奥希替尼间歇插入多西他赛治疗海南南部肺腺癌并骨转移T790M基因突变阳性患者的临床研究

doi:10.3760/cma.j.issn.1673-422X.2019.07.002

摘要/Abstract

摘要： 目的探讨奥希替尼间歇插入多西他赛治疗海南南部肺腺癌并骨转移T790M基因突变阳性患者的临床应用。方法入组2018年1月—2018年10月海南省第三人民医院收治的海南南部肺腺癌并骨转移T790M基因突变阳性患者，根据治疗用药分为奥希替尼间歇插入化疗组（n=32）和奥希替尼组（n=28）。奥希替尼间歇插入化疗组患者口服奥希替尼80 mg 1次/d，待病情进展插入静脉滴注多西他赛75 mg/m2化疗，1次/3周，待肿瘤治疗评价稳定或缓解，则口服奥希替尼80 mg 1次/d维持直至进展后再行多西他赛化疗。奥希替尼组患者口服奥希替尼80 mg 1次/d。两组患者均联合应用唑来膦酸。比较两组患者的有效率、疾病控制率、总生存期及不良反应发生率。结果奥希替尼间歇插入化疗组患者的有效率为62.5%（20/32），高于奥希替尼组的35.7%（10/28），两组差异有统计学意义（χ2=4.286，P=0.038）；奥希替尼间歇插入化疗组患者的疾病控制率为93.8%（30/32），高于奥希替尼组的67.9%（19/28），两组差异有统计学意义（χ2=6.687，P=0.010）。奥希替尼间歇插入化疗组患者的中位总生存期为10.0个月，较奥希替尼组的9.0个月有所延长，两组差异有统计学意义（χ2=5.917，P=0.015）。两组患者不良反应均为Ⅰ或Ⅱ级，给予对症治疗后得到缓解和改善。结论奥希替尼间歇插入多西他赛化疗治疗海南南部肺腺癌并骨转移T790M基因突变阳性患者安全有效，能够延长患者生存期。

关键词: 肺肿瘤, 奥希替尼, 多西他赛, 骨转移, 海南南部

Abstract: ObjectiveTo study the clinical application of intercalated combination of osimertinib and docetaxel in T790M mutationpositive lung adenocarcinoma patients with bone metastasis in the southern Hainan Province. MethodsT790M mutationpositive lung adenocarcinoma patients with bone metastasis in the southern Hainan Province treated at the Third People′s Hospital of Hainan Province from January 2018 to October 2018 were enrolled, and they were divided into intercalated combination of osimertinib and docetaxel group (n=32) and osimertinib group (n=28) according to the treatment. The patients in intercalated combination of osimertinib and docetaxel group received oral osimertinib (80 mg, qd), and received docetaxel (75 mg/m2, repeated in threeweek intervals) when taking to tumor progression, and oral osimertinib treatment (80 mg, qd) was maintained until tumor partial response or stable disease after chemotherapy. The patients in osimertinib group received oral osimertinib (80 mg, qd). The patients in both groups received zoledronic acid. The response rate, disease control rate, overall survival (OS) and the incidence of adverse reactions of both groups were contrastively analyzed. ResultsThe response rate of intercalated combination of osimertinib and docetaxel group (62.5%, 20/32) was higher than that of osimertinib group (35.7%, 10/28), and disease control rate (93.8%, 30/32) was also higher than that of osimertinib group (67.9%, 19/28), with statistically significant differences (χ2=4.286, P=0.038; χ2=6.687, P=0.010). The median OS of intercalated combination of osimertinib and docetaxel group was 10.0 months, which was longer than that of osimertinib group (9.0 months), with statistically significant difference (χ2=5.917, P=0.015). Moreover, the adverse reactions in both groups were all grade Ⅰ or Ⅱ, which could be relieved or improved through symptomatic treatment. ConclusionIntercalated treatment of osimertinib with docetaxel is safe and effective in T790M mutationpositive lung adenocarcinoma patients with bone metastasis in the southern Hainan Province. It can prolong the survival time of patients.

