Author: Kashiwazaki, Hiromi; Kakizaki, Masatoshi; Ikehara, Yuzuru; Togayachi, Akira; Narimatsu, Hisashi; Watanabe, Rihito
Title: Mice lacking α1,3â€fucosyltransferase 9 exhibit modulation of in vivo immune responses against pathogens Cord-id: 05rzrskg Document date: 2014_5_29
ID: 05rzrskg
Snippet: Carbohydrate structures, including Lewis X (Le(x)), which is not synthesized in mutant mice that lack α1,3â€fucosyltransferase 9 (Fut9(−/−)), are involved in cell–cell recognition and inflammation. However, immunological alteration in Fut9(−/−) mice has not been studied. Thus, the inflammatory response of Fut9(−/−) mice was examined using the highly neurovirulent mouse hepatitis virus (MHV) JHMV srr7 strain. Pathological study revealed that inflammation induced in the brains of F
Document: Carbohydrate structures, including Lewis X (Le(x)), which is not synthesized in mutant mice that lack α1,3â€fucosyltransferase 9 (Fut9(−/−)), are involved in cell–cell recognition and inflammation. However, immunological alteration in Fut9(−/−) mice has not been studied. Thus, the inflammatory response of Fut9(−/−) mice was examined using the highly neurovirulent mouse hepatitis virus (MHV) JHMV srr7 strain. Pathological study revealed that inflammation induced in the brains of Fut9(−/−) mice after infection was more extensive compared with that of wildâ€type mice, although viral titers obtained from the brains of mutant mice were lower than those of wildâ€type mice. Furthermore, the reduction in cell numbers in the spleens of wildâ€type mice after infection was not observed in the infected Fut9(−/−) mice. Although there were no clear differences in the levels of cytokines examined in the brains between Fut9(−/−) and wildâ€type mice except for interferonâ€Î² (IFNâ€Î²) expression, some of those in the spleens, including interferonâ€Î³ (IFNâ€Î³), interleukinâ€6 (ILâ€6), and monocyte chemoattractant proteinâ€1 (MCPâ€1), showed higher levels in Fut9(−/−) than in wildâ€type mice. Furthermore, Fut9(−/−) mice were refractory to the in vivo inoculation of endotoxin (LPS) compared with wildâ€type mice. These results indicate that Le(x) structures are involved in host responses against viral or bacterial challenges.
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