Becker Marc, Lemmermann Niels A W, Ebert Stefan, Baars Pamela, Renzaho Angelique, Podlech Jürgen, Stassen Michael, Reddehase Matthias J
Institute for Immunology, Research Center for Immunotherapy (FZI) at the University Medical Center of the Johannes Gutenberg University, Mainz, Germany.
Institute for Virology, Research Center for Immunotherapy (FZI) at the University Medical Center of the Johannes Gutenberg University, Mainz, Germany.
Cell Mol Immunol. 2015 Mar;12(2):192-201. doi: 10.1038/cmi.2014.73. Epub 2014 Aug 25.
The succinct metaphor, 'the immune system's loaded gun', has been used to describe the role of mast cells (MCs) due to their storage of a wide range of potent pro-inflammatory and antimicrobial mediators in secretory granules that can be released almost instantly on demand to fight invaders. Located at host-environment boundaries and equipped with an arsenal of pattern recognition receptors, MCs are destined to be rapid innate sensors of pathogens penetrating endothelial and epithelial surfaces. Although the importance of MCs in antimicrobial and antiparasitic defense has long been appreciated, their role in raising the alarm against viral infections has been noted only recently. Work on cytomegalovirus (CMV) infection in the murine model has revealed MCs as players in a novel cross-talk axis between innate and adaptive immune surveillance of CMV, in that infection of MCs, which is associated with MC degranulation and release of the chemokine CCL5, enhances the recruitment of protective CD8 T cells to extravascular sites of virus replication, specifically to lung interstitium and alveolar epithelium. Here, we have expanded on these studies by investigating the conditions for MC activation and the consequent degranulation in response to host infection. Surprisingly, the data revealed two temporally and mechanistically distinct waves of MC activation: an almost instant indirect activation that depended on TLR3/TRIF signaling and delayed activation by direct infection of MCs that did not involve TLR3/TRIF signaling. Cell type-specific Cre-recombination that yielded eGFP-expressing reporter virus selectively originating from MCs identified MC as a new in vivo, first-hit target cell of productive murine CMV infection.
简洁的比喻“免疫系统上膛的枪”已被用于描述肥大细胞(MCs)的作用,因为它们在分泌颗粒中储存了多种强效促炎和抗菌介质,这些介质几乎可应要求立即释放以对抗入侵者。MCs位于宿主与环境的边界,配备了一系列模式识别受体,注定会成为穿透内皮和上皮表面的病原体的快速固有传感器。尽管MCs在抗微生物和抗寄生虫防御中的重要性早已得到认可,但它们在针对病毒感染发出警报方面的作用直到最近才被注意到。对小鼠模型中巨细胞病毒(CMV)感染的研究表明,MCs是CMV固有免疫和适应性免疫监视之间新的相互作用轴中的参与者,因为MCs的感染与MC脱颗粒和趋化因子CCL5的释放相关,可增强保护性CD8 T细胞向病毒复制的血管外部位,特别是肺间质和肺泡上皮的募集。在此,我们通过研究MC激活的条件以及宿主感染后随之而来的脱颗粒情况,对这些研究进行了扩展。令人惊讶的是,数据揭示了MC激活的两个在时间和机制上不同的阶段:一个几乎立即发生的间接激活,它依赖于TLR3/TRIF信号传导;以及由MCs直接感染导致的延迟激活,这一过程不涉及TLR3/TRIF信号传导。通过细胞类型特异性Cre重组产生选择性源自MCs的表达eGFP的报告病毒,确定MC为有活性的小鼠CMV感染在体内的新的首个命中靶细胞。