Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury

Chronic pain is a common and often debilitating problem that affects 100 million Americans. A better understanding of pain’s molecular mechanisms is necessary for developing safe and effective therapeutics. Microglial activation has been implicated as a mediator of chronic pain in numerous preclinic...

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Autores principales: Huck, Nolan A., Donovan, Lauren J., Shen, Huaishuang, Jordan, Claire E., Muwanga, Gabriella P.B., Bridges, Caldwell M., Forman, Thomas E., Cordonnier, Stephanie A., Haight, Elena S., Dale-Huang, Fiona, Takemura, Yoshinori, Tawfik, Vivianne L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Special Issue on Basic mechanisms and targets in pain neurobiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9755061/
https://www.ncbi.nlm.nih.gov/pubmed/36531615
http://dx.doi.org/10.1016/j.ynpai.2022.100106
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author Huck, Nolan A.
Donovan, Lauren J.
Shen, Huaishuang
Jordan, Claire E.
Muwanga, Gabriella P.B.
Bridges, Caldwell M.
Forman, Thomas E.
Cordonnier, Stephanie A.
Haight, Elena S.
Dale-Huang, Fiona
Takemura, Yoshinori
Tawfik, Vivianne L.
author_facet Huck, Nolan A.
Donovan, Lauren J.
Shen, Huaishuang
Jordan, Claire E.
Muwanga, Gabriella P.B.
Bridges, Caldwell M.
Forman, Thomas E.
Cordonnier, Stephanie A.
Haight, Elena S.
Dale-Huang, Fiona
Takemura, Yoshinori
Tawfik, Vivianne L.
author_sort Huck, Nolan A.
collection PubMed
description Chronic pain is a common and often debilitating problem that affects 100 million Americans. A better understanding of pain’s molecular mechanisms is necessary for developing safe and effective therapeutics. Microglial activation has been implicated as a mediator of chronic pain in numerous preclinical studies; unfortunately, translational efforts using known glial modulators have largely failed, perhaps at least in part due to poor specificity of the compounds pursued, or an incomplete understanding of microglial reactivity. In order to achieve a more granular understanding of the role of microglia in chronic pain as a means of optimizing translational efforts, we utilized a clinically-informed mouse model of complex regional pain syndrome (CRPS), and monitored microglial activation throughout pain progression. We discovered that while both males and females exhibit spinal cord microglial activation as evidenced by increases in Iba1, activation is attenuated and delayed in females. We further evaluated the expression of the newly identified microglia-specific marker, TMEM119, and identified two distinct populations in the spinal cord parenchyma after peripheral injury: TMEM119+ microglia and TMEM119- infiltrating myeloid lineage cells, which are comprised of Ly6G + neutrophils and Ly6G- macrophages/monocytes. Neurons are sensitized by inflammatory mediators released in the CNS after injury; however, the cellular source of these cytokines remains somewhat unclear. Using multiplex in situ hybridization in combination with immunohistochemistry, we demonstrate that spinal cord TMEM119+ microglia are the cellular source of cytokines IL6 and IL1β after peripheral injury. Taken together, these data have important implications for translational studies: 1) microglia remain a viable analgesic target for males and females, so long as duration after injury is considered; 2) the analgesic properties of microglial modulators are likely at least in part related to their suppression of microglial-released cytokines, and 3) a limited number of neutrophils and macrophages/monocytes infiltrate the spinal cord after peripheral injury but have unknown impact on pain persistence or resolution. Further studies to uncover glial-targeted therapeutic interventions will need to consider sex, timing after injury, and the exact target population of interest to have the specificity necessary for translation.
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spelling pubmed-97550612022-12-17 Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury Huck, Nolan A. Donovan, Lauren J. Shen, Huaishuang Jordan, Claire E. Muwanga, Gabriella P.B. Bridges, Caldwell M. Forman, Thomas E. Cordonnier, Stephanie A. Haight, Elena S. Dale-Huang, Fiona Takemura, Yoshinori Tawfik, Vivianne L. Neurobiol Pain Special Issue on Basic mechanisms and targets in pain neurobiology Chronic pain is a common and often debilitating problem that affects 100 million Americans. A better understanding of pain’s molecular mechanisms is necessary for developing safe and effective therapeutics. Microglial activation has been implicated as a mediator of chronic pain in numerous preclinical studies; unfortunately, translational efforts using known glial modulators have largely failed, perhaps at least in part due to poor specificity of the compounds pursued, or an incomplete understanding of microglial reactivity. In order to achieve a more granular understanding of the role of microglia in chronic pain as a means of optimizing translational efforts, we utilized a clinically-informed mouse model of complex regional pain syndrome (CRPS), and monitored microglial activation throughout pain progression. We discovered that while both males and females exhibit spinal cord microglial activation as evidenced by increases in Iba1, activation is attenuated and delayed in females. We further evaluated the expression of the newly identified microglia-specific marker, TMEM119, and identified two distinct populations in the spinal cord parenchyma after peripheral injury: TMEM119+ microglia and TMEM119- infiltrating myeloid lineage cells, which are comprised of Ly6G + neutrophils and Ly6G- macrophages/monocytes. Neurons are sensitized by inflammatory mediators released in the CNS after injury; however, the cellular source of these cytokines remains somewhat unclear. Using multiplex in situ hybridization in combination with immunohistochemistry, we demonstrate that spinal cord TMEM119+ microglia are the cellular source of cytokines IL6 and IL1β after peripheral injury. Taken together, these data have important implications for translational studies: 1) microglia remain a viable analgesic target for males and females, so long as duration after injury is considered; 2) the analgesic properties of microglial modulators are likely at least in part related to their suppression of microglial-released cytokines, and 3) a limited number of neutrophils and macrophages/monocytes infiltrate the spinal cord after peripheral injury but have unknown impact on pain persistence or resolution. Further studies to uncover glial-targeted therapeutic interventions will need to consider sex, timing after injury, and the exact target population of interest to have the specificity necessary for translation. Elsevier 2022-10-12 /pmc/articles/PMC9755061/ /pubmed/36531615 http://dx.doi.org/10.1016/j.ynpai.2022.100106 Text en © 2022 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Special Issue on Basic mechanisms and targets in pain neurobiology
Huck, Nolan A.
Donovan, Lauren J.
Shen, Huaishuang
Jordan, Claire E.
Muwanga, Gabriella P.B.
Bridges, Caldwell M.
Forman, Thomas E.
Cordonnier, Stephanie A.
Haight, Elena S.
Dale-Huang, Fiona
Takemura, Yoshinori
Tawfik, Vivianne L.
Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
title Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
title_full Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
title_fullStr Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
title_full_unstemmed Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
title_short Sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
title_sort sex-distinct microglial activation and myeloid cell infiltration in the spinal cord after painful peripheral injury
topic Special Issue on Basic mechanisms and targets in pain neurobiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9755061/
https://www.ncbi.nlm.nih.gov/pubmed/36531615
http://dx.doi.org/10.1016/j.ynpai.2022.100106
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