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Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance

The rostral ventromedial medulla (RVM) exerts bidirectional descending modulation of pain attributable to the activity of electrophysiologically identified pronociceptive ON and antinociceptive OFF neurons. Here, we report that GABAergic ON neurons specifically express G protein–coupled estrogen rec...

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Autores principales: Jiao, Yingfu, Gao, Po, Dong, Li, Ding, Xiaowei, Meng, Youqiang, Qian, Jiahong, Gao, Ting, Wang, Ruoxi, Jiang, Tao, Zhang, Yunchun, Kong, Dexu, Wu, Yi, Chen, Sihan, Xu, Saihong, Tang, Dan, Luo, Ping, Wu, Meimei, Meng, Li, Wen, Daxiang, Wu, Changhao, Zhang, Guohua, Shi, Xueyin, Yu, Weifeng, Rong, Weifang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9797334/
https://www.ncbi.nlm.nih.gov/pubmed/36346677
http://dx.doi.org/10.1172/JCI154588
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author Jiao, Yingfu
Gao, Po
Dong, Li
Ding, Xiaowei
Meng, Youqiang
Qian, Jiahong
Gao, Ting
Wang, Ruoxi
Jiang, Tao
Zhang, Yunchun
Kong, Dexu
Wu, Yi
Chen, Sihan
Xu, Saihong
Tang, Dan
Luo, Ping
Wu, Meimei
Meng, Li
Wen, Daxiang
Wu, Changhao
Zhang, Guohua
Shi, Xueyin
Yu, Weifeng
Rong, Weifang
author_facet Jiao, Yingfu
Gao, Po
Dong, Li
Ding, Xiaowei
Meng, Youqiang
Qian, Jiahong
Gao, Ting
Wang, Ruoxi
Jiang, Tao
Zhang, Yunchun
Kong, Dexu
Wu, Yi
Chen, Sihan
Xu, Saihong
Tang, Dan
Luo, Ping
Wu, Meimei
Meng, Li
Wen, Daxiang
Wu, Changhao
Zhang, Guohua
Shi, Xueyin
Yu, Weifeng
Rong, Weifang
author_sort Jiao, Yingfu
collection PubMed
description The rostral ventromedial medulla (RVM) exerts bidirectional descending modulation of pain attributable to the activity of electrophysiologically identified pronociceptive ON and antinociceptive OFF neurons. Here, we report that GABAergic ON neurons specifically express G protein–coupled estrogen receptor (GPER). GPER(+) neurons exhibited characteristic ON-like responses upon peripheral nociceptive stimulation. Optogenetic activation of GPER(+) neurons facilitated, but their ablation abrogated, pain. Furthermore, activation of GPER caused depolarization of ON cells, potentiated pain, and ameliorated morphine analgesia through desensitizing μ-type opioid receptor–mediated (MOR-mediated) activation of potassium currents. In contrast, genetic ablation or pharmacological blockade of GPER attenuated pain, enhanced morphine analgesia, and delayed the development of morphine tolerance in diverse preclinical pain models. Our data strongly indicate that GPER is a marker for GABAergic ON cells and illuminate the mechanisms underlying hormonal regulation of pain and analgesia, thus highlighting GPER as a promising target for the treatment of pain and opioid tolerance.
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spelling pubmed-97973342023-01-10 Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance Jiao, Yingfu Gao, Po Dong, Li Ding, Xiaowei Meng, Youqiang Qian, Jiahong Gao, Ting Wang, Ruoxi Jiang, Tao Zhang, Yunchun Kong, Dexu Wu, Yi Chen, Sihan Xu, Saihong Tang, Dan Luo, Ping Wu, Meimei Meng, Li Wen, Daxiang Wu, Changhao Zhang, Guohua Shi, Xueyin Yu, Weifeng Rong, Weifang J Clin Invest Research Article The rostral ventromedial medulla (RVM) exerts bidirectional descending modulation of pain attributable to the activity of electrophysiologically identified pronociceptive ON and antinociceptive OFF neurons. Here, we report that GABAergic ON neurons specifically express G protein–coupled estrogen receptor (GPER). GPER(+) neurons exhibited characteristic ON-like responses upon peripheral nociceptive stimulation. Optogenetic activation of GPER(+) neurons facilitated, but their ablation abrogated, pain. Furthermore, activation of GPER caused depolarization of ON cells, potentiated pain, and ameliorated morphine analgesia through desensitizing μ-type opioid receptor–mediated (MOR-mediated) activation of potassium currents. In contrast, genetic ablation or pharmacological blockade of GPER attenuated pain, enhanced morphine analgesia, and delayed the development of morphine tolerance in diverse preclinical pain models. Our data strongly indicate that GPER is a marker for GABAergic ON cells and illuminate the mechanisms underlying hormonal regulation of pain and analgesia, thus highlighting GPER as a promising target for the treatment of pain and opioid tolerance. American Society for Clinical Investigation 2023-01-03 /pmc/articles/PMC9797334/ /pubmed/36346677 http://dx.doi.org/10.1172/JCI154588 Text en © 2023 Jiao et al. https://creativecommons.org/licenses/by/4.0/This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Jiao, Yingfu
Gao, Po
Dong, Li
Ding, Xiaowei
Meng, Youqiang
Qian, Jiahong
Gao, Ting
Wang, Ruoxi
Jiang, Tao
Zhang, Yunchun
Kong, Dexu
Wu, Yi
Chen, Sihan
Xu, Saihong
Tang, Dan
Luo, Ping
Wu, Meimei
Meng, Li
Wen, Daxiang
Wu, Changhao
Zhang, Guohua
Shi, Xueyin
Yu, Weifeng
Rong, Weifang
Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance
title Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance
title_full Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance
title_fullStr Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance
title_full_unstemmed Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance
title_short Molecular identification of bulbospinal ON neurons by GPER, which drives pain and morphine tolerance
title_sort molecular identification of bulbospinal on neurons by gper, which drives pain and morphine tolerance
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9797334/
https://www.ncbi.nlm.nih.gov/pubmed/36346677
http://dx.doi.org/10.1172/JCI154588
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