Key words: Lung neoplasms, Osimertinib, Docetaxel, Bone metastasis, Southern Hainan Province

陈珑，林玲，王翠英，王琳，何冬雷，冯军. 奥希替尼间歇插入多西他赛治疗海南南部肺腺癌并骨转移T790M基因突变阳性患者的临床研究[J]. 国际肿瘤学杂志, 2019, 46(7): 399-403.

Chen Long, Lin Ling, Wang Cuiying, Wang Lin, He Donglei, Feng Jun. Clinical research of intercalated combination of osimertinib and docetaxel in T790M mutationpositive lung adenocarcinoma patients with bone metastasis in the southern Hainan Province[J]. Journal of International Oncology, 2019, 46(7): 399-403.

参考文献

［1］ Cetin K, Christiansen CF, Jacobsen JB, et al. Bone metastasis, skeletalrelated events, and mortality in lung cancer patients: a Danish populationbased cohort study［J］. Lung Cancer, 2014, 86(2): 247254. DOI: 10.1016/j.lungcan.2014.08.022. ［2］ Reck M, Popat S, Reinmuth N, et al. Metastasis non small cell lung cancer (NSCLC): ESMO Clinical Practice Guidelines for diagnosis, treatment and follow up［J］. Ann Oncol, 2014, 25 Suppl 3: iii27iii39. DOI: 10.1093/annonc/mdu199. ［3］ Yashima H, Shimizu K, Araki T, et al. Assessment of DDR2, BRAF, EGFR and KRAS mutations as therapeutic targets in nonadenocarcinoma lung cancer patients［J］. Mol Clin Oncol, 2014, 2(5): 714718. DOI: 10.3892/mco.2014.302. ［4］中国临床肿瘤学会指南工作委员会. 中国临床肿瘤学会原发性肺癌诊疗指南（2018年版）［M］. 人民卫生出版社, 2018: 4950. ［5］ Su KY, Chen HY, Li KC, et al. Pretreatment epidermal growth factor receptor (EGFR) T790M mutation predicts shorter EGFR tyrosine kinase inhibitor response duration in patients with nonsmall cell lung cancer［J］. J Clin Oncol, 2012, 30(4): 433440. DOI: 10.1200/JCO.2011.38.3224. ［6］刘曦光. 化疗与埃克替尼间插治疗在EGFR突变型非小细胞肺癌术后辅助治疗中的疗效与安全性［D］. 广州: 南方医科大学, 2016. ［7］王洁, 皮灿. 奥希替尼与培美曲塞联合铂类化疗在EGFRT790M阳性非小细胞肺癌患者中的疗效比较［J］. 循证医学, 2018, 18(1): 3639. ［8］ Wu YL, Lee JS, Thongprasert S, et al. Intercalated combination of chemotherapy and erlotinib for patients with advanced stage nonsmallcell lung cancer (FASTACT2): a randomized, double blind trial［J］. Lancet Oncl, 2013, 14(8): 777786. DOI: 10.1016/S14702045(13)702547. ［9］ Cheng Y, Murakami H, Yang PC, et al. Randomized phase Ⅱ trial of gefitinib with and without pemetrexed as firstline therapy in patients with advanced nonsquamous nonsmallcell lung cancer with activating epidermal growth factor receptor mutations［J］. J Clin Oncol, 2016, 34(27): 32583266. DOI: 10.1200/JCO.2016.66.9218. ［10］钱琳. 晚期非小细胞肺癌患者进行单药多西他赛二线治疗的临床研究［J］. 临床医药文献杂志, 2018, 15(5): 105106. ［11］ Jnne PA, Yang JC, Kim DW, et al. AZD9291 in EGFR inhibitorresistant nonsmallcell lung cancer［J］. N Engl J Med, 2015, 372(18): 16891699. DOI: 10.1056/NEJMoa1411817. ［12］ Zhou T, Zeng SX, Ye DW, et al. A multicenter, randomized clinical trial comparing the threeweekly docetaxel regimen plus prednisone versus mitoxantone plus prednisone for Chinese patients with metastatic castration refractory prostate cancer［J］. PLoS One, 2015, 7: e0117002. DOI: 10.1371/journal.pone.0117002. ［13］胡林军，李长岭，寿建忠，等. 多西他赛治疗转移性去势抵抗性前列腺癌的耐受剂量及其与预后的关系［J］. 中华泌尿外科杂志, 2019, 40(1): 3136. DOI: 10.3760/cma.j.issn.10006702.2019.01.006.

