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Agios Publishes Groundbreaking Research in Nature Uncovering the New Role of IDH1 Gene Mutation in Brain Cancer –Findings Validate Cancer Metabolism as an Approach to Identify New Ways to Treat Cancer– –Opens Potential for New Class of Cancer Drugs Targeting Metabolic Enzymes– Cambridge, MA – November 23, 2009 –Agios Pharmaceuticals today announced that its scientists have established, for the first time, that the mutated IDH1 gene has a novel enzyme activity consistent with a cancer-causing gene, or oncogene. This breakthrough discovery shows that the mutated form of IDH1 produces a metabolite, 2-hydroxyglutarate (2HG), which may contribute to the formation and malignant progression of gliomas, the most common type of brain cancers. This discovery appears to reverse the previously held belief that IDH1 was non functional for cancer-causing activity. It is also one of the first reported instances where a metabolic enzyme such as IDH1 is shown to play a role in cancer formation, in this case through altered metabolic activity. This finding creates opportunities for therapeutic intervention in brain cancer and other cancers where IDH1 mutations are present using new drugs that can target the IDH1 metabolic pathway. The Agios research also identified an exciting new biomarker, 2HG, that could be used to develop an important diagnostic. The research was published on November 22 by the journal Nature, in a paper entitled “Cancer-associated IDH1 mutations produce 2-hydroxyglutarate (2HG)”. [1] “This groundbreaking work is profound for the field,” said Professor Lew Cantley, Ph.D., Director of the Cancer Center at the Beth Israel Deaconess Medical Center, a founder of Agios and a supporting author. “The team at Agios has demonstrated that what was previously considered an inactive enzyme is in reality an active oncogene and a potential therapeutic target. This has fundamentally changed our understanding of the field. Additionally, there is an easily measured metabolic biomarker, 2HG, that will help in the diagnosis and treatment of any related therapeutics that arise from this work.” “Agios’ founding principles included the belief that targeting important metabolic pathways of cancers could make a fundamental difference in the treatment of the disease. Our IDH1 discovery is a great example of the power of the team and of our approach in targeting cancer metabolic pathways. In just four months, scientists at Agios unraveled very complex biology to advance a new understanding of gliomas and the role of IDH1 and corresponding biomarkers,” said David Schenkein, M.D., Chief Executive Officer, Agios. “We are able to do this by utilizing a unique approach of integrating deep biology and leveraging our proprietary platform for cancer metabolism research. “We are looking forward to developing potential therapeutics specifically targeting IDH1 for patients with these devastating diseases, and to leveraging our unique cross functional approach to cancer metabolism research in order to discover insights into other targets and pathways,” added Schenkein. About the metabolic enzyme IDH1 and its role in cancer The insight from this new research at Agios is the first to reveal the function of the mutated IDH1 gene and provides critical insight into the mechanism by which this mutation leads to the development of brain cancer. Reports to date about the role of IDH1 have suggested that the gene functions as a tumor suppressor that, when mutationally inactivated, may contribute to brain tumor growth. The most recent research from Agios scientists published in Nature [1] suggests that it is activation of a metabolic pathway – rather than inactivation of a tumor suppression function – that is the likely process for oncogene function of IDH1. About Gliomas About Cancer Metabolism About Agios Pharmaceuticals [1] Dang et al. Cancer-associated IDH1 mutations produce 2-hydroxyglutarate. Nature 2009;In press. DOI: 10.1038/nature08617 [2] Parsons, D. W. et al. An integrated genomic analysis of human glioblastoma multiforme. Science 321, 1807-12 (2008); Yan, H. et al. IDH1 and IDH2 mutations in gliomas. N Engl J Med 360, 765-73 (2009). Media Contacts: U.S. Europe [ back to top ] |
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