Purine nucleoside phosphorylase inhibition ameliorates age-associated lower urinary tract dysfunctions
Lori A. Birder, … , Roger R. Dmochowski, Edwin K. Jackson
Lori A. Birder, … , Roger R. Dmochowski, Edwin K. Jackson
Published September 10, 2020
Citation Information: JCI Insight. 2020;5(20):e140109. https://doi.org/10.1172/jci.insight.140109.
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Research Article Aging

Purine nucleoside phosphorylase inhibition ameliorates age-associated lower urinary tract dysfunctions

Abstract

In the aging population, lower urinary tract (LUT) dysfunction is common and often leads to storage and voiding difficulties classified into overlapping symptom syndromes. Despite prevalence and consequences of these syndromes, LUT disorders continue to be undertreated simply because there are few therapeutic options. LUT function and structure were assessed in aged (>25 months) male and female Fischer 344 rats randomized to oral treatment with a purine nucleoside phosphorylase (PNPase inhibitor) 8-aminoguanine (8-AG) or vehicle for 6 weeks. The bladders of aged rats exhibited multiple abnormalities: tactile insensitivity, vascular remodeling, reduced collagen-fiber tortuosity, increased bladder stiffness, abnormal smooth muscle morphology, swelling of mitochondria, and increases in urodamaging purine metabolites. Treatment of aged rats with 8-AG restored all evaluated histological, ultrastructural, and physiological abnormalities toward that of a younger state. 8-AG is an effective treatment that ameliorates key age-related structural and physiologic bladder abnormalities. Because PNPase inhibition blocks metabolism of inosine to hypoxanthine and guanosine to guanine, likely uroprotective effects of 8-AG are mediated by increased bladder levels of uroprotective inosine and guanosine and reductions in urodamaging hypoxanthine and xanthine. These findings demonstrate that 8-AG has translational potential for treating age-associated LUT dysfunctions and resultant syndromes in humans.

Authors

Lori A. Birder, Amanda Wolf-Johnston, Alan J. Wein, Fangzhou Cheng, Mara Grove-Sullivan, Anthony J. Kanai, Alan M. Watson, Donna Stoltz, Simon C. Watkins, Anne M. Robertson, Diane Newman, Roger R. Dmochowski, Edwin K. Jackson

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Figure 4

Western immunoblotting revealed significant aging-associated alterations in proteins linked to mitochondrial dynamics and quality control within the bladder mucosa.

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Western immunoblotting revealed significant aging-associated alterations...
(A–D) Mitofusin 2 (MFN2; n = young 14; aged 16; aged + 8-AG 16) (A), a protein involved in mitochondrial fusion; Dynamin-|related protein (B) (DRP-1; n = young 4; aged 5; aged + 8-AG 4), which is involved in mitochondrial fission; Parkin (C) (n = young 4; aged 5; aged + 8-AG 4), which plays a role in mitophagy; and cleaved caspase-3 (D) (n = young 8; aged 9; aged + 8-AG 8), which is activated upon initiation of apoptosis. In all cases, treatment with 8-aminoguanine (8-AG) restored changes similar to a younger state. Representative immunoblotting is inset within each graph. Cleaved caspase-3 (top of inset) is normalized to total caspase-3 (bottom of inset). All samples were run on the same blot, but representative samples were not contiguous. Data are presented as mean ± SEM. Ordinary 1-way ANOVA was used to evaluate significance. *P < 0.05; **P < 0.01.