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头颈部区域 SMARCB1 缺陷型癌:一种细胞病理学特征。

SMARCB1-deficient carcinomas of the head and neck region: a cytopathologic characterization.

机构信息

Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, New York.

Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, New York.

出版信息

J Am Soc Cytopathol. 2020 Nov-Dec;9(6):494-501. doi: 10.1016/j.jasc.2020.07.134. Epub 2020 Jul 30.

Abstract

INTRODUCTION

SMARCB1 encodes for a component of the SWI/SNF complex and is widely implicated in carcinogenesis. In the head and neck, SMARCB1-deficient carcinomas typically arise in the sinonasal tract but can be found at other sites. EZH2 inhibitors have emerged as potential targeted therapy against SWI/SNF-deficient tumors. We sought to characterize the cytomorphology of head and neck carcinomas with SMARCB1 deficiencies to identify potential candidates for targeted therapy.

MATERIALS AND METHODS

Head and neck carcinomas with SMARCB1 mutations were retrospectively identified and confirmed to be SMARCB1-deficient by both molecular (fluorescent in-situ hybridization or next generation sequencing) and immunohistochemical means. Cases with positive cytology were reviewed and their cytologic features cataloged.

RESULTS

A total of 19 specimens from 13 patients were reviewed, including 8 specimens from 7 sinonasal carcinomas, 4 specimens from 3 thyroid carcinomas, 3 specimens from 2 skin carcinomas, and 4 specimens from 1 carcinoma of unknown primary origin. High-grade features were common, including mitoses (11 of 19) necrosis (13 of 19) and multinucleation (16 of 19). Tumors showed either dense cytoplasm with distinct cell borders (10 of 19) or delicate cytoplasm with indistinct cell borders (9 of 19). Most tumors showed no distinct epithelial differentiation (12 of 19), while some (7 of 19) showed glandular or signet ring features. A minor cohort demonstrated rhabdoid cells (4 of 19).

CONCLUSIONS

Head and neck carcinomas with SMARCB1 deficiencies have a wide array of morphologies and tend to demonstrate high-grade features. Only a minor cohort demonstrate rhabdoid-type cells. Evaluation of SMARCB1 deficiency for potential targeted therapy should not be limited to tumors with rhabdoid morphology.

摘要

简介

SMARCB1 编码 SWI/SNF 复合物的一个组成部分,广泛参与肿瘤发生。在头颈部,SMARCB1 缺陷型癌通常发生在鼻窦,但也可发生在其他部位。EZH2 抑制剂已成为针对 SWI/SNF 缺陷型肿瘤的潜在靶向治疗药物。我们旨在研究头颈部 SMARCB1 缺陷型癌的细胞形态学特征,以确定潜在的靶向治疗候选者。

材料和方法

回顾性地确定了具有 SMARCB1 突变的头颈部癌,并通过分子(荧光原位杂交或下一代测序)和免疫组织化学方法证实为 SMARCB1 缺陷型。对细胞学阳性的病例进行了回顾,并对其细胞学特征进行了分类。

结果

共对 13 名患者的 19 个标本进行了回顾,包括 7 例鼻窦癌的 8 个标本、3 例甲状腺癌的 4 个标本、2 例皮肤癌的 3 个标本和 1 例原发灶不明癌的 4 个标本。高级别特征很常见,包括有丝分裂(19 例中有 11 例)、坏死(19 例中有 13 例)和多核(19 例中有 16 例)。肿瘤表现为致密细胞质伴清晰的细胞边界(19 例中有 10 例)或细腻细胞质伴不清晰的细胞边界(19 例中有 9 例)。大多数肿瘤没有明显的上皮分化(19 例中有 12 例),而一些肿瘤(19 例中有 7 例)表现出腺状或印戒细胞特征。一小部分肿瘤表现出横纹肌样细胞(19 例中有 4 例)。

结论

SMARCB1 缺陷型头颈部癌具有广泛的形态学特征,往往表现出高级别特征。只有一小部分肿瘤表现出横纹肌样细胞。对于潜在的靶向治疗,SMARCB1 缺陷的评估不应仅限于具有横纹肌样形态的肿瘤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/268f/7572880/6f88923bd387/nihms-1617921-f0001.jpg

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