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鼻内注射干扰素γ可延长小鼠被动IgA抗体对结核分枝杆菌肺部感染的保护作用。

Intranasal IFNgamma extends passive IgA antibody protection of mice against Mycobacterium tuberculosis lung infection.

作者信息

Reljic R, Clark S O, Williams A, Falero-Diaz G, Singh M, Challacombe S, Marsh P D, Ivanyi J

机构信息

Mucosal Biology Research Group, Guy's Campus, King's College London, London SE1 9RT, UK.

出版信息

Clin Exp Immunol. 2006 Mar;143(3):467-73. doi: 10.1111/j.1365-2249.2006.03012.x.

Abstract

Intranasal inoculation of mice with monoclonal IgA against the alpha-crystallin (acr1) antigen can diminish the tuberculous infection in the lungs. As this effect has been observed only over a short-term, we investigated if it could be extended by inoculation of IFNgamma 3 days before infection, and further co-inoculations with IgA, at 2 h before and 2 and 7 days after aerosol infection with Mycobacterium tuberculosis H37Rv. This treatment reduced the lung infection at 4 weeks more than either IgA or IFNgamma alone (i.e. 17-fold, from 4.2 x 10(7) to 2.5 x 10(6) CFU, P = 0.006), accompanied also by lower granulomatous infiltration of the lungs. IFNgamma added prior to infection of mouse peritoneal macrophages with IgA-opsonized bacilli resulted in a synergistic increase of nitric oxide and TNFalpha production and a 2-3 fold decrease in bacterial counts. Our improved results suggest, that combined treatment with IFNgamma and IgA could be developed towards prophylactic treatment of AIDS patients, or as an adjunct to chemotherapy.

摘要

用针对α-晶状体蛋白(acr1)抗原的单克隆IgA经鼻接种小鼠,可减轻肺部的结核感染。由于这种效应仅在短期内观察到,我们研究了在感染前3天接种IFNγ,以及在结核分枝杆菌H37Rv气溶胶感染前2小时、感染后2天和7天进一步联合接种IgA是否能延长这种效应。这种治疗在4周时比单独使用IgA或IFNγ更能减少肺部感染(即减少17倍,从4.2×10⁷降至2.5×10⁶CFU,P = 0.006),同时肺部的肉芽肿浸润也较少。在用IgA调理的杆菌感染小鼠腹腔巨噬细胞之前加入IFNγ,会导致一氧化氮和TNFα产生协同增加,细菌数量减少2至3倍。我们改进的结果表明,IFNγ和IgA联合治疗可用于开发艾滋病患者的预防性治疗,或作为化疗的辅助手段。

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