Structures of TGF-β with betaglycan and the signaling receptors reveal the mechanism whereby betaglycan potentiates receptor complex assembly and signaling

Author:

Wieteska ŁukaszORCID,Taylor Alexander B.ORCID,Punch EmmaORCID,Coleman Jonathan A.ORCID,Conway Isabella O.ORCID,Lin Yeu-FarnORCID,Byeon Chang-HyeockORCID,Hinck Cynthia S.,Krzysiak Troy,Ishima RiekoORCID,López-Casillas FernandoORCID,Cherepanov PeterORCID,Bernard Daniel J.ORCID,Hill Caroline S.ORCID,Hinck Andrew P.ORCID

Abstract

AbstractBetaglycan (BG) is a transmembrane co-receptor of the transforming growth factor-β (TGF-β) family of signaling ligands. It is essential for embryonic development and tissue homeostasis and fertility in adults. It functions by enabling binding of the three TGF-β isoforms to their signaling receptors and is additionally required for inhibin A (InhA) activity. Despite its requirement for the functions of TGF-βs and InhA in vivo, structural information explaining BG ligand selectivity and its mechanism of action is lacking. Here, we determine the structure of TGF-β bound both to BG and the signaling receptors, TGFBR1 and TGFBR2. We identify key regions responsible for ligand engagement, which has revealed novel binding interfaces that differ from those described for the closely related co-receptor of the TGF-β family, endoglin, thus demonstrating remarkable evolutionary adaptation to enable ligand selectivity. Finally, we provide a structural explanation for the hand-off mechanism underlying TGF-β signal potentiation.

Publisher

Cold Spring Harbor Laboratory

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