首页> 外文期刊>Virchows Archiv >Differentiated dysplasia is a frequent precursor or associated lesion in invasive squamous cell carcinoma of the oral cavity and pharynx
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Differentiated dysplasia is a frequent precursor or associated lesion in invasive squamous cell carcinoma of the oral cavity and pharynx

机译:异型增生是口腔和咽部浸润性鳞状细胞癌的常见前体或相关病变

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摘要

The source of precursor lesions of squamous cell carcinoma (SCC) of the oral cavity and pharynx, their classification, and grading are controversial. In contrast, vulvar and penile cancer precursor lesions are known to be related to human papillomavirus or chronic inflammation and can be described using the vulvar intraepithelial neoplasia (VIN) classification system (VIN 1–3) or as differentiated vulvar intraepithelial neoplasia (dVIN), respectively. Oral and pharyngeal SCC precursor lesions are more etiologically diverse, and the spectrum of lesions may thus be wider. No international consensus exists regarding the histological types of precursor lesions or the significance of individual types. We therefore reviewed resection specimens and preceding biopsies of 155 patients with SCC of the oral cavity and pharynx (excluding tonsils) and identified five basic patterns of SCC-associated or precursor lesions: (1) pleomorphic (22/155), (2) basaloid (5/155), (3) differentiated (63/155), (4) mixed (42/155), and (5) verrucous (12/155). Keratinization was a common but variable feature in differentiated, mixed, and verrucous dysplasia. In 11/155 patients, no precursor lesion could be identified. Progression of isolated differentiated dysplasia (ranging from months to years) was documented in 13/155 (8 %) of patients. Our data suggest that full-thickness epithelial dysplasia of pleomorphic or basaloid type is present in <20 % of oral and pharyngeal SCC, and differentiated dysplasia is a frequent precursor or associated in situ lesion. Failure to recognize differentiated dysplasia results in the underdiagnosis of many patients at risk for invasive carcinoma. These results indicate a need to refine criteria to distinguish differentiated dysplasia from morphologically related lichenoid lesions.
机译:口腔和咽部鳞状细胞癌(SCC)的前体病变的来源,其分类和分级存在争议。相比之下,外阴和阴茎癌前体病变已知与人类乳头瘤病毒或慢性炎症有关,可以使用外阴上皮内瘤变(VIN)分类系统(VIN 1–3)或分化型外阴上皮内瘤变(dVIN)进行描述,分别。口腔和咽SCC前体病变在病因上更加多样,因此病变范围可能更广。关于前体病变的组织学类型或单个类型的意义,没有国际共识。因此,我们审查了155例口腔和咽部SCC(扁桃体除外)患者的切除标本和先前的活检,并确定了SCC相关或前体病变的五种基本模式:(1)多形性(22/155),(2)基底基底样(5/155),(3)区分(63/155),(4)混合(42/155)和(5)疣状(12/155)。角化是分化,混合和疣状不典型增生的常见但可变的特征。在11/155名患者中,未发现前体病变。在13/155(8%)的患者中记录了孤立的分化异常增生的进展(数月至数年不等)。我们的数据表明,口腔和咽部鳞状细胞癌的<20%存在多形或基底型全厚度上皮发育不良,分化的发育异常是常见的前体或相关的原位病变。无法识别分化异常的增生导致许多处于浸润性癌风险中的患者的诊断不足。这些结果表明需要完善标准,以区分分化异常的增生和形态相关的苔藓样病变。

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