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Limited Redundancy of Survival Signals from the Type 1 Insulin-Like Growth Factor Receptor*
71
Citations
62
References
2001
Year
ApoptosisImmunologyMitochondrial Raf TranslocationCell DeathCell ProliferationInsulin SignalingInflammationMetabolic SyndromeType 1Signaling PathwaySurvival SignalFibroblast Growth FactorInsulin DeliveryCell SignalingHealth SciencesGrowth HormoneInsulin ManagementLimited RedundancyEndocrinologyCell BiologyTumor MicroenvironmentSurvival SignalsSignal TransductionDiabetesDiabetes MellitusSystems BiologyMedicine
The type 1 insulin-like growth factor receptor (IGF-IR) is effective in protecting cells from a variety of apoptotic injuries. In 32D murine hemopoietic cells, the IGF-IR sends three separate survival signals, through insulin receptor substrate-1, Shc, and mitochondrial Raf translocation. We report here that these three pathways for survival have a limited redundancy. If one of these pathways is blocked, the IGF-IR can still protect 32D cells from apoptosis induced by interleukin-3 withdrawal. However, when two of the three pathways are inactivated, the receptor is no longer capable to protect cells from apoptosis. The survival signal can use any two pathway combinations.
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