substrate availability together mediate and sustain cell transformation from one condition to another.
Conclusion: Evidence is presented that demonstrates opposite changes in metabolic phenotypes induced by TGF-beta, a cell-transforming agent, and tumor growth-inhibiting phytochemicals such as genistein and Avemar, or novel synthetic anti-leukemic drugs such as STI571 (Gleevec). Intermediary metabolic enzymes that mediate the growth signaling pathways and promote malignant cell transformation may serve as high-efficacy nongenetic novel _targets for cancer therapies.
Similar articles
-
Use of metabolic pathway flux information in anticancer drug design.Ernst Schering Found Symp Proc. 2007;(4):189-203. doi: 10.1007/2789_2008_094. Ernst Schering Found Symp Proc. 2007. PMID: 18811058 Review.
-
Fermented wheat germ extract inhibits glycolysis/pentose cycle enzymes and induces apoptosis through poly(ADP-ribose) polymerase activation in Jurkat T-cell leukemia tumor cells.J Biol Chem. 2002 Nov 29;277(48):46408-14. doi: 10.1074/jbc.M206150200. Epub 2002 Sep 25. J Biol Chem. 2002. PMID: 12351627
-
Genistein inhibits nonoxidative ribose synthesis in MIA pancreatic adenocarcinoma cells: a new mechanism of controlling tumor growth.Pancreas. 2001 Jan;22(1):1-7. doi: 10.1097/00006676-200101000-00001. Pancreas. 2001. PMID: 11138960
-
TGFbeta1 represses proliferation of pancreatic carcinoma cells which correlates with Smad4-independent inhibition of ERK activation.Oncogene. 2000 Sep 14;19(39):4531-41. doi: 10.1038/sj.onc.1203806. Oncogene. 2000. PMID: 11002426
-
Metabolic biomarker and kinase drug _target discovery in cancer using stable isotope-based dynamic metabolic profiling (SIDMAP).Curr Cancer Drug _targets. 2003 Dec;3(6):445-53. doi: 10.2174/1568009033481769. Curr Cancer Drug _targets. 2003. PMID: 14683502 Review.
Cited by
-
Clinical consequences of hyperglycemia during remission induction therapy for pediatric acute lymphoblastic leukemia.Leukemia. 2009 Feb;23(2):245-50. doi: 10.1038/leu.2008.289. Epub 2008 Oct 16. Leukemia. 2009. PMID: 18923438 Free PMC article.
-
NMR-based metabonomic analysis of HUVEC cells during replicative senescence.Aging (Albany NY). 2020 Feb 17;12(4):3626-3646. doi: 10.18632/aging.102834. Epub 2020 Feb 17. Aging (Albany NY). 2020. PMID: 32074082 Free PMC article.
-
Tracer-based metabolomics: concepts and practices.Clin Biochem. 2010 Nov;43(16-17):1269-77. doi: 10.1016/j.clinbiochem.2010.07.027. Epub 2010 Aug 14. Clin Biochem. 2010. PMID: 20713038 Free PMC article. Review.
-
Characterizing phenotype with tracer based metabolomics.Metabolomics. 2006;2:31-39. doi: 10.1007/s11306-006-0017-3. Epub 2006 May 20. Metabolomics. 2006. PMID: 25540606 Free PMC article.
-
Metabolic analysis of senescent human fibroblasts reveals a role for AMP in cellular senescence.Biochem J. 2003 Dec 1;376(Pt 2):403-11. doi: 10.1042/BJ20030816. Biochem J. 2003. PMID: 12943534 Free PMC article.
Publication types
MeSH terms
Substances
Grants and funding
LinkOut - more resources
Full Text Sources
Medical
