仑伐替尼联合PD-1单抗及GEMOX方案在晚期胆道恶性肿瘤治疗中的临床观察

doi:10.3969/j.issn.1004-583X.2024.05.004

摘要/Abstract

摘要：

目的探讨靶免(仑伐替尼+信迪利单抗)联合GEMOX(吉西他滨+奥沙利铂)在胆道恶性肿瘤复发转移患者中的临床效果和安全性。方法选择2015年1月到2024年1月在我院中西医结合肿瘤科及肝胆外科接受靶免(仑伐替尼+信迪利单抗)联合GEMOX(吉西他滨+奥沙利铂)方案的复发转移的晚期胆道恶性肿瘤患者24例,主要观察终点设置为总体生存期(overall survival, OS)和无进展生存时间(progression-free survival,PFS),次要观察终点设置为客观缓解率(ORR)、疾病控制率(DCR)、安全性。借助肿瘤标记物(CEA、CA125、CA199)变化、不良反应、生活质量评分,影像学改变等各项数据综合评估靶免(仑伐替尼+信迪利单抗)联合GEMOX(吉西他滨+奥沙利铂)方案治疗晚期胆道恶性肿瘤复发转移的安全性和整体临床效果。结果部分缓解(PR)8例,稳定(SD)8例,进展(PD)8例,ORR 33.3%(8/24),DCR 66.7%(16/24),中位OS 13个月,中位PFS 8个月。治疗后CA199水平明显低于治疗前(P<0.05)。主要不良反应为皮疹(14/24,58.3%)、白细胞下降(22/24,91.6%)、贫血(20/24,83.3%),其中有1例因严重不良事件退出治疗,1例患者在治疗期间死于胆道梗阻合并感染。结论采用靶免(仑伐替尼+信迪利单抗)联合GEMOX(吉西他滨+奥沙利铂)方案治疗晚期胆道恶性肿瘤复发转移患者具有较高的安全性和有效性,可以在临床使用。

关键词: 胆道肿瘤, 复发转移, 化疗, 靶向, 免疫, 临床应用

Abstract:

Objective To evaluate the clinical efficacy and safety of gemcitabine and oxaliplatin (GEMOX) combined with target-immunity therapy (lenvatinib and programmed cell death 1 [PD-1] monoclonal antibody) in patients with advanced biliary tract cancer (BTC). Methods Twenty-four patients with advanced BTC received GEMOX combined with target-immunity therapy visited Integrative Oncology Department or Hepatobiliary Surgery Department of our hospital from January 2015 to January 2024 were recruited. The primary end points were set as overall survival (OS) and progression-free survival (PFS), and the secondary end points were objective response rate (ORR), disease control rate (DCR) and safety. The safety and overall clinical efficacy of GEMOX combined with target-immunity therapy regimen on advanced BTC were comprehensively evaluated via tumor marker indexes (carcinoembryonic antigen [CEA], carbohydrate antigen 125 [CA125], CA199), adverse reactions rates, quality of life scores, imaging indicators, and other data. Results None of the 24 patients had complete remission (CR). ORR was 33.3% (8/24, 8 patients had PR), DCR was 66.7% (16/24; 8 patients had SD and 8 patients had PD, respectively), median OS was 13 months and median PFS was 8 months. After treatment, the levels of CA199 were significantly lower than those before treatment (P<0.05). The incidence of adverse events in 24 patients were rash (14/24, 58.3%), leucopenia (22/24, 91.6%), anemia (20/24, 83.3%). One patient had serious adverse events and withdrew from treatment, one patient died of biliary obstruction with infection during treatment. Conclusion GEMOX combined with target-immunity therapy regimen is safe and effective in the treatment of advanced BTC, it may be used clinically.

Key words: biliary tract neoplasms, recurrence and metastasis, chemotherapy, targeting, immunization, clinical application

中图分类号:

R735.8

邬晓敏, 方益鹏, 章真, 章烨, 金成. 仑伐替尼联合PD-1单抗及GEMOX方案在晚期胆道恶性肿瘤治疗中的临床观察[J]. 临床荟萃, 2024, 39(5): 408-412.

Wu Xiaomin, Fang Yipeng, Zhang Zhen, Zhang Ye, Jin Cheng. Clinical application of GEMOX combined with target-immunity therapy in patients with advanced biliary tract cancer[J]. Clinical Focus, 2024, 39(5): 408-412.

