| Literature DB >> 32540868 |
Jie Liang1, Junyi J Zhang1, Hsin-I Huang1, Masashi Kanayama1, Nourhan Youssef1, Yingai J Jin2, Estefany Y Reyes1, Clare L Abram3, Shigao Yang4, Clifford A Lowell3, Donghai Wang1,4, Ling Shao5, Mari L Shinohara1,6, Jennifer Y Zhang2, Gianna Elena Hammer7,6.
Abstract
C-type lectin receptors (CLRs) play key roles in antifungal defense. CLR-induced NF-κB is central to CLR functions in immunity, and thus, molecules that control the amplitude of CLR-induced NF-κB could profoundly influence host defense against fungal pathogens. However, little is known about the mechanisms that negatively regulate CLR-induced NF-κB, and molecules which act on the CLR family broadly and which directly regulate acute CLR-signaling cascades remain unidentified. Here, we identify the ubiquitin-editing enzyme A20 as a negative regulator of acute NF-κB activation downstream of multiple CLR pathways. Absence of A20 suppression results in exaggerated CLR responses in cells which are A20 deficient and also cells which are A20 haplosufficient, including multiple primary immune cells. Loss of a single allele of A20 results in enhanced defense against systemic Candida albicans infection and prolonged host survival. Thus, A20 restricts CLR-induced innate immune responses in vivo and is a suppressor of host defense against systemic fungal infection.Entities:
Keywords: A20; C-type lectin receptors; NF-κB; TRAF6; cytokines; dendritic cells; fungal immunity; innate immunity; ubiquitination
Year: 2020 PMID: 32540868 PMCID: PMC7440764 DOI: 10.1128/IAI.00048-20
Source DB: PubMed Journal: Infect Immun ISSN: 0019-9567 Impact factor: 3.441