Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats

Nonsteroidal anti-inflammatory drugs (NSAIDs) can produce adverse effects by inhibiting prostaglandin (PG) synthesis. A PGE(1) analogue, misoprostol, is often utilized to alleviate NSAID-related gastrointestinal side effects. This study examined the effect of misoprostol on celecoxib renal toxicity....

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Autores principales: Cooper, Dustin L., Murrell, Derek E., Conder, Christopher M., Palau, Victoria E., Campbell, Grace E., Lynch, Shaun P., Denham, James W., Hanley, Angela V., Bullins, Kenny W., Panus, Peter C., Singh, Krishna, Harirforoosh, Sam
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3931696/
https://www.ncbi.nlm.nih.gov/pubmed/24586517
http://dx.doi.org/10.1371/journal.pone.0089087
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author Cooper, Dustin L.
Murrell, Derek E.
Conder, Christopher M.
Palau, Victoria E.
Campbell, Grace E.
Lynch, Shaun P.
Denham, James W.
Hanley, Angela V.
Bullins, Kenny W.
Panus, Peter C.
Singh, Krishna
Harirforoosh, Sam
author_facet Cooper, Dustin L.
Murrell, Derek E.
Conder, Christopher M.
Palau, Victoria E.
Campbell, Grace E.
Lynch, Shaun P.
Denham, James W.
Hanley, Angela V.
Bullins, Kenny W.
Panus, Peter C.
Singh, Krishna
Harirforoosh, Sam
author_sort Cooper, Dustin L.
collection PubMed
description Nonsteroidal anti-inflammatory drugs (NSAIDs) can produce adverse effects by inhibiting prostaglandin (PG) synthesis. A PGE(1) analogue, misoprostol, is often utilized to alleviate NSAID-related gastrointestinal side effects. This study examined the effect of misoprostol on celecoxib renal toxicity. Additionally, the effects of these drugs on cardiovascular parameters were evaluated. Four randomized rat groups were orally gavaged for 9 days, two groups receiving vehicle and two groups receiving misoprostol (100 µg/kg) twice daily. Celecoxib (40 mg/kg) was co-administered once daily to one vehicle and one misoprostol group from days 3 to 9. Urine and blood samples were collected and blood pressure parameters were measured during the study period. Hearts and kidneys were harvested on final day. Day 2 urinary electrolyte samples revealed significant reductions in sodium excretion in misoprostol (0.12±0.05 µmol/min/100 g) and misoprostol+celecoxib groups (0.07±0.02 µmol/min/100 g). At day 3, all treatment groups showed significantly reduced sodium excretion. Potassium excretion diminished significantly in vehicle+celecoxib and misoprostol+celecoxib groups from day 3 onward. Urinary kidney injury molecule-1 levels were significantly increased in vehicle+celecoxib (0.65±0.02 vs. 0.35±0.07 ng/mL, p = 0.0002) and misoprostol+celecoxib (0.61±0.06 vs. 0.37±0.06 ng/mL, p = 0.0015) groups when compared to baseline; while plasma levels of cardiac troponin I increased significantly in vehicle+celecoxib (p = 0.0040) and misoprostol+misoprostol (p = 0.0078) groups when compared to vehicle+vehicle. Blood pressure parameters increased significantly in all misoprostol treated groups. Significant elevation in diastolic (p = 0.0071) and mean blood pressure (p = 0.0153) was noted in misoprostol+celecoxib compared to vehicle+celecoxib. All treatments produced significant tubular dilatation/necrosis compared to control. No significant myocardial changes were noticed; however, three animals presented with pericarditis. Kidney, heart, and plasma celecoxib levels revealed no significant change between vehicle+celecoxib and misoprostol+celecoxib. Concomitant misoprostol administration did not prevent celecoxib renal toxicity, and instead exacerbated renal side effects. Misoprostol did not alter plasma or tissue celecoxib concentrations suggesting no pharmacokinetic interaction between celecoxib and misoprostol.
