Proinflammatory and Th1 Cytokine Alterations following Ultraviolet Radiation Enhancement of Disease Due to Influenza Infection in Mice

doi:10.1093/toxsci/67.1.88

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Toxicological Sciences 67, 88-97 (2002)
Copyright © 2002 by the Society of Toxicology

IMMUNOTOXICOLOGY

Proinflammatory and Th1 Cytokine Alterations following Ultraviolet Radiation Enhancement of Disease Due to Influenza Infection in Mice

Lisa K. Ryan^,1, Lisa R. Copeland, Mary J. Daniels, Elisabeth R. Costa and Mary Jane K. Selgrade

Immunotoxicology Branch, Experimental Toxicology Division, National Health and Environmental Effects Research Laboratory, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina 27711

Exposure of rodents to immunosuppressive agents such as ozone,dioxin, or ultraviolet radiation (UVR) leads to increased morbidityand mortality following influenza virus infection. However,these adverse effects are not related to the suppression ofvirus-specific immune responses. Our laboratory showed thatUVR increased the morbidity, mortality, and pathogenesis ofinfluenza virus without affecting protective immunity to thevirus, as measured by resistance to reinfection, suggestingthat UVR and other immunosuppressive pollutants such as dioxinand ozone may exacerbate early responses that contribute tothe pathogenesis of a primary viral infection. In the presentstudy, we examined the mechanism of UVR-enhanced mortality inthe absence of effects on virus-specific immunity and testedthe hypothesis that modulation of cytokine levels was associatedwith increased deaths and body weight loss. BALB/c mice wereexposed to 8.2 kJ/m² UVR and were infected 3 days later witha sublethal influenza virus infection (LD₄₀ of mouse-adaptedHong Kong influenza A/68, H₃N₂). Influx of inflammatory cells,proinflammatory cytokines, and cytokines produced by T-helperlymphocytes (Th1 and Th2) were measured in lung homogenates(LH) as well as in bronchoalveolar lavage fluid (BAL). UVR preexposuredecreased the influenza-induced lymphocytic influx 5 days afterinfection, but did not alter macrophage and neutrophil influxinto the lung, or increase virus titers significantly. Althoughinterferon (IFN)- ${gamma}$ , total interleukin (IL)-12, IL-6, and TNF- ${alpha}$ were altered in mice that received UVR exposure prior to infection,no clear association was made that correlated with the UVR-inducedincrease in body weight loss and mortality due to influenzainfection.

Key Words: T-helper lymphocytes; cytokines; influenza virus; mice; ultraviolet radiation; inflammation.

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