Colomer Ramon, Miranda Jesús, Romero-Laorden Nuria, Hornedo Javier, González-Cortijo Lucía, Mouron Silvana, Bueno Maria J, Mondéjar Rebeca, Quintela-Fandino Miguel
Department of Medicine, Universidad Autónoma de Madrid (UAM), Madrid, Spain.
Chair of Personalised Precision Medicine, Universidad Autonoma de Madrid (UAM - Fundación Instituto Roche), Madrid, Spain.
EClinicalMedicine. 2023 Jun 1;60:102029. doi: 10.1016/j.eclinm.2023.102029. eCollection 2023 Jun.
Next Generation Sequencing (NGS) panels are increasingly used in advanced patients with cancer to guide therapy. There is, however, controversy about when should these panels be used, and about their impact on the clinical course.
In an observational study of 139 patients with cancer having an NGS test [from January 1st, 2017 to December 30th, 2020, in two hospitals (Hospital Universitario de La Princesa and Hospital Universitario Quironsalud Madrid) from Spain], we evaluated whether the clinical course (progression-free survival, PFS) was influenced by drug-based criteria [druggable alterations, receiving a recommended drug, having a favourable ESCAT category (ESMO Scale for Clinical Actionability of molecular Targets)] or clinical judgement criteria.
In 111 of 139 cases that were successfully profiled, PFS was not significantly influenced by either having druggable alterations [median PFS for patients with druggable alterations was 170 (95% C.I.: 139-200) days compared to 299 (95% C.I.: 114-483) for those without; = 0.37], receiving a proposed matching agent [median PFS for patients receiving a genomics-informed drug was 195 days (95% C.I.: 144-245), compared with 156 days for those that did not (95% C.I.: 85-226); = 0.50], or having favourable ESCAT categories [median PFS for patients with ESCAT I-III was 183 days (95% C.I.: 104-261), compared with 180 (95% C.I.:144-215) for patients with ESCAT IV-X; = 0.87]. In contrast, NGS testing performed within clinical judgement showed a significantly improved PFS [median PFS for patients that were profiled under the recommended scenarios was 319 days (95% C.I.: 0-658), compared to 123 days (95% C.I.: 89-156) in the non-recommended categories; = 0.0020].
According to our data, real-world outcomes after NGS testing provide evidence of the benefit of clinical judgement in patients with either advanced cancers that routinely need multiple genetic markers, patients with advanced rare cancers, or patients that are screened for molecular clinical trials. By contrast, NGS does not seem to be valuable when performed in cases with a poor PS, rapidly progressing cancer, short expected lifetime, or cases with no standard therapeutic options.
RC, NR-L and MQF are recipients of the PMP22/00032 grant, funded by the ISCIII and co-funded by the European Regional Development Fund (ERDF). The study also received funds from the CRIS Contra el Cancer Foundation.
新一代测序(NGS)检测板越来越多地用于晚期癌症患者以指导治疗。然而,关于何时应使用这些检测板以及它们对临床病程的影响存在争议。
在一项对139例接受NGS检测的癌症患者的观察性研究中(2017年1月1日至2020年12月30日,来自西班牙的两家医院——拉普拉西公主大学医院和马德里基隆萨尔医院),我们评估了临床病程(无进展生存期,PFS)是否受基于药物的标准(可靶向改变、接受推荐药物、具有良好的ESCAT分类[分子靶点临床可操作性的ESMO量表])或临床判断标准的影响。
在139例成功分析的病例中的111例中,PFS不受是否有可靶向改变[有可靶向改变的患者的中位PFS为170天(95%置信区间:139 - 200),而无可靶向改变的患者为299天(95%置信区间:114 - 483);P = 0.37]、是否接受推荐的匹配药物[接受基于基因组学信息的药物的患者的中位PFS为195天(95%置信区间:144 - 245),未接受的患者为156天(95%置信区间:85 - 226);P = 0.50]或是否具有良好的ESCAT分类[ESCAT I - III级患者的中位PFS为183天(95%置信区间:104 - 261),ESCAT IV - X级患者为180天(95%置信区间:144 - 215);P = 0.87]的影响。相比之下,在临床判断下进行的NGS检测显示PFS有显著改善[在推荐情况下进行分析的患者的中位PFS为319天(95%置信区间:0 - 658),非推荐情况下为123天(95%置信区间:89 - 156);P = 0.0020]。
根据我们的数据,NGS检测后的实际临床结果为临床判断对常规需要多个基因标志物的晚期癌症患者、晚期罕见癌症患者或接受分子临床试验筛查的患者有益提供了证据。相比之下,在体能状态差、癌症进展迅速、预期寿命短或没有标准治疗选择的情况下进行NGS检测似乎没有价值。
RC、NR - L和MQF是PMP22/00032资助的获得者,该资助由西班牙国家卫生系统研究所(ISCIII)资助,并由欧洲区域发展基金(ERDF)共同资助。该研究还获得了CRIS抗癌基金会的资金。
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