Vestibular Mast Cell Density in Vulvodynia: A Case-Controlled Study

Overview

Journal J Low Genit Tract Dis

Specialty Gynecology & Obstetrics

Date 2016 May 26

PMID 27224531

Citations 7

Authors

Dimitrios Papoutsis

Hope K Haefner

Christopher P Crum

Anthony W Opipari Jr

Barbara D Reed

Affiliations

Soon will be listed here.

Abstract

Objectives: To identify whether mast cell densities in vulvar biopsies from the vestibule are associated with vulvodynia.

Methods: We enrolled 100 women aged 19 to 59 years with confirmed vulvodynia cases, 100 racially matched controls, and 100 black control women. All had vulvar biopsies performed at the 7 o'clock position of the vestibule, which were then immunostained to detect c-KIT protein. The numbers of c-KIT positive mast cells per ×400 magnification field were manually counted, and t tests and logistic regression were used to assess the association with case-control status.

Results: Of the biopsies, 235 were adequate samples for c-KIT testing for mast cells. The mast cell density was substantially lower in black control women (13.9 ± 10.9) in comparison to white control women (22.5 ± 13.2 p < 0.001): hence the analysis was confined to white cases and racially matched control women. Compared with racially matched controls, cases were younger, more likely to be married, and reported a higher household income. The average number of mast cells per ×400 magnification field overall was 19.1 ± 13.2 (range, 0-62). There was no difference in the mast cell count between racially matched cases (22.4 ± 13.9 per ×400 field) and controls (22.5 ± 13.2) in either the univariate or multivariable analyses. Within the group of cases, there was no difference in mast cell density based on the presence or absence of a variety of urogenital symptoms.

Conclusions: No difference in mast cell density in biopsies of the vestibule was found between white cases and racially matched controls. Black control women have a lower mast cell density compared with white control women.

Citing Articles

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Chakrabarty A, Liao Z, Mu Y, Smith P J Pain. 2017; 19(3):264-277.

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