Activation of Notch-1 signaling maintains the neoplastic phenotype in human Ras-transformed cells |
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| Authors: | Weijzen Sanne Rizzo Paola Braid Mike Vaishnav Radhika Jonkheer Suzanne M Zlobin Andrei Osborne Barbara A Gottipati Sridevi Aster Jon C Hahn William C Rudolf Michael Siziopikou Kalliopi Kast W Martin Miele Lucio |
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| Institution: | Cancer Immunology Program, Cardinal Bernardin Cancer Center, Loyola University Chicago, Maywood, Illinois, USA. |
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| Abstract: | Truncated Notch receptors have transforming activity in vitro and in vivo. However, the role of wild-type Notch signaling in neoplastic transformation remains unclear. Ras signaling is deregulated in a large fraction of human malignancies and is a major target for the development of novel cancer treatments. We show that oncogenic Ras activates Notch signaling and that wild-type Notch-1 is necessary to maintain the neoplastic phenotype in Ras-transformed human cells in vitro and in vivo. Oncogenic Ras increases levels and activity of the intracellular form of wild-type Notch-1, and upregulates Notch ligand Delta-1 and also presenilin-1, a protein involved in Notch processing, through a p38-mediated pathway. These observations place Notch signaling among key downstream effectors of oncogenic Ras and suggest that it might be a novel therapeutic target. |
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