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Exposure to Mycobacteria Primes the Immune System for Evolutionarily Diverse Heat Shock Proteins

机译:暴露于分枝​​杆菌会引发进化上多样化的热休克蛋白的免疫系统

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During stress conditions, such as infection, the synthesis of heat shock proteins (HSPs) in microorganisms is upregulated. Since a high degree of homology exists within each HSP family, we postulated that exposure to microorganisms could prime the immune system for evolutionarily diverse HSPs. We tested this hypothesis by priming mice with three microorganisms, namely, Mycobacterium bovis BCG, Mycobacterium vaccae, and Chlamydia pneumoniae. After this, mice received a dose of the various HSPs. We found that BCG and M. vaccae but not C. pneumoniae primed the immune system for the induction of secondary immunoglobulin G (IgG) responses to most of the HSPs tested. Analysis of the IgG1 and IgG2a profile and gamma interferon production induced against the HSPs revealed the induction of a mixture of responses. We also observed that sera from mice treated with M. vaccae and HSP70 were cross-reactive, but no antibody complexes were observed in their kidneys, which frequently are targets for autoantibody reactions. Our findings add further support for the use of HSPs as effective vaccine adjuvants.
机译:在压力条件下,例如感染,微生物中热激蛋白(HSP)的合成被上调。由于每个HSP家族都存在高度同源性,因此我们推测暴露于微生物可能会引发进化多样的HSP的免疫系统。我们通过用三种微生物,即牛分枝杆菌BCG,牛痘分枝杆菌和肺炎衣原体三种微生物引发小鼠,检验了这一假设。此后,小鼠接受了一剂各种HSP。我们发现BCG和 M。 vaccae ,而不是 C。肺炎引发了免疫系统,以诱导对大多数测试的HSP的次级免疫球蛋白G(IgG)的反应。 IgG1和IgG2a谱分析以及针对HSP诱导的γ干扰素产生的分析揭示了反应混合物的诱导。我们还观察到用 M处理过的小鼠的血清。 vaccae 和HSP70具有交叉反应性,但在肾脏中未观察到抗体复合物,而肾脏通常是自身抗体反应的靶标。我们的发现为将HSP用作有效疫苗佐剂提供了进一步的支持。

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