A Smac Mimetic Rescue Screen Reveals Roles for Inhibitor of Apoptosis Proteins in Tumor Necrosis Factor-α Signaling

Alex Gaither(Pathways Behavioral Services), Dale Porter(Pathways Behavioral Services), Yao Yao(Pathways Behavioral Services), Jason Borawski(Pathways Behavioral Services), Guang Yang(Pathways Behavioral Services), Jerry Donovan(Pathways Behavioral Services), David R. Sage(Pathways Behavioral Services), Joanna Slisz(Pathways Behavioral Services), Mary Tran(Pathways Behavioral Services), Christopher Straub(Pathways Behavioral Services), Tim Ramsey(Pathways Behavioral Services), Vadim Iourgenko(Pathways Behavioral Services), Alan Huang(Pathways Behavioral Services), Yan Chen(Pathways Behavioral Services), Robert Schlegel(Pathways Behavioral Services), Mark Labow(Pathways Behavioral Services), Stephen E. Fawell(Pathways Behavioral Services), William R. Sellers(Pathways Behavioral Services), Leigh Zawel(Pathways Behavioral Services)
Cancer Research
December 15, 2007
10.1158/0008-5472.can-07-5173
Cited by 225Open Access
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Abstract

Smac mimetic compounds targeting the inhibitor of apoptosis proteins (IAP) baculoviral IAP repeat-3 domain are presumed to reduce the threshold for apoptotic cell death by alleviating caspase-9 repression. We explored this tenet in an unbiased manner by searching for small interfering RNAs that are able to confer resistance to the Smac mimetic compound LBW242. Among the screening hits were multiple components of the tumor necrosis factor alpha (TNFalpha) signaling pathway as well as X-linked inhibitor of apoptosis (XIAP) itself. Here, we show that in a subset of highly sensitive tumor cell lines, activity of LBW242 is dependent on TNFalpha signaling. Mechanistic studies indicate that in this context, XIAP is a positive modulator of TNFalpha induction whereas cellular inhibitor of apoptosis protein 1 negatively regulates TNFalpha-mediated apoptosis.

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