对神经增生性前庭大腺炎患者切除的前庭组织进行 CD117 和 PGP9.5 免疫组化染色。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Alexandra Drian, Sue W Goldstein, Noel N Kim, Andrew S Goldstein, Rose Hartzell-Cushanick, Alyssa Yee, Irwin Goldstein
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引用次数: 0

摘要

背景:神经增生性前庭大腺炎(NPV)是一种以严重异感和痛觉减退为特征的诱发性生殖器疼痛,切除的前庭组织可通过免疫组化染色(>8个CD117阳性免疫染色细胞/100×显微视野)而非苏木精和伊红染色确认:2019年6月至2022年12月期间接受前庭大扫除术的符合NPV标准的患者(n = 65)组成研究队列。我们采用免疫组化染色法评估前庭组织的病理学,包括通过 CD117(肥大细胞标记物)和蛋白基因产物 (PGP) 9.5(神经元标记物)定量肥大细胞和神经纤维。我们通过人工计数和计算机辅助组织测量法分析了 725 张免疫染色组织切片(100×和 200×)的显微照片,并将这些数据与临床评估结果进行了关联:结果:结果包括 1:00-11:00 点钟和 12:00 点钟前庭区域的 CD117 和 PGP9.5 免疫染色密度,以及评估性功能、疼痛、痛苦和症状改善的患者报告结果:所有65名NPV患者(中位年龄26岁)中,有45名终生性NPV患者和20名获得性NPV患者,均有PROs和外阴镜检查记录的剧烈疼痛,CD117免疫阳性细胞>8个/100×显微视野。1:00-11:00 点钟和 12:00 点钟前庭区域的细胞计数中位值相似(分别为 28.5 和 29.5 个/100×视野)。同样,通过蛋白基因产物(PGP)9.5(神经元标记物)也能检测到神经纤维。)我们通过人工计数和计算机辅助组织测量法分析了 725 张免疫染色组织切片(100×和 200×)的显微照片,并将这些数据与临床评估结果进行了关联:结果:结果包括 1:00-11:00 点钟和 12:00 点钟前庭区域的 CD117 和 PGP9.5 免疫染色密度,以及评估性功能、疼痛、痛苦和症状改善的患者报告结果:所有65名NPV患者(中位年龄26岁)中,有45名终生性NPV患者和20名获得性NPV患者,均有PROs和外阴镜检查记录的剧烈疼痛,CD117免疫阳性细胞>8个/100×显微视野。1:00-11:00 点钟和 12:00 前庭区域的细胞计数中位值相似(分别为 28.5 和 29.5 个/100×视野)。同样,CD117 免疫染色的中位面积在两个区域也相似(0.69% 和 0.73%)。在这些相同区域,PGP9.5 免疫染色的中位面积分别为 0.47% 和 0.31%。用棉签测试确定的疼痛评分在终身与获得性 NPV 患者中明显较高,在 1:00-11:00 点钟区域达到统计学意义(P < .001)。终身性 NPV 患者与获得性 NPV 患者相比,麦吉尔疼痛问卷情感分量表维度的中位数得分也明显更高(P = .011)。苏木精和伊红结果与肥大细胞或神经元标记物的密度之间没有相关性。值得注意的是,63%的患者群报告患有与肥大细胞异常活动相关的其他疾病:NPV的病理变化主要位于前庭上皮基底膜和上皮下基质,外阴镜检查无明显发现,因此临床诊断具有挑战性:这项研究的优点包括检查了大量组织,据我们所知,这是首次对 12:00 前庭进行评估。主要局限是标本来自疾病状态下的单一时间点,且缺乏对照组织:用 CD117 和 PGP9.5 对切除的前庭组织进行免疫组化染色,通过组织计量学方法确认了 NPV,表明 NPV 是一种涉及所有前庭区域的现场疾病,为那些疼痛被忽视并遭受负面社会心理影响的患者提供了验证,并使人们认识到这种染色可以促进知识的发展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunohistochemical staining with CD117 and PGP9.5 of excised vestibular tissue from patients with neuroproliferative vestibulodynia.

