FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice

Male late-onset hypogonadism is an age-related disease, the core mechanism of which is dysfunction of senescent Leydig cells. Recent studies have shown that elimination of senescent cells can restore proper homeostasis to aging tissue. In the present study, we found that the fork head box O (FOXO) t...

Descripción completa

Detalles Bibliográficos
Autores principales: Zhang, Chi, Xie, Yun, Chen, Haicheng, Lv, Linyan, Yao, Jiahui, Zhang, Min, Xia, Kai, Feng, Xin, Li, Yanqing, Liang, Xiaoyan, Sun, Xiangzhou, Deng, Chunhua, Liu, Guihua
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals 2020
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7053614/
https://www.ncbi.nlm.nih.gov/pubmed/31959736
http://dx.doi.org/10.18632/aging.102682
_version_ 1783503070990172160
author Zhang, Chi
Xie, Yun
Chen, Haicheng
Lv, Linyan
Yao, Jiahui
Zhang, Min
Xia, Kai
Feng, Xin
Li, Yanqing
Liang, Xiaoyan
Sun, Xiangzhou
Deng, Chunhua
Liu, Guihua
author_facet Zhang, Chi
Xie, Yun
Chen, Haicheng
Lv, Linyan
Yao, Jiahui
Zhang, Min
Xia, Kai
Feng, Xin
Li, Yanqing
Liang, Xiaoyan
Sun, Xiangzhou
Deng, Chunhua
Liu, Guihua
author_sort Zhang, Chi
collection PubMed
description Male late-onset hypogonadism is an age-related disease, the core mechanism of which is dysfunction of senescent Leydig cells. Recent studies have shown that elimination of senescent cells can restore proper homeostasis to aging tissue. In the present study, we found that the fork head box O (FOXO) transcription factor FOXO4 was specially expressed in human Leydig cells and that its translocation to the nucleus in the elderly was related to decreased testosterone synthesis. Using hydrogen peroxide-induced senescent TM3 Leydig cells as an in vitro model, we observed that FOXO4 maintains the viability of senescent Leydig cells and suppresses their apoptosis. By disrupting the FOXO4-p53 interaction, FOXO4-DRI, a specific FOXO4 blocker, selectively induced p53 nuclear exclusion and apoptosis in senescent Leydig cells. In naturally aged mice, FOXO4-DRI improved the testicular microenvironment and alleviated age-related testosterone secretion insufficiency. These findings reveal the therapeutic potential of FOXO4-DRI for the treatment of male late-onset hypogonadism.
format Online
Article
Text
id pubmed-7053614
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Impact Journals
record_format MEDLINE/PubMed
spelling pubmed-70536142020-03-12 FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice Zhang, Chi Xie, Yun Chen, Haicheng Lv, Linyan Yao, Jiahui Zhang, Min Xia, Kai Feng, Xin Li, Yanqing Liang, Xiaoyan Sun, Xiangzhou Deng, Chunhua Liu, Guihua Aging (Albany NY) Research Paper Male late-onset hypogonadism is an age-related disease, the core mechanism of which is dysfunction of senescent Leydig cells. Recent studies have shown that elimination of senescent cells can restore proper homeostasis to aging tissue. In the present study, we found that the fork head box O (FOXO) transcription factor FOXO4 was specially expressed in human Leydig cells and that its translocation to the nucleus in the elderly was related to decreased testosterone synthesis. Using hydrogen peroxide-induced senescent TM3 Leydig cells as an in vitro model, we observed that FOXO4 maintains the viability of senescent Leydig cells and suppresses their apoptosis. By disrupting the FOXO4-p53 interaction, FOXO4-DRI, a specific FOXO4 blocker, selectively induced p53 nuclear exclusion and apoptosis in senescent Leydig cells. In naturally aged mice, FOXO4-DRI improved the testicular microenvironment and alleviated age-related testosterone secretion insufficiency. These findings reveal the therapeutic potential of FOXO4-DRI for the treatment of male late-onset hypogonadism. Impact Journals 2020-01-20 /pmc/articles/PMC7053614/ /pubmed/31959736 http://dx.doi.org/10.18632/aging.102682 Text en Copyright © 2020 Zhang et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Zhang, Chi
Xie, Yun
Chen, Haicheng
Lv, Linyan
Yao, Jiahui
Zhang, Min
Xia, Kai
Feng, Xin
Li, Yanqing
Liang, Xiaoyan
Sun, Xiangzhou
Deng, Chunhua
Liu, Guihua
FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice
title FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice
title_full FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice
title_fullStr FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice
title_full_unstemmed FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice
title_short FOXO4-DRI alleviates age-related testosterone secretion insufficiency by targeting senescent Leydig cells in aged mice
title_sort foxo4-dri alleviates age-related testosterone secretion insufficiency by targeting senescent leydig cells in aged mice
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7053614/
https://www.ncbi.nlm.nih.gov/pubmed/31959736
http://dx.doi.org/10.18632/aging.102682
work_keys_str_mv AT zhangchi foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT xieyun foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT chenhaicheng foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT lvlinyan foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT yaojiahui foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT zhangmin foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT xiakai foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT fengxin foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT liyanqing foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT liangxiaoyan foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT sunxiangzhou foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT dengchunhua foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice
AT liuguihua foxo4drialleviatesagerelatedtestosteronesecretioninsufficiencybytargetingsenescentleydigcellsinagedmice

Ejemplares similares