Department of Microbiology and Immunology, University of Louisville School of Medicine, Louisville, KY 40292, USA.
Sci Signal. 2010 Feb 16;3(109):ra11. doi: 10.1126/scisignal.2000697.
Crosstalk between complement and Toll-like receptors (TLRs) coordinates innate immunity. We report a previously unknown immune subversion mechanism involving microbial exploitation of communication between complement and TLRs. Porphyromonas gingivalis, a major oral and systemic pathogen with complement C5 convertase-like activity, synergizes with C5a (fragment of complement protein C5) to increase cyclic adenosine monophosphate (cAMP) concentrations, resulting in suppression of macrophage immune function and enhanced pathogen survival in vitro and in vivo. This synergy required TLR2 signaling, a pertussis toxin- and thapsigargin-sensitive C5a receptor pathway, with protein kinase A and glycogen synthase kinase-3beta as downstream effectors. Antagonistic blockade of the C5a receptor abrogated this evasive strategy and may thus have important therapeutic implications for periodontitis and atherosclerosis, diseases in which P. gingivalis is implicated. This first demonstration of complement-TLR crosstalk for immunosuppressive cAMP signaling indicates that pathogens may not simply undermine complement or TLRs (or both) as separate entities, but may also exploit their crosstalk pathways.
补体和 Toll 样受体 (TLRs) 之间的串扰协调先天免疫。我们报告了一种以前未知的免疫颠覆机制,涉及微生物利用补体和 TLR 之间的通讯。牙龈卟啉单胞菌是一种主要的口腔和全身病原体,具有补体 C5 转化酶样活性,与 C5a(补体蛋白 C5 的片段)协同作用可增加环磷酸腺苷 (cAMP) 浓度,导致巨噬细胞免疫功能抑制和病原体在体外和体内的存活增强。这种协同作用需要 TLR2 信号转导、百日咳毒素和毒蕈碱敏感的 C5a 受体途径,以及蛋白激酶 A 和糖原合酶激酶-3β作为下游效应物。C5a 受体的拮抗阻断消除了这种逃避策略,因此可能对牙周炎和动脉粥样硬化等疾病具有重要的治疗意义,这些疾病与牙龈卟啉单胞菌有关。这是补体-TLR 串扰用于免疫抑制 cAMP 信号的首次证明,表明病原体可能不仅简单地破坏补体或 TLRs(或两者)作为单独的实体,还可能利用它们的串扰途径。
