A partial form of inherited human USP18 deficiency underlies infection and inflammation

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Martin-Fernandez, Marta | Buta, Sofija | Le Voyer, Tom | Li, Zhi | Dynesen, Lasse Toftdal | Vuillier, Françoise | Franklin, Lina | Ailal, Fatima | Muglia Amancio, Alice | Malle, Louise | Gruber, Conor | Benhsaien, Ibtihal | Altman, Jennie | Taft, Justin | Deswarte, Caroline | Roynard, Manon | Nieto-Patlan, Alejandro | Moriya, Kunihiko | Rosain, Jérémie | Boddaert, Nathalie | Bousfiha, Aziz | Crow, Yanick | Jankovic, Dragana | Sher, Alan | Casanova, Jean-Laurent | Pellegrini, Sandra | Bustamante, Jacinta | Bogunovic, Dusan

Edité par CCSD ; Rockefeller University Press -

International audience. Human USP18 is an interferon (IFN)-stimulated gene product and a negative regulator of type I IFN (IFN-I) signaling. It also removes covalently linked ISG15 from proteins, in a process called deISGylation. In turn, ISG15 prevents USP18 from being degraded by the proteasome. Autosomal recessive complete USP18 deficiency is life-threatening in infancy owing to uncontrolled IFN-I–mediated autoinflammation. We report three Moroccan siblings with autoinflammation and mycobacterial disease who are homozygous for a new USP18 variant. We demonstrate that the mutant USP18 (p.I60N) is normally stabilized by ISG15 and efficient for deISGylation but interacts poorly with the receptor-anchoring STAT2 and is impaired in negative regulation of IFN-I signaling. We also show that IFN-γ–dependent induction of IL-12 and IL-23 is reduced owing to IFN-I–mediated impairment of myeloid cells to produce both cytokines. Thus, insufficient negative regulation of IFN-I signaling by USP18-I60N underlies a specific type I interferonopathy, which impairs IL-12 and IL-23 production by myeloid cells, thereby explaining predisposition to mycobacterial disease.

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