Platelet activating factor (PAF) is a phospholipid inter and intra-cellular mediator implicated in intestinal injury primarily via induction of an inflammatory cascade. We find that PAF also has direct pathologic effects on intestinal epithelial cells. PAF induces Cl^- channel activation which is associated with intracellular acidosis and apoptosis. Using the rat small intestinal epithelial cell line IEC-6, electrophysiologic experiments demonstrated that PAF induces Cl^- channel activation. This PAF activated Cl^- current was inhibited by Ca²⁺ chelation and a calcium calmodulin Kinase II inhibitor suggesting PAF activation of a Ca²⁺ activated Cl^- channel. To determine the pathologic consequences of Cl^- channel activation, microfluorimetry experiments were performed which revealed PAF induced intracellular acidosis which is also inhibited by the Cl^- channel inhibitor 4, 4' diisothiocyanostilbene-2, 2' disulfonic acid and Ca²⁺ chelation. PAF-induced intracellular acidosis is associated with caspase 3 activation and DNA fragmentation. PAF-induced caspase activation was abolished in cells transfected with a pH compensatory Na/H exchanger (NHE1) construct to enhance H⁺ extruding ability and prevent intracellular acidosis. As ClC-3 is a known intestinal Cl^- channel dependent on both Ca²⁺ and calcium calmodulin Kinase II phosphorylation, we generated ClC-3 knockdown cells using shRNA. PAF induced Cl^- current, acidosis and apoptosis were all significantly decreased in ClC-3 knockdown cells. Our data suggest a novel mechanism of PAF-induced injury by which PAF induces intracellular acidosis via activation of the Ca²⁺ dependent Cl^- channel ClC-3 resulting in apoptosis of intestinal epithelial cells.