Mutational Profiling of Driver Tumor Suppressor and Oncogenic Genes in Brazilian Malignant Pleural Mesotheliomas.

Pathobiology : journal of immunopathology, molecular and cellular biology Pub Date : 2020-01-01 Epub Date: 2020-05-05 DOI:10.1159/000507373

Nathália C Campanella, Eduardo Caetano Silva, Gustavo Dix, Fabiana de Lima Vazquez, Flávia Escremim de Paula, Gustavo N Berardinelli, Marcelo Balancin, Roger Chammas, Rossana V Mendoza Lopez, Henrique César S Silveira, Vera Luiza Capelozzi, Rui Manuel Reis

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引用次数: 12

Abstract

Background: Malignant pleural mesothelioma (MPM) is a highly lethal disease comprising a heterogeneous group of tumors with challenging to predict biological behavior. The diagnosis is complex, and the histologic classification includes 2 major subtypes of MPM: epithelioid (∼60% of cases) and sarcomatous (∼20%). Its identification depends upon pathological investigation supported by clinical and radiological evidence and more recently ancillary molecular testing. Treatment options are currently limited, with no known targeted therapies available.

Objectives: To elucidate the mutation profile of driver tumor suppressor and oncogenic genes in a cohort of Brazilian patients.

Methods: We sequenced 16 driver genes in a series of 43 Brazilian malignant mesothelioma (MM) patients from 3 distinct Brazilian centers. Genomic DNA was extracted from formalin-fixed paraffin-embedded tumor tissue blocks, and the TERT promoter region was amplified by PCR followed by direct capillary sequencing. The Illumina TruSight Tumor 15 was used to evaluate 250 amplicons from 15 genes associated with solid tumors (AKT1, GNA11, NRAS, BRAF, GNAQ, PDGFRA, EGFR, KIT, PIK3CA, ERBB2, KRAS, RET, FOXL2, MET,and TP53). Library preparation with the TruSight Tumor 15 was performed before sequencing at the MiSeq platform. Data analysis was performed using Sophia DDM software.

Results: Out of 43 MPM patients, 38 (88.4%) were epithelioid subtype and 5 (11.6%) were sarcomatoid histotype. Asbestos exposure was present in 15 (39.5%) patients with epithelioid MPM and 3 (60%) patients with sarcomatoid MPM. We found a TERT promoter mutation in 11.6% of MM, and the c.-146C>T mutation was the most common event. The next-generation sequencing was successful in 33 cases. A total of 18 samples showed at least 1 pathogenic, with a median of 1.8 variants, ranging from 1 to 6. The most mutated genes were TP53 and ERBB2 with 7 variants each, followed by NRAS BRAF, PI3KCA, EGFR and PDGFRA with 2 variants each. KIT, AKT1, and FOXL2 genes exhibited 1 variant each. Interestingly, 2 variants observed in the PDGFRA gene are classic imatinib-sensitive therapy.

Conclusions: We concluded that Brazilian MPM harbor mutation in classic tumor suppressor and oncogenic genes, which might help in the guidance of personalized treatment of MPM.

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巴西恶性胸膜间皮瘤驱动肿瘤抑制基因和致癌基因的突变分析。

背景:恶性胸膜间皮瘤(Malignant pleural mesothelioma, MPM)是一种高度致死性疾病，由异质性肿瘤组成，其生物学行为难以预测。MPM的诊断很复杂，组织学分类包括2种主要亚型:上皮样(约60%的病例)和肉瘤(约20%)。其鉴定依赖于病理调查支持的临床和放射证据和最近的辅助分子检测。目前治疗方案有限，没有已知的靶向治疗方法。目的:阐明巴西患者队列中驱动肿瘤抑制基因和致癌基因的突变谱。方法:我们对来自巴西3个不同中心的43例巴西恶性间皮瘤(MM)患者的16个驱动基因进行了测序。从福尔马林固定石蜡包埋的肿瘤组织块中提取基因组DNA，通过PCR扩增TERT启动子区域，然后进行直接毛细管测序。Illumina TruSight Tumor 15用于评估来自实体瘤相关的15个基因(AKT1、GNA11、NRAS、BRAF、GNAQ、PDGFRA、EGFR、KIT、PIK3CA、ERBB2、KRAS、RET、FOXL2、MET和TP53)的250个扩增子。在MiSeq平台测序之前，使用TruSight Tumor 15进行文库准备。采用Sophia DDM软件进行数据分析。结果:43例MPM患者中，上皮样亚型38例(88.4%)，肉瘤样组织型5例(11.6%)。15例(39.5%)上皮样MPM患者和3例(60%)肉瘤样MPM患者存在石棉暴露。我们在11.6%的MM中发现TERT启动子突变，其中c - 146c >T突变是最常见的事件。新一代测序在33例中取得了成功。共有18份样本显示至少1种致病性，中位数为1.8种变异，范围从1到6。突变最多的基因是TP53和ERBB2，各有7个变异，其次是NRAS BRAF、PI3KCA、EGFR和PDGFRA，各有2个变异。KIT、AKT1和FOXL2基因各有1个变异。有趣的是，在PDGFRA基因中观察到的2个变异是经典的伊马替尼敏感治疗。结论:巴西MPM存在经典抑癌基因和致癌基因突变，有助于指导MPM的个体化治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Pathobiology : journal of immunopathology, molecular and cellular biology

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