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Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats

Cancer cachexia occurs in up to 85% of advanced cancer patients, affecting different tissues and organs, mainly the liver, which plays a central role in body metabolism control. However, liver responses to cancer cachexia progression are still poorly understood. Considering the possible different ch...

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Autores principales: Miyaguti, Natália Angelo da Silva, Chiocchetti, Gabriela de Matuoka e, Salgado, Carla de Moraes, Lopes-Aguiar, Leisa, Viana, Lais Rosa, Blanchard, Lea, dos Santos, Rogério Willians, Gomes-Marcondes, Maria Cristina Cintra
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8705353/
https://www.ncbi.nlm.nih.gov/pubmed/34940589
http://dx.doi.org/10.3390/metabo11120831
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author Miyaguti, Natália Angelo da Silva
Chiocchetti, Gabriela de Matuoka e
Salgado, Carla de Moraes
Lopes-Aguiar, Leisa
Viana, Lais Rosa
Blanchard, Lea
dos Santos, Rogério Willians
Gomes-Marcondes, Maria Cristina Cintra
author_facet Miyaguti, Natália Angelo da Silva
Chiocchetti, Gabriela de Matuoka e
Salgado, Carla de Moraes
Lopes-Aguiar, Leisa
Viana, Lais Rosa
Blanchard, Lea
dos Santos, Rogério Willians
Gomes-Marcondes, Maria Cristina Cintra
author_sort Miyaguti, Natália Angelo da Silva
collection PubMed
description Cancer cachexia occurs in up to 85% of advanced cancer patients, affecting different tissues and organs, mainly the liver, which plays a central role in body metabolism control. However, liver responses to cancer cachexia progression are still poorly understood. Considering the possible different challenges provided by the rodent’s phase of life and the cachexia progression, we evaluated the liver metabolic alterations affected by Walker-256 tumour growth in weanling and young-adult rats. For this, we applied a metabolomics approach associated with protein and gene expression analyses. Higher amino acid levels and impaired glucose metabolism were important features in tumour-bearing animals’ liver tissue. The weanling hosts had more pronounced cachexia, with higher carcass spoliation, liver lipid metabolism and impaired CII and CIV mitochondrial complexes. The liver alterations in young adult tumour-bearing rats were related to energy status and nucleotide metabolites, such as uridine, NAD+, xanthosine, hypoxanthine and inosine. In conclusion, the Walker-256 tumour-induced cachexia impaired liver metabolism, being more severe in the weanling hosts. Further studies are needed to correlate these changes in the preclinical model, which can be correlated to the clinical features of cancer cachexia, allowing for a translational potential involving the liver function and its responses to potential treatments.
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spelling pubmed-87053532021-12-25 Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats Miyaguti, Natália Angelo da Silva Chiocchetti, Gabriela de Matuoka e Salgado, Carla de Moraes Lopes-Aguiar, Leisa Viana, Lais Rosa Blanchard, Lea dos Santos, Rogério Willians Gomes-Marcondes, Maria Cristina Cintra Metabolites Article Cancer cachexia occurs in up to 85% of advanced cancer patients, affecting different tissues and organs, mainly the liver, which plays a central role in body metabolism control. However, liver responses to cancer cachexia progression are still poorly understood. Considering the possible different challenges provided by the rodent’s phase of life and the cachexia progression, we evaluated the liver metabolic alterations affected by Walker-256 tumour growth in weanling and young-adult rats. For this, we applied a metabolomics approach associated with protein and gene expression analyses. Higher amino acid levels and impaired glucose metabolism were important features in tumour-bearing animals’ liver tissue. The weanling hosts had more pronounced cachexia, with higher carcass spoliation, liver lipid metabolism and impaired CII and CIV mitochondrial complexes. The liver alterations in young adult tumour-bearing rats were related to energy status and nucleotide metabolites, such as uridine, NAD+, xanthosine, hypoxanthine and inosine. In conclusion, the Walker-256 tumour-induced cachexia impaired liver metabolism, being more severe in the weanling hosts. Further studies are needed to correlate these changes in the preclinical model, which can be correlated to the clinical features of cancer cachexia, allowing for a translational potential involving the liver function and its responses to potential treatments. MDPI 2021-12-01 /pmc/articles/PMC8705353/ /pubmed/34940589 http://dx.doi.org/10.3390/metabo11120831 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Miyaguti, Natália Angelo da Silva
Chiocchetti, Gabriela de Matuoka e
Salgado, Carla de Moraes
Lopes-Aguiar, Leisa
Viana, Lais Rosa
Blanchard, Lea
dos Santos, Rogério Willians
Gomes-Marcondes, Maria Cristina Cintra
Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats
title Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats
title_full Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats
title_fullStr Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats
title_full_unstemmed Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats
title_short Walker-256 Tumour-Induced Cachexia Altered Liver Metabolomic Profile and Function in Weanling and Adult Rats
title_sort walker-256 tumour-induced cachexia altered liver metabolomic profile and function in weanling and adult rats
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8705353/
https://www.ncbi.nlm.nih.gov/pubmed/34940589
http://dx.doi.org/10.3390/metabo11120831
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