Ozone inhalation stimulates expression of a neutrophil chemotactic protein, macrophage inflammatory protein 2

KE Driscoll, L Simpson, J Carter, D Hassenbein… - Toxicology and applied …, 1993 - Elsevier
KE Driscoll, L Simpson, J Carter, D Hassenbein, GD Leikauf
Toxicology and applied pharmacology, 1993Elsevier
Short-term exposure of humans and animals to ozone results in increased lung neutrophils;
however, the mechanisms underlying this response are not completely understood. We
examined the potential involvement of the neutrophil chemotactic factor, macrophage
inflammatory protein 2 (MIP-2), in ozone-induced inflammation. Exposure-response
relationships for ozone and MIP-2 expression were characterized by exposing C57B1/6
mice to 0.1-2 ppm ozone for 3 hr and determining lung levels of MIP-2 mRNA 6 hr after …
Short-term exposure of humans and animals to ozone results in increased lung neutrophils; however, the mechanisms underlying this response are not completely understood. We examined the potential involvement of the neutrophil chemotactic factor, macrophage inflammatory protein 2 (MIP-2), in ozone-induced inflammation. Exposure-response relationships for ozone and MIP-2 expression were characterized by exposing C57B1/6 mice to 0.1-2 ppm ozone for 3 hr and determining lung levels of MIP-2 mRNA 6 hr after exposure. Temporal relationships between ozone and MIP-2 were determined by exposing mice (2 ppm ozone × 3 hr) and characterizing MIP-2 mRNA expression 0, 2, 6, and 24 hr after exposure. Neutrophils in lung lavage fluid were determined in both exposure-response and time course studies. Ozone concentrations ≥1.0 ppm increased MIP-2 mRNA and this increase corresponded with recruitment of neutrophils. MIP-2 mRNA was increased immediately after ozone exposure and decreased to control levels by 24 hr. To examine the role of direct oxidant effects in ozone-induced MIP-2 expression, alveolar macrophages were exposed in vitro for 4 hr to 10−10-10−5 M hydrogen peroxide and MIP-2 expression was characterized. MIP-2 mRNA levels in lung macrophages were increased by ≥10−9 M hydrogen peroxide. In summary, our findings suggest the chemotactic protein MIP-2 may be responsible, at least in part, for ozone-induced increases in lung neutrophils and indicate that direct exposure of alveolar macrophages to an oxidant is sufficient to induce MIP-2 expression.
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