Real-World Study on Implementation of Genomic Tests for Advanced Lung Adenocarcinoma in Brazil.

IF 3.2 Q2 ONCOLOGY

JCO Global Oncology Pub Date : 2024-11-01 Epub Date: 2024-11-21 DOI:10.1200/GO-24-00354

Rodrigo Dienstmann, Leonard M da Silva, Fernanda Orpinelli Ramos do Rego, Amanda Muniz Rodrigues, Fernanda Christtanini Koyama, Layla Testa Galindo, Carolina de Bustamante Fernandes, Bruno Batista de Souza, Rafael Duarte Paes, Tatiane Montella, Pedro de Marchi, Breno Jeha Araújo, Bruno Lemos Ferrari, Clarissa Mathias, Emilio Pereira, Mariano Gustavo Zalis, Chesley Leslin, Carlos Gil Ferreira

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Abstract

Purpose: Tissue inadequacy and operational challenges may limit lung cancer comprehensive biomarker testing. Here, we describe the initial implementation of a tailored tissue molecular journey at Oncoclínicas Precision Medicine Laboratory in Brazil, which includes fast-track (FT) non-next-generation sequencing (NGS) assays combined with a broad NGS panel.

Methods: From 2021 to 2023, all nonsquamous lung cancer samples eligible for the patient support program "Lung Mapping Consortium" at Oncoclínicas & Co were evaluated using the FT panel (immunohistochemistry for PD-L1 and anaplastic lymphoma kinase [ALK], polymerase chain reaction for EGFR and BRAF, and fluorescence in situ hybridization for ROS1) plus a broad DNA and RNA sequencing panel of 180 genes (custom ARCHER panel).

Results: From 1,272 samples received by the laboratory, 3% had no tissue for any molecular testing, 20% was not eligible for broad NGS panel as per pathologist assessment (tumor purity and quantity), additional 12% did not reach presequencing analytical thresholds (nucleic acid quantity and/or quality), and 3% had postsequencing failure. Most frequent alterations were KRAS mutations (28.4%, KRAS^G12C 9.7%), EGFR mutations (23.6%, exon20 insertions 2.9%), ALK fusions (6.4%), MET exon 14 skipping (4.4%), ERBB2 mutations (3.4%), ROS1 fusions (3.1%), and BRAF^V600E (1.9%). In 35% of the samples, FT non-NGS tests were the only molecular diagnostics: EGFR mutations (14%), ALK fusions (4.4%), ROS1 fusions (1.8%), and BRAF^V600E (0.7%). Overall, high PD-L1 expression (≥50%) was found in 12.3%.

Conclusion: This study provides data on the molecular epidemiology of lung adenocarcinoma in Brazil, confirming high prevalence of EGFR mutations, ALK fusions, and MET exon 14 skipping alteration. Biomarker detection is largely affected by biospecimen collection and processing, with one third of the patients eligible for non-NGS testing only, which presents reduced coverage and sensitivity for actionable drivers.

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在巴西实施晚期肺腺癌基因组检验的真实世界研究。

目的：组织不足和操作挑战可能会限制肺癌综合生物标记物检测。在此，我们介绍了巴西 Oncoclínicas 精确医学实验室（Oncoclínicas Precision Medicine Laboratory）量身定制的组织分子之旅的初步实施情况，其中包括快速通道（FT）非下一代测序（NGS）测定与广泛的 NGS 面板相结合：从 2021 年到 2023 年，Oncoclínicas & Co 公司使用 FT 面板（PD-L1 和无性淋巴瘤激酶 [ALK]的免疫组化、EGFR 和 BRAF 的聚合酶链反应以及 ROS1 的荧光原位杂交）加上包含 180 个基因的广泛 DNA 和 RNA 测序面板（定制 ARCHER 面板）对所有符合 "肺部图谱联盟 "患者支持计划的非鳞状肺癌样本进行评估：在实验室收到的 1,272 份样本中，3% 的样本没有进行任何分子检测的组织，20% 的样本根据病理学家的评估（肿瘤纯度和数量）不符合进行广泛 NGS 面板检测的条件，另外 12% 的样本未达到测序前分析阈值（核酸数量和/或质量），3% 的样本测序后失败。最常见的改变是KRAS突变（28.4%，KRASG12C 9.7%）、EGFR突变（23.6%，exon20插入2.9%）、ALK融合（6.4%）、MET外显子14跳越（4.4%）、ERBB2突变（3.4%）、ROS1融合（3.1%）和BRAFV600E（1.9%）。在 35% 的样本中，FT 非 NGS 检测是唯一的分子诊断方法：表皮生长因子受体突变（14%）、ALK 融合（4.4%）、ROS1 融合（1.8%）和 BRAFV600E（0.7%）。总体而言，12.3%的患者存在PD-L1高表达（≥50%）：这项研究提供了巴西肺腺癌分子流行病学的数据，证实了表皮生长因子受体（EGFR）突变、ALK融合和MET第14外显子跳变的高患病率。生物标志物检测在很大程度上受到生物样本采集和处理的影响，三分之一的患者只符合非 NGS 检测条件，这降低了可操作驱动因素的覆盖率和灵敏度。

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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