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Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal

Morphine belongs among the most commonly used opioids in medical practice due to its strong analgesic effects. However, sustained administration of morphine leads to the development of tolerance and dependence and may cause long-lasting alterations in nervous tissue. Although proteomic approaches en...

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Autores principales: Drastichova, Zdenka, Skrabalova, Jitka, Jedelsky, Petr, Neckar, Jan, Kolar, Frantisek, Novotny, Jiri
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3467212/
https://www.ncbi.nlm.nih.gov/pubmed/23056601
http://dx.doi.org/10.1371/journal.pone.0047167
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author Drastichova, Zdenka
Skrabalova, Jitka
Jedelsky, Petr
Neckar, Jan
Kolar, Frantisek
Novotny, Jiri
author_facet Drastichova, Zdenka
Skrabalova, Jitka
Jedelsky, Petr
Neckar, Jan
Kolar, Frantisek
Novotny, Jiri
author_sort Drastichova, Zdenka
collection PubMed
description Morphine belongs among the most commonly used opioids in medical practice due to its strong analgesic effects. However, sustained administration of morphine leads to the development of tolerance and dependence and may cause long-lasting alterations in nervous tissue. Although proteomic approaches enabled to reveal changes in multiple gene expression in the brain as a consequence of morphine treatment, there is lack of information about the effect of this drug on heart tissue. Here we studied the effect of 10-day morphine exposure and subsequent drug withdrawal (3 or 6 days) on the rat heart proteome. Using the iTRAQ technique, we identified 541 proteins in the cytosol, 595 proteins in the plasma membrane-enriched fraction and 538 proteins in the mitochondria-enriched fraction derived from the left ventricles. Altogether, the expression levels of 237 proteins were altered by morphine treatment or withdrawal. The majority of changes (58 proteins) occurred in the cytosol after a 3-day abstinence period. Significant alterations were found in the expression of heat shock proteins (HSP27, α-B crystallin, HSP70, HSP10 and HSP60), whose levels were markedly up-regulated after morphine treatment or withdrawal. Besides that morphine exposure up-regulated MAPK p38 (isoform CRA_b) which is a well-known up-stream mediator of phosphorylation and activation of HSP27 and α-B crystallin. Whereas there were no alterations in the levels of proteins involved in oxidative stress, several changes were determined in the levels of pro- and anti-apoptotic proteins. These data provide a complex view on quantitative changes in the cardiac proteome induced by morphine treatment or withdrawal and demonstrate great sensitivity of this organ to morphine.
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spelling pubmed-34672122012-10-10 Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal Drastichova, Zdenka Skrabalova, Jitka Jedelsky, Petr Neckar, Jan Kolar, Frantisek Novotny, Jiri PLoS One Research Article Morphine belongs among the most commonly used opioids in medical practice due to its strong analgesic effects. However, sustained administration of morphine leads to the development of tolerance and dependence and may cause long-lasting alterations in nervous tissue. Although proteomic approaches enabled to reveal changes in multiple gene expression in the brain as a consequence of morphine treatment, there is lack of information about the effect of this drug on heart tissue. Here we studied the effect of 10-day morphine exposure and subsequent drug withdrawal (3 or 6 days) on the rat heart proteome. Using the iTRAQ technique, we identified 541 proteins in the cytosol, 595 proteins in the plasma membrane-enriched fraction and 538 proteins in the mitochondria-enriched fraction derived from the left ventricles. Altogether, the expression levels of 237 proteins were altered by morphine treatment or withdrawal. The majority of changes (58 proteins) occurred in the cytosol after a 3-day abstinence period. Significant alterations were found in the expression of heat shock proteins (HSP27, α-B crystallin, HSP70, HSP10 and HSP60), whose levels were markedly up-regulated after morphine treatment or withdrawal. Besides that morphine exposure up-regulated MAPK p38 (isoform CRA_b) which is a well-known up-stream mediator of phosphorylation and activation of HSP27 and α-B crystallin. Whereas there were no alterations in the levels of proteins involved in oxidative stress, several changes were determined in the levels of pro- and anti-apoptotic proteins. These data provide a complex view on quantitative changes in the cardiac proteome induced by morphine treatment or withdrawal and demonstrate great sensitivity of this organ to morphine. Public Library of Science 2012-10-09 /pmc/articles/PMC3467212/ /pubmed/23056601 http://dx.doi.org/10.1371/journal.pone.0047167 Text en © 2012 Drastichova et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Drastichova, Zdenka
Skrabalova, Jitka
Jedelsky, Petr
Neckar, Jan
Kolar, Frantisek
Novotny, Jiri
Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal
title Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal
title_full Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal
title_fullStr Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal
title_full_unstemmed Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal
title_short Global Changes in the Rat Heart Proteome Induced by Prolonged Morphine Treatment and Withdrawal
title_sort global changes in the rat heart proteome induced by prolonged morphine treatment and withdrawal
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3467212/
https://www.ncbi.nlm.nih.gov/pubmed/23056601
http://dx.doi.org/10.1371/journal.pone.0047167
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