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链接本文: https://huicui.hebmu.edu.cn/CN/10.3969/j.issn.1004-583X.2024.05.004

https://huicui.hebmu.edu.cn/CN/Y2024/V39/I5/408

图/表 8

参考文献 23

[1]	Valle JW, Kelley RK, Nervi B, et al. Biliary tract cancer[J]. Lancet, 2021, 397(10272):428-444. doi: 10.1016/S0140-6736(21)00153-7 pmid: 33516341
[2]	Nakachi K, Ikeda M, Konishi M, et al. Adjuvant S-1 compared with observation in resected biliary tract cancer (JCOG1202, ASCOT): A multicentre, open-label, randomised, controlled, phase 3 trial[J]. Lancet, 2023, 401(10372):195-203. doi: 10.1016/S0140-6736(22)02038-4 pmid: 36681415
[3]	Subbiah V, Lassen U, Élez E, et al. Dabrafenib plus trametinib in patients with BRAFV600E-mutated biliary tract cancer (ROAR): A phase 2, open-label, single-arm, multicentre basket trial[J]. Lancet Oncol, 2020, 21(9):1234-1243. doi: S1470-2045(20)30321-1 pmid: 32818466
[4]	Ioka T, Kanai M, Kobayashi S, et al. Randomized phase III study of gemcitabine, cisplatin plus S-1 versus gemcitabine, cisplatin for advanced biliary tract cancer (KHBO1401- MITSUBA)[J]. J Hepatobiliary Pancreat Sci, 2023, 30(1):102-110.
[5]	Jiang Q, Huang J, Zhang B, et al. Efficacy and safety of anti-PD1/PDL1 in advanced biliary tract cancer: A systematic review and meta-analysis[J]. Front Immunol, 2022, 13:801909.
[6]	Zhu C, Xue J, Wang Y, Wang S, et al. Efficacy and safety of lenvatinib combined with PD-1/PD-L1 inhibitors plus Gemox chemotherapy in advanced biliary tract cancer[J]. Front Immunol, 2023, 14:1109292.
[7]	Dong X, Zhang Z, Zhang Q, et al. Triple therapy in biliary tract cancers: GemOX plus immune checkpoint inhibitor in combination with lenvatinib or NGS-guided targeted therapy[J]. J Cancer Res Clin Oncol, 2023, 149(5):1917-1927.
[8]	Shi GM, Huang XY, Wu D, et al. Toripalimab combined with lenvatinib and GEMOX is a promising regimen as first-line treatment for advanced intrahepatic cholangiocarcinoma: A single-center, single-arm, phase 2 study[J]. Signal Transduct Target Ther, 2023, 8(1):106.
[9]	Vogel A, Bridgewater J, Edeline J, et al. Biliary tract cancer: ESMO Clinical Practice Guideline for diagnosis, treatment and follow-up[J]. Ann Oncol, 2023, 34(2):127-140.
[10]	Fung S, Syed YY. Durvalumab: A review in advanced biliary tract cancer[J]. Target Oncol, 2023, 18(6):965-972. doi: 10.1007/s11523-023-01007-y pmid: 37943483
[11]	Vogel A, Bathon M, Saborowski A. Immunotherapies in clinical development for biliary tract cancer[J]. Expert Opin Investig Drugs, 2021, 30(4):351-363.
[12]	Harding JJ, Khalil DN, Fabris L, et al. Rational development of combination therapies for biliary tract cancers[J]. J Hepatol, 2023, 78(1):217-228.
[13]	Benson AB, D'Angelica MI, Abrams T, et al. NCCN guidelines^® insights: Biliary tract cancers, version 2.2023[J]. J Natl Compr Canc Netw, 2023, 21(7):694-704.
[14]	Feng K, Liu Y, Zhao YT, et al. Efficacy and biomarker analysis of nivolumab plus gemcitabine and cisplatin in patients with unresectable or metastatic biliary tract cancers: Results from a phase II study[J]. J Immunother Cancer, 2020, 8(1):e000367.
[15]	Sahai V, Griffith KA, Beg MS, et al. A randomized phase 2 trial of nivolumab, gemcitabine, and cisplatin or nivolumab and ipilimumab in previously untreated advanced biliary cancer: BilT-01[J]. Cancer, 2022, 128(19):3523-3530. doi: 10.1002/cncr.34394 pmid: 35895381
[16]	Chen X, Wang D, Liu J, et al. Genomic alterations in biliary tract cancer predict prognosis and immunotherapy outcomes[J]. J Immunother Cancer, 2021, 9(11):e003214.
[17]	Liu F, Hao X, Liu B, et al. Bile liquid biopsy in biliary tract cancer[J]. Clin Chim Acta, 2023, 551:117593.
[18]	Zhang T, Yang X, Yang X, et al. Different interventional time of hepatic arterial infusion with PD-1 inhibitor for advanced biliary tract cancer: A multicenter retrospective study[J]. Am J Cancer Res, 2022, 12(7):3455-3463. pmid: 35968352
[19]	Galluzzi L, Buqué A, Kepp O, et al. Immunological effects of conventional chemotherapy and targeted anticancer agents[J]. Cancer Cell, 2015, 28(6):690-714. doi: S1535-6108(15)00389-X pmid: 26678337
[20]	Sun W, Patel A, Normolle D, et al. A phase 2 trial of regorafenib as a single agent in patients with chemotherapy-refractory, advanced, and metastatic biliary tract adenocarcinoma[J]. Cancer, 2019, 125(6):902-909. doi: 10.1002/cncr.31872 pmid: 30561756
[21]	Galluzzi L, Vitale I, Aaronson SA, et al. Molecular mechanisms of cell death: Recommendations of the nomenclature committee on cell death 2018[J]. Cell Death Differ, 2018, 25(3):486-541. doi: 10.1038/s41418-017-0012-4 pmid: 29362479
[22]	Patel SA, Minn AJ. Combination cancer therapy with immune checkpoint blockade: Mechanisms and strategies[J]. Immunity, 2018, 48(3):417-433. doi: S1074-7613(18)30083-9 pmid: 29562193
[23]	Zhu S, Zhang T, Zheng L, et al. Combination strategies to maximize the benefits of cancer immunotherapy[J]. J Hematol Oncol, 2021, 14(1):156.

