Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet

Introduction: Metabolic disorders are an important health concern that threatens life and burdens society severely. ClC-3 is a member of the chloride voltage-gated channel family, and ClC-3 deletion improved the phenotypes of dysglycemic metabolism and the impairment of insulin sensitivity. However,...

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Autores principales: Jing, Zhenghui, Zhang, Haifeng, Wen, Yunjie, Cui, Shiyu, Ren, Yuhua, Liu, Rong, Duan, Sirui, Zhao, Wenbao, Fan, Lihong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Cell and Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10242048/
https://www.ncbi.nlm.nih.gov/pubmed/37287451
http://dx.doi.org/10.3389/fcell.2023.1196684
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author Jing, Zhenghui
Zhang, Haifeng
Wen, Yunjie
Cui, Shiyu
Ren, Yuhua
Liu, Rong
Duan, Sirui
Zhao, Wenbao
Fan, Lihong
author_facet Jing, Zhenghui
Zhang, Haifeng
Wen, Yunjie
Cui, Shiyu
Ren, Yuhua
Liu, Rong
Duan, Sirui
Zhao, Wenbao
Fan, Lihong
author_sort Jing, Zhenghui
collection PubMed
description Introduction: Metabolic disorders are an important health concern that threatens life and burdens society severely. ClC-3 is a member of the chloride voltage-gated channel family, and ClC-3 deletion improved the phenotypes of dysglycemic metabolism and the impairment of insulin sensitivity. However, the effects of a healthy diet on transcriptome and epigenetics in ClC-3(−/−) mice were not explained in detail. Methods: Here, we performed transcriptome sequencing and Reduced Representation Bisulfite Sequencing for the liver of 3 weeks old WT and ClC-3(−/−) mice consuming a normal diet to insight into the epigenetic and transcriptomic alterations of ClC-3 deficient mice. Results: In the present study, we found that ClC-3(−/−) mice that were younger than 8 weeks old had smaller bodies compared to ClC-3(+/+) mice with ad libitum self-feeding normal diet, and ClC-3(−/−) mice that were older than 10 weeks old had a similar body weight. Except for the spleen, lung, and kidney, the average weight of the heart, liver, and brain in ClC-3(−/−) mice was lower than that in ClC-3(+/+) mice. TG, TC, HDL, and LDL in fasting ClC-3(−/−) mice were not significantly different from those in ClC-3(+/+) mice. Fasting blood glucose in ClC-3(−/−) mice was lower than that in ClC-3(+/+) mice; the glucose tolerance test indicated the response to blood glucose increasing for ClC-3(−/−) mice was torpid, but the efficiency of lowering blood glucose was much higher once started. Transcriptomic sequencing and reduced representation bisulfite sequencing for the liver of unweaned mice indicated that ClC-3 deletion significantly changed transcriptional expression and DNA methylation levels of glucose metabolism-related genes. A total of 92 genes were intersected between DEGs and DMRs-targeted genes, of which Nos3, Pik3r1, Socs1, and Acly were gathered in type II diabetes mellitus, insulin resistance, and metabolic pathways. Moreover, Pik3r1 and Acly expressions were obviously correlated with DNA methylation levels, not Nos3 and Socs1. However, the transcriptional levels of these four genes were not different between ClC-3(−/−) and ClC-3(+/+) mice at the age of 12 weeks. Discussion: ClC-3 influenced the methylated modification to regulate glucose metabolism, of which the gene expressions could be driven to change again by a personalized diet-style intervention.
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spelling pubmed-102420482023-06-07 Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet Jing, Zhenghui Zhang, Haifeng Wen, Yunjie Cui, Shiyu Ren, Yuhua Liu, Rong Duan, Sirui Zhao, Wenbao Fan, Lihong Front Cell Dev Biol Cell and Developmental Biology Introduction: Metabolic disorders are an important health concern that threatens life and burdens society severely. ClC-3 is a member of the chloride voltage-gated channel family, and ClC-3 deletion improved the phenotypes of dysglycemic metabolism and the impairment of insulin sensitivity. However, the effects of a healthy diet on transcriptome and epigenetics in ClC-3(−/−) mice were not explained in detail. Methods: Here, we performed transcriptome sequencing and Reduced Representation Bisulfite Sequencing for the liver of 3 weeks old WT and ClC-3(−/−) mice consuming a normal diet to insight into the epigenetic and transcriptomic alterations of ClC-3 deficient mice. Results: In the present study, we found that ClC-3(−/−) mice that were younger than 8 weeks old had smaller bodies compared to ClC-3(+/+) mice with ad libitum self-feeding normal diet, and ClC-3(−/−) mice that were older than 10 weeks old had a similar body weight. Except for the spleen, lung, and kidney, the average weight of the heart, liver, and brain in ClC-3(−/−) mice was lower than that in ClC-3(+/+) mice. TG, TC, HDL, and LDL in fasting ClC-3(−/−) mice were not significantly different from those in ClC-3(+/+) mice. Fasting blood glucose in ClC-3(−/−) mice was lower than that in ClC-3(+/+) mice; the glucose tolerance test indicated the response to blood glucose increasing for ClC-3(−/−) mice was torpid, but the efficiency of lowering blood glucose was much higher once started. Transcriptomic sequencing and reduced representation bisulfite sequencing for the liver of unweaned mice indicated that ClC-3 deletion significantly changed transcriptional expression and DNA methylation levels of glucose metabolism-related genes. A total of 92 genes were intersected between DEGs and DMRs-targeted genes, of which Nos3, Pik3r1, Socs1, and Acly were gathered in type II diabetes mellitus, insulin resistance, and metabolic pathways. Moreover, Pik3r1 and Acly expressions were obviously correlated with DNA methylation levels, not Nos3 and Socs1. However, the transcriptional levels of these four genes were not different between ClC-3(−/−) and ClC-3(+/+) mice at the age of 12 weeks. Discussion: ClC-3 influenced the methylated modification to regulate glucose metabolism, of which the gene expressions could be driven to change again by a personalized diet-style intervention. Frontiers Media S.A. 2023-05-23 /pmc/articles/PMC10242048/ /pubmed/37287451 http://dx.doi.org/10.3389/fcell.2023.1196684 Text en Copyright © 2023 Jing, Zhang, Wen, Cui, Ren, Liu, Duan, Zhao and Fan. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cell and Developmental Biology
Jing, Zhenghui
Zhang, Haifeng
Wen, Yunjie
Cui, Shiyu
Ren, Yuhua
Liu, Rong
Duan, Sirui
Zhao, Wenbao
Fan, Lihong
Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet
title Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet
title_full Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet
title_fullStr Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet
title_full_unstemmed Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet
title_short Epigenetic and transcriptomic alterations in the ClC-3-deficient mice consuming a normal diet
title_sort epigenetic and transcriptomic alterations in the clc-3-deficient mice consuming a normal diet
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10242048/
https://www.ncbi.nlm.nih.gov/pubmed/37287451
http://dx.doi.org/10.3389/fcell.2023.1196684
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