Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance

Background: Obesity is characterized by adipose tissue dysregulation and predisposes individuals to insulin resistance and type 2 diabetes. At the molecular level, adipocyte dysfunction has been linked to obesity-triggered oxidative stress and protein carbonylation, considering protein carbonylation...

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Autores principales: Navarro-Ruiz, M. Carmen, Soler-Vázquez, M. Carmen, Díaz-Ruiz, Alberto, Peinado, Juan R., Nieto Calonge, Andrea, Sánchez-Ceinos, Julia, Tercero-Alcázar, Carmen, López-Alcalá, Jaime, Rangel-Zuñiga, Oriol A., Membrives, Antonio, López-Miranda, José, Malagón, María M., Guzmán-Ruiz, Rocío
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9775537/
https://www.ncbi.nlm.nih.gov/pubmed/36551793
http://dx.doi.org/10.3390/biomedicines10123032
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author Navarro-Ruiz, M. Carmen
Soler-Vázquez, M. Carmen
Díaz-Ruiz, Alberto
Peinado, Juan R.
Nieto Calonge, Andrea
Sánchez-Ceinos, Julia
Tercero-Alcázar, Carmen
López-Alcalá, Jaime
Rangel-Zuñiga, Oriol A.
Membrives, Antonio
López-Miranda, José
Malagón, María M.
Guzmán-Ruiz, Rocío
author_facet Navarro-Ruiz, M. Carmen
Soler-Vázquez, M. Carmen
Díaz-Ruiz, Alberto
Peinado, Juan R.
Nieto Calonge, Andrea
Sánchez-Ceinos, Julia
Tercero-Alcázar, Carmen
López-Alcalá, Jaime
Rangel-Zuñiga, Oriol A.
Membrives, Antonio
López-Miranda, José
Malagón, María M.
Guzmán-Ruiz, Rocío
author_sort Navarro-Ruiz, M. Carmen
collection PubMed
description Background: Obesity is characterized by adipose tissue dysregulation and predisposes individuals to insulin resistance and type 2 diabetes. At the molecular level, adipocyte dysfunction has been linked to obesity-triggered oxidative stress and protein carbonylation, considering protein carbonylation as a link between oxidative stress and metabolic dysfunction. The identification of specific carbonylated proteins in adipose tissue could provide novel biomarkers of oxidative damage related to metabolic status (i.e prediabetes). Thus, we aimed at characterizing the subcutaneous and omental human adipose tissue carbonylome in obesity-associated insulin resistance. Methods: 2D-PAGE was used to identify carbonylated proteins, and clinical correlations studies and molecular biology approaches including intracellular trafficking, reactive oxygen species assay, and iron content were performed using in vitro models of insulin resistance. Results: The carbonylome of human adipose tissue included common (serotransferrin, vimentin, actin, and annexin A2) and depot-specific (carbonic anhydrase and α-crystallin B in the subcutaneous depot; and α-1-antitrypsin and tubulin in the omental depot) differences that point out the complexity of oxidative stress at the metabolic level, highlighting changes in carbonylated transferrin expression. Posterior studies using in vitro prediabetic model evidence alteration in transferrin receptor translocation, linked to the prediabetic environment. Finally, ligand-receptor molecular docking studies showed a reduced affinity for carbonylated transferrin binding to its receptor compared to wild-type transferrin, emphasizing the role of transferrin carbonylation in the link between oxidative stress and metabolic dysfunction. Conclusions: The adipose tissue carbonylome contributes to understanding the molecular mechanism driving adipocyte dysfunction and identifies possible adipose tissue carbonylated targets in obesity-associated insulin resistance.
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spelling pubmed-97755372022-12-23 Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance Navarro-Ruiz, M. Carmen Soler-Vázquez, M. Carmen Díaz-Ruiz, Alberto Peinado, Juan R. Nieto Calonge, Andrea Sánchez-Ceinos, Julia Tercero-Alcázar, Carmen López-Alcalá, Jaime Rangel-Zuñiga, Oriol A. Membrives, Antonio López-Miranda, José Malagón, María M. Guzmán-Ruiz, Rocío Biomedicines Article Background: Obesity is characterized by adipose tissue dysregulation and predisposes individuals to insulin resistance and type 2 diabetes. At the molecular level, adipocyte dysfunction has been linked to obesity-triggered oxidative stress and protein carbonylation, considering protein carbonylation as a link between oxidative stress and metabolic dysfunction. The identification of specific carbonylated proteins in adipose tissue could provide novel biomarkers of oxidative damage related to metabolic status (i.e prediabetes). Thus, we aimed at characterizing the subcutaneous and omental human adipose tissue carbonylome in obesity-associated insulin resistance. Methods: 2D-PAGE was used to identify carbonylated proteins, and clinical correlations studies and molecular biology approaches including intracellular trafficking, reactive oxygen species assay, and iron content were performed using in vitro models of insulin resistance. Results: The carbonylome of human adipose tissue included common (serotransferrin, vimentin, actin, and annexin A2) and depot-specific (carbonic anhydrase and α-crystallin B in the subcutaneous depot; and α-1-antitrypsin and tubulin in the omental depot) differences that point out the complexity of oxidative stress at the metabolic level, highlighting changes in carbonylated transferrin expression. Posterior studies using in vitro prediabetic model evidence alteration in transferrin receptor translocation, linked to the prediabetic environment. Finally, ligand-receptor molecular docking studies showed a reduced affinity for carbonylated transferrin binding to its receptor compared to wild-type transferrin, emphasizing the role of transferrin carbonylation in the link between oxidative stress and metabolic dysfunction. Conclusions: The adipose tissue carbonylome contributes to understanding the molecular mechanism driving adipocyte dysfunction and identifies possible adipose tissue carbonylated targets in obesity-associated insulin resistance. MDPI 2022-11-24 /pmc/articles/PMC9775537/ /pubmed/36551793 http://dx.doi.org/10.3390/biomedicines10123032 Text en © 2022 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
Navarro-Ruiz, M. Carmen
Soler-Vázquez, M. Carmen
Díaz-Ruiz, Alberto
Peinado, Juan R.
Nieto Calonge, Andrea
Sánchez-Ceinos, Julia
Tercero-Alcázar, Carmen
López-Alcalá, Jaime
Rangel-Zuñiga, Oriol A.
Membrives, Antonio
López-Miranda, José
Malagón, María M.
Guzmán-Ruiz, Rocío
Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance
title Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance
title_full Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance
title_fullStr Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance
title_full_unstemmed Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance
title_short Influence of Protein Carbonylation on Human Adipose Tissue Dysfunction in Obesity and Insulin Resistance
title_sort influence of protein carbonylation on human adipose tissue dysfunction in obesity and insulin resistance
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9775537/
https://www.ncbi.nlm.nih.gov/pubmed/36551793
http://dx.doi.org/10.3390/biomedicines10123032
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