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Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis

Glutamine supplementation in specific groups of critically ill patients results in favourable clinical outcome. Enhancement of citrulline and arginine synthesis by glutamine could serve as a potential mechanism. However, while receiving optimal enteral nutrition, uptake and enteral metabolism of glu...

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Autores principales: Vermeulen, Mechteld A. R., Brinkmann, Saskia J. H., Buijs, Nikki, Beishuizen, Albertus, Bet, Pierre M., Houdijk, Alexander P. J., van Goudoever, Johannes B., van Leeuwen, Paul A. M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4855021/
https://www.ncbi.nlm.nih.gov/pubmed/27200186
http://dx.doi.org/10.1155/2016/1373060
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author Vermeulen, Mechteld A. R.
Brinkmann, Saskia J. H.
Buijs, Nikki
Beishuizen, Albertus
Bet, Pierre M.
Houdijk, Alexander P. J.
van Goudoever, Johannes B.
van Leeuwen, Paul A. M.
author_facet Vermeulen, Mechteld A. R.
Brinkmann, Saskia J. H.
Buijs, Nikki
Beishuizen, Albertus
Bet, Pierre M.
Houdijk, Alexander P. J.
van Goudoever, Johannes B.
van Leeuwen, Paul A. M.
author_sort Vermeulen, Mechteld A. R.
collection PubMed
description Glutamine supplementation in specific groups of critically ill patients results in favourable clinical outcome. Enhancement of citrulline and arginine synthesis by glutamine could serve as a potential mechanism. However, while receiving optimal enteral nutrition, uptake and enteral metabolism of glutamine in critically ill patients remain unknown. Therefore we investigated the effect of a therapeutically relevant dose of L-glutamine on synthesis of L-citrulline and subsequent L-arginine in this group. Ten versus ten critically ill patients receiving full enteral nutrition, or isocaloric isonitrogenous enteral nutrition including 0.5 g/kg L-alanyl-L-glutamine, were studied using stable isotopes. A cross-over design using intravenous and enteral tracers enabled splanchnic extraction (SE) calculations. Endogenous rate of appearance and SE of glutamine citrulline and arginine was not different (SE controls versus alanyl-glutamine: glutamine 48 and 48%, citrulline 33 versus 45%, and arginine 45 versus 42%). Turnover from glutamine to citrulline and arginine was not higher in glutamine-administered patients. In critically ill nonseptic patients receiving adequate nutrition and a relevant dose of glutamine there was no extra citrulline or arginine synthesis and glutamine SE was not increased. This suggests that for arginine synthesis enhancement there is no need for an additional dose of glutamine when this population is adequately fed. This trial is registered with NTR2285.
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spelling pubmed-48550212016-05-19 Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis Vermeulen, Mechteld A. R. Brinkmann, Saskia J. H. Buijs, Nikki Beishuizen, Albertus Bet, Pierre M. Houdijk, Alexander P. J. van Goudoever, Johannes B. van Leeuwen, Paul A. M. J Nutr Metab Clinical Study Glutamine supplementation in specific groups of critically ill patients results in favourable clinical outcome. Enhancement of citrulline and arginine synthesis by glutamine could serve as a potential mechanism. However, while receiving optimal enteral nutrition, uptake and enteral metabolism of glutamine in critically ill patients remain unknown. Therefore we investigated the effect of a therapeutically relevant dose of L-glutamine on synthesis of L-citrulline and subsequent L-arginine in this group. Ten versus ten critically ill patients receiving full enteral nutrition, or isocaloric isonitrogenous enteral nutrition including 0.5 g/kg L-alanyl-L-glutamine, were studied using stable isotopes. A cross-over design using intravenous and enteral tracers enabled splanchnic extraction (SE) calculations. Endogenous rate of appearance and SE of glutamine citrulline and arginine was not different (SE controls versus alanyl-glutamine: glutamine 48 and 48%, citrulline 33 versus 45%, and arginine 45 versus 42%). Turnover from glutamine to citrulline and arginine was not higher in glutamine-administered patients. In critically ill nonseptic patients receiving adequate nutrition and a relevant dose of glutamine there was no extra citrulline or arginine synthesis and glutamine SE was not increased. This suggests that for arginine synthesis enhancement there is no need for an additional dose of glutamine when this population is adequately fed. This trial is registered with NTR2285. Hindawi Publishing Corporation 2016 2016-04-20 /pmc/articles/PMC4855021/ /pubmed/27200186 http://dx.doi.org/10.1155/2016/1373060 Text en Copyright © 2016 Mechteld A. R. Vermeulen et al. https://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Clinical Study
Vermeulen, Mechteld A. R.
Brinkmann, Saskia J. H.
Buijs, Nikki
Beishuizen, Albertus
Bet, Pierre M.
Houdijk, Alexander P. J.
van Goudoever, Johannes B.
van Leeuwen, Paul A. M.
Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis
title Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis
title_full Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis
title_fullStr Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis
title_full_unstemmed Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis
title_short Enteral Glutamine Administration in Critically Ill Nonseptic Patients Does Not Trigger Arginine Synthesis
title_sort enteral glutamine administration in critically ill nonseptic patients does not trigger arginine synthesis
topic Clinical Study
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4855021/
https://www.ncbi.nlm.nih.gov/pubmed/27200186
http://dx.doi.org/10.1155/2016/1373060
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