The extracellular matrix molecules versican and hyaluronan in urethral and vaginal tissues in stress urinary incontinence

Purpose Abnormal extracellular matrix (ECM) changes are correlated with stress urinary incontinence (SUI). The ECM components versican (Vcan) and hyaluronan (HA) play key roles in regulating tissue inflammation and maintaining connective tissue homeostasis. We analyzed the localization and expressio...

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Bibliographic Details
Published in:Neurourology and urodynamics 2021-03, Vol.40 (3), p.771-782
Main Authors: Harten, Ingrid A., Evanko, Stephen P., Choe, Chong H., Lee, Eugene W., Patel, Bhavin N., Bogdani, Marika, Wight, Thomas N., Lee, Una J.
Format: Article
Language:English
Subjects:
Abundance
Connective tissues
Distension
Elastin
Enzymes
Epitopes
Extracellular matrix
Gene expression
Homeostasis
hyaluronan
Hyaluronic acid
Immunohistochemistry
inflammation
Localization
stress urinary incontinence
Urinary incontinence
Vagina
Versican
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Summary:Purpose Abnormal extracellular matrix (ECM) changes are correlated with stress urinary incontinence (SUI). The ECM components versican (Vcan) and hyaluronan (HA) play key roles in regulating tissue inflammation and maintaining connective tissue homeostasis. We analyzed the localization and expression of these ECM components in urethral and vaginal tissues from a rat model of urinary incontinence and from human clinical specimens. Methods Nulliparous rats underwent vaginal distension (VD), a rodent model of SUI, or a sham procedure. Tissues were harvested from six rats per group at days 1, 4, and 21 for immunohistochemistry and RNA expression analysis of ECM components. Periurethral vaginal samples from female patients with SUI were also examined. Results High‐intensity staining for Vcan was observed 1 day after procedure in both control and VD animals. This level of abundance persisted at day 4 in VD compared to control, with concurrent reduced messenger RNA (mRNA) expression of the Vcan‐degrading enzymes ADAMTS5 and ADAMTS9 and reduced staining for the Vcan cleavage epitope DPEAAE. Abundance of HA was not different between VD and control, however mRNA expression of the HA synthase Has2 was significantly reduced in VD tissues at day 4. Abundant Vcan staining was observed in 60% of SUI patient samples, which was strongest in regions of disrupted elastin. Conclusion Reduction of Vcan‐degrading enzymes and HA synthases at day 4 postsurgery indicates a potential delay in ECM turnover associated with SUI. Abundant Vcan is associated with inflammation and elastin fiber network disruption, warranting further investigation to determine its role in SUI pathogenesis.
ISSN:0733-2467
1520-6777
DOI:10.1002/nau.24635