Changes in abdominal subcutaneous adipose tissue phenotype following menopause is associated with increased visceral fat mass

Julie Abildgaard*, Thorkil Ploug, Elaf Al-Saoudi, Thomas Wagner, Carsten Thomsen, Caroline Ewertsen, Michael Bzorek, Bente Klarlund Pedersen, Anette Tønnes Pedersen, Birgitte Lindegaard

*Corresponding author for this work

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Abstract

Menopause is associated with a redistribution of adipose tissue towards central adiposity, known to cause insulin resistance. In this cross-sectional study of 33 women between 45 and 60 years, we assessed adipose tissue inflammation and morphology in subcutaneous adipose tissue (SAT) and visceral adipose tissue (VAT) across menopause and related this to menopausal differences in adipose tissue distribution and insulin resistance. We collected paired SAT and VAT biopsies from all women and combined this with anthropometric measurements and estimated whole-body insulin sensitivity. We found that menopause was associated with changes in adipose tissue phenotype related to metabolic dysfunction. In SAT, postmenopausal women showed adipocyte hypertrophy, increased inflammation, hypoxia and fibrosis. The postmenopausal changes in SAT was associated with increased visceral fat accumulation. In VAT, menopause was associated with adipocyte hypertrophy, immune cell infiltration and fibrosis. The postmenopausal changes in VAT phenotype was associated with decreased insulin sensitivity. Based on these findings we suggest, that menopause is associated with changes in adipose tissue phenotype related to metabolic dysfunction in both SAT and VAT. Whereas increased SAT inflammation in the context of menopause is associated with VAT accumulation, VAT morphology is related to insulin resistance.

Original languageEnglish
Article number14750
JournalScientific Reports
Volume11
Issue number1
Number of pages12
ISSN2045-2322
DOIs
Publication statusPublished - Dec 2021

Bibliographical note

Funding Information:
The Centre for Physical Activity Research (CFAS) is supported by TrygFonden (Grants ID 101390 and ID 20045). During the study period, the Centre of Inflammation and Metabolism (CIM) was supported by a grant from the Danish National Research Foundation (DNRF55).

Funding Information:
Funding was provided by Augustinus Fonden (Grant no. 17-2354).

Publisher Copyright:
© 2021, The Author(s).

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