Litcius/Paper detail

Competitive binding of CD226/TIGIT with poliovirus receptor regulates macrophage polarization and is involved in vascularized skin graft rejection

Dongliang Zhang, Yitian Liu, Jingchang Ma, Zhigang Xu, Chujun Duan, Yuling Wang, Xuemei Li, Juntao Han, Ran Zhuang

2023American Journal of Transplantation17 citationsDOIOpen Access PDF

Abstract

End-stage organ failure often requires solid organ transplantation. Nevertheless, transplant rejection remains an unresolved issue. The induction of donor-specific tolerance is the ultimate goal in transplantation research. In this study, an allograft vascularized skin rejection model using BALB/c-C57/BL6 mice was established to evaluate the regulation of the poliovirus receptor signaling pathway using CD226 knockout or T cell immunoglobulin and ITIM domain (TIGIT)–crystallizable fragment (Fc) recombinant protein treatment. In the TIGIT-Fc–treated and CD226 knockout groups, graft survival time prolonged significantly, with a regulatory T cell proportion increase and M2-type macrophage polarization. Donor-reactive recipient T cells became hyporesponsive while responding normally after a third-party antigen challenge. In both groups, serum interleukin (IL)-1β, IL-6, IL-12p70, IL-17A, tumor necrosis factor–α, interferon gamma, and monocyte chemoattractant protein-1 levels decreased, and the IL-10 level increased. In vitro, M2 markers, such as Arg1 and IL-10, were markedly increased by TIGIT-Fc, whereas iNOS, IL-1β, IL-6, IL-12p70, tumor necrosis factor–α, and interferon gamma levels decreased. CD226-Fc exerted the opposite effect. TIGIT suppressed TH1 and TH17 differentiation by inhibiting macrophage SHP-1 phosphorylation and enhanced ERK1/2-MSK1 phosphorylation and nuclear translocation of CREB. In conclusion, CD226 and TIGIT competitively bind to poliovirus receptor with activating and inhibitory functions, respectively. Mechanistically, TIGIT promotes IL-10 transcription from macrophages by activating the ERK1/2-MSK1-CREB pathway and enhancing M2-type polarization. CD226/TIGIT–poliovirus receptor are crucial regulatory molecules of allograft rejection.

Topics & Concepts

MedicineMacrophage polarizationTIGITReceptorImmunologyMacrophageCancer researchInternal medicineImmune systemCD8BiologyIn vitroBiochemistryImmune Cell Function and InteractionImmune cells in cancerExtracellular vesicles in disease
Competitive binding of CD226/TIGIT with poliovirus receptor regulates macrophage polarization and is involved in vascularized skin graft rejection | Litcius