多生物标志物检测组织消耗和完成率与单基因检测和 OncomineDxTargetTest 在晚期非小细胞肺癌中的研究应用:一项单中心分析。
Multiple Biomarker Testing Tissue Consumption and Completion Rates With Single-gene Tests and Investigational Use of Oncomine Dx Target Test for Advanced Non-Small-cell Lung Cancer: A Single-center Analysis.
机构信息
Navigant Consulting, Inc, San Francisco, CA.
OmniSeq, LLC, Buffalo, NY.
出版信息
Clin Lung Cancer. 2019 Jan;20(1):20-29.e8. doi: 10.1016/j.cllc.2018.08.010. Epub 2018 Aug 23.
INTRODUCTION
First-line targeted therapies have been developed for advanced non-small-cell lung cancer (NSCLC). However, small biopsy samples pose a challenge to testing all relevant biomarkers. The present study characterized clinician-ordered single-gene lung cancer testing and evaluated tissue stewardship and the ability to successfully determine mutation status with single-gene testing or investigational use of the Oncomine Dx Target Test.
MATERIALS AND METHODS
Clinician-submitted orders for 3659 single-gene tests (EGFR, ALK, ROS1, BRAF, KRAS, ERBB2, MET, RET, FGFR1) across 1402 samples at a large US-based commercial reference laboratory and 169 investigational Oncomine Dx Target Tests were retrospectively evaluated. The testing success rates and tissue consumption were evaluated by sample type, test type, and number of single-gene tests per sample.
RESULTS
The large majority of lung tissue samples submitted for clinical testing were small (70.5% core needle biopsies; 10.0% fine needle aspirations). With single-gene testing, mutation status was successfully reported for ≥ 1 biomarker for 88.4% of the clinical samples. The success rates decreased and tissue consumption increased with testing of additional biomarkers. Investigational Oncomine Dx Target Tests were permitted 1 tissue slide each and demonstrated success rates similar to single-gene testing for ≥ 5 biomarkers on core needle biopsies, ≥ 4 biomarkers on fine needle aspirations, and ≥ 2 biomarkers on surgical resection specimens.
CONCLUSION
Tissue stewardship is important to enable successful completion of genetic testing and informed NSCLC treatment decisions. Preliminary assessment of the investigational Oncomine Dx Target Test suggests it could facilitate access to multiple biomarker testing using small tissue samples to support therapy decisions for patients with advanced NSCLC.
简介
针对晚期非小细胞肺癌(NSCLC)已开发出一线靶向疗法。然而,小活检样本在测试所有相关生物标志物方面存在挑战。本研究描述了临床医生要求的单基因肺癌检测,并评估了组织管理以及通过单基因检测或使用 Oncomine Dx Target Test 进行研究性检测成功确定突变状态的能力。
材料和方法
回顾性评估了一家大型美国商业参考实验室的 1402 个样本中 3659 个单基因检测(EGFR、ALK、ROS1、BRAF、KRAS、ERBB2、MET、RET、FGFR1)的临床医生提交的订单和 169 项研究性 Oncomine Dx Target Test。通过样本类型、检测类型以及每个样本的单基因检测数量评估检测成功率和组织消耗。
结果
提交用于临床检测的绝大多数肺组织样本较小(70.5%为芯针活检;10.0%为细针抽吸)。通过单基因检测,88.4%的临床样本成功报告了≥1 种生物标志物的突变状态。随着额外生物标志物的检测,成功率降低,组织消耗增加。研究性的 Oncomine Dx Target Test 每个允许使用 1 个组织载玻片,并且在芯针活检上≥5 种生物标志物、细针抽吸上≥4 种生物标志物和手术切除标本上≥2 种生物标志物的检测中,其成功率与单基因检测相似。
结论
组织管理对于成功完成基因检测和为 NSCLC 治疗决策提供信息至关重要。对研究性 Oncomine Dx Target Test 的初步评估表明,它可以通过使用小组织样本进行多种生物标志物检测,为晚期 NSCLC 患者的治疗决策提供便利。
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