Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity

Inflammation is an important mediator of obesity-related complications such as the metabolic syndrome but its causes and mechanisms are unknown. As the complement system is a key mediator of inflammation, we studied whether it is activated in acquired obesity in subcutaneous adipose tissue (AT) and...

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Autores principales: Kaye, Sanna, Lokki, A. Inkeri, Hanttu, Anna, Nissilä, Eija, Heinonen, Sini, Hakkarainen, Antti, Lundbom, Jesper, Lundbom, Nina, Saarinen, Lilli, Tynninen, Olli, Muniandy, Maheswary, Rissanen, Aila, Kaprio, Jaakko, Meri, Seppo, Pietiläinen, Kirsi H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2017
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5432622/
https://www.ncbi.nlm.nih.gov/pubmed/28559893
http://dx.doi.org/10.3389/fimmu.2017.00545
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author Kaye, Sanna
Lokki, A. Inkeri
Hanttu, Anna
Nissilä, Eija
Heinonen, Sini
Hakkarainen, Antti
Lundbom, Jesper
Lundbom, Nina
Saarinen, Lilli
Tynninen, Olli
Muniandy, Maheswary
Rissanen, Aila
Kaprio, Jaakko
Meri, Seppo
Pietiläinen, Kirsi H.
author_facet Kaye, Sanna
Lokki, A. Inkeri
Hanttu, Anna
Nissilä, Eija
Heinonen, Sini
Hakkarainen, Antti
Lundbom, Jesper
Lundbom, Nina
Saarinen, Lilli
Tynninen, Olli
Muniandy, Maheswary
Rissanen, Aila
Kaprio, Jaakko
Meri, Seppo
Pietiläinen, Kirsi H.
author_sort Kaye, Sanna
collection PubMed
description Inflammation is an important mediator of obesity-related complications such as the metabolic syndrome but its causes and mechanisms are unknown. As the complement system is a key mediator of inflammation, we studied whether it is activated in acquired obesity in subcutaneous adipose tissue (AT) and isolated adipocytes. We used a special study design of genetically matched controls of lean and heavy groups, rare monozygotic twin pairs discordant for body mass index (BMI) [n = 26, within-pair difference (Δ) in body mass index, BMI >3 kg/m(2)] with as much as 18 kg mean Δweight. Additionally, 14 BMI-concordant (BMI <3 kg/m(2)) served as a reference group. The detailed measurements included body composition (DEXA), fat distribution (MRI), glucose, insulin, adipokines, C3a and SC5b-9 levels, and the expression of complement and insulin signaling pathway-related genes in AT and adipocytes. In both AT and isolated adipocytes, the classical and alternative pathway genes were upregulated, and the terminal pathway genes downregulated in the heavier co-twins of the BMI-discordant pairs. The upregulated genes included C1q, C1s, C2, ficolin-1, factor H, receptors for C3a and C5a (C5aR1), and the iC3b receptor (CR3). While the terminal pathway components C5 and C6 were downregulated, its inhibitor clusterin was upregulated. Complement gene upregulation in AT and adipocytes correlated positively with adiposity and hyperinsulinemia and negatively with the expression of insulin signaling-related genes. Plasma C3a, but not SC5b-9, levels were elevated in the heavier co-twins. There were no differences between the co-twins in BMI-concordant pairs. Obesity is associated with increased expression of the early, but not late, complement pathway components and of key receptors. The twins with acquired obesity have therefore an inflated inflammatory activity in the AT. The results suggest that complement is likely involved in orchestrating clearance of apoptotic debris and inflammation in the AT.
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spelling pubmed-54326222017-05-30 Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity Kaye, Sanna Lokki, A. Inkeri Hanttu, Anna Nissilä, Eija Heinonen, Sini Hakkarainen, Antti Lundbom, Jesper Lundbom, Nina Saarinen, Lilli Tynninen, Olli Muniandy, Maheswary Rissanen, Aila Kaprio, Jaakko Meri, Seppo Pietiläinen, Kirsi H. Front Immunol Immunology Inflammation is an important mediator of obesity-related complications such as the metabolic syndrome but its causes and mechanisms are unknown. As the complement system is a key mediator of inflammation, we studied whether it is activated in acquired obesity in subcutaneous adipose tissue (AT) and isolated adipocytes. We used a special study design of genetically matched controls of lean and heavy groups, rare monozygotic twin pairs discordant for body mass index (BMI) [n = 26, within-pair difference (Δ) in body mass index, BMI >3 kg/m(2)] with as much as 18 kg mean Δweight. Additionally, 14 BMI-concordant (BMI <3 kg/m(2)) served as a reference group. The detailed measurements included body composition (DEXA), fat distribution (MRI), glucose, insulin, adipokines, C3a and SC5b-9 levels, and the expression of complement and insulin signaling pathway-related genes in AT and adipocytes. In both AT and isolated adipocytes, the classical and alternative pathway genes were upregulated, and the terminal pathway genes downregulated in the heavier co-twins of the BMI-discordant pairs. The upregulated genes included C1q, C1s, C2, ficolin-1, factor H, receptors for C3a and C5a (C5aR1), and the iC3b receptor (CR3). While the terminal pathway components C5 and C6 were downregulated, its inhibitor clusterin was upregulated. Complement gene upregulation in AT and adipocytes correlated positively with adiposity and hyperinsulinemia and negatively with the expression of insulin signaling-related genes. Plasma C3a, but not SC5b-9, levels were elevated in the heavier co-twins. There were no differences between the co-twins in BMI-concordant pairs. Obesity is associated with increased expression of the early, but not late, complement pathway components and of key receptors. The twins with acquired obesity have therefore an inflated inflammatory activity in the AT. The results suggest that complement is likely involved in orchestrating clearance of apoptotic debris and inflammation in the AT. Frontiers Media S.A. 2017-05-16 /pmc/articles/PMC5432622/ /pubmed/28559893 http://dx.doi.org/10.3389/fimmu.2017.00545 Text en Copyright © 2017 Kaye, Lokki, Hanttu, Nissilä, Heinonen, Hakkarainen, Lundbom, Lundbom, Saarinen, Tynninen, Muniandy, Rissanen, Kaprio, Meri and Pietiläinen. http://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) or licensor 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 Immunology
Kaye, Sanna
Lokki, A. Inkeri
Hanttu, Anna
Nissilä, Eija
Heinonen, Sini
Hakkarainen, Antti
Lundbom, Jesper
Lundbom, Nina
Saarinen, Lilli
Tynninen, Olli
Muniandy, Maheswary
Rissanen, Aila
Kaprio, Jaakko
Meri, Seppo
Pietiläinen, Kirsi H.
Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity
title Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity
title_full Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity
title_fullStr Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity
title_full_unstemmed Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity
title_short Upregulation of Early and Downregulation of Terminal Pathway Complement Genes in Subcutaneous Adipose Tissue and Adipocytes in Acquired Obesity
title_sort upregulation of early and downregulation of terminal pathway complement genes in subcutaneous adipose tissue and adipocytes in acquired obesity
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5432622/
https://www.ncbi.nlm.nih.gov/pubmed/28559893
http://dx.doi.org/10.3389/fimmu.2017.00545
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