(005) Immunohistochemical Staining of the 12:00 Vestibule in NPV Patients: First Ever Assessment

Abstract

Abstract Introduction In 2004, Bornstein and colleagues performed immunohistochemical (IHC) staining of excised vestibular specimens in patients with vestibular pain. They demonstrated that these specimens contained > 8 CD117 immunopositive stained cells per high-power field (HPF), consistent with mast cells, and excess S100 stained immunopositive cells, consistent with nerves-far more compared to control tissue. However, Bornstein et al. only studied the 1:00-11:00 vestibule in this condition, now referred to as neuroproliferative vestibulodynia (NPV). To the best of our knowledge, the 12:00 region of the vestibule, below the clitoral frenulae and above the urethral meatus, has not been examined with IHC staining. Pain in the 12:00 region can be particularly bothersome for patients and poses several challenges for successful treatment. Objective To report IHC staining findings in the excised 12:00 vestibule specimen and associated clinical characteristics of NPV patients. Methods Retrospective chart review performed. Slides of IHC-stained vestibular tissue specimens from the 12:00 vestibule were examined and high-resolution digital microscopy images were captured under 100x and 200x magnification. A least 2 photomicrographs at both magnifications were taken for each slide that included representative areas of epithelial basement membrane and the adjacent subepithelial regions. Fractional area of positive immunostaining in all photomicrographs was assessed and mean values calculated using computer-assisted histometry by ImageJ. Results A total of 50 patients had complete vestibulectomy including 12:00 and 3 had regional vestibulectomy for only the 12:00 area. Using manual counting as applied by Bornstein et al., 53 excised 12:00 specimens stained for CD117 had a median immunopositive cell count, consistent with mast cells, of 29.5, greater than the described 8 mast cells per HPF. Using computer-assisted histometry, tissue stained for CD117 had a median fractional area of 0.73 in the 12:00 region. Tissues stained for PGP9.5 had a median fractional area of 0.31 in the 12:00 region. Overall, there was no difference between lifelong NPV (LNPV) and acquired NPV (ANPV) patients in the cell count or median fractional area for CD117-immunopositive or PGP9.5-immunopositive staining in the 12:00 region. In LNPV patients who had excision of both the 1:00-11:00 and 12:00 regions, the 12:00 region had significantly less PGP9.5 immunopositive fractional area than the 1:00-11:00 region of the vestibule (p = 0.001). Their H&E pathology findings, including severity grading of the subepithelial inflammatory infiltrate, did not predict the IHC assessment of either CD117 or PGP9.5 in the 12:00 region. The median cotton-tipped swab test pain score was 5 out of 10 for the 12:00 region vs 7 for the rest of the vestibule. Conclusions Current surgical practices often do not include the 12:00 region, likely due to lack of data demonstrating excess mast cells and nerves in this specific region. Our results suggest that there are, in fact, a high density of immunopositive histochemical stains consistent with mast cells and nerves in the 12:00 region and high reported pain scores in both 12:00 and 1:00-11:00 vestibule. Thus, NPV surgical treatments should include, when appropriate, the 12:00 vestibule, as NPV is a field disease involving the entire vestibule. Disclosure No.