Modified natural porcine surfactant modulates tobacco smoke-induced stress response in human monocytes.

Abstract Tobacco smoke (TS) is a potent source of oxidants and oxidative stress is an important mechanism by which TS exerts its toxicity in the lung. We have shown that TS induces heat shock (HS)/stress protein (HSP) synthesis in human monocytes. Pulmonary surfactant (PS) whose major physiological function is to confer mechanical stability to alveoli, also modulates oxidative metabolism and other pro-inflammatory functions of monocytes-macrophages. In order to determine whether PS alters the stress response induced by TS, we incubated human peripheral blood monocytes overnight with modified natural porcine surfactant (Curosurf ® ) ( 1mg ml ) before exposure to TS. Curosurf ® decreased TS-induced, but not HS-induced, expression of the major cytosolic, inducible 72kD HSP (Hsp70). Furthermore, TS-generated superoxide anions production was significantly decreased by Curosurf ® in an acellular system, suggesting a direct scavenging effect of PS. We also examined the effects of TS and PS on monocytes ultrastructure. Monocytes incubated with Curosurf ® presented smoother cell membranes than control monocytes, while TS-induced monocyte vacuolization was, at least in part, prevented by Curosurf ® . Taken together, our data suggest that PS plays a protective role against oxygen radical-mediated, TS-induced cellular stress responses.