Female sex hormones inversely regulate acute kidney disease susceptibility throughout life

激素 医学 内科学 内分泌学 肾脏疾病 生理学 疾病
作者
Yuichiro Kitai,Naoya Toriu,Takahisa Yoshikawa,Yoshiki Sahara,Sonoko Kinjo,Yoko Shimizu,Yuki Sato,Akiko Oguchi,Ryo Yamada,Makiko Kondo,Eiichiro Uchino,Keisuke Taniguchi,Hiroyuki Arai,Takayoshi Sasako,Hironori Haga,Shingo Fukuma,Naoto Kubota,Takashi Kadowaki,Minoru Takasato,Yasuhiro Murakawa,Motoko Yanagita
出处
期刊:Kidney International [Elsevier BV]
被引量:2
标识
DOI:10.1016/j.kint.2024.08.034
摘要

While epidemiological and experimental studies have demonstrated kidney-protective effects of estrogen and female sex in adulthood, some epidemiological data showed deterioration of kidney function during puberty when estrogen production increases. However, molecular mechanisms explaining these conflicting phenomena remain unknown. Here, we showed that the pubertal sex hormone surge in female mice increases susceptibility to kidney ischemia reperfusion injury partly via downregulation of insulin-like growth factor 1 receptor (IGF-1R) expression in proximal tubules. Adult mice ovariectomized pre-pubertally (at postnatal day 21) showed strong tolerance to kidney ischemia, which was partly reversed by the administration of 17β-estradiol, while adult mice ovariectomized post-pubertally (at 8 weeks of age) were vulnerable to kidney ischemia. Kidney tubular IGF-1R protein expression decreased during postnatal growth but was highly expressed in adult mice ovariectomized pre-pubertally and in infant mice, which might be partly explained by different expression of an E3 ligase (MDM2) of IGF-1R. Mice deficient of Igf-1r in proximal tubules (iIGF-1RKO mice) during postnatal kidney growth showed increased susceptibility to ischemic injury. RNA-seq and western blotting analysis using proximal tubular cells from pre-pubertally ovariectomized iIGF-1RKO and control mice revealed altered expression of cell cycle-associated molecules such as cyclin D1. These results suggest that Igf-1r deletion during postnatal growth renders proximal tubular cells susceptible to ischemia possibly via altered cell cycle regulation. Thus, our findings provide evidence that exposure to pubertal sex hormones leads to increased susceptibility to kidney ischemia, which is partly mediated by modulation of IGF-1R signaling.Graphical abstract
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