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Volume 20 Issue 10, October 2019

TNFAIP3 variants in human evolution

A20, encoded by TNFAIP3, is a negative-feedback inhibitor of NF-κB. Grey and colleagues identify natural human variants of TNFAIP3 that lower A20 activity and increase autoinflammatory responses. These alleles were inherited by descendants of Denisovans who crossed the Wallace line to inhabit Oceania.

See Zammit et al.

Image: Shane Grey and Nathan Zammit. Cover Design: Erin Dewalt

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  • A new study has identified various previously unknown mutations in the genes encoding human and mouse A20 that affect its phosphorylation and its function as an inhibitor of the transcription factor NF-κB, with implications for immunity and inflammatory disease.

    • Arne Martens
    • Geert van Loo
    News & Views
  • Transcription-factor paralogs are not equivalent and serve distinct roles in immune cells. Analysis of the RUNX family of transcription factors reveals insights into the non-redundant roles of RUNX1 and RUNX3.

    • Wooseok Seo
    • Ichiro Taniuchi
    News & Views
  • Cellular metabolic screening identifies hyper-respiration, induced by gain-of-function mutations in the gene encoding succinate dehydrogenase, as a disease-driving immunometabolic trait of B cells from patients with primary antibody deficiency.

    • Hu Zeng
    • Hongbo Chi
    News & Views
  • A specifically engineered Zika subunit vaccine based on the viral envelope protein mediates protective immunity in mice without inducing the cross-reactive antibodies responsible for antibody-dependent enhancement of infection with dengue virus.

    • Franz X. Heinz
    • Karin Stiasny
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  • Zhu and colleagues discuss the forces that affect the ligand recognition, receptor triggering and signal transduction downstream of immunoreceptors, and their implication on lineage decision and effector function.

    • Cheng Zhu
    • Wei Chen
    • Kaitao Li
    Perspective
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