Inflammatory Profiles Induced by Intranasal Immunization with Ricin Toxin-immune Complexes.

Q3 Medicine
Lindsey E Tolman, Nicholas J Mantis
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引用次数: 0

Abstract

The underlying contribution of immune complexes in modulating adaptive immunity in mucosal tissues remains poorly understood. In this report, we examined, in mice, the proinflammatory response elicited by intranasal delivery of the biothreat agent ricin toxin (RT) in association with two toxin-neutralizing mAbs, SylH3 and PB10. We previously demonstrated that ricin-immune complexes (RICs) induce the rapid onset of high-titer toxin-neutralizing Abs that persist for months. We now demonstrate that such responses are dependent on CD4+ T cell help, because treatment of mice with an anti-CD4 mAb abrogated the onset of RT-specific Abs following intranasal RICs exposure. To define the inflammatory environment associated with RIC exposure, we collected bronchoalveolar lavage fluid (BALF) and sera from mice 6, 12, and 18 h after they had received RT or RICs by the intranasal route. A 32-plex cytometric bead array revealed an inflammatory profile elicited by RT that was dominated by IL-6 (>1500-fold increase in BALF) and secondarily by KC (CXCL1), G-CSF, GM-CSF, and MCP-1. RICs induced inflammatory profiles in both BALF and serum response that were similar to RT, albeit at markedly reduced levels. These results demonstrate that RICs retain the capacity to induce local and systemic inflammatory cytokines/chemokines that, in turn, may influence Ag sampling and presentation in the lung mucosa and draining lymph nodes. A better understanding of the fate of immune complexes following intranasal delivery has implications for the development of mucosal vaccines for biothreats and emerging infectious diseases.

蓖麻毒素-免疫复合物鼻内免疫诱发的炎症特征
人们对免疫复合物在调节粘膜组织适应性免疫中的潜在作用仍然知之甚少。在本报告中,我们研究了小鼠鼻内注射生物威胁制剂蓖麻毒素(RT)与两种毒素中和 mAbs(SylH3 和 PB10)引起的促炎反应。我们以前曾证明,蓖麻毒素免疫复合物(RICs)可诱导高滴度毒素中和抗体的快速产生,并可持续数月之久。我们现在证明,这种反应依赖于 CD4+ T 细胞的帮助,因为用抗 CD4 mAb 处理小鼠会减弱鼻内 RICs 暴露后 RT 特异性抗体的产生。为了确定与 RIC 暴露相关的炎症环境,我们在小鼠经鼻内途径接受 RT 或 RIC 6、12 和 18 小时后收集了它们的支气管肺泡灌洗液(BALF)和血清。32 重细胞计数珠阵列显示 RT 引发的炎症特征主要是 IL-6(在 BALF 中增加了 1500 倍以上),其次是 KC (CXCL1)、G-CSF、GM-CSF 和 MCP-1。RICs 在 BALF 和血清反应中诱导的炎症特征与 RT 相似,但水平明显降低。这些结果表明,RICs 仍有能力诱导局部和全身性炎症细胞因子/凝血因子,而这些细胞因子/凝血因子反过来又可能影响 Ag 在肺粘膜和引流淋巴结中的取样和表现。更好地了解鼻内给药后免疫复合物的去向对开发针对生物威胁和新发传染病的粘膜疫苗具有重要意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
3.70
自引率
0.00%
发文量
0
审稿时长
4 weeks
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