TY - JOUR
T1 - Lost in translation
T2 - Dysregulation of cap-dependent translation and cancer
AU - Bjornsti, Mary Ann
AU - Houghton, Peter J.
N1 - Funding Information:
The authors were supported by USPHS grants CA58755 (M.A.B.), CA23099 (P.J.H. and M.A.B.), CA77776 (P.J.H.), CA96696 (P.J.H.), CA21765, and ALSAC.
PY - 2004/6
Y1 - 2004/6
N2 - Activation of the phosphatidylinositol 3′ kinase-Akt pathway has long been associated with malignant transformation and antiapoptotic signaling. Mutations downstream of Akt that activate the TOR kinase are found in tumor-prone syndromes, while overexpression of translation initiation complex components, such as eIF4E, occurs frequently in human cancer. However, direct roles for TOR signaling or eIF4E overexpression, in the genesis of cancer, have been lacking. Recent papers, including one by Avdulov et al. (2004) in this issue of Cancer Cell, clearly establish that dysregulation of cap-dependent translation confers malignant characteristics and induces cancer by suppressing apoptosis, underscoring the potential of therapeutics that selectively target the Akt-TOR-eIF4E pathway.
AB - Activation of the phosphatidylinositol 3′ kinase-Akt pathway has long been associated with malignant transformation and antiapoptotic signaling. Mutations downstream of Akt that activate the TOR kinase are found in tumor-prone syndromes, while overexpression of translation initiation complex components, such as eIF4E, occurs frequently in human cancer. However, direct roles for TOR signaling or eIF4E overexpression, in the genesis of cancer, have been lacking. Recent papers, including one by Avdulov et al. (2004) in this issue of Cancer Cell, clearly establish that dysregulation of cap-dependent translation confers malignant characteristics and induces cancer by suppressing apoptosis, underscoring the potential of therapeutics that selectively target the Akt-TOR-eIF4E pathway.
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U2 - 10.1016/j.ccr.2004.05.027
DO - 10.1016/j.ccr.2004.05.027
M3 - Review article
C2 - 15193254
AN - SCOPUS:2942518250
SN - 1535-6108
VL - 5
SP - 519
EP - 523
JO - Cancer Cell
JF - Cancer Cell
IS - 6
ER -