How the immune mousetrap works: structural evidence for the immunomodulatory action of a peptide from influenza NS1 protein

Author:

Zabrodskaya YanaORCID,Tsvetkov VladimirORCID,Shurygina Anna-PolinaORCID,Vasyliev Kirill,Shaldzhyan AramORCID,Gorshkov AndreyORCID,Kuklin AlexanderORCID,Fedorova Natalya,Egorov VladimirORCID

Abstract

AbstractOne of the critical stages of the T-cell immune response is the dimerization of the intramembrane domains of T-cell receptors (TCR). Structural similarities between the immunosuppressive domains of viral proteins and the transmembrane domains of TCR have led several authors to hypothesize the mechanism of immune response suppression by highly pathogenic viruses: viral proteins embed themselves in the membrane and act on the intramembrane domain of the TCRalpha subunit, hindering its functional oligomerization. It has also been suggested that this mechanism is used by influenza A virus in NS1-mediated immunosuppression. We have shown that the peptide corresponding to the primary structure of the potential immunosuppressive domain of NS1 protein (G51) can reduce concanavalin A-induced proliferation of PBMC cells, as well as in vitro, G51 can affect the oligomerization of the core peptide corresponding to the intramembrane domain of TCR, using AFM and small-angle neutron scattering.The results obtained usingin celluloandin vitromodel systems suggest the presence of functional interaction between the NS1 fragment and the intramembrane domain of the TCR alpha subunit. We have proposed a possible scheme for such interaction obtained by computer modeling.This suggests the existence of another NS1-mediated mechanism of immunosuppression in influenza.Abstract Figure

Publisher

Cold Spring Harbor Laboratory

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