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喉黏液囊肿中的 DNA 罕见拷贝数改变。

DNA rare copy number alterations in Reinke's Edema.

机构信息

Faculdade de Ciências Médicas da Santa Casa de São Paulo, São Paulo, SP, Brazil; São Camilo Oncologia.

Universidade Estadual Paulista (UNESP), Faculdade de Medicina, Departamento de Especialidades Cirúrgicas e Anestesiologia, Botucatu, SP, Brazil.

出版信息

Braz J Otorhinolaryngol. 2023 Mar-Apr;89(2):279-284. doi: 10.1016/j.bjorl.2022.09.002. Epub 2022 Sep 22.

Abstract

INTRODUCTION

Reinke's Edema (RE) is a laryngeal lesion related to excessive tobacco smoking, voice overuse, and laryngopharyngeal reflux. Although the risk of malignancy has been considered low in literature, RE is classified among precancerous lesions.

OBJECTIVES

We investigated DNA Copy Number Alterations (CNAs) in specimens of RE and its potential association with malignant progression.

METHODS

We used array-based comparative genomic hybridization (aCGH, Agilent 4 × 180 K platform) to study eight RE cases. All patients were heavy tobacco users for at least 30 years, and none of them progressed to cancer in the follow-up (>8 years). Two RE presented mild dysplasia, one moderate dysplasia, and no histological alterations were found in the remaining five cases. CNAs were compared with the Database of Genomic Variants (DGV) and genes mapped on altered regions had their functions annotated.

RESULTS

Six of eight patients showed different rare copy number alterations on chromosomes 2q37.3, 4q13.1, 4q13.3, 7q11.22, 10p14, and 13q34. A gain of the whole chromosome 8 were detected in one case. Of interest, four of eight RE cases showed copy number imbalances involving genes previously described in several tumor types (RASA3, COL6A3, LINC00707, LINP1, SMR3A, and SMR3B).

CONCLUSION

The genomic imbalances herein found in RE have the potential to contribute to the phenotype but with limited or no risk of cancer. A long-term follow-up in a large series of patients could clarify the mechanisms involved in the malignant progression of RE.

摘要

简介

任克氏水肿(RE)是一种与过度吸烟、过度用嗓和喉咽反流有关的喉部病变。尽管文献中认为其恶变风险较低,但 RE 被归类为癌前病变。

目的

我们研究了 RE 标本中的 DNA 拷贝数改变(CNAs)及其与恶性进展的潜在关联。

方法

我们使用基于阵列的比较基因组杂交(aCGH,Agilent 4×180 K 平台)研究了 8 例 RE 病例。所有患者均为重度烟草使用者,吸烟史至少 30 年,在随访中(>8 年)均未发展为癌症。其中 2 例为轻度异型增生,1 例为中度异型增生,其余 5 例未见组织学改变。我们将 CNAs 与基因组变异数据库(DGV)进行比较,并对发生改变的区域上的基因进行功能注释。

结果

8 例患者中有 6 例在染色体 2q37.3、4q13.1、4q13.3、7q11.22、10p14 和 13q34 上显示出不同的罕见拷贝数改变。1 例患者出现整条 8 号染色体获得。有趣的是,8 例 RE 中有 4 例出现涉及多种肿瘤类型(RASA3、COL6A3、LINC00707、LINP1、SMR3A 和 SMR3B)的基因拷贝数失衡。

结论

RE 中发现的基因组失衡有可能导致表型改变,但恶变风险有限或不存在。对大量患者进行长期随访可能有助于阐明 RE 恶性进展中涉及的机制。

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