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牙源性角化囊肿和角化性成釉细胞瘤的实体型是否应归类为同一实体?九例临床病理分析及文献复习。

Should the solid variant of odontogenic keratocyst and keratoameloblastoma be classified as the same entity? A clinicopathological analysis of nine cases and a review of the literature.

机构信息

Department of Oral Pathology, Peking University School and Hospital of Stomatology, Beijing, China; Research Unit of Precision Pathologic Diagnosis in Tumors of the Oral and Maxillofacial Regions, Chinese Academy of Medical Sciences, Beijing, China; National Clinical Research Center for Oral Diseases, Peking University School and Hospital of Stomatology, Beijing, China.

Department of Oral Pathology, Peking University School and Hospital of Stomatology, Beijing, China.

出版信息

Pathology. 2021 Jun;53(4):478-486. doi: 10.1016/j.pathol.2020.09.028. Epub 2021 Feb 5.

Abstract

The solid variant of odontogenic keratocyst (SOKC) is an extremely rare odontogenic lesion, which remains poorly defined even in the 2017 World Health Organization odontogenic tumour classification. It is difficult to distinguish between SOKC and so called keratoameloblastoma (KAB), both rare lesions that have similarities in clinical, histological and biological characteristics. Here, we report clinicopathological data and results of molecular analysis of nine cases with a literature review. First, they were compared to previously reported cases of SOKC and/or KAB, and many overlaps were found in clinical and pathological characteristics. Second, we performed PCR analysis for BRAF V600E mutation. Although ameloblastoma-like epithelia were often encountered, none exhibited BRAF V600E mutation, which has been reported to occur frequently in ameloblastomas but not in odontogenic keratocysts (OKCs). One of two cases of SOKC in the present series from which fresh frozen tissue specimens were available was found to harbour PTCH1 mutations, indicating that these were more likely to be a subtype of OKC. Moreover, we also examined the differences between SOKC and primary intraosseous carcinoma (PIOC) with regard to the expression of cytokeratins (pan-CK, CK5/6, CK7, CK8/18, CK10, CK14 and CK19), p53 and Ki-67. The proportions of p53-and Ki-67-positive cells were significantly higher in PIOC than in SOKC. These findings suggest that immunostaining for p53 and Ki-67 would be useful to differentiate between SOKC and PIOC. We also conducted a review of SOKC and KAB cases reported in the English language literature.

摘要

牙源性角化囊性瘤的实体型(SOKC)是一种极为罕见的牙源性肿瘤,即使在 2017 年世界卫生组织牙源性肿瘤分类中,其定义仍不明确。SOKC 与所谓的角化性成釉细胞瘤(KAB)之间难以区分,这两种罕见病变在临床、组织学和生物学特征上具有相似性。在此,我们报告了 9 例病例的临床病理数据和分子分析结果,并进行了文献复习。首先,将其与先前报道的 SOKC 和/或 KAB 病例进行比较,发现临床和病理特征存在许多重叠。其次,我们进行了 BRAF V600E 突变的 PCR 分析。尽管经常遇到类似于成釉细胞瘤的上皮,但均未显示 BRAF V600E 突变,该突变已报道在成釉细胞瘤中频繁发生,但不在牙源性角化囊肿(OKC)中发生。本研究系列中来自两个 SOKC 病例的新鲜冷冻组织标本中,有一个发现存在 PTCH1 突变,这表明它们更可能是 OKC 的一个亚型。此外,我们还研究了 SOKC 和原发性骨内癌(PIOC)在细胞角蛋白(pan-CK、CK5/6、CK7、CK8/18、CK10、CK14 和 CK19)、p53 和 Ki-67 表达方面的差异。PIOC 中 p53 和 Ki-67 阳性细胞的比例明显高于 SOKC。这些发现表明,p53 和 Ki-67 的免疫染色有助于区分 SOKC 和 PIOC。我们还对英文文献中报道的 SOKC 和 KAB 病例进行了复习。

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