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A common signaling cascade may underlie "addiction" to the Src, BCR-ABL, and EGF receptor oncogenes.


ABSTRACT: "Oncogene addiction" describes an unexplained dependency of cancer cells on a particular cellular pathway for survival or proliferation. We report that differential attenuation rates of prosurvival and proapoptotic signals in oncogene-dependent cells contribute to cell death following oncogene inactivation. Src-, BCR-ABL-, and EGF receptor-dependent cells exhibit a similar profile of signal attenuation following oncogene inactivation characterized by rapid diminution of phospho-ERK, -Akt, and -STAT3/5, and a delayed accumulation of the proapoptotic effector phospho-p38 MAPK. These findings implicate a transient imbalance in survival and apoptotic oncogenic outputs in the apoptotic response to oncogene inactivation. Moreover, these observations implicate a common profile of signal attenuation for multiple oncogenes and suggest that "addiction" associated with apoptosis reflects an active rather than a passive process.

SUBMITTER: Sharma SV 

PROVIDER: S-EPMC2673136 | biostudies-literature | 2006 Nov

REPOSITORIES: biostudies-literature

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A common signaling cascade may underlie "addiction" to the Src, BCR-ABL, and EGF receptor oncogenes.

Sharma Sreenath V SV   Gajowniczek Patrycja P   Way Inna P IP   Lee Diana Y DY   Jiang Jane J   Yuza Yuki Y   Classon Marie M   Haber Daniel A DA   Settleman Jeffrey J  

Cancer cell 20061101 5


"Oncogene addiction" describes an unexplained dependency of cancer cells on a particular cellular pathway for survival or proliferation. We report that differential attenuation rates of prosurvival and proapoptotic signals in oncogene-dependent cells contribute to cell death following oncogene inactivation. Src-, BCR-ABL-, and EGF receptor-dependent cells exhibit a similar profile of signal attenuation following oncogene inactivation characterized by rapid diminution of phospho-ERK, -Akt, and -S  ...[more]

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