Nature Communications (Nov 2024)

TBK1-associated adapters TANK and AZI2 protect mice against TNF-induced cell death and severe autoinflammatory diseases

  • Andrea Ujevic,
  • Daniela Knizkova,
  • Alzbeta Synackova,
  • Michaela Pribikova,
  • Tijana Trivic,
  • Anna Dalinskaya,
  • Ales Drobek,
  • Veronika Niederlova,
  • Darina Paprckova,
  • Roldan De Guia,
  • Petr Kasparek,
  • Jan Prochazka,
  • Juraj Labaj,
  • Olha Fedosieieva,
  • Bernhard Florian Roeck,
  • Ondrej Mihola,
  • Zdenek Trachtulec,
  • Radislav Sedlacek,
  • Ondrej Stepanek,
  • Peter Draber

DOI
https://doi.org/10.1038/s41467-024-54399-4
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 18

Abstract

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Abstract The cytokine TNF can trigger highly proinflammatory RIPK1-dependent cell death. Here, we show that the two adapter proteins, TANK and AZI2, suppress TNF-induced cell death by regulating the activation of TBK1 kinase. Mice lacking either TANK or AZI2 do not show an overt phenotype. Conversely, animals deficient in both adapters are born in a sub-Mendelian ratio and suffer from severe multi-organ inflammation, excessive antibody production, male sterility, and early mortality, which can be rescued by TNFR1 deficiency and significantly improved by expressing a kinase-dead form of RIPK1. Mechanistically, TANK and AZI2 both recruit TBK1 to the TNF receptor signaling complex, but with distinct kinetics due to interaction with different complex components. While TANK binds directly to the adapter NEMO, AZI2 is recruited later via deubiquitinase A20. In summary, our data show that TANK and AZI2 cooperatively sustain TBK1 activity during different stages of TNF receptor assembly to protect against autoinflammation.