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spelling pubmed-39316962014-02-25 Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats Cooper, Dustin L. Murrell, Derek E. Conder, Christopher M. Palau, Victoria E. Campbell, Grace E. Lynch, Shaun P. Denham, James W. Hanley, Angela V. Bullins, Kenny W. Panus, Peter C. Singh, Krishna Harirforoosh, Sam PLoS One Research Article Nonsteroidal anti-inflammatory drugs (NSAIDs) can produce adverse effects by inhibiting prostaglandin (PG) synthesis. A PGE(1) analogue, misoprostol, is often utilized to alleviate NSAID-related gastrointestinal side effects. This study examined the effect of misoprostol on celecoxib renal toxicity. Additionally, the effects of these drugs on cardiovascular parameters were evaluated. Four randomized rat groups were orally gavaged for 9 days, two groups receiving vehicle and two groups receiving misoprostol (100 µg/kg) twice daily. Celecoxib (40 mg/kg) was co-administered once daily to one vehicle and one misoprostol group from days 3 to 9. Urine and blood samples were collected and blood pressure parameters were measured during the study period. Hearts and kidneys were harvested on final day. Day 2 urinary electrolyte samples revealed significant reductions in sodium excretion in misoprostol (0.12±0.05 µmol/min/100 g) and misoprostol+celecoxib groups (0.07±0.02 µmol/min/100 g). At day 3, all treatment groups showed significantly reduced sodium excretion. Potassium excretion diminished significantly in vehicle+celecoxib and misoprostol+celecoxib groups from day 3 onward. Urinary kidney injury molecule-1 levels were significantly increased in vehicle+celecoxib (0.65±0.02 vs. 0.35±0.07 ng/mL, p = 0.0002) and misoprostol+celecoxib (0.61±0.06 vs. 0.37±0.06 ng/mL, p = 0.0015) groups when compared to baseline; while plasma levels of cardiac troponin I increased significantly in vehicle+celecoxib (p = 0.0040) and misoprostol+misoprostol (p = 0.0078) groups when compared to vehicle+vehicle. Blood pressure parameters increased significantly in all misoprostol treated groups. Significant elevation in diastolic (p = 0.0071) and mean blood pressure (p = 0.0153) was noted in misoprostol+celecoxib compared to vehicle+celecoxib. All treatments produced significant tubular dilatation/necrosis compared to control. No significant myocardial changes were noticed; however, three animals presented with pericarditis. Kidney, heart, and plasma celecoxib levels revealed no significant change between vehicle+celecoxib and misoprostol+celecoxib. Concomitant misoprostol administration did not prevent celecoxib renal toxicity, and instead exacerbated renal side effects. Misoprostol did not alter plasma or tissue celecoxib concentrations suggesting no pharmacokinetic interaction between celecoxib and misoprostol. Public Library of Science 2014-02-21 /pmc/articles/PMC3931696/ /pubmed/24586517 http://dx.doi.org/10.1371/journal.pone.0089087 Text en © 2014 Cooper 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
Cooper, Dustin L.
Murrell, Derek E.
Conder, Christopher M.
Palau, Victoria E.
Campbell, Grace E.
Lynch, Shaun P.
Denham, James W.
Hanley, Angela V.
Bullins, Kenny W.
Panus, Peter C.
Singh, Krishna
Harirforoosh, Sam
Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats
title Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats
title_full Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats
title_fullStr Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats
title_full_unstemmed Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats
title_short Exacerbation of Celecoxib-Induced Renal Injury by Concomitant Administration of Misoprostol in Rats
title_sort exacerbation of celecoxib-induced renal injury by concomitant administration of misoprostol in rats
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3931696/
https://www.ncbi.nlm.nih.gov/pubmed/24586517
http://dx.doi.org/10.1371/journal.pone.0089087
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