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Lack of transglutaminase 2 diminished T-cell responses in mice

Cited 12 time in Web of Science Cited 13 time in Scopus
Authors

Kim, Jin-Hee; Hong, Jun Man; Jeong, Eui Man; Lee, Wang Jae; Kim, Hang-Rae; Kang, Jae Seung; Kim, In-Gyu; Hwang, Young-il

Issue Date
2014-07
Publisher
Blackwell Publishing Inc.
Citation
Immunology, Vol.142 No.3, pp.506-516
Abstract
Transglutaminase 2 (TG2) has been reported to play a role in dendritic cell activation and B-cell differentiation after immunization. Its presence and role in T cells, however, has not been explored. In the present study, we determined the expression of TG2 on mouse T cells, and evaluated its role by comparing the behaviours of wild-type and TG2-/- T cells after activation. In our results, naive T cells minimally expressed TG2, expression of which was increased after activation. T-cell proliferation, expression of activation markers such as CD69 and CD25, and secretions of interleukin-2 and interferon- were suppressed in the absence of TG2, presumably due, in part, to diminished nuclear factor-B activation. These effects on T cells seemed to be reflected in the in vivo immune response, the contact hypersensitivity reaction elicited by 2,4-dinitro-1-fluorobenzene, with lowered peak responses in the TG2-/- mice. When splenic T cells from mice immunized with tumour lysate-loaded wild-type dendritic cells were re-challenged ex vivo with the same antigen, the profile of surface markers including CD44, CD62L, and CD127 strongly indicated lesser generation of memory CD8+ T cells in TG2-/- mice. In the TG2-/-CD8+ T cells, moreover, Eomes expression was markedly decreased. These results indicate possible roles of TG2 in CD8+ T-cell activation and CD8+ memory T-cell generation.
ISSN
0019-2805
URI
https://hdl.handle.net/10371/202643
DOI
https://doi.org/10.1111/imm.12282
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  • College of Medicine
Research Area Function, Immune modulation by metabolites, T-cell anergy, differentiation of memory CD8+ T cells, metabolism

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