Differentiation of CD8+ T cells into effector cells is enhanced by physiological range hyperthermia

生物 细胞毒性T细胞 CD8型 脾细胞 抗原 效应器 细胞生物学 CD28 免疫学 分子生物学 生物化学 体外
作者
Thomas A. Mace,Lingwen Zhong,Casey L. Kilpatrick,Evan R. Zynda,Chen-Ting Lee,Maegan L. Capitano,Hans Minderman,Elizabeth A. Repasky
出处
期刊:Journal of Leukocyte Biology [Oxford University Press]
卷期号:90 (5): 951-962 被引量:98
标识
DOI:10.1189/jlb.0511229
摘要

In this study, we asked whether exposure to different physiologically relevant temperatures (33°C, 37°C, and 39.5°C) could affect subsequent antigen-specific, activation-related events of naive CD8(+) T cells. We observed that temporary exposure of CD62L(hi)CD44(lo) Pmel-1 CD8(+) cells to 39.5°C prior to their antigen-dependent activation with gp100(25-33) peptide-pulsed C57BL/6 splenocytes resulted in a greater percentage of cells, which eventually differentiated into CD62L(lo)CD44(hi) effector cells compared with cells incubated at 33°C and 37°C. However, the proliferation rate of naive CD8(+) T cells was not affected by mild heating. While exploring these effects further, we observed that mild heating of CD8(+) T cells resulted in the reversible clustering of GM1(+) CD-microdomains in the plasma membrane. This could be attributable to a decrease in line tension in the plasma membrane, as we also observed an increase in membrane fluidity at higher temperatures. Importantly, this same clustering phenomenon was observed in CD8(+) T cells isolated from spleen, LNs, and peripheral blood following mild whole-body heating of mice. Further, we observed that mild heating also resulted in the clustering of TCRβ and the CD8 coreceptor but not CD71R. Finally, we observed an enhanced rate of antigen-specific conjugate formation with APCs following mild heating, which could account for the difference in the extent of differentiation. Overall, these novel findings may help us to further understand the impact of physiologically relevant temperature shifts on the regulation of antigen-specific CD8(+) T cell activation and the subsequent generation of effector cells.
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