Structural and functional analysis of the TGF-β mimic, TGM-2: an immunomodulatory helminth protein
Emmaculate Yaah Ntang, Kyle T. Cunningham, Shashi P. Singh, Claire Ciancia, Anna Sanders, Sergio Lilla, Ananya Mukundan, Stephen M. Ghogomu, Andrew P. Hinck, Rick M. Maizels

TL;DR
This study explores how a helminth protein, TGM-2, mimics TGF-β to modulate the immune system and reduce inflammation.
Contribution
The study reveals the structural and functional roles of TGM-2 domains in immune modulation and TGF-β-like activity.
Findings
Domains 1–3 of TGM-2 bind TGFBR1 and TGFBR2, while domains 4 and 5 bind CD44 more strongly.
Full-length TGM-2 activates the pSMAD pathway and converts CD4+ T cells into Tregs.
TGM-2 and its truncated form reduce allergic airway inflammation in mice.
Abstract
The extraordinary prevalence of helminths is attributable to secretion of molecules that manipulate the host immune system, facilitating their survival. Among the secretory products of the murine intestinal helminth Heligmosomoides polygyrus are 10 mimic proteins with functional resemblance to the mammalian immunosuppressive cytokine, TGF-β, but structurally distinct with five Complement Control Protein (CCP) domains, designated TGM-1 to −10. Here we dissect the structure and function of the mimic TGM-2 and its domains. We generated eight protein truncations lacking N- or C-terminal domains, for testing through pulldowns, mass spectrometric analysis and isothermal titration calorimetry, confirming affinity for TGFBR1 (ALK5), TGFBR2, and the co-receptor CD44. We observed that domains 1–3 bind TGFBR1 and TGFBR2, while domains 4 and 5 exhibit stronger binding to the CD44 co-receptor than…
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Taxonomy
TopicsTGF-β signaling in diseases · Asthma and respiratory diseases · Parasites and Host Interactions
