鉴别外阴上皮内瘤变的诊断和20种组织学特征的预测价值的跨亚专科观察者间的一致。

IF 3.7 3区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY
Shula A Schechter, May P Chan, Selvaraj Muthusamy, Stephanie L Skala, Grace Y Wang
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引用次数: 1

摘要

上下文。-:分化外阴上皮内瘤变(dVIN)是一种不依赖于人乳头瘤病毒的病变,有可能迅速发展为侵袭性鳞状细胞癌(SCC)。dVIN的组织病理学特征多样,与硬化性地衣(LS)和慢性单纯地衣(LSC)有重叠特征,由于外阴的解剖位置,可由皮肤病理学家或妇科病理学家诊断。-:确定dVIN的显著组织病理学特征,特别是那些预测SCC进展的特征,并评估在同一亚专科和跨亚专科诊断dVIN的观察者之间的一致性。1名普通外科病理学家、2名受过病理学训练的皮肤病理学家和1名对最终诊断不知情的妇科病理学家被要求记录20个组织病理学特征,并提供他们对dVIN (n = 65)、LS (n = 126)、LSC (n = 112)和LS合并LSC (n = 6)病例的最终解释。-: 4项诊断和10项组织病理特征的观察者间一致性中等。Logistic回归分析表明,角蛋白珍珠、基底多形性和基底层紊乱是诊断dVIN的自变量(系数分别为1.95、1.97和0.91;P < 0.001)和进展为SCC(系数分别为1.96、1.20和1.08;P < 0.001)。-: dVIN没有单一的病理组织学特征;然而,角蛋白珍珠、基底多形性和基底层紊乱的存在应引起对dVIN和并发SCC的高度怀疑。皮肤科和妇科病理学的专业知识对诊断dVIN是有益的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Interobserver Agreement Across Subspecialties for Diagnosis of Differentiated Vulvar Intraepithelial Neoplasia and Predictive Values of 20 Histologic Features.

Context.—: Differentiated vulvar intraepithelial neoplasia (dVIN) is a human papillomavirus-independent lesion with the potential for rapid progression to invasive squamous cell carcinoma (SCC). The histopathologic features of dVIN are diverse, have overlapping characteristics with lichen sclerosus (LS) and lichen simplex chronicus (LSC), and may be diagnosed by dermatopathologists or gynecologic pathologists because of the vulva's anatomic location.

Objectives.—: To identify the salient histopathologic features of dVIN, particularly those that predict progression to SCC, and to evaluate interobserver agreement in diagnosing dVIN within the same subspecialty and across subspecialties.

Design.—: One general surgical pathologist, 2 pathology-trained dermatopathologists, and 1 gynecologic pathologist blinded to the final diagnoses were asked to record 20 histopathologic features and to provide their final interpretations on cases of dVIN (n = 65), LS (n = 126), LSC (n = 112), and LS with LSC (n = 6).

Results.—: Interobserver agreement for the 4 diagnoses and 10 histopathologic features was moderate. Logistic regression analysis indicated that keratin pearls, basal pleomorphism, and basal layer disarray were independent variables for diagnosing dVIN (coefficients 1.95, 1.97, and 0.91, respectively; P < .001) and progression to SCC (coefficients 1.96, 1.20, and 1.08, respectively; P < .001).

Conclusions.—: There is no single histopathologic feature pathognomonic for dVIN; however, the presence of keratin pearls, basal pleomorphism, and basal layer disarray should raise high suspicion for dVIN and concurrent SCC. Expertise in both dermatologic and gynecologic pathology is beneficial for diagnosing dVIN.

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来源期刊
CiteScore
9.20
自引率
2.20%
发文量
369
审稿时长
3-8 weeks
期刊介绍: Welcome to the website of the Archives of Pathology & Laboratory Medicine (APLM). This monthly, peer-reviewed journal of the College of American Pathologists offers global reach and highest measured readership among pathology journals. Published since 1926, ARCHIVES was voted in 2009 the only pathology journal among the top 100 most influential journals of the past 100 years by the BioMedical and Life Sciences Division of the Special Libraries Association. Online access to the full-text and PDF files of APLM articles is free.
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