Increased renal cellular senescence in murine high-fat diet: effect of the senolytic drug quercetin

内分泌学 内科学 衰老 血脂异常 肾功能 医学 槲皮素 生物 糖尿病 生物化学 抗氧化剂
作者
Seo Rin Kim,Kai Jiang,Mikołaj Ogrodnik,Xiaojun Chen,Xiang-Yang Zhu,Hannah Lohmeier,Leena Ahmed,Hui Tang,Tamar Tchkonia,LaTonya J. Hickson,James L. Kirkland,Lilach O. Lerman
出处
期刊:Translational Research [Elsevier]
卷期号:213: 112-123 被引量:107
标识
DOI:10.1016/j.trsl.2019.07.005
摘要

Obesity and dyslipidemia can be associated with cellular senescence, and may impair kidney function. However, whether senescence contributes to renal dysfunction in these conditions remains unclear. Quercetin is an abundant dietary flavonoid that selectively clears inhibiting PI3K/AKT and p53/p21/serpines and inducing apoptosis. We hypothesized that high-fat-diet-induced obesity causes renal senescence, which would be mitigated by quercetin. C57BL/6J mice fed either standard chow or high-fat diets (HFDs) were treated with quercetin (50 mg/kg) or vehicle 5-days biweekly via oral gavage for 10 weeks. Subsequently, renal function was studied in vivo using magnetic resonance imaging, and renal senescence and histology were evaluated ex vivo. Mice fed with a HFD developed obesity and hypercholesterolemia, whereas renal size remained unchanged. Murine obesity impaired renal function and cortical oxygenation, and induced glomerulomegaly. Renal markers of senescence (eg, expression of p16, p19, and p53) and its secretory phenotype were upregulated in the obese hypercholesterolemic compared to lean mice in renal tubular cells, but attenuated in quercetin-treated murine kidneys, as was renal fibrosis. Quercetin treatment also increased renal cortical oxygenation and decreased plasma creatinine levels in obese mice, whereas body weight and cholesterol levels were unaltered. Therefore, murine obesity and dyslipidemia induce renal tissue senescence and impairs kidney function, which is alleviated by chronic senolytic treatment. These findings implicate senescence in loss of kidney function in murine dyslipidemia and obesity, and support further studies of senolytic therapy in obesity.
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