Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling

BACKGROUND: Glucocorticoids, such as prednisolone, are widely used anti-inflammatory drugs, but therapy is hampered by a broad range of metabolic side effects including skeletal muscle wasting and insulin resistance. Therefore, development of improved synthetic glucocorticoids that display similar e...

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Autores principales: Ellero-Simatos, Sandrine, Szymańska, Ewa, Rullmann, Ton, Dokter, Wim HA, Ramaker, Raymond, Berger, Ruud, van Iersel, Thijs MP, Smilde, Age K, Hankemeier, Thomas, Alkema, Wynand
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4064315/
https://www.ncbi.nlm.nih.gov/pubmed/23199229
http://dx.doi.org/10.1186/gm395
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author Ellero-Simatos, Sandrine
Szymańska, Ewa
Rullmann, Ton
Dokter, Wim HA
Ramaker, Raymond
Berger, Ruud
van Iersel, Thijs MP
Smilde, Age K
Hankemeier, Thomas
Alkema, Wynand
author_facet Ellero-Simatos, Sandrine
Szymańska, Ewa
Rullmann, Ton
Dokter, Wim HA
Ramaker, Raymond
Berger, Ruud
van Iersel, Thijs MP
Smilde, Age K
Hankemeier, Thomas
Alkema, Wynand
author_sort Ellero-Simatos, Sandrine
collection PubMed
description BACKGROUND: Glucocorticoids, such as prednisolone, are widely used anti-inflammatory drugs, but therapy is hampered by a broad range of metabolic side effects including skeletal muscle wasting and insulin resistance. Therefore, development of improved synthetic glucocorticoids that display similar efficacy as prednisolone but reduced side effects is an active research area. For efficient development of such new drugs, in vivo biomarkers, which can predict glucocorticoid metabolic side effects in an early stage, are needed. In this study, we aim to provide the first description of the metabolic perturbations induced by acute and therapeutic treatments with prednisolone in humans using urine metabolomics, and to derive potential biomarkers for prednisolone-induced metabolic effects. METHODS: A randomized, double blind, placebo-controlled trial consisting of two protocols was conducted in healthy men. In protocol 1, volunteers received placebo (n = 11) or prednisolone (7.5 mg (n = 11), 15 mg (n = 13) or 30 mg (n = 12)) orally once daily for 15 days. In protocol 2, volunteers (n = 6) received placebo at day 0 and 75 mg prednisolone at day 1. We collected 24 h urine and serum samples at baseline (day 0), after a single dose (day 1) and after prolonged treatment (day 15) and obtained mass-spectrometry-based urine and serum metabolic profiles. RESULTS: At day 1, high-dose prednisolone treatment increased levels of 13 and 10 proteinogenic amino acids in urine and serum respectively, as well as levels of 3-methylhistidine, providing evidence for an early manifestation of glucocorticoid-induced muscle wasting. Prednisolone treatment also strongly increased urinary carnitine derivatives at day 1 but not at day 15, which might reflect adaptive mechanisms under prolonged treatment. Finally, urinary levels of proteinogenic amino acids at day 1 and of N-methylnicotinamide at day 15 significantly correlated with the homeostatic model assessment of insulin resistance and might represent biomarkers for prednisolone-induced insulin resistance. CONCLUSION: This study provides evidence that urinary metabolomics represents a noninvasive way of monitoring the effect of glucocorticoids on muscle protein catabolism after a single dose and can derive new biomarkers of glucocorticoid-induced insulin resistance. It might, therefore, help the development of improved synthetic glucocorticoids. TRIAL REGISTRATION: ClinicalTrials.gov NCT00971724
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spelling pubmed-40643152014-06-21 Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling Ellero-Simatos, Sandrine Szymańska, Ewa Rullmann, Ton Dokter, Wim HA Ramaker, Raymond Berger, Ruud van Iersel, Thijs MP Smilde, Age K Hankemeier, Thomas Alkema, Wynand Genome Med Research BACKGROUND: Glucocorticoids, such as prednisolone, are widely used anti-inflammatory drugs, but therapy is hampered by a broad range of metabolic side effects including skeletal muscle wasting and insulin resistance. Therefore, development of improved synthetic glucocorticoids that display similar efficacy as prednisolone but reduced side effects is an active research area. For efficient development of such new drugs, in vivo biomarkers, which can predict glucocorticoid metabolic side effects in an early stage, are needed. In this study, we aim to provide the first description of the metabolic perturbations induced by acute and therapeutic treatments with prednisolone in humans using urine metabolomics, and to derive potential biomarkers for prednisolone-induced metabolic effects. METHODS: A randomized, double blind, placebo-controlled trial consisting of two protocols was conducted in healthy men. In protocol 1, volunteers received placebo (n = 11) or prednisolone (7.5 mg (n = 11), 15 mg (n = 13) or 30 mg (n = 12)) orally once daily for 15 days. In protocol 2, volunteers (n = 6) received placebo at day 0 and 75 mg prednisolone at day 1. We collected 24 h urine and serum samples at baseline (day 0), after a single dose (day 1) and after prolonged treatment (day 15) and obtained mass-spectrometry-based urine and serum metabolic profiles. RESULTS: At day 1, high-dose prednisolone treatment increased levels of 13 and 10 proteinogenic amino acids in urine and serum respectively, as well as levels of 3-methylhistidine, providing evidence for an early manifestation of glucocorticoid-induced muscle wasting. Prednisolone treatment also strongly increased urinary carnitine derivatives at day 1 but not at day 15, which might reflect adaptive mechanisms under prolonged treatment. Finally, urinary levels of proteinogenic amino acids at day 1 and of N-methylnicotinamide at day 15 significantly correlated with the homeostatic model assessment of insulin resistance and might represent biomarkers for prednisolone-induced insulin resistance. CONCLUSION: This study provides evidence that urinary metabolomics represents a noninvasive way of monitoring the effect of glucocorticoids on muscle protein catabolism after a single dose and can derive new biomarkers of glucocorticoid-induced insulin resistance. It might, therefore, help the development of improved synthetic glucocorticoids. TRIAL REGISTRATION: ClinicalTrials.gov NCT00971724 BioMed Central 2012-11-30 /pmc/articles/PMC4064315/ /pubmed/23199229 http://dx.doi.org/10.1186/gm395 Text en Copyright © 2013 Ellero-Simatos 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
Ellero-Simatos, Sandrine
Szymańska, Ewa
Rullmann, Ton
Dokter, Wim HA
Ramaker, Raymond
Berger, Ruud
van Iersel, Thijs MP
Smilde, Age K
Hankemeier, Thomas
Alkema, Wynand
Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
title Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
title_full Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
title_fullStr Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
title_full_unstemmed Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
title_short Assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
title_sort assessing the metabolic effects of prednisolone in healthy volunteers using urine metabolic profiling
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4064315/
https://www.ncbi.nlm.nih.gov/pubmed/23199229
http://dx.doi.org/10.1186/gm395
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