T Cell-Intrinsic Vitamin A Metabolism and Its Signaling Are Targets for Memory T Cell-Based Cancer Immunotherapy

Fumihiro Fujiki,Soyoko Morimoto,Akiko Katsuhara, Akane Okuda, Saeka Ogawa, Eriko Ueda, Maki Miyazaki,Ayako Isotani,Masahito Ikawa,Sumiyuki Nishida,Hiroko Nakajima,Akihiro Tsuboi,Yoshihiro Oka,Jun Nakata,Naoki Hosen,Atsushi Kumanogoh,Yusuke Oji,Haruo Sugiyama

FRONTIERS IN IMMUNOLOGY（2022）

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摘要

Memory T cells play an essential role in infectious and tumor immunity. Vitamin A metabolites such as retinoic acid are immune modulators, but the role of vitamin A metabolism in memory T-cell differentiation is unclear. In this study, we identified retinol dehydrogenase 10 (Rdh10), which metabolizes vitamin A to retinal (RAL), as a key molecule for regulating T cell differentiation. T cell-specific Rdh10 deficiency enhanced memory T-cell formation through blocking RAL production in infection model. Epigenetic profiling revealed that retinoic acid receptor (RAR) signaling activated by vitamin A metabolites induced comprehensive epigenetic repression of memory T cell-associated genes, including TCF7, thereby promoting effector T-cell differentiation. Importantly, memory T cells generated by Rdh deficiency and blocking RAR signaling elicited potent anti-tumor responses in adoptive T-cell transfer setting. Thus, T cell differentiation is regulated by vitamin A metabolism and its signaling, which should be novel targets for memory T cell-based cancer immunotherapy.

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关键词

vitamin A, RDH10, memory T cell, retinoic acid, cancer immunotherapy, vitamin A metabolism, effector T cell

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