笑对人生 (2022-10-03 23:59):
#paper doi: 10.1038/s41416-022-01913-4. Comprehensive assessment of actionable genomic alterations in primary colorectal carcinoma using targeted next-generation sequencing. Br J Cancer. 2022 Oct;127(7):1304-1311. 这是一篇设计思路较为简单的原发结直肠癌体细胞突变检测文章,检测项目包括SNV(单核苷酸变异)、small INDELS(小的插入或缺失)、CNV(拷贝数变异)、TMB(肿瘤突变负荷)和microsatellite status(微卫星状态)。使用基于扩增子的靶向二代测序技术,设计靶向测序panel为428 cancer-related genes。使用的测序平台为Ion Proton sequencer using the Ion PI chip。临床样本的主要信息为澳大利亚队列,575份原发CRC(结肠腺癌)的FFPE样本,按取样部位划分,45.6%来自右侧colon(结肠),剩下54.4%来自左侧结肠。该篇文章主要的亮点是在对突变数据进行解读时,始终围绕着临床用药进行对比或探讨。主要值得关注的发现包括(1)在MSI-H的CRCs,BRAF是突变频率最高的原癌基因,占比为71%,其次是抑癌基因RNF43(63%)、KMT2C(50%)、APC(48%)、FAT1(48%)、ATM(39%)和ARID1A(39%)。在MSS的CRC中,APC和TP53是突变频率最高的抑癌基因,占比分别是74%和67%,突变频率最高的原癌基因是KRAS(47%)、PIK3CA(21%)和BRAF(13%)。413基因的拷贝数变异图谱也发现了MSI-H和MSS间存在差异。(2)MSI-H组患者的TMBs中位值显著高于MSS组。左侧结肠,只有5.6%是MSI-H,右侧结肠,1/3是MSI-H。47%的MSI-H患者存在至少一种loss of function(功能丧失)的突变导致ICIs治疗不佳。在MSS且RAS/RAF野生型突变的CRC患者中,59%含有至少一个可采取anti-EGFR靶向治疗的actionable mutation。actionable mutation理解为目前具有明确治疗策略的突变。随着NGS高通量测序的普及,肿瘤基因检测会报告大量的突变,其中包含具有临床意义的突变,而这些突变又包括可评估预后的突变、目前已经有批准的或正在临床试验的靶向药基因突变。(3)根据生物标志物(未找到具体标准),对复发晚期(III或IV)的CRC患者,分成6类,分别是MSI、On-label、On-label plus Off-label、Off-label、WT-RAS/RAF和WT-RAS/RAF plus Off-label。这里的on-label是指按药物包装上标注的适应症使用,off-label意为超出所标注的适应症用药。
Comprehensive assessment of actionable genomic alterations in primary colorectal carcinoma using targeted next-generation sequencing
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Abstract:
BACKGROUND: The clinical utility of comprehensive genomic profiling (CGP) for guiding treatment has gradually become the standard-of-care procedure for colorectal carcinoma (CRC). Here, we comprehensively assess emerging targeted therapy biomarkers using CGP in primary CRC.METHODS: A total of 575 primary CRCs were sequenced by ACTOnco® assay for genomic alterations, tumour mutational burden (TMB), and microsatellite instability (MSI).RESULTS: Eighteen percent of patients were detected as MSI-High (MSI-H), and the remaining cases were classified as microsatellite stable (MSS). Driver mutation prevalence in MSS CRCs were APC (74%), TP53 (67%), KRAS (47%), PIK3CA (21%) and BRAF (13%). The median TMBs for MSI-H and MSS patients were 37.8 mutations per mega base (mut/Mb) and 3.9 mut/Mb, respectively. Forty-seven percent of MSI-H CRC harboured at least one loss-of-function mutations in genes that may hamper immune checkpoint blockade. Among MSS RAS/RAF wild-type CRCs, 59% had at least one actionable mutation that may compromise the efficacy of anti-EGFR therapy. For late-stage CRC, 51% of patients are eligible for standard care actionability and the remaining 49% could be enrolled in clinical trials with investigational drugs.CONCLUSIONS: This study highlights the essential role of CGP for identifying rational targeted therapy options in CRC.
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