Department of Thoracic Surgery, The Affiliated Hospital of Qingdao University, China.
Hangzhou Jichenjunchuang Medical Laboratory, Co., Ltd., China.
Mol Oncol. 2023 May;17(5):765-778. doi: 10.1002/1878-0261.13348. Epub 2022 Dec 13.
ALK rearrangement is called the 'diamond mutation' in non-small cell lung cancer (NSCLC). Accurately identifying patients who are candidates for ALK inhibitors is a key step in making clinical treatment decisions. In this study, a total of 783 ALK rearrangement-positive NSCLC cases were identified by DNA-based next-generation sequencing (NGS), including 731 patients with EML4-ALK and 52 patients with other ALK rearrangements. Diverse genomic breakpoints of ALK rearrangements were identified. Approximately 94.4% (739/783) of the cases carried ALK rearrangements with genomic breakpoints in the introns of ALK and its partner genes, and 2.8% (21/739) of these cases resulted in frameshift transcripts of ALK. Meanwhile, 5.6% (44/783) of the ALK rearrangement-positive cases had breakpoints in the exons that would be expected to result in abnormal transcripts. RNA-based NGS was performed to analyse the aberrant fusions at the transcript level. Some of these rearranged DNAs were not transcribed, and the others were fixed by some mechanisms so that the fusion kinase proteins could be expressed. Altogether, these findings emphasize that, when using DNA-based NGS, functional RNA fusions should be confirmed in cases with uncommon/frameshift rearrangement by RNA-based assays.
ALK 重排被称为非小细胞肺癌(NSCLC)中的“钻石突变”。准确识别适合接受 ALK 抑制剂治疗的患者是做出临床治疗决策的关键步骤。在这项研究中,通过基于 DNA 的下一代测序(NGS)共鉴定出 783 例 ALK 重排阳性 NSCLC 病例,其中 731 例为 EML4-ALK,52 例为其他 ALK 重排。鉴定出 ALK 重排的不同基因组断点。大约 94.4%(739/783)的病例携带 ALK 重排,其基因组断点位于 ALK 及其伙伴基因的内含子中,并且 2.8%(21/739)的这些病例导致 ALK 的移码转录本。同时,5.6%(44/783)的 ALK 重排阳性病例在外显子中具有断点,预计会导致异常转录本。进行基于 RNA 的 NGS 以分析转录本水平的异常融合。这些重排 DNA 中的一些没有转录,而另一些则通过某些机制固定,以使融合激酶蛋白能够表达。总之,这些发现强调了在使用基于 DNA 的 NGS 时,对于不常见/移码重排的病例,应通过基于 RNA 的检测来确认功能性 RNA 融合。
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