Substrate-specific recognition of IKKs mediated by USP16 facilitates autoimmune inflammation
Jian-shuai Yu, Tao Huang, Yu Zhang, Xin-tao Mao, Ling-jie Huang, Yining Li, Ting-Ting Wu, Jiang-yan Zhong, Qian Cao, Yi‐yuan Li, Jin Jin
Abstract
-deficient mice. In this study, we found that IKKβ ubiquitination on lysine-238 was substantially increased during inflammation. Using mass spectrometry, we identified USP16 as an essential regulator of the IKKβ ubiquitination level that selectively affected p105 phosphorylation without directly affecting p65 or IκBα phosphorylation. Furthermore, USP16 was highly expressed in colon macrophages in patients with IBD, and myeloid-conditional USP16-knockout mice exhibited reduced IBD severity. Our study provides a new theoretical basis for IBD pathogenesis and targeted precision intervention therapy.
Topics & Concepts
InflammationSubstrate (aquarium)BiologyImmunologyMedicineComputational biologyEcologyInflammasome and immune disordersNF-κB Signaling Pathwaysinterferon and immune responses