Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs

Institut for Veterinær- og Husdyrvidenskab

Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › fagfællebedømt

Standard

Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs. / Mentzel, Caroline M. Junker; Cardoso, Tainã Figueiredo; Pipper, Christian Bressen; Jacobsen, Mette Juul; Jørgensen, Claus Bøttcher; Cirera, Susanna; Fredholm, Merete.

I: Molecular Genetics and Genomics, Bind 293, Nr. 1, 2018, s. 129–136.

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › fagfællebedømt

Harvard

Mentzel, CMJ, Cardoso, TF, Pipper, CB, Jacobsen, MJ, Jørgensen, CB, Cirera, S & Fredholm, M 2018, 'Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs', Molecular Genetics and Genomics, bind 293, nr. 1, s. 129–136. https://doi.org/10.1007/s00438-017-1369-2

APA

Mentzel, C. M. J., Cardoso, T. F., Pipper, C. B., Jacobsen, M. J., Jørgensen, C. B., Cirera, S., & Fredholm, M. (2018). Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs. Molecular Genetics and Genomics, 293(1), 129–136. https://doi.org/10.1007/s00438-017-1369-2

Vancouver

Mentzel CMJ, Cardoso TF, Pipper CB, Jacobsen MJ, Jørgensen CB, Cirera S o.a. Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs. Molecular Genetics and Genomics. 2018;293(1):129–136. https://doi.org/10.1007/s00438-017-1369-2

Author

Mentzel, Caroline M. Junker ; Cardoso, Tainã Figueiredo ; Pipper, Christian Bressen ; Jacobsen, Mette Juul ; Jørgensen, Claus Bøttcher ; Cirera, Susanna ; Fredholm, Merete. / Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs. I: Molecular Genetics and Genomics. 2018 ; Bind 293, Nr. 1. s. 129–136.

Bibtex

@article{2807e248fd7845328f7753370b64d4f9,

title = "Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs",

abstract = "The aim of this study was to elucidate the relative impact of three phenotypes often used to characterize obesity on perturbation of molecular pathways involved in obesity. The three obesity-related phenotypes are (1) body mass index (BMI), (2) amount of subcutaneous adipose tissue (SATa), and (3) amount of retroperitoneal adipose tissue (RPATa). Although it is generally accepted that increasing amount of RPATa is {\textquoteleft}unhealthy{\textquoteright}, a direct comparison of the relative impact of the three obesity-related phenotypes on gene expression has, to our knowledge, not been performed previously. We have used multiple linear models to analyze altered gene expression of selected obesity-related genes in tissues collected from 19 female pigs phenotypically characterized with respect to the obesity-related phenotypes. Gene expression was assessed by high-throughput qPCR in RNA from liver, skeletal muscle and abdominal adipose tissue. The stringent statistical approach used in the study has increased the power of the analysis compared to the classical approach of analysis in divergent groups of individuals. Our approach led to the identification of key components of cellular pathways that are modulated in the three tissues in association with changes in the three obesity-relevant phenotypes (BMI, SATa and RPATa). The deregulated pathways are involved in biosynthesis and transcript regulation in adipocytes, in lipid transport, lipolysis and metabolism, and in inflammatory responses. Deregulation seemed more comprehensive in liver (23 genes) compared to abdominal adipose tissue (10 genes) and muscle (3 genes). Notably, the study supports the notion that excess amount of intra-abdominal adipose tissue is associated with a greater metabolic disease risk. Our results provide molecular support for this notion by demonstrating that increasing amount of RPATa has a higher impact on perturbation of cellular pathways influencing obesity and obesity-related metabolic traits compared to increase in BMI and amount of SATa.",

author = "Mentzel, {Caroline M. Junker} and Cardoso, {Tain{\~a} Figueiredo} and Pipper, {Christian Bressen} and Jacobsen, {Mette Juul} and J{\o}rgensen, {Claus B{\o}ttcher} and Susanna Cirera and Merete Fredholm",

year = "2018",

doi = "10.1007/s00438-017-1369-2",

language = "English",

volume = "293",

pages = "129–136",

journal = "Molecular Genetics and Genomics",

issn = "1617-4615",

publisher = "Springer",

number = "1",

}

RIS

TY - JOUR

T1 - Deregulation of obesity-relevant genes is associated with progression in BMI and the amount of adipose tissue in pigs

