Severe impairment in liver insulin signaling fails to alter hepatic insulin action in conscious mice
Christoph Buettner, … , Silvana Obici, Luciano Rossetti
Christoph Buettner, … , Silvana Obici, Luciano Rossetti
Published May 2, 2005
Citation Information: J Clin Invest. 2005;115(5):1306-1313. https://doi.org/10.1172/JCI23109.
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Severe impairment in liver insulin signaling fails to alter hepatic insulin action in conscious mice

Abstract

Insulin exerts its potent effects on hepatic glucose fluxes via direct and indirect mechanisms. Whereas a liver-specific insulin receptor (IR) knockout (LIRKO) mouse exhibits glucose intolerance as well as insulin resistance, it is unclear whether a more acute decrease in the expression of hepatic IR would be sufficient to induce hepatic insulin resistance. Here we report that the downregulation of hepatic IR expression by up to 95% does not modify hepatic insulin action. The i.p. administration (2 injections over 1 week) of an antisense oligodeoxynucleotide (ASO) directed to reduce insulin expression downregulated hepatic IR expression in C57BL6J mice. A high dose of IR-ASO decreased IR protein approximately 95%, while a control-ASO failed to modify IR expression. At this dose, the IR-ASO also decreased IR expression in adipose tissue but did not significantly decrease IR expression in hypothalamus or skeletal muscle. Insulin action was assessed with insulin clamp studies in conscious mice. The rate of glucose infusion during the clamp studies was comparable in control-ASO– and IR-ASO–treated mice. Importantly, the depletion of liver IR protein markedly impaired downstream insulin signaling in the liver, but it failed to modify the rate of glucose production. Thus, near ablation of liver IR does not alter insulin action on glucose production.

Authors

Christoph Buettner, Rima Patel, Evan D. Muse, Sanjay Bhanot, Brett P. Monia, Rob McKay, Silvana Obici, Luciano Rossetti

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IR-ASO treatment impairs insulin signaling. (A) Experimental design for ...
IR-ASO treatment impairs insulin signaling. (A) Experimental design for treatment with IR-ASO and control-ASO and acute in vivo stimulation with i.p. insulin (100 mU). (B) Effect of IR-ASO compared with control-ASO on IR and Akt activation in liver extracts after acute insulin stimulation. IR activation was assessed with a phosphospecific antibody for tyrosine 1146 IR. Akt activation was assessed with phospho-specific antibodies against serine 473 (S473) and threonine 308 (T308) of Akt. For normalization purposes, membranes were stripped and reprobed with the housekeeping genes actin and GAPDH, as well as the transcription factor Stat3.