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

Author:

Birder Lori A12,Wolf-Johnston Amanda S1,Zabbarova Irina1,Ikeda Youko1,Robertson Anne M3,Cardozo Ricardo3,Azari Fatemeh3,Kanai Anthony J12,Kuchel George A4,Jackson Edwin K2

Affiliation:

1. Department of Medicine, University of Pittsburgh School of Medicine , Pittsburgh, Pennsylvania , USA

2. Department of Pharmacology and Chemical Biology, University of Pittsburgh School of Medicine , Pittsburgh , Pennsylvania , USA

3. Department of Mechanical Engineering and Materials Science, University of Pittsburgh , Pittsburgh, Pennsylvania , USA

4. UConn Center on Aging, University of Connecticut , Farmington, Connecticut , USA

Abstract

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.

Funder

National Institutes of Health

Publisher

Oxford University Press (OUP)

Subject

Geriatrics and Gerontology,Aging

Reference47 articles.

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