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Leucine and Protein Metabolism in Obese Zucker Rats

Branched-chain amino acids (BCAAs) are circulating nutrient signals for protein accretion, however, they increase in obesity and elevations appear to be prognostic of diabetes. To understand the mechanisms whereby obesity affects BCAAs and protein metabolism, we employed metabolomics and measured ra...

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Autores principales: She, Pengxiang, Olson, Kristine C., Kadota, Yoshihiro, Inukai, Ayami, Shimomura, Yoshiharu, Hoppel, Charles L., Adams, Sean H., Kawamata, Yasuko, Matsumoto, Hideki, Sakai, Ryosei, Lang, Charles H., Lynch, Christopher J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3603883/
https://www.ncbi.nlm.nih.gov/pubmed/23527196
http://dx.doi.org/10.1371/journal.pone.0059443
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author She, Pengxiang
Olson, Kristine C.
Kadota, Yoshihiro
Inukai, Ayami
Shimomura, Yoshiharu
Hoppel, Charles L.
Adams, Sean H.
Kawamata, Yasuko
Matsumoto, Hideki
Sakai, Ryosei
Lang, Charles H.
Lynch, Christopher J.
author_facet She, Pengxiang
Olson, Kristine C.
Kadota, Yoshihiro
Inukai, Ayami
Shimomura, Yoshiharu
Hoppel, Charles L.
Adams, Sean H.
Kawamata, Yasuko
Matsumoto, Hideki
Sakai, Ryosei
Lang, Charles H.
Lynch, Christopher J.
author_sort She, Pengxiang
collection PubMed
description Branched-chain amino acids (BCAAs) are circulating nutrient signals for protein accretion, however, they increase in obesity and elevations appear to be prognostic of diabetes. To understand the mechanisms whereby obesity affects BCAAs and protein metabolism, we employed metabolomics and measured rates of [1-(14)C]-leucine metabolism, tissue-specific protein synthesis and branched-chain keto-acid (BCKA) dehydrogenase complex (BCKDC) activities. Male obese Zucker rats (11-weeks old) had increased body weight (BW, 53%), liver (107%) and fat (∼300%), but lower plantaris and gastrocnemius masses (−21–24%). Plasma BCAAs and BCKAs were elevated 45–69% and ∼100%, respectively, in obese rats. Processes facilitating these rises appeared to include increased dietary intake (23%), leucine (Leu) turnover and proteolysis [35% per g fat free mass (FFM), urinary markers of proteolysis: 3-methylhistidine (183%) and 4-hydroxyproline (766%)] and decreased BCKDC per g kidney, heart, gastrocnemius and liver (−47–66%). A process disposing of circulating BCAAs, protein synthesis, was increased 23–29% by obesity in whole-body (FFM corrected), gastrocnemius and liver. Despite the observed decreases in BCKDC activities per gm tissue, rates of whole-body Leu oxidation in obese rats were 22% and 59% higher normalized to BW and FFM, respectively. Consistently, urinary concentrations of eight BCAA catabolism-derived acylcarnitines were also elevated. The unexpected increase in BCAA oxidation may be due to a substrate effect in liver. Supporting this idea, BCKAs were elevated more in liver (193–418%) than plasma or muscle, and per g losses of hepatic BCKDC activities were completely offset by increased liver mass, in contrast to other tissues. In summary, our results indicate that plasma BCKAs may represent a more sensitive metabolic signature for obesity than BCAAs. Processes supporting elevated BCAA]BCKAs in the obese Zucker rat include increased dietary intake, Leu and protein turnover along with impaired BCKDC activity. Elevated BCAAs/BCKAs may contribute to observed elevations in protein synthesis and BCAA oxidation.
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spelling pubmed-36038832013-03-22 Leucine and Protein Metabolism in Obese Zucker Rats She, Pengxiang Olson, Kristine C. Kadota, Yoshihiro Inukai, Ayami Shimomura, Yoshiharu Hoppel, Charles L. Adams, Sean H. Kawamata, Yasuko Matsumoto, Hideki Sakai, Ryosei Lang, Charles H. Lynch, Christopher J. PLoS One Research Article Branched-chain amino acids (BCAAs) are circulating nutrient signals for protein accretion, however, they increase in obesity and elevations appear to be prognostic of diabetes. To understand the mechanisms whereby obesity affects BCAAs and protein metabolism, we employed metabolomics and measured rates of [1-(14)C]-leucine metabolism, tissue-specific protein synthesis and branched-chain keto-acid (BCKA) dehydrogenase complex (BCKDC) activities. Male obese Zucker rats (11-weeks old) had increased body weight (BW, 53%), liver (107%) and fat (∼300%), but lower plantaris and gastrocnemius masses (−21–24%). Plasma BCAAs and BCKAs were elevated 45–69% and ∼100%, respectively, in obese rats. Processes facilitating these rises appeared to include increased dietary intake (23%), leucine (Leu) turnover and proteolysis [35% per g fat free mass (FFM), urinary markers of proteolysis: 3-methylhistidine (183%) and 4-hydroxyproline (766%)] and decreased BCKDC per g kidney, heart, gastrocnemius and liver (−47–66%). A process disposing of circulating BCAAs, protein synthesis, was increased 23–29% by obesity in whole-body (FFM corrected), gastrocnemius and liver. Despite the observed decreases in BCKDC activities per gm tissue, rates of whole-body Leu oxidation in obese rats were 22% and 59% higher normalized to BW and FFM, respectively. Consistently, urinary concentrations of eight BCAA catabolism-derived acylcarnitines were also elevated. The unexpected increase in BCAA oxidation may be due to a substrate effect in liver. Supporting this idea, BCKAs were elevated more in liver (193–418%) than plasma or muscle, and per g losses of hepatic BCKDC activities were completely offset by increased liver mass, in contrast to other tissues. In summary, our results indicate that plasma BCKAs may represent a more sensitive metabolic signature for obesity than BCAAs. Processes supporting elevated BCAA]BCKAs in the obese Zucker rat include increased dietary intake, Leu and protein turnover along with impaired BCKDC activity. Elevated BCAAs/BCKAs may contribute to observed elevations in protein synthesis and BCAA oxidation. Public Library of Science 2013-03-20 /pmc/articles/PMC3603883/ /pubmed/23527196 http://dx.doi.org/10.1371/journal.pone.0059443 Text en © 2013 She 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
She, Pengxiang
Olson, Kristine C.
Kadota, Yoshihiro
Inukai, Ayami
Shimomura, Yoshiharu
Hoppel, Charles L.
Adams, Sean H.
Kawamata, Yasuko
Matsumoto, Hideki
Sakai, Ryosei
Lang, Charles H.
Lynch, Christopher J.
Leucine and Protein Metabolism in Obese Zucker Rats
title Leucine and Protein Metabolism in Obese Zucker Rats
title_full Leucine and Protein Metabolism in Obese Zucker Rats
title_fullStr Leucine and Protein Metabolism in Obese Zucker Rats
title_full_unstemmed Leucine and Protein Metabolism in Obese Zucker Rats
title_short Leucine and Protein Metabolism in Obese Zucker Rats
title_sort leucine and protein metabolism in obese zucker rats
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3603883/
https://www.ncbi.nlm.nih.gov/pubmed/23527196
http://dx.doi.org/10.1371/journal.pone.0059443
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