Nuclear expression of E2F4 induces cell death via multiple pathways in normal human intestinal epithelial crypt cells but not in colon cancer cells

doi:10.1152/ajpgi.00050.2007

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Am J Physiol Gastrointest Liver Physiol 293: G758-G772, 2007. First published July 26, 2007; doi:10.1152/ajpgi.00050.2007
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MUCOSAL BIOLOGY

Nuclear expression of E2F4 induces cell death via multiple pathways in normal human intestinal epithelial crypt cells but not in colon cancer cells

Hugo Garneau,¹^,* Laetitia Alvarez,¹^,* Marie-Christine Paquin,¹ Carine Lussier,¹ Claudine Rancourt,² Éric Tremblay,¹ Jean-Francois Beaulieu,¹ and Nathalie Rivard¹

¹Département d'Anatomie et Biologie Cellulaire and ²Département de Microbiologie-Infectiologie, Faculté de Médecine et des Sciences de la Santé, Université de Sherbrooke, Sherbrooke, Quebec, Canada

Submitted 26 January 2007 ; accepted in final form 25 July 2007

E2F transcription factors control cell cycle progression. Thelocalization of E2F4 in intestinal epithelial cells is cellcycle dependent, being cytoplasmic in quiescent differentiatedcells but nuclear in proliferative cells. However, whether nucleartranslocation of E2F4 alone is sufficient to trigger intestinalepithelial cell proliferation remains to be established. Adenovirusesexpressing fusion proteins between green fluorescent protein(GFP) and wild-type (wt)E2F4 or GFP and nuclear localizationsignal (NLS)-tagged E2F4 were used to infect normal human intestinalepithelial crypt cells (HIEC). In contrast to expression ofwtE2F4, persistent expression of E2F4 into the nucleus of HIECtriggered phosphatidylserine exposure, cytoplasmic shrinkage,zeiosis, formation of apoptotic bodies, and activation of caspase9 and caspase 3. Inhibition of caspase activities by zVAD-fmkpartially inhibited cell death induced by E2F4-NLS. An inductionof p53, phosphorylated Ser15-p53, PUMA, FAS, BAX, RIP, and phosphorylatedJNK1 was also observed in HIEC expressing E2F4-NLS comparedwith wtE2F4-expressing cells. E2F1 and p14ARF expression remainedunaltered. Downregulation of p53 expression by RNA interferenceattenuated cell death induced by E2F4-NLS. By contrast, thelevel of cell death was negligible in colon cancer cells despitethe strong expression of E2F4 into the nucleus. In conclusion,deregulated nuclear E2F4 expression induces apoptosis via multiplepathways in normal intestinal epithelial cells but not in coloncancer cells. Hence, mutations that deregulate E2F4 localizationmay provide an initial proliferative advantage but at the sametime accelerate cell death. However, intestinal cells acquiringmutations (e.g., p53, Bax loci, etc.) may escape apoptosis,thereby revealing the full mitogenic potential of the E2F4 transcriptionfactor.

E2F; intestinal epithelial crypt apoptosis; p53; colon cancer

Address for reprint requests and other correspondence: N. Rivard, Département d'Anatomie et de Biologie Cellulaire, Faculté de Médecine et des Sciences de la Santé, Université de Sherbrooke, Sherbrooke, QC, J1H5N4, Canada (e-mail: nathalie.rivard{at}usherbrooke.ca)