Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging

In addition to their extended lifespans, slow-aging growth hormone receptor/binding protein gene-disrupted (knockout) (GHR-KO) mice are hypoinsulinemic and highly sensitive to the action of insulin. It has been proposed that this insulin sensitivity is important for their longevity and increased hea...

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Autores principales: Arum, Oge, Boparai, Ravneet K, Saleh, Jamal K, Wang, Feiya, Dirks, Angela L, Turner, Jeremy G, Kopchick, John J, Liu, Jun-Li, Khardori, Romesh K, Bartke, Andrzej
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BlackWell Publishing Ltd 2014
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Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4326932/
https://www.ncbi.nlm.nih.gov/pubmed/25244225
http://dx.doi.org/10.1111/acel.12262
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author Arum, Oge
Boparai, Ravneet K
Saleh, Jamal K
Wang, Feiya
Dirks, Angela L
Turner, Jeremy G
Kopchick, John J
Liu, Jun-Li
Khardori, Romesh K
Bartke, Andrzej
author_facet Arum, Oge
Boparai, Ravneet K
Saleh, Jamal K
Wang, Feiya
Dirks, Angela L
Turner, Jeremy G
Kopchick, John J
Liu, Jun-Li
Khardori, Romesh K
Bartke, Andrzej
author_sort Arum, Oge
collection PubMed
description In addition to their extended lifespans, slow-aging growth hormone receptor/binding protein gene-disrupted (knockout) (GHR-KO) mice are hypoinsulinemic and highly sensitive to the action of insulin. It has been proposed that this insulin sensitivity is important for their longevity and increased healthspan. We tested whether this insulin sensitivity of the GHR-KO mouse is necessary for its retarded aging by abrogating that sensitivity with a transgenic alteration that improves development and secretory function of pancreatic β-cells by expressing Igf-1 under the rat insulin promoter 1 (RIP::IGF-1). The RIP::IGF-1 transgene increased circulating insulin content in GHR-KO mice, and thusly fully normalized their insulin sensitivity, without affecting the proliferation of any non-β-cell cell types. Multiple (nonsurvivorship) longevity-associated physiological and endocrinological characteristics of these mice (namely beneficial blood glucose regulatory control, altered metabolism, and preservation of memory capabilities) were partially or completely normalized, thus supporting the causal role of insulin sensitivity for the decelerated senescence of GHR-KO mice. We conclude that a delayed onset and/or decreased pace of aging can be hormonally regulated.
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spelling pubmed-43269322015-02-19 Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging Arum, Oge Boparai, Ravneet K Saleh, Jamal K Wang, Feiya Dirks, Angela L Turner, Jeremy G Kopchick, John J Liu, Jun-Li Khardori, Romesh K Bartke, Andrzej Aging Cell Original Articles In addition to their extended lifespans, slow-aging growth hormone receptor/binding protein gene-disrupted (knockout) (GHR-KO) mice are hypoinsulinemic and highly sensitive to the action of insulin. It has been proposed that this insulin sensitivity is important for their longevity and increased healthspan. We tested whether this insulin sensitivity of the GHR-KO mouse is necessary for its retarded aging by abrogating that sensitivity with a transgenic alteration that improves development and secretory function of pancreatic β-cells by expressing Igf-1 under the rat insulin promoter 1 (RIP::IGF-1). The RIP::IGF-1 transgene increased circulating insulin content in GHR-KO mice, and thusly fully normalized their insulin sensitivity, without affecting the proliferation of any non-β-cell cell types. Multiple (nonsurvivorship) longevity-associated physiological and endocrinological characteristics of these mice (namely beneficial blood glucose regulatory control, altered metabolism, and preservation of memory capabilities) were partially or completely normalized, thus supporting the causal role of insulin sensitivity for the decelerated senescence of GHR-KO mice. We conclude that a delayed onset and/or decreased pace of aging can be hormonally regulated. BlackWell Publishing Ltd 2014-12 2014-09-20 /pmc/articles/PMC4326932/ /pubmed/25244225 http://dx.doi.org/10.1111/acel.12262 Text en © 2014 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd. http://creativecommons.org/licenses/by/3.0/ This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Arum, Oge
Boparai, Ravneet K
Saleh, Jamal K
Wang, Feiya
Dirks, Angela L
Turner, Jeremy G
Kopchick, John J
Liu, Jun-Li
Khardori, Romesh K
Bartke, Andrzej
Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging
title Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging
title_full Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging
title_fullStr Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging
title_full_unstemmed Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging
title_short Specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (GHR-KO) mice attenuates phenotypic features of slow aging
title_sort specific suppression of insulin sensitivity in growth hormone receptor gene-disrupted (ghr-ko) mice attenuates phenotypic features of slow aging
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4326932/
https://www.ncbi.nlm.nih.gov/pubmed/25244225
http://dx.doi.org/10.1111/acel.12262
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