Data from Deficiency of Phospholipase A<sub>2</sub> Group 7 Decreases Intestinal Polyposis and Colon Tumorigenesis in <i>Apc<sup>Min</sup></i><sup>/+</sup> Mice

Abstract

<div>Abstract<p>Platelet-activating factor (PAF) is a naturally occurring phospholipid that mediates diverse effects such as physiological and pathological inflammation, immunosuppression, and cancer. Several lines of evidence support both positive and negative roles for PAF in carcinogenesis. PAF stimulates cell growth, oncogenic transformation, and metastasis, but can also limit proliferation and induce apoptosis. The biological context and microenvironment seem to define whether PAF has pro- or anticarcinogenic effects. To investigate the role of exacerbated PAF signaling in colon cancer, we conducted cell-based and <i>in vivo</i> studies using genetically engineered mice lacking expression of phospholipase A<sub>2</sub> group 7 (PLA2G7), an enzyme that specifically metabolizes PAF and structurally related glycerophospholipids. Absence of <i>Pla2g7</i> robustly decreased intestinal polyposis and colon tumor formation in <i>Apc<sup>Min</sup></i><sup>/+</sup> mice, suggesting an antitumorigenic role for PAF in settings characterized by aberrant function of the tumor suppressor <i>Adenomatous polyposis coli (Apc)</i>. In colonic epithelial cells, exposure to a PAF analog led to dephosphorylation of Akt at serine-473 and induction of apoptosis. The mechanism of this response involved formation of a complex between β-arrestin 1 and the Akt phosphatase PHLPP2, and activation of the intrinsic pathway of apoptosis. Our results suggest that strategies based on inhibiting PLA2G7 activity or increasing PAF-mediated signaling hold promise for the treatment of intestinal malignancies that harbor mutations in <i>APC</i>. <i>Cancer Res; 73(9); 2806–16. ©2013 AACR</i>.</p></div>