Ossabaw Pig Demonstrates Detrusor Fibrosis and Detrusor Underactivity Associated with Oxidative Stress in Metabolic Syndrome

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Abstract

Metabolic Syndrome (MetS) has detrimental effects on the bladder, including detrusor underactivity. The progression and mechanism of disease are poorly understood. A swine model for diabetic bladder dysfunction (DBD) was established because of the pig's human-sized bladder and its ability to develop MetS by dietary modification alone. The hypothesis of this study is that this swine model will demonstrate oxidative stress associated with MetS, which contributes to both bladder fibrosis and detrusor underactivity (DU). Ossabaw pigs underwent dietary modification consisting of a hypercaloric, atherogenic diet for 10 mo to induce MetS, and were compared with a group of control (lean) pigs. Urodynamic studies were performed in both groups to confirm DU. Thiobarbituric acid reactive substances (TBARS) detected in the urine were used to measure oxidative stress activity in the urinary tract, and urinary IL17a was used to detect profibrotic activity. MetS was confirmed by assessing body weight, blood pressure, glucose tolerance, total cholesterol, and triglycerides. The MetS group exhibited an increase in the relative levels of urinary TBARS and IL17a. Bladder pressures at capacity were lower in the MetS group, suggesting DU. Histologic analysis of a cohort of control (lean) and MetS pigs revealed that as compared with the control pigs, the MetS pigs had significantly more collagen in the muscularis layer, but not in the submucosa or mucosa layer. In conclusion, the Ossabaw pig model for diet-induced MetS is associated with oxidative stress and profibrotic activity in the bladder, which results in DU. This has previously been shown in mice and rats, but never in pigs. This novel model will better represent human MetS and DBD because the mechanism and size of the pig bladder more closely resemble that of a human, resulting in a more valid model and facilitating further study into the signaling mechanisms responsible for this impairment.

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Journal

Journal ID (nlm-ta): Comp Med

Journal ID (iso-abbrev): Comp Med

Journal ID (publisher-id): cm

Title: Comparative Medicine

Publisher: American Association for Laboratory Animal Science

ISSN (Print): 1532-0820

Publication date (Print): October 2020

Publication date (Electronic): October 2020

Volume: 70

Issue: 5

Pages: 329-334

Affiliations

[1 ]Indiana University School of Medicine Department of Urology, Indianapolis, Indiana

[2 ]Temple University College of Engineering, Philadelphia, Pennsylvania

[3 ]Department of Anatomy, Cell Biology, and Physiology, and

[4 ]Department of Medicine, Endocrinology Division, Indiana University School of Medicine, Indianapolis, Indiana

[5 ]Purdue Weldon School of Biomedical Engineering, Purdue University, West Lafayette, Indiana

[6 ]University of Michigan, Department of Pulmonary and Critical Care Medicine, Ann Arbor, Michigan

Author notes

[* ]Corresponding author. Email: crpowell@ 123456iupui.edu

This article contains supplemental materials online.

Article

Accession ID: PMC7574218 Pmcid ID: PMC7574218 Pmc-uid ID: 7574218 Publisher ID: 2020000329

DOI: 10.30802/AALAS-CM-20-000004

PMC ID: 7574218

PubMed ID: 32972487

SO-VID: 2b9d1659-9703-4d42-a6c5-a2be15168600

History

Date received : 19 January 2020

Date revision received : 25 March 2020

Date accepted : 21 April 2020

Page count

Pages: 6

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