Keratocystoma: A Distinctive Salivary Gland Neoplasm Characterized by RUNX2 Rearrangements.

Justin A Bishop, Masato Nakaguro, Makoto Urano, Yoshinari Yamamoto, Yoshitaka Utsumi, Rong Li, Ilan Weinreb, Yoji Nagashima, Chiraag Gangahar, Katsushige Yamashiro, Kimio Hashimoto, Lisa M Rooper, Brian Carlile, Richard C Wang, Jeffrey Gagan, Toshitaka Nagao
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Abstract

Keratocystoma is a rare salivary gland lesion that has been reported primarily in children and young adults. Because of a scarcity of reported cases, very little is known about it, including its molecular underpinnings, biological potential, and histologic spectrum. Purported to be a benign neoplasm, keratocystoma bears a striking histologic resemblance to benign lesions like metaplastic Warthin tumor on one end of the spectrum and squamous cell carcinoma on the other end. This overlap can cause diagnostic confusion, and it raises questions about the boundaries and definition of keratocystoma as an entity. This study seeks to utilize molecular tools to evaluate the pathogenesis of keratocystoma as well as its relationship with its histologic mimics. On the basis of targeted RNA sequencing (RNA-seq) results on a sentinel case, RUNX2 break-apart fluorescence in situ hybridization (FISH) was successfully performed on 4 cases diagnosed as keratocystoma, as well as 13 cases originally diagnosed as tumors that morphologically resemble keratocystoma: 6 primary squamous cell carcinomas, 3 metaplastic/dysplastic Warthin tumors, 2 atypical squamous cysts, 1 proliferating trichilemmal tumor, and 1 cystadenoma. RNA-seq and/or reverse transcriptase-PCR were attempted on all FISH-positive cases. Seven cases were positive for RUNX2 rearrangement, including 3 of 4 tumors originally called keratocystoma, 2 of 2 called atypical squamous cyst, 1 of 1 called proliferating trichilemmal tumor, and 1 of 6 called squamous cell carcinoma. RNA-seq and/or reverse transcriptase-PCR identified IRF2BP2::RUNX2 in 6 of 7 cases; for the remaining case, the partner remains unknown. The cases positive for RUNX2 rearrangement arose in the parotid glands of 4 females and 3 males, ranging from 8 to 63 years old (mean, 25.4 years; median, 15 years). The RUNX2-rearranged cases had a consistent histologic appearance: variably sized cysts lined by keratinizing squamous epithelium, plus scattered irregular squamous nests, with essentially no cellular atypia or mitotic activity. The background was fibrotic, often with patchy chronic inflammation and/or giant cell reaction. One case originally called squamous cell carcinoma was virtually identical to the other cases, except for a single focus of small nerve invasion. The FISH-negative case that was originally called keratocystoma had focal cuboidal and mucinous epithelium, which was not found in any FISH-positive cases. The tumors with RUNX2 rearrangement were all treated with surgery only, and for the 5 patients with follow-up, there were no recurrences or metastases (1 to 120 months), even for the case with perineural invasion. Our findings solidify that keratocystoma is a cystic neoplastic entity, one which appears to consistently harbor RUNX2 rearrangements, particularly IRF2BP2::RUNX2. Having a diagnostic genetic marker now allows for a complete understanding of this rare tumor. They arise in the parotid gland and affect a wide age range. Keratocystoma has a consistent morphologic appearance, which includes large squamous-lined cysts that mimic benign processes like metaplastic Warthin tumor and also small, irregular nests that mimic squamous cell carcinoma. Indeed, RUNX2 analysis has considerable promise for resolving these differential diagnoses. Given that one RUNX2-rearranged tumor had focal perineural invasion, it is unclear whether that finding is within the spectrum of keratocystoma or whether it could represent malignant transformation. Most important, all RUNX2-rearranged cases behaved in a benign manner.
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角化囊肿:一种以 RUNX2 重排为特征的独特唾液腺肿瘤
角化囊瘤是一种罕见的唾液腺病变,主要发生在儿童和年轻人身上。由于报道的病例很少,对其知之甚少,包括其分子基础,生物学潜力和组织学谱。角化细胞瘤被认为是一种良性肿瘤,在组织学上与良性病变如化生沃氏瘤和鳞状细胞癌有惊人的相似之处。这种重叠可引起诊断混淆,并引起对角化囊瘤作为一个实体的界限和定义的疑问。本研究旨在利用分子工具来评估角化囊瘤的发病机制及其与组织模拟物的关系。在1例前哨病例靶向RNA测序(RNA-seq)结果的基础上,对4例确诊为角化囊瘤的患者,以及13例原诊断为形态类似角化囊瘤的患者,分别进行RUNX2分离荧光原位杂交(FISH),其中6例为原发性鳞状细胞癌,3例为化生/发育异常沃辛瘤,2例为非典型鳞状囊肿,1例为增生性毛突瘤,1例为囊腺瘤。对所有fish阳性病例进行RNA-seq和/或逆转录- pcr。RUNX2重排阳性7例,其中4例为角化囊瘤3例,2例为非典型鳞状囊肿2例,1例为增生性毛管肿瘤1例,6例为鳞状细胞癌1例。RNA-seq和/或逆转录- pcr在7例中鉴定出IRF2BP2::RUNX2;对于其余的病例,合作伙伴仍然未知。RUNX2重排阳性病例出现在腮腺中,女性4例,男性3例,年龄8 ~ 63岁,平均25.4岁;中位数,15年)。runx2重排的病例具有一致的组织学表现:大小不一的囊肿由角质化的鳞状上皮排列,加上分散的不规则鳞状巢,基本上没有细胞异型性或有丝分裂活性。背景为纤维化,常伴有斑片状慢性炎症和/或巨细胞反应。一个最初被称为鳞状细胞癌的病例几乎与其他病例相同,除了一个小的神经浸润病灶。最初称为角化细胞瘤的fish阴性病例具有局灶立方和粘液上皮,这在任何fish阳性病例中都没有发现。发生RUNX2重排的肿瘤均行手术治疗,随访5例患者,1 ~ 120个月无复发、无转移,甚至有侵袭神经周围的病例。我们的研究结果巩固了角化细胞瘤是一种囊性肿瘤实体,它似乎始终存在RUNX2重排,特别是IRF2BP2::RUNX2。现在有了一种诊断性的遗传标记,就可以对这种罕见的肿瘤有一个完整的了解。它们起源于腮腺,影响广泛的年龄范围。角化细胞瘤具有一致的形态学外观,包括大的鳞状内衬囊肿,类似良性过程,如化生沃氏瘤,也有小的,不规则的巢,类似鳞状细胞癌。事实上,RUNX2分析在解决这些鉴别诊断方面具有相当大的前景。考虑到一例runx2重排肿瘤有局灶性神经周围浸润,尚不清楚这一发现是否属于角化囊瘤的范围,或者是否代表恶性转化。最重要的是,所有runx2重新排列的情况都表现良好。
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