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Fluorescence in Situ Hybridization (FISH) for Detecting Anaplastic Lymphoma Kinase (ALK) Rearrangement in Lung Cancer: Clinically Relevant Technical Aspects

机译:荧光原位杂交(鱼类)用于检测肺癌中的促进淋巴瘤激酶(ALK)重排:临床相关技术方面

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摘要

In 2011, the Vysis Break Apart ALK fluorescence in situ hybridization (FISH) assay was approved by the United States Food and Drug Administration as a companion diagnostic for detecting ALK rearrangement in lung cancer patients who may benefit from treatment of tyrosine kinase inhibitor therapy. This assay is the current “gold standard”. According to updated ALK testing guidelines from the College of American Pathologists, the International Association for the Study of Lung Cancer and the Association for Molecular Pathology published in 2018, ALK immunohistochemistry is formally an alternative to ALK FISH, and simultaneous detection of multiple hot spots, including, at least, ALK, ROS1, RET, MET, ERBB2, BRAF and KRAS genes is also recommended while performing next generation sequencing (NGS)-based testing. Therefore, ALK status in a specimen can be tested by different methods and platforms, even in the same institution or laboratory. In this review, we discuss several clinically relevant technical aspects of ALK FISH, including pros and cons of the unique two-step (50- to 100-cell) analysis approach employed in the Vysis Break Apart ALK FISH assay, including: the preset cutoff value of ≥15% for a positive resu technical aspects and biology of discordant results obtained by different methods; and incidental findings, such as ALK copy number gain or amplification and co-existent driver mutations. These issues have practical implications for ALK testing in the clinical laboratory following the updated guidelines.
机译:2011年,通过美国食品和药物管理批准,分裂杂交(鱼类)分析Alap荧光作为检测可能受益于酪氨酸激酶抑制作用治疗的肺癌患者Alk重排的伴侣诊断。该测定是目前的“黄金标准”。根据美国病理学家学院的最新的ALK测试指南,国际肺癌研究协会和2018年出版的分子病理学协会,ALK免疫组化是ALK FISH的替代品,同时检测多个热点,在执行下一代测序(NGS)的测试时,还推荐至少包括ALK,ROS1,RET,MET,ERBB2,BRAF和KRAS基因。因此,即使在同一机构或实验室中,也可以通过不同的方法和平台测试标本中的ALK状态。在本次审查中,我们讨论了Alk Fish的几个临床相关技术方面,包括在群体中使用的独特两步(50至100个细胞)分析方法的优缺点,包括:预设截止阳性结果的值≥15%;不同方法获得的不间断结果的技术方面和生物学;和偶然的发现,如ALK拷贝数增益或扩增和共存驾驶员突变。这些问题在更新的准则之后对临床实验室中的ALK测试具有实际影响。

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