曲妥珠单抗联合紫杉醇治疗 EGFR-TKI 治疗进展后 HER2 过表达的 EGFR 突变型 NSCLC 患者。
Trastuzumab and paclitaxel in patients with EGFR mutated NSCLC that express HER2 after progression on EGFR TKI treatment.
机构信息
Department of Thoracic Oncology, Netherlands Cancer Institute-Antoni van Leeuwenhoek Hospital, Amsterdam, The Netherlands.
Department of Pulmonary Diseases, VU University Medical Center, Amsterdam, The Netherlands.
出版信息
Br J Cancer. 2018 Aug;119(5):558-564. doi: 10.1038/s41416-018-0194-7. Epub 2018 Jul 31.
BACKGROUND
HER2 expression and amplification are observed in ~15% of tumour biopsies from patients with a sensitising EGFR mutation who develop EGFR TKI resistance. It is unknown whether HER2 targeting in this setting can result in tumour responses.
METHODS
A single arm phase II study was performed to study the safety and efficacy of trastuzumab and paclitaxel treatment in patients with a sensitising EGFR mutation who show HER2 expression in a tumour biopsy (IHC ≥ 1) after progression on EGFR TKI treatment. Trastuzumab (first dose 4 mg/kg, thereafter 2 mg/kg) and paclitaxel (60 mg/m) were dosed weekly until disease progression or unacceptable toxicity. The primary end-point was tumour response rate according to RECIST v1.1.
RESULTS
Twenty-four patients were enrolled. Nine patients were exon 21 L858R positive and fifteen exon 19 del positive. Median HER2 IHC was 2+ (range 1-3). For 21 patients, gene copy number by in situ hybridisation could be calculated: 5 copies/nucleus (n = 9), 5-10 copies (n = 8), and >10 copies (n = 4). An objective response was observed in 11/24 (46%) patients. Highest response rates were seen for patients with 3+ HER2 IHC (12 patients, ORR 67%) or HER2 copy number ≥10 (4 patients, ORR 100%). Median tumour change in size was 42% decrease (range -100% to +53%). Median duration of response was 5.6 (95% confidence interval [CI], 3.8 to 7.3) months. Treatment toxicity was mild with four patients experiencing grade ≥3 toxicity, including fatigue, neuropathy, neutropaenia, urinary tract infection, and pneumonitis.
CONCLUSIONS
Trastuzumab-paclitaxel induces objective tumour responses in 46% of EGFR TKI pretreated patients with an activating EGFR mutation and HER2 expression. The treatment was well tolerated. The relation between response rate and HER2 expression level and copy number suggests effective HER2 targeting by trastuzumab, although the combination with paclitaxel does not allow to determine the relative contribution of the individual drugs in terms of treatment efficacy.
背景
在接受 EGFR TKI 治疗后出现 EGFR 敏感突变耐药的患者中,约有 15%的肿瘤活检标本中观察到 HER2 表达和扩增。目前尚不清楚在这种情况下针对 HER2 是否可以使肿瘤产生应答。
方法
进行了一项单臂 II 期研究,以研究在 EGFR TKI 治疗进展后肿瘤活检中 HER2 表达(IHC≥1)的具有敏感 EGFR 突变的患者中,曲妥珠单抗联合紫杉醇治疗的安全性和疗效。曲妥珠单抗(首剂 4mg/kg,随后 2mg/kg)和紫杉醇(60mg/m)每周给药,直至疾病进展或出现不可接受的毒性。主要终点是根据 RECIST v1.1 评估的肿瘤缓解率。
结果
共纳入 24 例患者。9 例患者为外显子 21 L858R 阳性,15 例患者为外显子 19 del 阳性。中位 HER2 IHC 为 2+(范围 1-3)。对于 21 例患者,通过原位杂交可以计算基因拷贝数:5 个核/拷贝(n=9),5-10 个拷贝(n=8),和>10 个拷贝(n=4)。24 例患者中,21 例可计算基因拷贝数,其中 9 例为 5 个核/拷贝(n=9),8 例为 5-10 个拷贝(n=8),4 例为>10 个拷贝(n=4)。24 例患者中,21 例可计算基因拷贝数,其中 9 例为 5 个核/拷贝(n=9),8 例为 5-10 个拷贝(n=8),4 例为>10 个拷贝(n=4)。24 例患者中,21 例可计算基因拷贝数,其中 9 例为 5 个核/拷贝(n=9),8 例为 5-10 个拷贝(n=8),4 例为>10 个拷贝(n=4)。24 例患者中,21 例可计算基因拷贝数,其中 9 例为 5 个核/拷贝(n=9),8 例为 5-10 个拷贝(n=8),4 例为>10 个拷贝(n=4)。观察到 11/24(46%)例患者出现客观缓解。HER2 IHC 为 3+的患者中,最高缓解率为 67%(12 例),HER2 拷贝数≥10 的患者中,最高缓解率为 100%(4 例)。中位肿瘤大小变化为 42%减少(范围-100%至+53%)。中位缓解持续时间为 5.6 个月(95%置信区间[CI],3.8 至 7.3)。治疗毒性轻微,有 4 例患者发生 3 级以上毒性,包括疲劳、神经病变、中性粒细胞减少症、尿路感染和肺炎。
结论
曲妥珠单抗联合紫杉醇在接受 EGFR TKI 预处理的具有激活型 EGFR 突变和 HER2 表达的患者中,可使 46%的患者产生客观肿瘤应答。该治疗方法耐受性良好。尽管联合紫杉醇治疗并不能确定两种药物在治疗效果方面的相对贡献,但根据 HER2 表达水平和拷贝数的关系提示曲妥珠单抗可有效靶向 HER2。
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