A structurally distinct TGF-β mimic from an intestinal helminth parasite potently induces regulatory T cells

来自肠道蠕虫寄生虫的一种结构独特的TGF-β类似物能够有效诱导调节性T细胞。

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作者:Chris J C Johnston ,Danielle J Smyth ,Ravindra B Kodali ,Madeleine P J White ,Yvonne Harcus ,Kara J Filbey ,James P Hewitson ,Cynthia S Hinck ,Alasdair Ivens ,Andrea M Kemter ,Anna O Kildemoes ,Thierry Le Bihan ,Dinesh C Soares ,Stephen M Anderton ,Thomas Brenn ,Stephen J Wigmore ,Hannah V Woodcock ,Rachel C Chambers ,Andrew P Hinck ,Henry J McSorley ,Rick M Maizels

Abstract

Helminth parasites defy immune exclusion through sophisticated evasion mechanisms, including activation of host immunosuppressive regulatory T (Treg) cells. The mouse parasite Heligmosomoides polygyrus can expand the host Treg population by secreting products that activate TGF-β signalling, but the identity of the active molecule is unknown. Here we identify an H. polygyrus TGF-β mimic (Hp-TGM) that replicates the biological and functional properties of TGF-β, including binding to mammalian TGF-β receptors and inducing mouse and human Foxp3+ Treg cells. Hp-TGM has no homology with mammalian TGF-β or other members of the TGF-β family, but is a member of the complement control protein superfamily. Thus, our data indicate that through convergent evolution, the parasite has acquired a protein with cytokine-like function that is able to exploit an endogenous pathway of immunoregulation in the host.

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