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A study from Watson School of Biological Sciences shows that Mutant p53 Drives Pancreatic Cancer Metastasis through Cell-Autonomous PDGF Receptor β Signaling. This study was published in the April 10, 2014 Cell by Prof. Dr Scott Lowe, Watson School of Biological Sciences, CSHL, New York; Prof. Dr Carol Prives, Department of Biological Sciences, Columbia University, New York; and others.

On the foundation of this interesting finding, Dr L Boominathan, Director-cum-chief Scientist of GBMD, reports here that:  Insight into the treatment of Metastatic Pancreatic/intestine/ovarian Cancer: Genistein suppresses the expression of  PDGF Receptor β via up regulation of its target gene. Given that tumor suppressor p53 is mutated in about 50% of different human cancers, this study suggests, for the first time, a therapeutic strategy as to how mutant p53 expressing human cancers can be cured.

Idea Proposed/Formulated byDr L Boominathan Ph.D.

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To citeBoominathan, Insight into the treatment of Metastatic Pancreatic/intestine/ovarian Cancer:  Genistein suppresses the expression of  PDGF Receptor β via up regulation of its target gene, 2/May/2014, 8.37 am, Genome-2-Bio-Medicine Discovery center (GBMD), http://genomediscovery.org

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