Laboratory of Bacteriology, Rocky Mountain Laboratories, Division of Intramural Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, MT United States of America.
PLoS Pathog. 2018 Apr 5;14(4):e1006959. doi: 10.1371/journal.ppat.1006959. eCollection 2018 Apr.
Lyme disease in humans is caused by several genospecies of the Borrelia burgdorferi sensu lato (s.l.) complex of spirochetal bacteria, including B. burgdorferi, B. afzelii and B. garinii. These bacteria exist in nature as obligate parasites in an enzootic cycle between small vertebrate hosts and Ixodid tick vectors, with humans representing incidental hosts. During the natural enzootic cycle, infected ticks in endemic areas feed not only upon naïve hosts, but also upon seropositive infected hosts. In the current study, we considered this environmental parameter and assessed the impact of the immune status of the blood-meal host on the phenotype of the Lyme disease spirochete within the tick vector. We found that blood from a seropositive host profoundly attenuates the infectivity (>104 fold) of homologous spirochetes within the tick vector without killing them. This dramatic neutralization of vector-borne spirochetes was not observed, however, when ticks and blood-meal hosts carried heterologous B. burgdorferi s.l. strains, or when mice lacking humoral immunity replaced wild-type mice as blood-meal hosts in similar experiments. Mechanistically, serum-mediated neutralization does not block induction of host-adapted OspC+ spirochetes during tick feeding, nor require tick midgut components. Significantly, this study demonstrates that strain-specific antibodies elicited by B. burgdorferi s.l. infection neutralize homologous bacteria within feeding ticks, before the Lyme disease spirochetes enter a host. The blood meal ingested from an infected host thereby prevents super-infection by homologous spirochetes, while facilitating transmission of heterologous B. burgdorferi s.l. strains. This finding suggests that Lyme disease spirochete diversity is stably maintained within endemic populations in local geographic regions through frequency-dependent selection of rare alleles of dominant polymorphic surface antigens.
人类莱姆病是由伯氏疏螺旋体 sensu lato (s.l.) 复合螺旋体细菌的几个基因型引起的,包括 B. burgdorferi、B. afzelii 和 B. garinii。这些细菌在自然环境中作为小脊椎动物宿主和硬蜱媒介之间的地方性动物寄生虫存在,人类是偶然宿主。在自然地方性动物寄生虫周期中,流行地区感染的蜱虫不仅以幼稚宿主为食,而且还以血清阳性感染宿主为食。在目前的研究中,我们考虑了这一环境参数,并评估了血液宿主的免疫状态对蜱媒莱姆病螺旋体表型的影响。我们发现,来自血清阳性宿主的血液会极大地减弱(>104 倍)同种螺旋体在蜱虫中的感染力,而不会杀死它们。然而,当蜱虫和血液宿主携带异源 B. burgdorferi s.l. 菌株时,或者当缺乏体液免疫的小鼠代替野生型小鼠作为类似实验中的血液宿主时,不会观察到这种对媒介传播螺旋体的显著中和作用。从机制上讲,血清介导的中和作用不会阻止在蜱虫叮咬期间诱导宿主适应性 OspC+ 螺旋体的产生,也不需要蜱虫中肠成分。重要的是,这项研究表明,由 B. burgdorferi s.l. 感染引起的特异性抗体在莱姆病螺旋体进入宿主之前,可中和在喂食蜱虫内的同源细菌。从感染宿主中摄入的血液餐因此可以防止同源螺旋体的超感染,同时促进异源 B. burgdorferi s.l. 菌株的传播。这一发现表明,通过对优势多态表面抗原的稀有等位基因的频率依赖性选择,莱姆病螺旋体的多样性在当地地理区域的地方性人群中得以稳定维持。
Zotero 插件
