The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes

Recent studies in mice and humans demonstrated the relevance of H(2)S synthesising enzymes, such as CTH, CBS, and MPST, in the physiology of adipose tissue and the differentiation of preadipocyte into adipocytes. Here, our objective was to investigate the combined role of CTH, CBS, and MPST in the p...

Descripción completa

Detalles Bibliográficos
Autores principales: Latorre, Jessica, Aroca, Angeles, Fernández-Real, José Manuel, Romero, Luis C., Moreno-Navarrete, José María
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9220337/
https://www.ncbi.nlm.nih.gov/pubmed/35739994
http://dx.doi.org/10.3390/antiox11061095
_version_ 1784732348891267072
author Latorre, Jessica
Aroca, Angeles
Fernández-Real, José Manuel
Romero, Luis C.
Moreno-Navarrete, José María
author_facet Latorre, Jessica
Aroca, Angeles
Fernández-Real, José Manuel
Romero, Luis C.
Moreno-Navarrete, José María
author_sort Latorre, Jessica
collection PubMed
description Recent studies in mice and humans demonstrated the relevance of H(2)S synthesising enzymes, such as CTH, CBS, and MPST, in the physiology of adipose tissue and the differentiation of preadipocyte into adipocytes. Here, our objective was to investigate the combined role of CTH, CBS, and MPST in the preservation of adipocyte protein persulfidation and adipogenesis. Combined partial CTH, CBS, and MPST gene knockdown was achieved treating fully human adipocytes with siRNAs against these transcripts (siRNA_MIX). Adipocyte protein persulfidation was analyzed using label-free quantitative mass spectrometry coupled with a dimedone-switch method for protein labeling and purification. Proteomic analysis quantified 216 proteins with statistically different levels of persulfidation in KD cells compared to control adipocytes. In fully differentiated adipocytes, CBS and MPST mRNA and protein levels were abundant, while CTH expression was very low. It is noteworthy that siRNA_MIX administration resulted in a significant decrease in CBS and MPST expression, without impacting on CTH. The combined partial knockdown of the CBS and MPST genes resulted in reduced cellular sulfide levels in parallel to decreased expression of relevant genes for adipocyte biology, including adipogenesis, mitochondrial biogenesis, and lipogenesis, but increased proinflammatory- and senescence-related genes. It should be noted that the combined partial knockdown of CBS and MPST genes also led to a significant disruption in the persulfidation pattern of the adipocyte proteins. Although among the less persulfidated proteins, we identified several relevant proteins for adipocyte adipogenesis and function, among the most persulfidated, key mediators of adipocyte inflammation and dysfunction as well as some proteins that might play a positive role in adipogenesis were found. In conclusion, the current study indicates that the combined partial elimination of CBS and MPST (but not CTH) in adipocytes affects the expression of genes related to the maintenance of adipocyte function and promotes inflammation, possibly by altering the pattern of protein persulfidation in these cells, suggesting that these enzymes were required for the functional maintenance of adipocytes.
format Online
Article
Text
id pubmed-9220337
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-92203372022-06-24 The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes Latorre, Jessica Aroca, Angeles Fernández-Real, José Manuel Romero, Luis C. Moreno-Navarrete, José María Antioxidants (Basel) Article Recent studies in mice and humans demonstrated the relevance of H(2)S synthesising enzymes, such as CTH, CBS, and MPST, in the physiology of adipose tissue and the differentiation of preadipocyte into adipocytes. Here, our objective was to investigate the combined role of CTH, CBS, and MPST in the preservation of adipocyte protein persulfidation and adipogenesis. Combined partial CTH, CBS, and MPST gene knockdown was achieved treating fully human adipocytes with siRNAs against these transcripts (siRNA_MIX). Adipocyte protein persulfidation was analyzed using label-free quantitative mass spectrometry coupled with a dimedone-switch method for protein labeling and purification. Proteomic analysis quantified 216 proteins with statistically different levels of persulfidation in KD cells compared to control adipocytes. In fully differentiated adipocytes, CBS and MPST mRNA and protein levels were abundant, while CTH expression was very low. It is noteworthy that siRNA_MIX administration resulted in a significant decrease in CBS and MPST expression, without impacting on CTH. The combined partial knockdown of the CBS and MPST genes resulted in reduced cellular sulfide levels in parallel to decreased expression of relevant genes for adipocyte biology, including adipogenesis, mitochondrial biogenesis, and lipogenesis, but increased proinflammatory- and senescence-related genes. It should be noted that the combined partial knockdown of CBS and MPST genes also led to a significant disruption in the persulfidation pattern of the adipocyte proteins. Although among the less persulfidated proteins, we identified several relevant proteins for adipocyte adipogenesis and function, among the most persulfidated, key mediators of adipocyte inflammation and dysfunction as well as some proteins that might play a positive role in adipogenesis were found. In conclusion, the current study indicates that the combined partial elimination of CBS and MPST (but not CTH) in adipocytes affects the expression of genes related to the maintenance of adipocyte function and promotes inflammation, possibly by altering the pattern of protein persulfidation in these cells, suggesting that these enzymes were required for the functional maintenance of adipocytes. MDPI 2022-05-31 /pmc/articles/PMC9220337/ /pubmed/35739994 http://dx.doi.org/10.3390/antiox11061095 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
Latorre, Jessica
Aroca, Angeles
Fernández-Real, José Manuel
Romero, Luis C.
Moreno-Navarrete, José María
The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes
title The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes
title_full The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes
title_fullStr The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes
title_full_unstemmed The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes
title_short The Combined Partial Knockdown of CBS and MPST Genes Induces Inflammation, Impairs Adipocyte Function-Related Gene Expression and Disrupts Protein Persulfidation in Human Adipocytes
title_sort combined partial knockdown of cbs and mpst genes induces inflammation, impairs adipocyte function-related gene expression and disrupts protein persulfidation in human adipocytes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9220337/
https://www.ncbi.nlm.nih.gov/pubmed/35739994
http://dx.doi.org/10.3390/antiox11061095
work_keys_str_mv AT latorrejessica thecombinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT arocaangeles thecombinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT fernandezrealjosemanuel thecombinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT romeroluisc thecombinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT morenonavarretejosemaria thecombinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT latorrejessica combinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT arocaangeles combinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT fernandezrealjosemanuel combinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT romeroluisc combinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes
AT morenonavarretejosemaria combinedpartialknockdownofcbsandmpstgenesinducesinflammationimpairsadipocytefunctionrelatedgeneexpressionanddisruptsproteinpersulfidationinhumanadipocytes

Ejemplares similares