Mutations in <i>STAT3</i> and <i>IL12RB1</i> impair the development of human IL-17–producing T cells

Ludovic de Beaucoudrey(Délégation Paris 5), Anne Puel(Délégation Paris 5), Orchidée Filipe‐Santos(Délégation Paris 5), Aurélie Cobat(Délégation Paris 5), Pegah Ghandil(Délégation Paris 5), Maya Chrabieh(Délégation Paris 5), Jacqueline Feinberg(Délégation Paris 5), Horst von Bernuth(Délégation Paris 5), Arina Samarina(Délégation Paris 5), Lucile Jannière(Délégation Paris 5), Claire Fieschi(Assistance Publique – Hôpitaux de Paris), Jean‐Louis Stephan(Centre Hospitalier Universitaire de Saint-Étienne), Cathérine Boileau(Assistance Publique – Hôpitaux de Paris), Stanislas Lyonnet(Délégation Paris 5), Guillaume Jondeau(Délégation Paris 7), Valérie Cormier‐Daire(Délégation Paris 5), Martine Le Merrer(Délégation Paris 5), C. Hoarau(Université de Tours), Yvon Lebranchu(Université de Tours), Olivier Lortholary, Marie‐Olivia Chandesris, François Tron(Inserm), Eleonora Gambineri(University of Florence), Lucia Bianchi(University of Florence), Carlos Rodríguez‐Gallego(Hospital Universitario de Gran Canaria Doctor Negrín), Simona Eva Zitnik(Ljubljana University Medical Centre), Julia Vasconcelos, Margarida Guedes(Hospital de Santo António), Artur Bonito Vítor(Hospital de São João), László Maródi(University of Debrecen), Helen Chapel(University of Oxford), Brenda Reid(University of Toronto), Chaim M. Roifman(University of Toronto), David Nadal(Office of Infectious Diseases), Janine Reichenbach(University Children's Hospital Zurich), Isabel Caragol(Vall d'Hebron Hospital Universitari), Ben‐Zion Garty(Schneider Children's Medical Center), Figen Doğu(Ankara University), Yıldız Çamcıoğlu(Istanbul University), Sanyie Gülle(Dr. Behçet Uz Çocuk Hastalıkları Hastanesi), Özden Sanal(Hacettepe University Hospital), Alain Fischer(Délégation Paris 5), Laurent Abel(Délégation Paris 5), Brigitta Stockinger(Medical Research Council), Capucine Pïcard(Délégation Paris 5), Jean‐Laurent Casanova(Délégation Paris 5)
The Journal of Experimental Medicine
June 30, 2008
10.1084/jem.20080321
Cited by 430Open Access
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Abstract

The cytokines controlling the development of human interleukin (IL) 17--producing T helper cells in vitro have been difficult to identify. We addressed the question of the development of human IL-17--producing T helper cells in vivo by quantifying the production and secretion of IL-17 by fresh T cells ex vivo, and by T cell blasts expanded in vitro from patients with particular genetic traits affecting transforming growth factor (TGF) beta, IL-1, IL-6, or IL-23 responses. Activating mutations in TGFB1, TGFBR1, and TGFBR2 (Camurati-Engelmann disease and Marfan-like syndromes) and loss-of-function mutations in IRAK4 and MYD88 (Mendelian predisposition to pyogenic bacterial infections) had no detectable impact. In contrast, dominant-negative mutations in STAT3 (autosomal-dominant hyperimmunoglobulin E syndrome) and, to a lesser extent, null mutations in IL12B and IL12RB1 (Mendelian susceptibility to mycobacterial diseases) impaired the development of IL-17--producing T cells. These data suggest that IL-12Rbeta1- and STAT-3--dependent signals play a key role in the differentiation and/or expansion of human IL-17-producing T cell populations in vivo.

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