Cell Reports (Sep 2014)

κB-Ras Proteins Regulate Both NF-κB-Dependent Inflammation and Ral-Dependent Proliferation

  • Andrea Oeckinghaus,
  • Thomas S. Postler,
  • Ping Rao,
  • Heike Schmitt,
  • Verena Schmitt,
  • Yenkel Grinberg-Bleyer,
  • Lars I. Kühn,
  • Christian W. Gruber,
  • Gustav E. Lienhard,
  • Sankar Ghosh

DOI
https://doi.org/10.1016/j.celrep.2014.08.015
Journal volume & issue
Vol. 8, no. 6
pp. 1793 – 1807

Abstract

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The transformation of cells generally involves multiple genetic lesions that undermine control of both cell death and proliferation. We now report that κB-Ras proteins act as regulators of NF-κB and Ral pathways, which control inflammation/cell death and proliferation, respectively. Cells lacking κB-Ras therefore not only show increased NF-κB activity, which results in increased expression of inflammatory mediators, but also exhibit elevated Ral activity, which leads to enhanced anchorage-independent proliferation (AIP). κB-Ras deficiency consequently leads to significantly increased tumor growth that can be dampened by inhibiting either Ral or NF-κB pathways, revealing the unique tumor-suppressive potential of κB-Ras proteins. Remarkably, numerous human tumors show reduced levels of κB-Ras, and increasing the level of κB-Ras in these tumor cells impairs their ability to undergo AIP, thereby implicating κB-Ras proteins in human disease.