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Mammalian Genetic Models with Minimal or Complex Phenotypes

Preserved Pancreatic β-Cell Development and Function in Mice Lacking the Insulin Receptor-Related Receptor

, , , , &
Pages 5624-5630 | Received 10 Jan 2001, Accepted 15 May 2001, Published online: 28 Mar 2023
 

Abstract

Receptors of the insulin/insulinlike growth factor (IGF) family have been implicated in the regulation of pancreatic β-cell growth and insulin secretion. The insulin receptor-related receptor (IRR) is an orphan receptor of the insulin receptor gene (Ir) subfamily. It is expressed at considerably higher levels in β cells than either insulin or IGF-1 receptors, and it has been shown to engage in heterodimer formation with insulin or IGF-1 receptors. To address whether IRR plays a physiologic role in β-cell development and regulation of insulin secretion, we have characterized mice lacking IRR and generated a combined knockout of Irand Irr. We report that islet morphology, β-cell mass, and secretory function are not affected in IRR-deficient mice. Moreover, lack of IRR does not impair compensatory β-cell hyperplasia in insulin-resistant Ir+/− mice, nor does it affect β-cell development and function in Ir−/− mice. We conclude that glucose-stimulated insulin secretion and embryonic β-cell development occur normally in mice lacking Irr.

ACKNOWLEDGMENTS

This work was supported by NIH grants DK58282, DK57539, and JDF 2000-893 to D.A. and by R37NS331999 to L.F.P.

We thank Jun Nakae for helpful comments on the manuscript.

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