Skeletal Muscle–Specific Deletion of Lipoprotein Lipase Enhances Insulin Signaling in Skeletal Muscle but Causes Insulin Resistance in Liver and Other Tissues-Reference-Cited by-同舟云学术

Skeletal Muscle–Specific Deletion of Lipoprotein Lipase Enhances Insulin Signaling in Skeletal Muscle but Causes Insulin Resistance in Liver and Other Tissues

Published:2008-10-24 Issue:1 Volume:58 Page:116-124
ISSN:0012-1797
Container-title:Diabetes
language:en
Short-container-title:

Author:

Wang Hong¹,Knaub Leslie A.¹,Jensen Dalan R.¹,Young Jung Dae²,Hong Eun-Gyoung²,Ko Hwi-Jin²,Coates Alison M.¹,Goldberg Ira J.³,de la Houssaye Becky A.⁴,Janssen Rachel C.⁴,McCurdy Carrie E.⁴,Rahman Shaikh M.⁴,Soo Choi Cheol⁵,Shulman Gerald I.⁶,Kim Jason K.²,Friedman Jacob E.⁴,Eckel Robert H.¹

Affiliation:

1. Division of Endocrinology, Metabolism and Diabetes, University of Colorado Denver Anschutz Medical Campus, Aurora, Colorado;

2. Department of Cellular & Molecular Physiology, Pennsylvania State University College of Medicine, Hershey, Pennsylvania;

3. Department of Medicine, Columbia University, New York City, New York;

4. Department of Pediatrics, University of Colorado Denver Anschutz Medical Campus, Aurora, Colorado;

5. Department of Internal Medicine, Yale University School of Medicine, New Haven, Connecticut;

6. Department of Internal Medicine, Department of Cellular & Molecular Physiology, Howard Hughes Medical Institute, Yale University School of Medicine, New Haven, Connecticut.

Abstract

OBJECTIVE Skeletal muscle–specific LPL knockout mouse (SMLPL−/−) were created to study the systemic impact of reduced lipoprotein lipid delivery in skeletal muscle on insulin sensitivity, body weight, and composition. RESEARCH DESIGN AND METHODS Tissue-specific insulin sensitivity was assessed using a hyperinsulinemic-euglycemic clamp and 2-deoxyglucose uptake. Gene expression and insulin-signaling molecules were compared in skeletal muscle and liver of SMLPL−/− and control mice. RESULTS Nine-week-old SMLPL−/− mice showed no differences in body weight, fat mass, or whole-body insulin sensitivity, but older SMLPL−/− mice had greater weight gain and whole-body insulin resistance. High-fat diet feeding accelerated the development of obesity. In young SMLPL−/− mice, insulin-stimulated glucose uptake was increased 58% in the skeletal muscle, but was reduced in white adipose tissue (WAT) and heart. Insulin action was also diminished in liver: 40% suppression of hepatic glucose production in SMLPL−/− vs. 90% in control mice. Skeletal muscle triglyceride was 38% lower, and insulin-stimulated phosphorylated Akt (Ser473) was twofold greater in SMLPL−/− mice without changes in IRS-1 tyrosine phosphorylation and phosphatidylinositol 3-kinase activity. Hepatic triglyceride and liver X receptor, carbohydrate response element–binding protein, and PEPCK mRNAs were unaffected in SMLPL−/− mice, but peroxisome proliferator–activated receptor (PPAR)-γ coactivator-1α and interleukin-1β mRNAs were higher, and stearoyl–coenzyme A desaturase-1 and PPARγ mRNAs were reduced. CONCLUSIONS LPL deletion in skeletal muscle reduces lipid storage and increases insulin signaling in skeletal muscle without changes in body composition. Moreover, lack of LPL in skeletal muscle results in insulin resistance in other key metabolic tissues and ultimately leads to obesity and systemic insulin resistance.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

Link

https://journals.org/diabetes/diabetes/article-pdf/58/1/116/513551/zdb00109000116.pdf

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