[1]	刘娜, 寇介丽, 杨枫, 刘桃桃, 李丹萍, 韩君蕊, 杨立洲. 血清miR-106b-5p、miR-760联合低剂量螺旋CT诊断早期肺癌的临床价值[J]. 国际肿瘤学杂志, 2024, 51(6): 321-325.
[2]	王丽, 刘志华, 杨伟洪, 蒋凤莲, 李全泳, 宋浩杰, 鞠文东. ROS1突变肺腺鳞癌合并脑梗死为主要表现的Trousseau综合征1例[J]. 国际肿瘤学杂志, 2024, 51(6): 382-384.
[3]	贺嘉慧, 胡钦勇. 基于GBD数据的中国和美国肺癌发病和死亡趋势及危险因素对比分析[J]. 国际肿瘤学杂志, 2024, 51(1): 29-36.
[4]	李雄安, 颜艳艳. 丙戊酸镁用于治疗继发癫痫的晚期肺癌脑转移患者1例报道[J]. 国际肿瘤学杂志, 2023, 50(3): 191-192.
[5]	宁婷婷, 胡钦勇, 李倩, 杨鹏程. 奥希替尼与埃克替尼一线治疗EGFR阳性转移性NSCLC临床疗效观察[J]. 国际肿瘤学杂志, 2023, 50(2): 65-70.
[6]	左小平, 刘晓川, 吴西强, 李周, 夏天, 刘国凤. 老年早期肺癌患者经胸腔镜肺切除术后心律失常发生的危险因素及预测模型构建[J]. 国际肿瘤学杂志, 2023, 50(12): 711-716.
[7]	陈郁, 许华, 刘海, 陈士新. 基于CT影像学特征的恶性肺纯磨玻璃结节患者病理分型预测模型构建[J]. 国际肿瘤学杂志, 2023, 50(11): 655-660.
[8]	张万芳, 王尤, 苏晶, 陈刚, 周福祥. 肺原发尤文肉瘤/原始神经外胚层瘤1例[J]. 国际肿瘤学杂志, 2023, 50(1): 62-64.
[9]	杨莎, 杨晓华, 王苏华, 薛晓燕, 徐俊. 老年肺癌胸腔镜手术后下肢深静脉血栓的危险因素分析及预测模型的建立和验证[J]. 国际肿瘤学杂志, 2022, 49(9): 532-536.
[10]	王津, 张耀圣, 孙婷婷, 王丹, 胡乃东. 以前胸壁聚集性多发蕈状肿物为表现的肺腺鳞状细胞癌皮肤转移1例[J]. 国际肿瘤学杂志, 2022, 49(9): 575-576.
[11]	陈煌婧, 朱鹏飞, 张晴, 陈桂芳, 杨春林, 何英. 超声造影和CT引导下经皮穿刺活检在周围型肺肿块诊断中临床价值的比较[J]. 国际肿瘤学杂志, 2022, 49(8): 459-463.
[12]	蔡刚祥, 李境, 许斌. 肺癌新辅助免疫治疗研究进展[J]. 国际肿瘤学杂志, 2022, 49(6): 366-370.
[13]	韩丛丛, 付帅, 谢超, 张建军, 张秋景, 祝情情, 刘杰. 吉非替尼、培美曲塞和贝伐珠单抗一线治疗EGFR突变晚期肺腺癌的有效性和安全性[J]. 国际肿瘤学杂志, 2022, 49(6): 376-379.
[14]	王永洪, 何弢, 李星, 罗启余, 王乔羽. 信迪利单抗致晚期鳞状细胞肺癌患者致死性中毒性表皮坏死松解症1例[J]. 国际肿瘤学杂志, 2022, 49(6): 380-382.
[15]	张静娴, 易丹, 李小江. 抗体偶联药物在非小细胞肺癌中的应用[J]. 国际肿瘤学杂志, 2022, 49(5): 296-301.