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Journal of Endocrinology (1998) 159, R9-R12       DOI: 10.1677/joe.0.159R009
© 1998 Society for Endocrinology
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Journal of Endocrinology, Vol 159, Issue 2, R9-R12
Copyright © 1998 by Society for Endocrinology


Articles

Effect of fasting on insulin receptor-related receptor messenger ribonucleic acid in rat kidney

D Chrysis, BM Moats-Staats, and LE Underwood


The insulin receptor-related receptor (IRR), a member of the insulin receptor tyrosine kinase family, has structural homology to the insulin receptor (IR) and the IGF-I receptor (IGF-IR). The ligand, gene regulation and biological function of the IRR are not known. Because mRNAs for both the IR and IGF-IR are increased by nutrient restriction, we used RNase protection assays to assess the effects of fasting 48 h on IRR mRNA in kidneys of rats. We compared the changes in IRR with those in IR and IGF-IR mRNAs. We observed a significant increase in steady state levels of IRR (ratio of IRR mRNA to beta-actin in fed P<0.01), suggesting that the ligand for IRR also might be regulated by nutrients.


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