Independent tissue contributors to obesity-associated insulin resistance
Yvo H.A.M. Kusters, Casper G. Schalkwijk, Alfons J.H.M. Houben, M. Eline Kooi, Lucas Lindeboom, Jos Op ’t Roodt, Peter J. Joris, Jogchum Plat, Ronald P. Mensink, Eugene J. Barrett, Coen D.A. Stehouwer
Yvo H.A.M. Kusters, Casper G. Schalkwijk, Alfons J.H.M. Houben, M. Eline Kooi, Lucas Lindeboom, Jos Op ’t Roodt, Peter J. Joris, Jogchum Plat, Ronald P. Mensink, Eugene J. Barrett, Coen D.A. Stehouwer
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Clinical Research and Public Health Endocrinology Metabolism

Independent tissue contributors to obesity-associated insulin resistance

Abstract

BACKGROUND. Induction of insulin resistance is a key pathway through which obesity increases risk of type 2 diabetes, hypertension, dyslipidemia, and cardiovascular events. Although the detrimental effects of obesity on insulin sensitivity are incompletely understood, accumulation of visceral, subcutaneous, and liver fat and impairment of insulin-induced muscle microvascular recruitment (MVR) may be involved. As these phenotypic changes often coincide in obesity, we aimed to unravel whether they independently contribute to insulin resistance and thus constitute separate targets for intervention. METHODS. We measured visceral (VAT) and subcutaneous adipose tissue (SAT) volumes and intrahepatic lipid (IHL) content by MRI, and whole body glucose disposal (WBGD) and MVR (using contrast-enhanced ultrasound) responses to a euglycemic insulin clamp in lean (n = 25) and abdominally obese men (n = 52). Abdominally obese men were randomized to dietary weight loss intervention or habitual diet. RESULTS. Obesity-associated increases in VAT, SAT, and IHL, along with the decrease in MVR, contributed independently to insulin resistance. Moreover, a dietary weight loss intervention reduced insulin resistance, and mediation analyses showed that decreased IHL and insulin-induced MVR, but not decreased VAT or SAT volumes, independently contributed to improved insulin resistance seen with weight loss. CONCLUSION. Quantifying the mutually independent contributions of visceral and subcutaneous adipose tissue, intrahepatic lipid, and insulin-induced muscle microvascular recruitment reveals distinct targets for treating obesity-associated insulin resistance. TRIAL REGISTRATION. Clinicaltrials.gov NCT01675401. FUNDING. Funding was from the Top Institute Food and Nutrition.

Authors

Yvo H.A.M. Kusters, Casper G. Schalkwijk, Alfons J.H.M. Houben, M. Eline Kooi, Lucas Lindeboom, Jos Op ’t Roodt, Peter J. Joris, Jogchum Plat, Ronald P. Mensink, Eugene J. Barrett, Coen D.A. Stehouwer

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Figure 4

Multiple mediator models.

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Multiple mediator models. (A) Multiple mediator model with visceral adip...
(A) Multiple mediator model with visceral adipose tissue (VAT), subcutaneous adipose tissue (SAT), log-transformed intrahepatic lipid (IHL), and muscle microvascular recruitment (MVR) as statistically significant mediators [percentage of total effect mediated (β of mediated effect (95% CI using the Monte Carlo method))] of the association between BMI and whole body glucose disposal (WBGD; n = 76, age-adjusted). The CIs of the mediators overlap, which implies that no mediator contributes more than the other. (B) Multiple mediator model with ΔIHL and ΔMVR as statistically significant mediators [percentage of total effect mediated (β of mediated effect (bootstrapped 95% CI))] of the association between the weight loss intervention and ΔWBGD (n = 49, age-adjusted). The variables ΔVAT and ΔSAT were not statistically significant mediators of this association. The confidence intervals of the mediators overlap, which implies that no mediator contributes more than the other.