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The IL-23/Th17 axis is involved in the adaptive immune response to Bacillus anthracis in humans

机译:IL-23 / Th17轴自适应免疫反应在人类炭疽杆菌

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The neutralization of toxins is considered essential for protection against lethal infection with Bacillus anthracis (BA), a select agent and bioterrorism threat. However, toxin-neutralizing activity alone would not be expected to provide sterile immunity. Therefore, we hypothesized that the development of an adaptive immune response against BA is required for bacterial clearance. We found that human monocyte-derived dendritic cells (hDCs) kill germinated BA bacilli, but not nongerminated BA spores. hDCs produce IL-1β, IL-6, IL-12, and IL-23, and these cytokines are differentially regulated by germination-proficient versus germination-deficient BA spores. Moreover, the IL-23 response to BA spores is regulated by IL-1R-mediated signaling. hDCs infected with germinating BA spores stimulated autologous CD4+ T cells to secrete IL-17A and IFN-γ in a contact-dependent and antigen-specific manner. The T-cell response to BA spores was not recapitulated by hDCs infected with germination-deficient BA spores, implying that the germination of spores into replicating bacilli triggers the proinflammatory cytokine response in hDCs. Our results provide primary evidence that hDCs can generate a BA-specific Th17 response, and help elucidate the mechanisms involved. These novel findings suggest that the IL-23/Th17 axis is involved in the immune response to anthrax in humans.
机译:的中和毒素被认为是对于防止致命的感染与炭疽杆菌(BA),选择代理和生物恐怖主义威胁。活动本身不会将提供无菌的免疫力。一种自适应免疫反应的发展对英航需要细菌清除率。我们发现人类monocyte-derived树突细胞(hDCs)杀死发芽英航杆菌,而不是nongerminated英航孢子。il - 6、il - 12和IL-23,这些细胞因子不同的规定germination-proficient与germination-deficient英航孢子。英航孢子是由IL-23响应IL-1R-mediated信号。英航孢子发芽刺激自体CD4 +T细胞分泌IL-17A和干扰素-γcontact-dependent和抗原特异的方式。英航孢子的t细胞反应重现hDCs感染germination-deficient英航孢子,暗示孢子萌发的复制杆菌引发的促炎细胞因子在hDCs响应。证据表明hDCs可以生成一个BA-specificTh17反应,有助于阐明机制参与。IL-23 / Th17轴是参与免疫应对人类炭疽。

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