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肺类癌不典型和大细胞神经内分泌癌的基因表达谱分析确定了具有特定基因组改变的三种转录组亚型。

Gene Expression Profiling of Lung Atypical Carcinoids and Large Cell Neuroendocrine Carcinomas Identifies Three Transcriptomic Subtypes with Specific Genomic Alterations.

机构信息

Department of Diagnostics and Public Health, Section of Anatomical Pathology, University and Hospital Trust of Verona, Verona, Italy.

ARC-Net Research Centre, University and Hospital Trust of Verona, Verona, Italy.

出版信息

J Thorac Oncol. 2019 Sep;14(9):1651-1661. doi: 10.1016/j.jtho.2019.05.003. Epub 2019 May 11.

DOI:10.1016/j.jtho.2019.05.003
PMID:31085341
Abstract

INTRODUCTION

DNA mutational profiling showed that atypical carcinoids (ACs) share alterations with large cell neuroendocrine carcinomas (LCNECs). Transcriptomic studies suggested that LCNECs are composed of two subtypes, one of which shares molecular anomalies with SCLC. The missing piece of information is the transcriptomic relationship between ACs and LCNECs, as a direct comparison is lacking in the literature.

METHODS

Transcriptomic and genomic alterations were investigated by next-generation sequencing in a discovery set of 14 ACs and 14 LCNECs and validated on 21 ACs and 18 LCNECs by using custom gene panels and immunohistochemistry for Men1 and Rb1.

RESULTS

A 58-gene signature distinguished three transcriptional clusters. Cluster 1 comprised 20 LCNECs and one AC harboring concurrent inactivation of tumor protein p53 gene (TP53) and retinoblastoma 1 gene (RB1) in the absence of menin 1 gene (MEN1) mutations; all cases lacked Rb1 nuclear immunostaining. Cluster 3 included 20 ACs and four LCNECs lacking RB1 alterations and having frequent MEN1 (37.5%) and TP53 mutations (16.7%); menin nuclear immunostaining was lost in 75% of cases. Cluster 2 included 14 ACs and eight LCNECs showing intermediate features: TP53, 40.9%; MEN1, 22.7%; and RB1, 18.2%. Patients in cluster C1 had a shorter cancer-specific survival than did patients in C2 or C3.

CONCLUSIONS

ACs and LCNECs comprise three different and clinically relevant molecular diseases, one AC-enriched group in which MEN1 inactivation plays a major role, one LCNEC-enriched group whose hallmark is RB1 inactivation, and one mixed group with intermediate molecular features. These data support a progression of malignancy that may be traced by using combined molecular and immunohistochemical analysis.

摘要

介绍

DNA 突变分析显示非典型类癌(AC)与大细胞神经内分泌癌(LCNEC)具有相同的改变。转录组研究表明 LCNEC 由两个亚型组成,其中一个亚型与小细胞肺癌(SCLC)具有分子异常。目前缺少 AC 和 LCNEC 之间转录组关系的相关信息,因为文献中缺乏直接比较。

方法

通过下一代测序对 14 例 AC 和 14 例 LCNEC 进行了转录组和基因组改变的研究,并使用定制基因面板和 Men1 和 Rb1 的免疫组织化学对 21 例 AC 和 18 例 LCNEC 进行了验证。

结果

一个包含 58 个基因的特征区分了三个转录簇。簇 1 包括 20 例 LCNEC 和 1 例同时存在肿瘤蛋白 p53 基因(TP53)和视网膜母细胞瘤 1 基因(RB1)失活而无 Men1 基因(MEN1)突变的 AC;所有病例均缺乏 Rb1 核免疫染色。簇 3 包括 20 例 AC 和 4 例缺乏 RB1 改变且 MEN1 频繁(37.5%)和 TP53 突变(16.7%)的 LCNEC;75%的病例失去了 menin 核免疫染色。簇 2 包括 14 例 AC 和 8 例显示中间特征的 LCNEC:TP53,40.9%;MEN1,22.7%;和 RB1,18.2%。C1 簇的患者癌症特异性生存率低于 C2 或 C3 簇的患者。

结论

AC 和 LCNEC 包含三种不同且具有临床意义的分子疾病,一种富含 AC 的疾病,其中 MEN1 失活起主要作用,一种富含 LCNEC 的疾病,其特征是 RB1 失活,一种混合组具有中间分子特征。这些数据支持恶性肿瘤的进展,可通过联合分子和免疫组织化学分析进行追踪。

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