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唾液腺癌导管内癌中复发性 RET 基因重排。

Recurrent RET Gene Rearrangements in Intraductal Carcinomas of Salivary Gland.

机构信息

Department of Pathology, University Health Network.

Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, ON, Canada.

出版信息

Am J Surg Pathol. 2018 Apr;42(4):442-452. doi: 10.1097/PAS.0000000000000952.

Abstract

Intraductal carcinoma (IC) is the World Health Organization designation for lesions previously called low-grade cribriform cystadenocarcinoma. The relationship of IC to salivary duct carcinoma (SDC) is controversial, but currently these are considered distinct entities. It is hypothesized that IC and SDC should have different genomic signatures that may be identifiable by next-generation sequencing. A total of 23 ICs were identified: 14 pure IC and 9 invasive carcinomas with an intraductal component. Five invasive carcinomas were subjected to next-generation paired-end RNA sequencing. Data analysis was performed using FusionSeq and Mutation detection algorithms (MuTect and VarScan) for variant callers. Gene fusion candidates were validated by fluorescence in situ hybridization and reverse transcription polymerase chain reaction, and mutations by Sanger sequencing. Among the 9 invasive carcinomas, all except 1 were apocrine SDCs with an intraductal component. The remaining case showed typical intercalated duct type IC with invasive adenocarcinoma. The 14 pure ICs had typical intercalated duct features (2 showed hybrid intercalated/apocrine features). RNA sequencing predicted a NCOA4-RET fusion, confirmed by reverse transcription polymerase chain reaction, in the intercalated duct type IC invasive component. Six additional cases of pure IC showed RET rearrangement by fluorescence in situ hybridization (7/15=47%). No apocrine carcinomas showed RET rearrangement. RNA sequencing and Sanger sequencing identified PIK3CA (p.E545K/p.H1047R) and/or HRAS (p.Q61R) hotspot mutations in 6 of 8 (75%) apocrine carcinomas. In conclusion, 2 distinctive types of intraductal lesions are emerging based on molecular analysis. Classic intercalated type ICs commonly harbor fusions involving RET and rarely show widespread invasion. Apocrine intraductal lesions are typically associated with widespread invasion with no pure examples and show similar PIK3CA and HRAS mutations to SDC.

摘要

导管内癌(IC)是世界卫生组织为以前称为低级别筛状囊腺癌的病变指定的名称。IC 与唾液腺癌(SDC)的关系存在争议,但目前认为它们是不同的实体。据推测,IC 和 SDC 应该具有不同的基因组特征,这些特征可以通过下一代测序来识别。共鉴定出 23 例 IC:14 例纯 IC 和 9 例伴有导管内成分的浸润性癌。对 5 例浸润性癌进行了下一代配对末端 RNA 测序。使用 FusionSeq 和突变检测算法(MuTect 和 VarScan)对数据进行分析,作为变体调用器。通过荧光原位杂交和逆转录聚合酶链反应验证基因融合候选物,通过 Sanger 测序验证突变。在 9 例浸润性癌中,除 1 例外,均为伴有导管内成分的大汗腺癌。其余病例表现为典型的中间导管型 IC 伴浸润性腺癌。14 例纯 IC 具有典型的中间导管特征(2 例显示混合中间/大汗腺特征)。RNA 测序预测中间导管型 IC 浸润成分存在 NCOA4-RET 融合,通过逆转录聚合酶链反应证实。另外 6 例纯 IC 显示 RET 重排通过荧光原位杂交(7/15=47%)。没有大汗腺癌显示 RET 重排。RNA 测序和 Sanger 测序在 6 例(75%)大汗腺癌中鉴定出 PIK3CA(p.E545K/p.H1047R)和/或 HRAS(p.Q61R)热点突变。总之,基于分子分析,出现了 2 种不同类型的导管内病变。经典的中间导管型 IC 通常含有涉及 RET 的融合,很少有广泛浸润。大汗腺导管内病变通常与广泛浸润相关,没有纯例,与 SDC 具有相似的 PIK3CA 和 HRAS 突变。

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