Hypoxanthine Induces Signs of Bladder Aging With Voiding Dysfunction and Lower Urinary Tract Remodeling.

IF 4.3 2区 医学 Q1 GERIATRICS & GERONTOLOGY Journals of Gerontology Series A-Biological Sciences and Medical Sciences Pub Date : 2024-06-01 DOI:10.1093/gerona/glad171
Lori A Birder, Amanda S Wolf-Johnston, Irina Zabbarova, Youko Ikeda, Anne M Robertson, Ricardo Cardozo, Fatemeh Azari, Anthony J Kanai, George A Kuchel, Edwin K Jackson
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Abstract

Background: Lower urinary tract syndrome (LUTS) is a group of urinary tract symptoms and signs that can include urinary incontinence. Advancing age is a major risk factor for LUTS; however, the underlying biochemical mechanisms of age-related LUTS remain unknown. Hypoxanthine (HX) is a purine metabolite associated with generation of tissue-damaging reactive oxygen species (ROS). This study tested the hypothesis that exposure of the adult bladder to HX-ROS over time damages key LUT elements, mimicking qualitatively some of the changes observed with aging.

Methods: Adult 3-month-old female Fischer 344 rats were treated with vehicle or HX (10 mg/kg/day; 3 weeks) administered in drinking water. Targeted purine metabolomics and molecular approaches were used to assess purine metabolites and biomarkers for oxidative stress and cellular damage. Biomechanical approaches assessed LUT structure and measurements of LUT function (using custom-metabolic cages and cystometry) were also employed.

Results: HX exposure increased biomarkers indicative of oxidative stress, pathophysiological ROS production, and depletion of cellular energy with declines in NAD+ levels. Moreover, HX treatment caused bladder remodeling and decreased the intercontraction interval and leak point pressure (surrogate measure to assess stress urinary incontinence).

Conclusions: These studies provide evidence that in adult rats chronic exposure to HX causes changes in voiding behavior and in bladder structure resembling alterations observed with aging. These results suggest that increased levels of uro-damaging HX were associated with ROS/oxidative stress-associated cellular damage, which may be central to age-associated development of LUTS, opening up potential opportunities for geroscience-guided interventions.

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次黄嘌呤诱发排尿功能障碍和下尿路重塑的膀胱衰老迹象
背景:下尿路综合征(LUTS)是一组尿路症状和体征,可包括尿失禁。年龄增长是导致下尿路综合征的一个主要风险因素,但与年龄相关的下尿路综合征的潜在生化机制仍不清楚。HX(次黄嘌呤)是一种嘌呤代谢物,与产生破坏组织的活性氧(ROS)有关。本研究测试了一个假设,即成年膀胱长期暴露于 HX-ROS 会损害 LUT 的关键元素,从而在质量上模仿衰老过程中观察到的一些变化:方法:成年 3 个月大的雌性费舍尔 344(F344)大鼠在饮用水中接受药物或 HX(10 毫克/千克/天;3 周)治疗。采用靶向嘌呤代谢组学和分子方法评估嘌呤代谢物以及氧化应激和细胞损伤的生物标志物。此外,还采用生物力学方法评估 LUT 结构,并测量 LUT 功能(使用定制代谢笼和膀胱测量法):结果:暴露于 HX 会增加表明氧化应激、病理生理 ROS 生成和细胞能量耗竭的生物标志物,并导致 NAD + 水平下降。此外,HX 治疗会导致膀胱重塑,并减少收缩间期和漏点压力(评估压力性尿失禁的替代指标):这些研究提供的证据表明,成年大鼠长期暴露于 HX 会导致排尿行为和膀胱结构发生变化,这些变化与衰老过程中观察到的变化相似。这些结果表明,泌尿系统损伤性 HX 水平的升高与 ROS/氧化应激相关的细胞损伤有关,这可能是与年龄相关的 LUTS 发展的核心原因,从而为地质科学指导的干预措施提供了潜在的机会。
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来源期刊
CiteScore
10.00
自引率
5.90%
发文量
233
审稿时长
3-8 weeks
期刊介绍: Publishes articles representing the full range of medical sciences pertaining to aging. Appropriate areas include, but are not limited to, basic medical science, clinical epidemiology, clinical research, and health services research for professions such as medicine, dentistry, allied health sciences, and nursing. It publishes articles on research pertinent to human biology and disease.
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