Phenotypic and functional features of human Th17 cells

doi:10.1084/jem.20070663

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doi:10.1084/jem.20070663
The Journal of Experimental Medicine, Vol. 204, No. 8, 1849-1861
The Rockefeller University Press, 0022-1007 $30.00
© Annunziato et al.

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Phenotypic and functional features of human Th17 cells

Francesco Annunziato¹, Lorenzo Cosmi¹, Veronica Santarlasci¹, Laura Maggi¹, Francesco Liotta¹, Benedetta Mazzinghi¹, Eliana Parente¹, Lucia Filì¹, Simona Ferri¹, Francesca Frosali¹, Francesco Giudici², Paola Romagnani¹, Paola Parronchi¹, Francesco Tonelli², Enrico Maggi¹, and Sergio Romagnani¹

¹ Center for Research, Transfer and High Education on Chronic, Inflammatory, Degenerative and Neoplastic Disorders (DENOTHE) and ² Department of Pathophysiology, University of Florence, Florence 50134, Italy

CORRESPONDENCE Sergio Romagnani:s.romagnani{at}dmi.unifi.it

T helper (Th) 17 cells represent a novel subset of CD4+ T cellsthat are protective against extracellular microbes, but areresponsible for autoimmune disorders in mice. However, theirproperties in humans are only partially known. We demonstratethe presence of Th17 cells, some of which produce both interleukin(IL)-17 and interferon (IFN)- ${gamma}$ (Th17/Th1), in the gut of patientswith Crohn's disease. Both Th17 and Th17/Th1 clones showed selectiveexpression of IL-23R, CCR6, and the transcription factor ROR ${gamma}$ t,and they exhibited similar functional features, such as theability to help B cells, low cytotoxicity, and poor susceptibilityto regulation by autologous regulatory T cells. Interestingly,these subsets also expressed the Th1-transcription factor T-bet,and stimulation of these cells in the presence of IL-12 down-regulatedthe expression of ROR ${gamma}$ t and the production of IL-17, but inducedIFN- ${gamma}$ . These effects were partially inhibited in presence ofIL-23. Similar receptor expression and functional capabilitieswere observed in freshly derived IL-17–producing peripheralblood and tonsillar CD4+ T cells. The demonstration of selectivemarkers for human Th17 cells may help us to understand theirpathogenic role. Moreover, the identification of a subset ofcells sharing features of both Th1 and Th17, which can arisefrom the modulation of Th17 cells by IL-12, may raise new issuesconcerning developmental and/or functional relationships betweenTh17 and Th1.

Abbreviations used: Ab, antibody; CD, Crohn's disease; CIA,collagen-induced arthritis; EAE, experimental autoimmune encephalomyelitis;PB, peripheral blood; RA, rheumatoid arthritis.

F. Annunziato and L. Cosmi contributed equally to this paper.

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