Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period

Reproduction requires adequate energy stores for parents and offspring to survive. Kiss1 neurons, which are essential for fertility, have the potential to serve as the central sensors of metabolic factors that signal to the reproductive axis the presence of stored calories. Paradoxically, obesity is...

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Autores principales: Qiu, Xiaoliang, Dao, Hoangha, Wang, Mengjie, Heston, Amelia, Garcia, Kaitlyn M., Sangal, Alisha, Dowling, Abigail R., Faulkner, Latrice D., Molitor, Scott C., Elias, Carol F., Hill, Jennifer W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4422586/
https://www.ncbi.nlm.nih.gov/pubmed/25946091
http://dx.doi.org/10.1371/journal.pone.0121974
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author Qiu, Xiaoliang
Dao, Hoangha
Wang, Mengjie
Heston, Amelia
Garcia, Kaitlyn M.
Sangal, Alisha
Dowling, Abigail R.
Faulkner, Latrice D.
Molitor, Scott C.
Elias, Carol F.
Hill, Jennifer W.
author_facet Qiu, Xiaoliang
Dao, Hoangha
Wang, Mengjie
Heston, Amelia
Garcia, Kaitlyn M.
Sangal, Alisha
Dowling, Abigail R.
Faulkner, Latrice D.
Molitor, Scott C.
Elias, Carol F.
Hill, Jennifer W.
author_sort Qiu, Xiaoliang
collection PubMed
description Reproduction requires adequate energy stores for parents and offspring to survive. Kiss1 neurons, which are essential for fertility, have the potential to serve as the central sensors of metabolic factors that signal to the reproductive axis the presence of stored calories. Paradoxically, obesity is often accompanied by infertility. Despite excess circulating levels of insulin and leptin, obese individuals exhibit resistance to both metabolic factors in many neuron types. Thus, resistance to insulin or leptin in Kiss1 neurons could lead to infertility. Single deletion of the receptors for either insulin or the adipokine leptin from Kiss1 neurons does not impair adult reproductive dysfunction. However, insulin and leptin signaling pathways may interact in such a way as to obscure their individual functions. We hypothesized that in the presence of genetic or obesity-induced concurrent insulin and leptin resistance, Kiss1 neurons would be unable to maintain reproductive function. We therefore induced a chronic hyperinsulinemic and hyperleptinemic state in mice lacking insulin receptors in Kiss1 neurons through high fat feeding and examined the impact on fertility. In an additional, genetic model, we ablated both leptin and insulin signaling in Kiss1 neurons (IR/LepR(Kiss) mice). Counter to our hypothesis, we found that the addition of leptin insensitivity did not alter the reproductive phenotype of IR(Kiss) mice. We also found that weight gain, body composition, glucose and insulin tolerance were normal in mice of both genders. Nonetheless, leptin and insulin receptor deletion altered pubertal timing as well as LH and FSH levels in mid-puberty in a reciprocal manner. Our results confirm that Kiss1 neurons do not directly mediate the critical role that insulin and leptin play in reproduction. However, during puberty kisspeptin neurons may experience a critical window of susceptibility to the influence of metabolic factors that can modify the onset of fertility.
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spelling pubmed-44225862015-05-12 Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period Qiu, Xiaoliang Dao, Hoangha Wang, Mengjie Heston, Amelia Garcia, Kaitlyn M. Sangal, Alisha Dowling, Abigail R. Faulkner, Latrice D. Molitor, Scott C. Elias, Carol F. Hill, Jennifer W. PLoS One Research Article Reproduction requires adequate energy stores for parents and offspring to survive. Kiss1 neurons, which are essential for fertility, have the potential to serve as the central sensors of metabolic factors that signal to the reproductive axis the presence of stored calories. Paradoxically, obesity is often accompanied by infertility. Despite excess circulating levels of insulin and leptin, obese individuals exhibit resistance to both metabolic factors in many neuron types. Thus, resistance to insulin or leptin in Kiss1 neurons could lead to infertility. Single deletion of the receptors for either insulin or the adipokine leptin from Kiss1 neurons does not impair adult reproductive dysfunction. However, insulin and leptin signaling pathways may interact in such a way as to obscure their individual functions. We hypothesized that in the presence of genetic or obesity-induced concurrent insulin and leptin resistance, Kiss1 neurons would be unable to maintain reproductive function. We therefore induced a chronic hyperinsulinemic and hyperleptinemic state in mice lacking insulin receptors in Kiss1 neurons through high fat feeding and examined the impact on fertility. In an additional, genetic model, we ablated both leptin and insulin signaling in Kiss1 neurons (IR/LepR(Kiss) mice). Counter to our hypothesis, we found that the addition of leptin insensitivity did not alter the reproductive phenotype of IR(Kiss) mice. We also found that weight gain, body composition, glucose and insulin tolerance were normal in mice of both genders. Nonetheless, leptin and insulin receptor deletion altered pubertal timing as well as LH and FSH levels in mid-puberty in a reciprocal manner. Our results confirm that Kiss1 neurons do not directly mediate the critical role that insulin and leptin play in reproduction. However, during puberty kisspeptin neurons may experience a critical window of susceptibility to the influence of metabolic factors that can modify the onset of fertility. Public Library of Science 2015-05-06 /pmc/articles/PMC4422586/ /pubmed/25946091 http://dx.doi.org/10.1371/journal.pone.0121974 Text en © 2015 Qiu et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Qiu, Xiaoliang
Dao, Hoangha
Wang, Mengjie
Heston, Amelia
Garcia, Kaitlyn M.
Sangal, Alisha
Dowling, Abigail R.
Faulkner, Latrice D.
Molitor, Scott C.
Elias, Carol F.
Hill, Jennifer W.
Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period
title Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period
title_full Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period
title_fullStr Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period
title_full_unstemmed Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period
title_short Insulin and Leptin Signaling Interact in the Mouse Kiss1 Neuron during the Peripubertal Period
title_sort insulin and leptin signaling interact in the mouse kiss1 neuron during the peripubertal period
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4422586/
https://www.ncbi.nlm.nih.gov/pubmed/25946091
http://dx.doi.org/10.1371/journal.pone.0121974
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