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Induction of HDAC2 expression upon loss of APC in colorectal tumorigenesis.

Cancer cell (2004-05-18)
Ping Zhu, Elke Martin, Jörg Mengwasser, Peter Schlag, Klaus-Peter Janssen, Martin Göttlicher
RÉSUMÉ

Inappropriate transcriptional repression involving histone deacetylases (HDACs) is a prominent cause for the development of leukemia. We now identify faulty expression of a specific mediator of transcriptional repression in a solid tumor. Loss of the adenomatosis polyposis coli (APC) tumor suppressor induces HDAC2 expression depending on the Wnt pathway and c-Myc. Increased HDAC2 expression is found in the majority of human colon cancer explants, as well as in intestinal mucosa and polyps of APC-deficient mice. HDAC2 is required for, and sufficient on its own to prevent, apoptosis of colonic cancer cells. Interference with HDAC2 by valproic acid largely diminishes adenoma formation in APC(min) mice. These findings point toward HDAC2 as a particularly relevant potential target in cancer therapy.

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Anticorps anti-acétyl-histone H3, from rabbit