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Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition

Background: Sclerostin was initially described as an inhibitor of the Wnt-β catenin bone-forming pathway, but it also exerts important effects on intermediate metabolism and body composition. Osteosarcopenia and altered body fat distribution are common findings in excessive drinkers. The role of scl...

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Autores principales: Martín González, Candelaria, Fernández Rodríguez, Camino María, Abreu González, Pedro, García Rodríguez, Alen, Alvisa Negrín, Julio César, Cabañas Perales, Elisa, González Navarrete, Lourdes, Vera Delgado, Víctor Eugenio, Ortega Toledo, Paula, González Reimers, Emilio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9268012/
https://www.ncbi.nlm.nih.gov/pubmed/35807755
http://dx.doi.org/10.3390/nu14132574
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author Martín González, Candelaria
Fernández Rodríguez, Camino María
Abreu González, Pedro
García Rodríguez, Alen
Alvisa Negrín, Julio César
Cabañas Perales, Elisa
González Navarrete, Lourdes
Vera Delgado, Víctor Eugenio
Ortega Toledo, Paula
González Reimers, Emilio
author_facet Martín González, Candelaria
Fernández Rodríguez, Camino María
Abreu González, Pedro
García Rodríguez, Alen
Alvisa Negrín, Julio César
Cabañas Perales, Elisa
González Navarrete, Lourdes
Vera Delgado, Víctor Eugenio
Ortega Toledo, Paula
González Reimers, Emilio
author_sort Martín González, Candelaria
collection PubMed
description Background: Sclerostin was initially described as an inhibitor of the Wnt-β catenin bone-forming pathway, but it also exerts important effects on intermediate metabolism and body composition. Osteosarcopenia and altered body fat distribution are common findings in excessive drinkers. The role of sclerostin in these patients is uncertain. We aim to analyze the behavior of sclerostin in excessive drinkers and its relationships with body composition (fat mass, lean mass, bone mass), handgrip strength, body mass index (BMI), liver function and ethanol intake. Methods: 107 male active heavy drinkers and 26 age-matched controls were included. Serum sclerostin was determined by ELISA. Body composition analysis was performed by double X-ray absorptiometry. Handgrip strength was recorded using a dynamometer. Liver function was assessed according to Child’s classification. Results: Sclerostin was higher among Child’s C patients, keeping a relationship with deranged liver function. Obesity, defined according to BMI, and body fat were strongly related to sclerostin, being independent of serum creatinine and of liver function. The relationship of sclerostin with total hip bone mineral density was displaced by BMI. Conclusion: Deranged liver function is associated with higher sclerostin levels in alcoholics. Raised sclerostin levels are related to fat deposition and increased BMI.
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spelling pubmed-92680122022-07-09 Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition Martín González, Candelaria Fernández Rodríguez, Camino María Abreu González, Pedro García Rodríguez, Alen Alvisa Negrín, Julio César Cabañas Perales, Elisa González Navarrete, Lourdes Vera Delgado, Víctor Eugenio Ortega Toledo, Paula González Reimers, Emilio Nutrients Article Background: Sclerostin was initially described as an inhibitor of the Wnt-β catenin bone-forming pathway, but it also exerts important effects on intermediate metabolism and body composition. Osteosarcopenia and altered body fat distribution are common findings in excessive drinkers. The role of sclerostin in these patients is uncertain. We aim to analyze the behavior of sclerostin in excessive drinkers and its relationships with body composition (fat mass, lean mass, bone mass), handgrip strength, body mass index (BMI), liver function and ethanol intake. Methods: 107 male active heavy drinkers and 26 age-matched controls were included. Serum sclerostin was determined by ELISA. Body composition analysis was performed by double X-ray absorptiometry. Handgrip strength was recorded using a dynamometer. Liver function was assessed according to Child’s classification. Results: Sclerostin was higher among Child’s C patients, keeping a relationship with deranged liver function. Obesity, defined according to BMI, and body fat were strongly related to sclerostin, being independent of serum creatinine and of liver function. The relationship of sclerostin with total hip bone mineral density was displaced by BMI. Conclusion: Deranged liver function is associated with higher sclerostin levels in alcoholics. Raised sclerostin levels are related to fat deposition and increased BMI. MDPI 2022-06-22 /pmc/articles/PMC9268012/ /pubmed/35807755 http://dx.doi.org/10.3390/nu14132574 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
Martín González, Candelaria
Fernández Rodríguez, Camino María
Abreu González, Pedro
García Rodríguez, Alen
Alvisa Negrín, Julio César
Cabañas Perales, Elisa
González Navarrete, Lourdes
Vera Delgado, Víctor Eugenio
Ortega Toledo, Paula
González Reimers, Emilio
Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition
title Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition
title_full Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition
title_fullStr Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition
title_full_unstemmed Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition
title_short Sclerostin in Excessive Drinkers: Relationships with Liver Function and Body Composition
title_sort sclerostin in excessive drinkers: relationships with liver function and body composition
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9268012/
https://www.ncbi.nlm.nih.gov/pubmed/35807755
http://dx.doi.org/10.3390/nu14132574
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