Evidence of Early Alterations in Adipose Tissue Biology and Function and Its Association with Obesity-related Inflammation and Insulin Resistance in Children

Overview

Journal Diabetes

Specialty Endocrinology

Date 2014 Nov 14

PMID 25392242

Citations 87

Authors

Kathrin Landgraf

Denise Rockstroh

Isabel V Wagner

Sebastian Weise

Roy Tauscher

Julian T Schwartze

Dennis Loffler

Ulf Buhligen

Magdalena Wojan

Holger Till

Jurgen Kratzsch

Wieland Kiess

Matthias Bluher

Antje Korner

Affiliations

Soon will be listed here.

Abstract

Accumulation of fat mass in obesity may result from hypertrophy and/or hyperplasia and is frequently associated with adipose tissue (AT) dysfunction in adults. Here we assessed early alterations in AT biology and function by comprehensive experimental and clinical characterization of 171 AT samples from lean and obese children aged 0 to 18 years. We show an increase in adipocyte size and number in obese compared with lean children beginning in early childhood. These alterations in AT composition in obese children were accompanied by decreased basal lipolytic activity and significantly enhanced stromal vascular cell proliferation in vitro, potentially underlying the hypertrophy and hyperplasia seen in obese children, respectively. Furthermore, macrophage infiltration, including the formation of crown-like structures, was increased in AT of obese children from 6 years on and was associated with higher hs-CRP serum levels. Clinically, adipocyte hypertrophy was not only associated with leptin serum levels but was highly and independently correlated with HOMA-IR as a marker of insulin resistance in children. In summary, we show that adipocyte hypertrophy is linked to increased inflammation in AT in obese children, thereby providing evidence that obesity-associated AT dysfunction develops in early childhood and is related to insulin resistance.

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