在血液阶段感染期间1型天然淋巴细胞迅速丢失。
Rapid loss of group 1 innate lymphoid cells during blood stage infection.
作者信息
Ng Susanna S, Souza-Fonseca-Guimaraes Fernando, Rivera Fabian de Labastida, Amante Fiona H, Kumar Rajiv, Gao Yulong, Sheel Meru, Beattie Lynette, Montes de Oca Marcela, Guillerey Camille, Edwards Chelsea L, Faleiro Rebecca J, Frame Teija, Bunn Patrick T, Vivier Eric, Godfrey Dale I, Pellicci Daniel G, Lopez J Alejandro, Andrews Katherine T, Huntington Nicholas D, Smyth Mark J, McCarthy James, Engwerda Christian R
机构信息
Immunology and Infection Laboratory QIMR Berghofer Medical Research Institute Herston QLD Australia.
School of Natural Sciences Griffith University Nathan QLD Australia.
出版信息
Clin Transl Immunology. 2018 Jan 12;7(1):e1003. doi: 10.1002/cti2.1003. eCollection 2018.
OBJECTIVES
Innate lymphoid cells (ILCs) share many characteristics with CD4 T cells, and group 1 ILCs share a requirement for T-bet and the ability to produce IFNγ with T helper 1 (Th1) cells. Given this similarity, and the importance of Th1 cells for protection against intracellular protozoan parasites, we aimed to characterise the role of group 1 ILCs during infection.
METHODS
We quantified group 1 ILCs in peripheral blood collected from subjects infected with with 3D7 as part of a controlled human malaria infection study, and in the liver and spleens of AS-infected mice. We used genetically-modified mouse models, as well as cell-depletion methods in mice to characterise the role of group 1 ILCs during AS infection.
RESULTS
In a controlled human malaria infection study, we found that the frequencies of circulating ILC1s and NK cells decreased as infection progressed but recovered after volunteers were treated with antiparasitic drug. A similar observation was made for liver and splenic ILC1s in AS ( AS)-infected mice. The decrease in mouse liver ILC1 frequencies was associated with increased apoptosis. We also identified a population of cells within the liver and spleen that expressed both ILC1 and NK cell markers, indicative of plasticity between these two cell lineages. Studies using genetic and cell-depletion approaches indicated that group 1 ILCs have a limited role in antiparasitic immunity during AS infection in mice.
DISCUSSION
Our results are consistent with a previous study indicating a limited role for natural killer (NK) cells during infection in mice. Additionally, a recent study reported the redundancy of ILCs in humans with competent B and T cells. Nonetheless, our results do not rule out a role for group 1 ILCs in human malaria in endemic settings given that blood stage infection was initiated intravenously in our experimental models, and thus bypassed the liver stage of infection, which may influence the immune response during the blood stage.
CONCLUSION
Our results show that ILC1s are lost early during mouse and human malaria, and this observation may help to explain the limited role for these cells in controlling blood stage infection.
目的
固有淋巴细胞(ILC)与CD4 T细胞具有许多共同特征,1型ILC与T辅助1(Th1)细胞一样需要T-bet并具有产生IFNγ的能力。鉴于这种相似性,以及Th1细胞对抵御细胞内原生动物寄生虫的重要性,我们旨在明确1型ILC在感染过程中的作用。
方法
作为一项对照人体疟疾感染研究的一部分,我们对感染3D7的受试者外周血中的1型ILC进行了定量分析,并对感染伯氏疟原虫(AS)的小鼠的肝脏和脾脏中的1型ILC进行了定量分析。我们使用基因改造小鼠模型以及小鼠体内的细胞清除方法来明确1型ILC在AS感染过程中的作用。
结果
在一项对照人体疟疾感染研究中,我们发现随着感染进展,循环中的ILC1和自然杀伤(NK)细胞频率降低,但在志愿者接受抗寄生虫药物治疗后恢复。在感染AS的小鼠的肝脏和脾脏ILC1中也观察到了类似现象。小鼠肝脏ILC1频率的降低与细胞凋亡增加有关。我们还在肝脏和脾脏中鉴定出一群同时表达ILC1和NK细胞标志物的细胞,这表明这两个细胞谱系之间具有可塑性。使用基因和细胞清除方法的研究表明,1型ILC在小鼠AS感染期间的抗寄生虫免疫中作用有限。
讨论
我们的结果与之前一项表明自然杀伤(NK)细胞在小鼠感染期间作用有限的研究一致。此外,最近一项研究报道了在具有正常B细胞和T细胞的人类中ILC的冗余性。尽管如此,鉴于我们的实验模型中血液阶段感染是通过静脉注射启动的,从而绕过了可能影响血液阶段免疫反应的感染肝脏阶段,我们的结果并不排除1型ILC在地方性环境中的人类疟疾中发挥作用。
结论
我们的结果表明,ILC1在小鼠和人类疟疾早期丢失,这一观察结果可能有助于解释这些细胞在控制血液阶段感染中的作用有限。
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