Type I interferon-mediated autoinflammation due to DNase II deficiency

Mathieu P. Rodero(Inserm), Alessandra Tesser(University of Trieste), Eva Bartok(University of Bonn), Gillian Rice(Manchester Academic Health Science Centre), Erika Della Mina(Inserm), Marine Depp(Inserm), Benoît Beitz(BIOASTER), Vincent Bondet(Inserm), Nicolas Cagnard(Délégation Paris 5), Darragh Duffy(Inserm), Michaël Dussiot(Délégation Paris 5), Marie‐Louise Frémond(Inserm), Marco Gattorno(Istituto Giannina Gaslini), Flavia Guillem(Délégation Paris 5), Naoki Kitabayashi(Inserm), Fabrice Porcheray(BIOASTER), Frédéric Rieux‐Laucat(Délégation Paris 5), Luís Seabra(Inserm), Carolina Uggenti(Inserm), Stefano Volpi(Istituto Giannina Gaslini), Leo Zeef(University of Manchester), Marie‐Alexandra Alyanakian(Hôpital Necker-Enfants Malades), Jacques Beltrand(Délégation Paris 5), Anna Monica Bianco(IRCCS Materno Infantile Burlo Garofolo), Nathalie Boddaert(Hôpital Necker-Enfants Malades), Chantal Brouzes(Hôpital Necker-Enfants Malades), Sophie Candon(Hôpital Necker-Enfants Malades), Roberta Caorsi(Istituto Giannina Gaslini), Marina Charbit(Hôpital Necker-Enfants Malades), Monique Fabrè(Hôpital Necker-Enfants Malades), Flavio Faletra(IRCCS Materno Infantile Burlo Garofolo), M Girard(Hôpital Necker-Enfants Malades), Annie Harroche(Hôpital Necker-Enfants Malades), Evelyn Hartmann(University of Bonn), Dominique Lasne(Université Paris-Sud), Annalisa Marcuzzi(University of Trieste), Bénédicte Neven(Délégation Paris 5), Patrick Nitschké(Délégation Paris 5), Tiffany Pascreau(Université Paris-Sud), Serena Pastore(IRCCS Materno Infantile Burlo Garofolo), Capucine Pïcard(Hôpital Necker-Enfants Malades), Paolo Picco(Istituto Giannina Gaslini), Elisa Piscianz(University of Trieste), Michel Polak(Délégation Paris 5), Pierre Quartier(Délégation Paris 5), Marion Rabant(Hôpital Necker-Enfants Malades), Gabriele Stocco(University of Trieste), Andrea Taddio(University of Trieste), Florence Uettwiller(Délégation Paris 5), Erica Valencic(IRCCS Materno Infantile Burlo Garofolo), Diego Vozzi(IRCCS Materno Infantile Burlo Garofolo), Gunther Hartmann(University of Bonn), Winfried Barchet(University of Bonn), Olivier Hermine(Délégation Paris 5), Brigitte Bader‐Meunier(Hôpital Necker-Enfants Malades), Alberto Tommasini(IRCCS Materno Infantile Burlo Garofolo), Yanick J. Crow(Délégation Paris 5)
Nature Communications
December 13, 2017
10.1038/s41467-017-01932-3
Cited by 225Open Access
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Abstract

Microbial nucleic acid recognition serves as the major stimulus to an antiviral response, implying a requirement to limit the misrepresentation of self nucleic acids as non-self and the induction of autoinflammation. By systematic screening using a panel of interferon-stimulated genes we identify two siblings and a singleton variably demonstrating severe neonatal anemia, membranoproliferative glomerulonephritis, liver fibrosis, deforming arthropathy and increased anti-DNA antibodies. In both families we identify biallelic mutations in DNASE2, associated with a loss of DNase II endonuclease activity. We record increased interferon alpha protein levels using digital ELISA, enhanced interferon signaling by RNA-Seq analysis and constitutive upregulation of phosphorylated STAT1 and STAT3 in patient lymphocytes and monocytes. A hematological disease transcriptomic signature and increased numbers of erythroblasts are recorded in patient peripheral blood, suggesting that interferon might have a particular effect on hematopoiesis. These data define a type I interferonopathy due to DNase II deficiency in humans.

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