Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways

Activation of mTORC1 is essential for anti-tumor function of iNKT cells. The mechanisms underlying impaired mTORC1 activation in intratumoral iNKT cells remain unclear. Via generating Vam6(+/-) mice and using flow cytometry, image approach, and RNA sequencing, we studied the role of Vam6 in controll...

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Autores principales: Bai, Shiyu, Wu, Qielan, Zhu, Shasha, Zhang, Yuwei, Chen, Xuran, Su, Miya, Pan, Jun, Li, Shuhang, Yue, Ting, Xu, Linfeng, Xie, Di, Tian, Chenxi, Zhao, Dan, Li, Xiang, Hou, Junjie, Wang, Lu, Fu, Sicheng, Xue, Yanhong, Jiang, Amin, Li, Dong, Xu, Tao, Tian, Zhigang, Zhou, Rongbin, Zhang, Huimin, Bai, Li
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9892639/
https://www.ncbi.nlm.nih.gov/pubmed/36741382
http://dx.doi.org/10.3389/fimmu.2022.1051045
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author Bai, Shiyu
Wu, Qielan
Zhu, Shasha
Zhang, Yuwei
Chen, Xuran
Su, Miya
Pan, Jun
Li, Shuhang
Yue, Ting
Xu, Linfeng
Xie, Di
Tian, Chenxi
Zhao, Dan
Li, Xiang
Hou, Junjie
Wang, Lu
Fu, Sicheng
Xue, Yanhong
Jiang, Amin
Li, Dong
Xu, Tao
Tian, Zhigang
Zhou, Rongbin
Zhang, Huimin
Bai, Li
author_facet Bai, Shiyu
Wu, Qielan
Zhu, Shasha
Zhang, Yuwei
Chen, Xuran
Su, Miya
Pan, Jun
Li, Shuhang
Yue, Ting
Xu, Linfeng
Xie, Di
Tian, Chenxi
Zhao, Dan
Li, Xiang
Hou, Junjie
Wang, Lu
Fu, Sicheng
Xue, Yanhong
Jiang, Amin
Li, Dong
Xu, Tao
Tian, Zhigang
Zhou, Rongbin
Zhang, Huimin
Bai, Li
author_sort Bai, Shiyu
collection PubMed
description Activation of mTORC1 is essential for anti-tumor function of iNKT cells. The mechanisms underlying impaired mTORC1 activation in intratumoral iNKT cells remain unclear. Via generating Vam6(+/-) mice and using flow cytometry, image approach, and RNA sequencing, we studied the role of Vam6 in controlling mTORC1 activation and intratumoral iNKT cell functions. Here, we find that increased Vam6 expression in intratumoral iNKT cells leads to impaired mTORC1 activation and IFN-γ production. Mechanistically, Vam6 in iNKT cells is essential for Rab7a-Vam6-AMPK complex formation and thus for recruitment of AMPK to lysosome to activate AMPK, a negative regulator of mTORC1. Additionally, Vam6 relieves inhibitory effect of VDAC1 on Rab7a-Vam6-AMPK complex formation at mitochondria-lysosome contact site. Moreover, we report that lactic acid produced by tumor cells increases Vam6 expression in iNKT cells. Given the key roles of increased Vam6 in promoting AMPK activation in intratumoral iNKT cells, reducing Vam6 expression signifificantly enhances the mTORC1 activation in intratumoral iNKT cells as well as their anti-tumor effificacy. Together, we propose Vam6 as a target for iNKT cell-based immunotherapy.
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spelling pubmed-98926392023-02-03 Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways Bai, Shiyu Wu, Qielan Zhu, Shasha Zhang, Yuwei Chen, Xuran Su, Miya Pan, Jun Li, Shuhang Yue, Ting Xu, Linfeng Xie, Di Tian, Chenxi Zhao, Dan Li, Xiang Hou, Junjie Wang, Lu Fu, Sicheng Xue, Yanhong Jiang, Amin Li, Dong Xu, Tao Tian, Zhigang Zhou, Rongbin Zhang, Huimin Bai, Li Front Immunol Immunology Activation of mTORC1 is essential for anti-tumor function of iNKT cells. The mechanisms underlying impaired mTORC1 activation in intratumoral iNKT cells remain unclear. Via generating Vam6(+/-) mice and using flow cytometry, image approach, and RNA sequencing, we studied the role of Vam6 in controlling mTORC1 activation and intratumoral iNKT cell functions. Here, we find that increased Vam6 expression in intratumoral iNKT cells leads to impaired mTORC1 activation and IFN-γ production. Mechanistically, Vam6 in iNKT cells is essential for Rab7a-Vam6-AMPK complex formation and thus for recruitment of AMPK to lysosome to activate AMPK, a negative regulator of mTORC1. Additionally, Vam6 relieves inhibitory effect of VDAC1 on Rab7a-Vam6-AMPK complex formation at mitochondria-lysosome contact site. Moreover, we report that lactic acid produced by tumor cells increases Vam6 expression in iNKT cells. Given the key roles of increased Vam6 in promoting AMPK activation in intratumoral iNKT cells, reducing Vam6 expression signifificantly enhances the mTORC1 activation in intratumoral iNKT cells as well as their anti-tumor effificacy. Together, we propose Vam6 as a target for iNKT cell-based immunotherapy. Frontiers Media S.A. 2023-01-19 /pmc/articles/PMC9892639/ /pubmed/36741382 http://dx.doi.org/10.3389/fimmu.2022.1051045 Text en Copyright © 2023 Bai, Wu, Zhu, Zhang, Chen, Su, Pan, Li, Yue, Xu, Xie, Tian, Zhao, Li, Hou, Wang, Fu, Xue, Jiang, Li, Xu, Tian, Zhou, Zhang and Bai https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Bai, Shiyu
Wu, Qielan
Zhu, Shasha
Zhang, Yuwei
Chen, Xuran
Su, Miya
Pan, Jun
Li, Shuhang
Yue, Ting
Xu, Linfeng
Xie, Di
Tian, Chenxi
Zhao, Dan
Li, Xiang
Hou, Junjie
Wang, Lu
Fu, Sicheng
Xue, Yanhong
Jiang, Amin
Li, Dong
Xu, Tao
Tian, Zhigang
Zhou, Rongbin
Zhang, Huimin
Bai, Li
Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways
title Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways
title_full Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways
title_fullStr Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways
title_full_unstemmed Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways
title_short Vam6 reduces iNKT cell function in tumor via modulating AMPK/mTOR pathways
title_sort vam6 reduces inkt cell function in tumor via modulating ampk/mtor pathways
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9892639/
https://www.ncbi.nlm.nih.gov/pubmed/36741382
http://dx.doi.org/10.3389/fimmu.2022.1051045
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