Dual functions of Aire CARD multimerization in the transcriptional regulation of T cell tolerance

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作者
Yu-San Huoh
Bin Wu
Sehoon Park
Darren Yang
Kushagra Bansal
Emily Greenwald
Wesley P. Wong
Diane Mathis
Sun Hur
机构
[1] Department of Biological Chemistry and Molecular Pharmacology Blavatnik Institute at Harvard Medical School,Wyss Institute for Biologically Inspired Engineering
[2] Program in Cellular and Molecular Medicine Boston Children’s Hospital,NTU Institute of Structural Biology, School of Biological Sciences
[3] Harvard University,Molecular Biology & Genetics Unit
[4] Department of Immunology Blavatnik Institute at Harvard Medical School,undefined
[5] Nanyang Technological University,undefined
[6] Jawaharlal Nehru Centre for Advanced Scientific Research,undefined
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Aggregate-like biomolecular assemblies are emerging as new conformational states with functionality. Aire, a transcription factor essential for central T cell tolerance, forms large aggregate-like assemblies visualized as nuclear foci. Here we demonstrate that Aire utilizes its caspase activation recruitment domain (CARD) to form filamentous homo-multimers in vitro, and this assembly mediates foci formation and transcriptional activity. However, CARD-mediated multimerization also makes Aire susceptible to interaction with promyelocytic leukemia protein (PML) bodies, sites of many nuclear processes including protein quality control of nuclear aggregates. Several loss-of-function Aire mutants, including those causing autoimmune polyendocrine syndrome type-1, form foci with increased PML body association. Directing Aire to PML bodies impairs the transcriptional activity of Aire, while dispersing PML bodies with a viral antagonist restores this activity. Our study thus reveals a new regulatory role of PML bodies in Aire function, and highlights the interplay between nuclear aggregate-like assemblies and PML-mediated protein quality control.
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