比较基因组杂交阵列和 DNA 测序指导转移性乳腺癌的治疗:一项多中心、前瞻性试验(SAFIR01/UNICANCER)。
Comparative genomic hybridisation array and DNA sequencing to direct treatment of metastatic breast cancer: a multicentre, prospective trial (SAFIR01/UNICANCER).
机构信息
Department of Medical Oncology, Institut Gustave Roussy, Villejuif, France; INSERM Unit U981, Institut Gustave Roussy, Villejuif, France; Université Paris Sud, le Kremlin Bicêtre, France.
Departement de Cancerologie Medicale, Université Lyon 1, Centre Léon Bérard, Lyon, France.
出版信息
Lancet Oncol. 2014 Mar;15(3):267-74. doi: 10.1016/S1470-2045(13)70611-9. Epub 2014 Feb 7.
BACKGROUND
Breast cancer is characterised by genomic alterations. We did a multicentre molecular screening study to identify abnormalities in individual patients with the aim of providing targeted therapy matched to individuals' genomic alterations.
METHODS
From June 16, 2011, to July 30, 2012, we recruited patients who had breast cancer with a metastasis accessible for biopsy in 18 centres in France. Comparative genomic hybridisation (CGH) array and Sanger sequencing on PIK3CA (exon 10 and 21) and AKT1 (exon 4) were used to assess metastatic biopsy samples in five centres. Therapeutic targets were decided on the basis of identified genomic alterations. The primary objective was to include 30% of patients in clinical trials testing a targeted therapy and, therefore, the primary outcome was the proportion of patients to whom a targeted therapy could be offered. For the primary endpoint, the analyses were done on the overall population registered for the trial. This trial is registered with ClinicalTrials.gov, number NCT01414933.
FINDINGS
423 patients were included, and biopsy samples were obtained from 407 (metastatic breast cancer was not found in four). CGH array and Sanger sequencing were feasible in 283 (67%) and 297 (70%) patients, respectively. A targetable genomic alteration was identified in 195 (46%) patients, most frequently in PIK3CA (74 [25%] of 297 identified genomic alterations), CCND1 (53 [19%]), and FGFR1 (36 [13%]). 117 (39%) of 297 patients with genomic tests available presented with rare genomic alterations (defined as occurring in less than 5% of the general population), including AKT1 mutations, and EGFR, MDM2, FGFR2, AKT2, IGF1R, and MET high-level amplifications. Therapy could be personalised in 55 (13%) of 423 patients. Of the 43 patients who were assessable and received targeted therapy, four (9%) had an objective response, and nine others (21%) had stable disease for more than 16 weeks. Serious (grade 3 or higher) adverse events related to biopsy were reported in four (1%) of enrolled patients, including pneumothorax (grade 3, one patient), pain (grade 3, one patient), haematoma (grade 3, one patient), and haemorrhagic shock (grade 3, one patient).
INTERPRETATION
Personalisation of medicine for metastatic breast cancer is feasible, including for rare genomic alterations.
FUNDING
French National Cancer Institute, Breast Cancer Research Foundation, Odyssea, Operation Parrains Chercheurs.
背景
乳腺癌的特征是存在基因组改变。我们进行了一项多中心分子筛选研究,以确定个体患者的异常情况,目的是为个体的基因组改变提供靶向治疗。
方法
从 2011 年 6 月 16 日至 2012 年 7 月 30 日,我们在法国的 18 个中心招募了有转移性乳腺癌且可进行活检的患者。在五个中心,我们使用比较基因组杂交(CGH)阵列和 Sanger 测序对 PIK3CA(外显子 10 和 21)和 AKT1(外显子 4)进行了评估。根据确定的基因组改变来决定治疗靶点。主要目的是将 30%的患者纳入测试靶向治疗的临床试验中,因此,主要终点是能够为靶向治疗提供的患者比例。对于主要终点,对整个试验注册人群进行了分析。该试验在 ClinicalTrials.gov 注册,编号为 NCT01414933。
结果
共纳入 423 例患者,其中 407 例(4 例未发现转移性乳腺癌)获得了活检样本。CGH 阵列和 Sanger 测序在 283 例(67%)和 297 例(70%)患者中分别是可行的。在 195 例(46%)患者中确定了可靶向的基因组改变,最常见的是 PIK3CA(297 例鉴定的基因组改变中有 74 例[25%])、CCND1(53 例[19%])和 FGFR1(36 例[13%])。在 297 例有基因组检测的患者中,117 例(39%)存在罕见的基因组改变(定义为发生在不到 5%的普通人群中),包括 AKT1 突变和 EGFR、MDM2、FGFR2、AKT2、IGF1R 和 MET 高水平扩增。在 423 例患者中,有 55 例(13%)可进行个体化治疗。在 43 例可评估且接受靶向治疗的患者中,有 4 例(9%)有客观缓解,另有 9 例(21%)的疾病稳定超过 16 周。在纳入的患者中,有 4 例(1%)报告了与活检相关的严重(3 级或更高)不良事件,包括气胸(3 级,1 例)、疼痛(3 级,1 例)、血肿(3 级,1 例)和出血性休克(3 级,1 例)。
解释
转移性乳腺癌的药物个体化治疗是可行的,包括罕见的基因组改变。
资金来源
法国国家癌症研究所、乳腺癌研究基金会、Odyssea、Operation Parrains Chercheurs。
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