序号	性别	分期	病理类型	是否转移	转移部位
1	女	Ⅳ	胆囊癌	是	肝脏
2	女	Ⅳ	肝内胆管癌	是	肝脏
3	男	Ⅳ	肝内胆管癌	是	肝脏
4	男	Ⅳ	胆囊癌	是	肝脏
5	女	Ⅳ	胆囊癌	是	第16组淋巴结
6	女	Ⅳ	肝内胆管癌	是	肝脏
7	男	Ⅳ	胆囊癌	是	肝脏
8	男	Ⅳ	肝门部胆管癌	是	肝脏
9	男	Ⅳ	胆囊癌	是	第16组淋巴结
10	男	Ⅳ	肝门部胆管癌	是	肝脏
11	女	Ⅳ	胆管下段癌	是	肝脏
12	男	Ⅳ	肝内胆管癌	是	肝脏
13	女	Ⅳ	胆囊癌	是	肝脏
14	女	Ⅳ	肝门部胆管癌	是	肝脏
15	男	Ⅳ	肝内胆管癌	是	肝脏
16	男	Ⅳ	胆管下段癌	是	肝脏
17	女	Ⅳ	胆囊癌	是	第16组淋巴结
18	女	Ⅳ	肝门部胆管癌	是	肝脏
19	男	Ⅳ	肝内胆管癌	是	肝脏
20	男	Ⅳ	胆管下段癌	是	肝脏
21	男	Ⅳ	胆囊癌	是	第16组淋巴结
22	男	Ⅳ	肝内胆管癌	是	肝脏
23	女	Ⅳ	胆管下段癌	是	肝脏
24	男	Ⅳ	肝内胆管癌	是	肝脏

序号	性别	分期	病理类型	是否转移	转移部位
1	女	Ⅳ	胆囊癌	是	肝脏
2	女	Ⅳ	肝内胆管癌	是	肝脏
3	男	Ⅳ	肝内胆管癌	是	肝脏
4	男	Ⅳ	胆囊癌	是	肝脏
5	女	Ⅳ	胆囊癌	是	第16组淋巴结
6	女	Ⅳ	肝内胆管癌	是	肝脏
7	男	Ⅳ	胆囊癌	是	肝脏
8	男	Ⅳ	肝门部胆管癌	是	肝脏
9	男	Ⅳ	胆囊癌	是	第16组淋巴结
10	男	Ⅳ	肝门部胆管癌	是	肝脏
11	女	Ⅳ	胆管下段癌	是	肝脏
12	男	Ⅳ	肝内胆管癌	是	肝脏
13	女	Ⅳ	胆囊癌	是	肝脏
14	女	Ⅳ	肝门部胆管癌	是	肝脏
15	男	Ⅳ	肝内胆管癌	是	肝脏
16	男	Ⅳ	胆管下段癌	是	肝脏
17	女	Ⅳ	胆囊癌	是	第16组淋巴结
18	女	Ⅳ	肝门部胆管癌	是	肝脏
19	男	Ⅳ	肝内胆管癌	是	肝脏
20	男	Ⅳ	胆管下段癌	是	肝脏
21	男	Ⅳ	胆囊癌	是	第16组淋巴结
22	男	Ⅳ	肝内胆管癌	是	肝脏
23	女	Ⅳ	胆管下段癌	是	肝脏
24	男	Ⅳ	肝内胆管癌	是	肝脏

项目	0级	1级	2级	3级	4级
皮肤	无	红斑	干性脱水、水疱、瘙痒	湿性皮炎、溃疡	剥脱性皮炎、坏死、需手术
白细胞下降(×10⁹)	≥4.0	3.0~3.9	2.0~2.9	1.0~1.9	<1.0
贫血(HB g/L)	≥110	95~109	80~94	65~79	<65

项目	0级	1级	2级	3级	4级
皮肤	无	红斑	干性脱水、水疱、瘙痒	湿性皮炎、溃疡	剥脱性皮炎、坏死、需手术
白细胞下降(×10⁹)	≥4.0	3.0~3.9	2.0~2.9	1.0~1.9	<1.0
贫血(HB g/L)	≥110	95~109	80~94	65~79	<65

组别	例数	CEA(μg/L)	CA125(kU/L)	CA199(kU/L)
治疗前	24	72.85±207.99	33.50±38.31	148.09±174.12
治疗后	24	8.91±13.52	32.56±45.07	67.16±59.07
t值		1.59	0.073	3.217
P值		0.125	0.942	0.004