The interaction of microbes with pattern recognition receptors (PRRs) is essential for protective immunity. While many PRRs that recognize mycobacteria have been identified, none is essentially required for host defense in vivo. Here, we have identified the C-type lectin receptor CLECSF8 (CLEC4D, MCL) as a key molecule in anti-mycobacterial host defense. Clecsf8-/- mice exhibit higher bacterial burdens and increased mortality upon M. tuberculosis infection. Additionally, Clecsf8 deficiency is associated with exacerbated pulmonary inflammation, characterized by enhanced neutrophil recruitment. Clecsf8-/- mice show reduced mycobacterial uptake by pulmonary leukocytes, but infection with opsonized bacteria can restore this phagocytic defect as well as decrease bacterial burdens. Notably, a CLECSF8 polymorphism identified in humans is associated with an increased susceptibility to pulmonary tuberculosis. We conclude that CLECSF8 plays a non-redundant role in anti-mycobacterial immunity in mouse and in man.
The C-type lectin receptor CLECSF8/CLEC4D is a key component of anti-mycobacterial immunity.
C 型凝集素受体 CLECSF8/CLEC4D 是抗分枝杆菌免疫的关键组成部分
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作者:Wilson Gillian J, Marakalala Mohlopheni J, Hoving Jennifer C, van Laarhoven Arjan, Drummond Rebecca A, Kerscher Bernhard, Keeton Roanne, van de Vosse Esther, Ottenhoff Tom H M, Plantinga Theo S, Alisjahbana Bachti, Govender Dhirendra, Besra Gurdyal S, Netea Mihai G, Reid Delyth M, Willment Janet A, Jacobs Muazzam, Yamasaki Sho, van Crevel Reinout, Brown Gordon D
| 期刊: | Cell Host & Microbe | 影响因子: | 18.700 |
| 时间: | 2015 | 起止号: | 2015 Feb 11; 17(2):252-9 |
| doi: | 10.1016/j.chom.2015.01.004 | 研究方向: | 其它 |
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