Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor

Endogenous hyperinsulinemia and insulin receptor (IR)/IGF-I receptor (IGF-IR) phosphorylation in tumors are associated with a worse prognosis in women with breast cancer. In vitro, insulin stimulation of the IR increases proliferation of breast cancer cells. However, in vivo studies demonstrating th...

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Autores principales: Gallagher, Emily Jane, Alikhani, Nyosha, Tobin-Hess, Aviva, Blank, Jeffrey, Buffin, Nicholas J., Zelenko, Zara, Tennagels, Norbert, Werner, Ulrich, LeRoith, Derek
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2013
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3781483/
https://www.ncbi.nlm.nih.gov/pubmed/23835331
http://dx.doi.org/10.2337/db13-0249
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author Gallagher, Emily Jane
Alikhani, Nyosha
Tobin-Hess, Aviva
Blank, Jeffrey
Buffin, Nicholas J.
Zelenko, Zara
Tennagels, Norbert
Werner, Ulrich
LeRoith, Derek
author_facet Gallagher, Emily Jane
Alikhani, Nyosha
Tobin-Hess, Aviva
Blank, Jeffrey
Buffin, Nicholas J.
Zelenko, Zara
Tennagels, Norbert
Werner, Ulrich
LeRoith, Derek
author_sort Gallagher, Emily Jane
collection PubMed
description Endogenous hyperinsulinemia and insulin receptor (IR)/IGF-I receptor (IGF-IR) phosphorylation in tumors are associated with a worse prognosis in women with breast cancer. In vitro, insulin stimulation of the IR increases proliferation of breast cancer cells. However, in vivo studies demonstrating that IR activation increases tumor growth, independently of IGF-IR activation, are lacking. We hypothesized that endogenous hyperinsulinemia increases mammary tumor growth by directly activating the IR rather than the IGF-IR or hybrid receptors. We aimed to determine whether stimulating the IR with the insulin analog AspB10 could increase tumor growth independently of IGF-IR signaling. We induced orthotopic mammary tumors in control FVB/n and hyperinsulinemic MKR mice, and treated them with the insulin analog AspB10, recombinant human IGF-I, or vehicle. Tumors from mice with endogenous hyperinsulinemia were larger and had greater IR phosphorylation, but not IGF-IR phosphorylation, than those from control mice. Chronic AspB10 administration also increased tumor growth and IR (but not IGF-IR) phosphorylation in tumors. IGF-I led to activation of both the IGF-IR and IR and probably hybrid receptors. Our results demonstrate that IR phosphorylation increases tumor growth, independently of IGF-IR/hybrid receptor phosphorylation, and warrant consideration when developing therapeutics targeting the IGF-IR, but not the IR.
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spelling pubmed-37814832014-10-01 Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor Gallagher, Emily Jane Alikhani, Nyosha Tobin-Hess, Aviva Blank, Jeffrey Buffin, Nicholas J. Zelenko, Zara Tennagels, Norbert Werner, Ulrich LeRoith, Derek Diabetes Original Research Endogenous hyperinsulinemia and insulin receptor (IR)/IGF-I receptor (IGF-IR) phosphorylation in tumors are associated with a worse prognosis in women with breast cancer. In vitro, insulin stimulation of the IR increases proliferation of breast cancer cells. However, in vivo studies demonstrating that IR activation increases tumor growth, independently of IGF-IR activation, are lacking. We hypothesized that endogenous hyperinsulinemia increases mammary tumor growth by directly activating the IR rather than the IGF-IR or hybrid receptors. We aimed to determine whether stimulating the IR with the insulin analog AspB10 could increase tumor growth independently of IGF-IR signaling. We induced orthotopic mammary tumors in control FVB/n and hyperinsulinemic MKR mice, and treated them with the insulin analog AspB10, recombinant human IGF-I, or vehicle. Tumors from mice with endogenous hyperinsulinemia were larger and had greater IR phosphorylation, but not IGF-IR phosphorylation, than those from control mice. Chronic AspB10 administration also increased tumor growth and IR (but not IGF-IR) phosphorylation in tumors. IGF-I led to activation of both the IGF-IR and IR and probably hybrid receptors. Our results demonstrate that IR phosphorylation increases tumor growth, independently of IGF-IR/hybrid receptor phosphorylation, and warrant consideration when developing therapeutics targeting the IGF-IR, but not the IR. American Diabetes Association 2013-10 2013-09-17 /pmc/articles/PMC3781483/ /pubmed/23835331 http://dx.doi.org/10.2337/db13-0249 Text en © 2013 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.
spellingShingle Original Research
Gallagher, Emily Jane
Alikhani, Nyosha
Tobin-Hess, Aviva
Blank, Jeffrey
Buffin, Nicholas J.
Zelenko, Zara
Tennagels, Norbert
Werner, Ulrich
LeRoith, Derek
Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor
title Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor
title_full Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor
title_fullStr Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor
title_full_unstemmed Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor
title_short Insulin Receptor Phosphorylation by Endogenous Insulin or the Insulin Analog AspB10 Promotes Mammary Tumor Growth Independent of the IGF-I Receptor
title_sort insulin receptor phosphorylation by endogenous insulin or the insulin analog aspb10 promotes mammary tumor growth independent of the igf-i receptor
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3781483/
https://www.ncbi.nlm.nih.gov/pubmed/23835331
http://dx.doi.org/10.2337/db13-0249
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