AU - Mentzel, Caroline M. Junker

AU - Cardoso, Tainã Figueiredo

AU - Pipper, Christian Bressen

AU - Jacobsen, Mette Juul

AU - Jørgensen, Claus Bøttcher

AU - Cirera, Susanna

AU - Fredholm, Merete

PY - 2018

Y1 - 2018

N2 - The aim of this study was to elucidate the relative impact of three phenotypes often used to characterize obesity on perturbation of molecular pathways involved in obesity. The three obesity-related phenotypes are (1) body mass index (BMI), (2) amount of subcutaneous adipose tissue (SATa), and (3) amount of retroperitoneal adipose tissue (RPATa). Although it is generally accepted that increasing amount of RPATa is ‘unhealthy’, a direct comparison of the relative impact of the three obesity-related phenotypes on gene expression has, to our knowledge, not been performed previously. We have used multiple linear models to analyze altered gene expression of selected obesity-related genes in tissues collected from 19 female pigs phenotypically characterized with respect to the obesity-related phenotypes. Gene expression was assessed by high-throughput qPCR in RNA from liver, skeletal muscle and abdominal adipose tissue. The stringent statistical approach used in the study has increased the power of the analysis compared to the classical approach of analysis in divergent groups of individuals. Our approach led to the identification of key components of cellular pathways that are modulated in the three tissues in association with changes in the three obesity-relevant phenotypes (BMI, SATa and RPATa). The deregulated pathways are involved in biosynthesis and transcript regulation in adipocytes, in lipid transport, lipolysis and metabolism, and in inflammatory responses. Deregulation seemed more comprehensive in liver (23 genes) compared to abdominal adipose tissue (10 genes) and muscle (3 genes). Notably, the study supports the notion that excess amount of intra-abdominal adipose tissue is associated with a greater metabolic disease risk. Our results provide molecular support for this notion by demonstrating that increasing amount of RPATa has a higher impact on perturbation of cellular pathways influencing obesity and obesity-related metabolic traits compared to increase in BMI and amount of SATa.

AB - The aim of this study was to elucidate the relative impact of three phenotypes often used to characterize obesity on perturbation of molecular pathways involved in obesity. The three obesity-related phenotypes are (1) body mass index (BMI), (2) amount of subcutaneous adipose tissue (SATa), and (3) amount of retroperitoneal adipose tissue (RPATa). Although it is generally accepted that increasing amount of RPATa is ‘unhealthy’, a direct comparison of the relative impact of the three obesity-related phenotypes on gene expression has, to our knowledge, not been performed previously. We have used multiple linear models to analyze altered gene expression of selected obesity-related genes in tissues collected from 19 female pigs phenotypically characterized with respect to the obesity-related phenotypes. Gene expression was assessed by high-throughput qPCR in RNA from liver, skeletal muscle and abdominal adipose tissue. The stringent statistical approach used in the study has increased the power of the analysis compared to the classical approach of analysis in divergent groups of individuals. Our approach led to the identification of key components of cellular pathways that are modulated in the three tissues in association with changes in the three obesity-relevant phenotypes (BMI, SATa and RPATa). The deregulated pathways are involved in biosynthesis and transcript regulation in adipocytes, in lipid transport, lipolysis and metabolism, and in inflammatory responses. Deregulation seemed more comprehensive in liver (23 genes) compared to abdominal adipose tissue (10 genes) and muscle (3 genes). Notably, the study supports the notion that excess amount of intra-abdominal adipose tissue is associated with a greater metabolic disease risk. Our results provide molecular support for this notion by demonstrating that increasing amount of RPATa has a higher impact on perturbation of cellular pathways influencing obesity and obesity-related metabolic traits compared to increase in BMI and amount of SATa.

U2 - 10.1007/s00438-017-1369-2

DO - 10.1007/s00438-017-1369-2

M3 - Journal article

C2 - 28913560

VL - 293

SP - 129

EP - 136

JO - Molecular Genetics and Genomics

JF - Molecular Genetics and Genomics

SN - 1617-4615

IS - 1

ER -

ID: 183612520