Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice

BACKGROUND: The effects of chronic treatment with tricyclic antidepressant (desipramine, DMI) on the hippocampal transcriptome in mice displaying high and low swim stress-induced analgesia (HA and LA lines) were studied. These mice displayed different depression-like behavioral responses to DMI: str...

Descripción completa

Detalles Bibliográficos
Autores principales: Lisowski, Pawel, Juszczak, Grzegorz R, Goscik, Joanna, Stankiewicz, Adrian M, Wieczorek, Marek, Zwierzchowski, Lech, Swiergiel, Artur H
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3831054/
https://www.ncbi.nlm.nih.gov/pubmed/24225037
http://dx.doi.org/10.1186/1471-2202-14-144
_version_ 1782291565072351232
author Lisowski, Pawel
Juszczak, Grzegorz R
Goscik, Joanna
Stankiewicz, Adrian M
Wieczorek, Marek
Zwierzchowski, Lech
Swiergiel, Artur H
author_facet Lisowski, Pawel
Juszczak, Grzegorz R
Goscik, Joanna
Stankiewicz, Adrian M
Wieczorek, Marek
Zwierzchowski, Lech
Swiergiel, Artur H
author_sort Lisowski, Pawel
collection PubMed
description BACKGROUND: The effects of chronic treatment with tricyclic antidepressant (desipramine, DMI) on the hippocampal transcriptome in mice displaying high and low swim stress-induced analgesia (HA and LA lines) were studied. These mice displayed different depression-like behavioral responses to DMI: stress-sensitive HA animals responded to DMI, while LA animals did not. RESULTS: To investigate the effects of DMI treatment on gene expression profiling, whole-genome Illumina Expression BeadChip arrays and qPCR were used. Total RNA isolated from hippocampi was used. Expression profiling was then performed and data were analyzed bioinformatically to assess the influence of stress susceptibility-specific phenotypes on hippocampal transcriptomic responses to chronic DMI. DMI treatment affected the expression of 71 genes in HA mice and 41 genes in LA mice. We observed the upregulation of Igf2 and the genes involved in neurogenesis (HA: Sema3f, Ntng1, Gbx2, Efna5, and Rora; LA: Otx2, Rarb, and Drd1a) in both mouse lines. In HA mice, we observed the upregulation of genes involved in neurotransmitter transport, the termination of GABA and glycine activity (Slc6a11, Slc6a9), glutamate uptake (Slc17a6), and the downregulation of neuropeptide Y (Npy) and corticotropin releasing hormone-binding protein (Crhbp). In LA mice, we also observed the upregulation of other genes involved in neuroprotection (Ttr, Igfbp2, Prlr) and the downregulation of genes involved in calcium signaling and ion binding (Adcy1, Cckbr, Myl4, Slu7, Scrp1, Zfp330). CONCLUSIONS: Several antidepressant treatment responses are similar in individuals with different sensitivities to stress, including the upregulation of Igf2 and the genes involved in neurogenesis. However, the findings also reveal that many responses to antidepressant treatments, involving the action of individual genes engaged in neurogenesis, neurotransmitter transport and neuroprotection, depend on constitutive hippocampal transcriptomic profiles and might be genotype dependent. The results suggest that, when and if this becomes feasible, antidepressant treatment should take into consideration individual sensitivity to stress.
format Online
Article
Text
id pubmed-3831054
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-38310542013-11-19 Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice Lisowski, Pawel Juszczak, Grzegorz R Goscik, Joanna Stankiewicz, Adrian M Wieczorek, Marek Zwierzchowski, Lech Swiergiel, Artur H BMC Neurosci Research Article BACKGROUND: The effects of chronic treatment with tricyclic antidepressant (desipramine, DMI) on the hippocampal transcriptome in mice displaying high and low swim stress-induced analgesia (HA and LA lines) were studied. These mice displayed different depression-like behavioral responses to DMI: stress-sensitive HA animals responded to DMI, while LA animals did not. RESULTS: To investigate the effects of DMI treatment on gene expression profiling, whole-genome Illumina Expression BeadChip arrays and qPCR were used. Total RNA isolated from hippocampi was used. Expression profiling was then performed and data were analyzed bioinformatically to assess the influence of stress susceptibility-specific phenotypes on hippocampal transcriptomic responses to chronic DMI. DMI treatment affected the expression of 71 genes in HA mice and 41 genes in LA mice. We observed the upregulation of Igf2 and the genes involved in neurogenesis (HA: Sema3f, Ntng1, Gbx2, Efna5, and Rora; LA: Otx2, Rarb, and Drd1a) in both mouse lines. In HA mice, we observed the upregulation of genes involved in neurotransmitter transport, the termination of GABA and glycine activity (Slc6a11, Slc6a9), glutamate uptake (Slc17a6), and the downregulation of neuropeptide Y (Npy) and corticotropin releasing hormone-binding protein (Crhbp). In LA mice, we also observed the upregulation of other genes involved in neuroprotection (Ttr, Igfbp2, Prlr) and the downregulation of genes involved in calcium signaling and ion binding (Adcy1, Cckbr, Myl4, Slu7, Scrp1, Zfp330). CONCLUSIONS: Several antidepressant treatment responses are similar in individuals with different sensitivities to stress, including the upregulation of Igf2 and the genes involved in neurogenesis. However, the findings also reveal that many responses to antidepressant treatments, involving the action of individual genes engaged in neurogenesis, neurotransmitter transport and neuroprotection, depend on constitutive hippocampal transcriptomic profiles and might be genotype dependent. The results suggest that, when and if this becomes feasible, antidepressant treatment should take into consideration individual sensitivity to stress. BioMed Central 2013-11-13 /pmc/articles/PMC3831054/ /pubmed/24225037 http://dx.doi.org/10.1186/1471-2202-14-144 Text en Copyright © 2013 Lisowski et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Lisowski, Pawel
Juszczak, Grzegorz R
Goscik, Joanna
Stankiewicz, Adrian M
Wieczorek, Marek
Zwierzchowski, Lech
Swiergiel, Artur H
Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
title Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
title_full Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
title_fullStr Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
title_full_unstemmed Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
title_short Stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
title_sort stress susceptibility-specific phenotype associated with different hippocampal transcriptomic responses to chronic tricyclic antidepressant treatment in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3831054/
https://www.ncbi.nlm.nih.gov/pubmed/24225037
http://dx.doi.org/10.1186/1471-2202-14-144
work_keys_str_mv AT lisowskipawel stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice
AT juszczakgrzegorzr stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice
AT goscikjoanna stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice
AT stankiewiczadrianm stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice
AT wieczorekmarek stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice
AT zwierzchowskilech stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice
AT swiergielarturh stresssusceptibilityspecificphenotypeassociatedwithdifferenthippocampaltranscriptomicresponsestochronictricyclicantidepressanttreatmentinmice

Ejemplares similares