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Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice

Certain life stressors having enduring physiological and behavioral consequences, in part by eliciting dramatic signaling shifts in monoamine neurotransmitters. High monoamine levels can overwhelm selective transporters like the serotonin transporter. This is when polyspecific transporters like plas...

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Autores principales: Weber, Brady L., Nicodemus, Marissa M., Hite, Allianna K., Spalding, Isabella R., Beaver, Jasmin N., Scrimshaw, Lauren R., Kassis, Sarah K., Reichert, Julie M., Ford, Matthew T., Russell, Cameron N., Hallal, Elayna M., Gilman, T. Lee
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10671398/
https://www.ncbi.nlm.nih.gov/pubmed/38003684
http://dx.doi.org/10.3390/ijms242216494
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author Weber, Brady L.
Nicodemus, Marissa M.
Hite, Allianna K.
Spalding, Isabella R.
Beaver, Jasmin N.
Scrimshaw, Lauren R.
Kassis, Sarah K.
Reichert, Julie M.
Ford, Matthew T.
Russell, Cameron N.
Hallal, Elayna M.
Gilman, T. Lee
author_facet Weber, Brady L.
Nicodemus, Marissa M.
Hite, Allianna K.
Spalding, Isabella R.
Beaver, Jasmin N.
Scrimshaw, Lauren R.
Kassis, Sarah K.
Reichert, Julie M.
Ford, Matthew T.
Russell, Cameron N.
Hallal, Elayna M.
Gilman, T. Lee
author_sort Weber, Brady L.
collection PubMed
description Certain life stressors having enduring physiological and behavioral consequences, in part by eliciting dramatic signaling shifts in monoamine neurotransmitters. High monoamine levels can overwhelm selective transporters like the serotonin transporter. This is when polyspecific transporters like plasma membrane monoamine transporter (PMAT, Slc29a4) are hypothesized to contribute most to monoaminergic signaling regulation. Here, we employed two distinct counterbalanced stressors—fear conditioning and swim stress—in mice to systematically determine how reductions in PMAT function affect heterotypic stressor responsivity. We hypothesized that male heterozygotes would exhibit augmented stressor responses relative to female heterozygotes. Decreased PMAT function enhanced context fear expression, an effect unexpectedly obscured by a sham stress condition. Impaired cued fear extinction retention and enhanced context fear expression in males were conversely unmasked by a sham swim condition. Abrogated corticosterone levels in male heterozygotes that underwent swim stress after context fear conditioning did not map onto any measured behaviors. In sum, male heterozygous mouse fear behaviors proved malleable in response to preceding stressor or sham stress exposure. Combined, these data indicate that reduced male PMAT function elicits a form of stress-responsive plasticity. Future studies should assess how PMAT is differentially affected across sexes and identify downstream consequences of the stress-shifted corticosterone dynamics.
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spelling pubmed-106713982023-11-18 Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice Weber, Brady L. Nicodemus, Marissa M. Hite, Allianna K. Spalding, Isabella R. Beaver, Jasmin N. Scrimshaw, Lauren R. Kassis, Sarah K. Reichert, Julie M. Ford, Matthew T. Russell, Cameron N. Hallal, Elayna M. Gilman, T. Lee Int J Mol Sci Article Certain life stressors having enduring physiological and behavioral consequences, in part by eliciting dramatic signaling shifts in monoamine neurotransmitters. High monoamine levels can overwhelm selective transporters like the serotonin transporter. This is when polyspecific transporters like plasma membrane monoamine transporter (PMAT, Slc29a4) are hypothesized to contribute most to monoaminergic signaling regulation. Here, we employed two distinct counterbalanced stressors—fear conditioning and swim stress—in mice to systematically determine how reductions in PMAT function affect heterotypic stressor responsivity. We hypothesized that male heterozygotes would exhibit augmented stressor responses relative to female heterozygotes. Decreased PMAT function enhanced context fear expression, an effect unexpectedly obscured by a sham stress condition. Impaired cued fear extinction retention and enhanced context fear expression in males were conversely unmasked by a sham swim condition. Abrogated corticosterone levels in male heterozygotes that underwent swim stress after context fear conditioning did not map onto any measured behaviors. In sum, male heterozygous mouse fear behaviors proved malleable in response to preceding stressor or sham stress exposure. Combined, these data indicate that reduced male PMAT function elicits a form of stress-responsive plasticity. Future studies should assess how PMAT is differentially affected across sexes and identify downstream consequences of the stress-shifted corticosterone dynamics. MDPI 2023-11-18 /pmc/articles/PMC10671398/ /pubmed/38003684 http://dx.doi.org/10.3390/ijms242216494 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Weber, Brady L.
Nicodemus, Marissa M.
Hite, Allianna K.
Spalding, Isabella R.
Beaver, Jasmin N.
Scrimshaw, Lauren R.
Kassis, Sarah K.
Reichert, Julie M.
Ford, Matthew T.
Russell, Cameron N.
Hallal, Elayna M.
Gilman, T. Lee
Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice
title Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice
title_full Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice
title_fullStr Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice
title_full_unstemmed Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice
title_short Heterotypic Stressors Unmask Behavioral Influences of PMAT Deficiency in Mice
title_sort heterotypic stressors unmask behavioral influences of pmat deficiency in mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10671398/
https://www.ncbi.nlm.nih.gov/pubmed/38003684
http://dx.doi.org/10.3390/ijms242216494
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