Murine endotoxin-induced uveitis, but not immune complex-induced uveitis, is dependent on the IL-8 receptor homolog

被引:22
作者
Brito, BE [1 ]
O'Rourke, LM [1 ]
Pan, YZ [1 ]
Huang, XN [1 ]
Park, JM [1 ]
Zamora, D [1 ]
Cook, DN [1 ]
Planck, SR [1 ]
Rosenbaum, JT [1 ]
机构
[1] Oregon Hlth & Sci Univ, Casey Eye Inst, Portland, OR 97201 USA
关键词
immune complexes; IL-8; MIP-1; alpha; endotoxin; uveitis; mouse;
D O I
10.1076/ceyr.19.1.76.5339
中图分类号
R77 [眼科学];
学科分类号
100212 ;
摘要
Purpose. To determine the roles of the murine interleukin-8 receptor homolog (mIL-8Rh, neutrophil chemokine CXC receptor 2) and macrophage inflammatory protein-la (MIP-1 alpha, a CC chemokine) in two eye inflammation models: endotoxin-induced uveitis (EIU) and immune complex-induced uveitis (reverse passive Arthus reaction (RPAR) uveitis). Methods. For the EIU model, 250 ng E.coli endotoxin was injected into the vitreous of mIL-8Rh(-/-) mice or heterozygous littermate mIL-8Rh(+/-) controls and into MIP-1 alpha(-/-) mice or congenic MIP-1 alpha(+/+) controls. Eyes were harvested after 24 h for histologic characterization of infiltrating cells and IL-6 bioassays. For the RPAR model, mouse antiserum against human serum albumin (HSA) was injected into the vitreous of mIL-8Rh(-/-), mIL-8Rh(+/-), MIP-1 alpha(-/-), and MIP-1 alpha(+/+) mice. Twenty-four hours later, animals were challenged with intravenous HSA. Eyes were harvested after 4 h for analysis. Results. RPAR resulted in the deposition of immune complexes at the ciliary area and iris with the subsequent development of uveitis. Genetic deficiency of mIL-8Rh reduced the median number of infiltrating cells in ETU by 63% (p < 0.01) but had no effect on RPAR-induced inflammation. In the EIU model, macrophages comprised a much higher percentage (45%) of infiltrating cells in mice lacking mIL-8Rh than in controls (17%). Loss of the MIP-1 alpha gene had no apparent effect on RPAR uveitis and a 39% reduction of infiltrating cells in EIU that was not statistically significant. IL-6 activity in aqueous humor was much less in mice with RPAR uveitis than in those with EIU, Neither gene deletion had a significant impact on IL-6 levels in either disease model. Conclusions. Chemokines acting via mIL-8Rh have a significant role in the induction of neutrophil infiltration during EIU but not during RPAR uveitis. MIP-1 alpha is not critical for either EIU or RPAR-induced uveitis. The differential dependence on IL-8-like chemokines is in accord with the two forms of uveitis having different etiologies and, therefore, potentially different optimal therapies.
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页码:76 / 85
页数:10
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