Abstract
A20 (also known as TNFAIP3) is a deubiquitinating enzyme (DUB) that ensures optimal immune responses in cells stimulated by cytokines, such as TNF and IL-1, or pathogen components, such as lipopolysaccharide. Deletion of A20 in mice results in multi-organ inflammation and death within 2 weeks 1. The anti-inflammatory functions of A20 have been attributed to its ability to negatively regulate NF-κB signaling 2. The picture that has emerged over the last decade is that A20 attenuates NF-κB signaling by removing polyubiquitin chains from specific NF-κB signaling proteins. A study published in this issue of EMBO reports by Sankar Ghosh and colleagues 3 now shows that A20 knockin mice expressing a catalytically inactive A20 mutant that can no longer remove ubiquitin are normal and do not have an inflammatory phenotype. These results challenge the notion that A20 exerts its NF-κB inhibitory and anti-inflammatory function by acting as a DUB.
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