Background: Neuroproliferative vestibulodynia (NPV), a provoked genital pain characterized by severe allodynia and hyperalgesia, is confirmed in excised vestibular tissue by immunohistochemical staining (>8 CD117-positive immunostained cells/100× microscopic field) rather than by hematoxylin and eosin staining.

Aim: In this study we sought to assess immunostaining of tissue samples obtained during vestibulectomy surgery and to correlate results with patient outcomes.

Methods: Patients (n = 65) meeting criteria for NPV who underwent vestibulectomy during the period from June 2019 through December 2022 formed the study cohort. We performed assessment of pathology of vestibular tissues by use of immunohistochemical staining, including quantitation of mast cells by CD117 (mast cell marker) and nerve fibers by protein gene product (PGP) 9.5 (neuronal marker). We analyzed 725 photomicrographs of immunostained tissue sections (100× and 200×) by manual counting and computer-assisted histometry and correlated these data to clinical assessments.

Outcomes: Outcomes included density of CD117 and PGP9.5 immunostaining in the 1:00-11:00 o'clock and 12:00 o'clock vestibular regions, and patient-reported outcomes assessing sexual function, pain, distress, and symptom improvement.

Results: All 65 NPV patients (median age 26 years), 45 with lifelong and 20 with acquired NPV, had severe pain documented by PROs and vulvoscopy and had >8 CD117-immunopositive cells/100× microscopic field. Median cell count values were similar in the 1:00-11:00 o'clock and 12:00 vestibular regions (28.5 and 29.5/100× field, respectively). Likewise, the marker) and nerve fibers by protein gene product (PGP) 9.5 (neuronal marker). We analyzed 725 photomicrographs of immunostained tissue sections (100× and 200×) by manual counting and computer-assisted histometry and correlated these data to clinical assessments.

Outcomes: Outcomes included density of CD117 and PGP9.5 immunostaining in the 1:00-11:00 o'clock and 12:00 o'clock vestibular regions, and patient-reported outcomes assessing sexual function, pain, distress, and symptom improvement.

Results: All 65 NPV patients (median age 26 years), 45 with lifelong and 20 with acquired NPV, had severe pain documented by PROs and vulvoscopy and had >8 CD117-immunopositive cells/100× microscopic field. Median cell count values were similar in the 1:00-11:00 o'clock and 12:00 vestibular regions (28.5 and 29.5/100× field, respectively). Likewise, the median area of CD117 immunostaining was similar in both regions (0.69% and 0.73%). The median area of PGP9.5 immunostaining was 0.47% and 0.31% in these same regions. Pain scores determined with cotton-tipped swab testing were nominally higher in lifelong vs acquired NPV patients, reaching statistical significance in the 1:00-11:00 o'clock region (P < .001). The median score for the McGill Pain Questionnaire affective subscale dimension was also significantly higher in lifelong vs acquired NPV patients (P = .011). No correlations were observed between hematoxylin and eosin results and density of mast cells or neuronal markers. Of note, 63% of the patient cohort reported having additional conditions associated with aberrant mast cell activity.

Clinical implications: The pathology of NPV is primarily localized to the vestibular epithelial basement membrane and subepithelial stroma with no visible vulvoscopic findings, making clinical diagnosis challenging.

Strengths and limitations: Strengths of this study include the large number of tissues examined with what is to our knowledge the first-ever assessment of the 12:00 vestibule. Major limitations are specimens from a single timepoint within the disease state and lack of control tissues.

Conclusions: Performing immunohistochemical staining of excised vestibular tissue with CD117 and PGP9.5 led to histometric confirmation of NPV, indications that NPV is a field disease involving all vestibular regions, validation for patients whose pain had been ignored and who had experienced negative psychosocial impact, and appreciation that such staining can advance knowledge.

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