Postreceptor insulin resistance contributes to human dyslipidemia and hepatic steatosis
Robert K. Semple, … , Stephen O’Rahilly, David B. Savage
Robert K. Semple, … , Stephen O’Rahilly, David B. Savage
Published January 26, 2009
Citation Information: J Clin Invest. 2009;119(2):315-322. https://doi.org/10.1172/JCI37432.
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Research Article

Postreceptor insulin resistance contributes to human dyslipidemia and hepatic steatosis

Abstract

Metabolic dyslipidemia is characterized by high circulating triglyceride (TG) and low HDL cholesterol levels and is frequently accompanied by hepatic steatosis. Increased hepatic lipogenesis contributes to both of these problems. Because insulin fails to suppress gluconeogenesis but continues to stimulate lipogenesis in both obese and lipodystrophic insulin-resistant mice, it has been proposed that a selective postreceptor defect in hepatic insulin action is central to the pathogenesis of fatty liver and hypertriglyceridemia in these mice. Here we show that humans with generalized insulin resistance caused by either mutations in the insulin receptor gene or inhibitory antibodies specific for the insulin receptor uniformly exhibited low serum TG and normal HDL cholesterol levels. This was due at least in part to surprisingly low rates of de novo lipogenesis and was associated with low liver fat content and the production of TG-depleted VLDL cholesterol particles. In contrast, humans with a selective postreceptor defect in AKT2 manifest increased lipogenesis, elevated liver fat content, TG-enriched VLDL, hypertriglyceridemia, and low HDL cholesterol levels. People with lipodystrophy, a disorder characterized by particularly severe insulin resistance and dyslipidemia, demonstrated similar abnormalities. Collectively these data from humans with molecularly characterized forms of insulin resistance suggest that partial postreceptor hepatic insulin resistance is a key element in the development of metabolic dyslipidemia and hepatic steatosis.

Authors

Robert K. Semple, Alison Sleigh, Peter R. Murgatroyd, Claire A. Adams, Les Bluck, Sarah Jackson, Alessandra Vottero, Dipak Kanabar, Valentine Charlton-Menys, Paul Durrington, Maria A. Soos, T. Adrian Carpenter, David J. Lomas, Elaine K. Cochran, Phillip Gorden, Stephen O’Rahilly, David B. Savage

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Figure 4

Abdominal and liver fat measurements in patients with severe insulin resistance.

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Abdominal and liver fat measurements in patients with severe insulin res...
Representative abdominal fat distribution (at the L4 vertebral level) (top row), together with T2-weighted HASTE transaxial images of the liver (middle row), and the corresponding liver fat spectra (bottom row) from 4 women. The control volunteer was a 38-year-old female (BMI, 24.2 kg/m2), INSR A1135E was a 17-year-old female (BMI, 21.5 kg/m2; patient 3 in Table 2), AKT2 R274H was a 40-year-old female (BMI, 26.7 kg/m2; patient 5 in Table 2), and LMNA was a 45-year-old woman (BMI, 25.0 kg/m2 with FPLD2; she was a compound heterozygote for LMNA S583L and T528M; ref. 40). VAT is shown in yellow. IHL, intrahepatic lipid as determined by magnetic resonance spectroscopy; SCAT, subcutaneous adipose tissue (red).