帕博利珠单抗联合XELOX方案治疗晚期胃癌的回顾性研究

doi:10.19401/j.cnki.1007-3639.2024.11.005

摘要/Abstract

摘要：

背景与目的：尽管目前针对胃癌的治疗手段已取得了显著进步，但晚期胃癌患者仍存在预后差、5年生存率偏低等问题，因此探究有效的治疗方案仍是临床研究的重点。帕博利珠单抗作为新型免疫检查点抑制剂，其临床应用效果及安全性仍需大量研究予以验证，因此本研究回顾性分析帕博利珠单抗联合XELOX方案治疗晚期胃癌的效果，以期为临床治疗提供参考。方法：回顾性收集2020年3月—2022年8月山西省肿瘤医院收治的晚期胃癌患者的临床资料。纳入标准：经临床组织病理学检查确诊为HER2阴性、未经治疗的晚期胃癌/食管胃结合部腺癌患者，符合相关诊断标准；TNM分期为Ⅳ期；年龄≥20岁；预计生存期≥6个月；治疗前器官无严重损伤者；Karnofsky评分>60分；临床资料完整者。排除标准：合并重要器官功能障碍者；合并甲状腺功能减退或亢进者；合并血液、凝血功能异常者；合并自身免疫性疾病者；哺乳、妊娠期女性；存在精神类疾病或诊断史者；伴有其他恶性肿瘤者；存在严重肝肾功能障碍者；临床资料不全者。通过纳入和排除标准选择91例晚期胃癌患者，其中45例接受XELOX方案治疗（对照组），46例接受帕博利珠单抗联合XELOX方案治疗（观察组），建立数据库后发现观察组1例患者的治疗信息存在逻辑错误，因此去除该病例，最终确定研究对象90例，对照组和观察组各45例。对比两组疗效、中位总生存期（overall survival，OS）、中位无进展生存期（progression-free survival，PFS）、不良反应、生活质量改善情况，以及治疗前后癌胚抗原（carcinoembryonic antigen，CEA）、糖类抗原19-9（carbohydrate antigen 19-9，CA19-9）、大肠杆菌、双歧杆菌、乳杆菌水平。本研究已获得山西省肿瘤医院伦理委员会批准（伦理编号：KY2023081）。结果：治疗后观察组疾病进展（progressive disease，PD）占20.0%（9/45），低于对照组的40.0%（18/45），但两组的疾病稳定（stable disease，SD）、完全缓解（complete response，CR）和部分缓解（partial response，PR）占比差异无统计学意义（P>0.05）。治疗后观察组的生活质量改善率为60.0%（27/45），高于对照组的37.8%（17/45）（P<0.05）。观察组的中位OS和中位PFS均大于对照组（P<0.05）。治疗后观察组的外周血CEA、CA19-9均低于对照组（P<0.05）。治疗后观察组的大肠杆菌数量低于对照组，双歧杆菌、乳杆菌数量均高于对照组（P <0.05）。两组不同等级恶心呕吐、腹泻、白细胞减少、皮疹及肝功能损害的发生率差异无统计学意义（P>0.05）。结论：帕博利珠单抗联合XELOX方案可调节肿瘤标志物在晚期胃癌患者中的水平，预防疾病进展，改善患者生活质量，还有助于维持肠道微生态平衡。

关键词: 帕博利珠单抗, XELOX方案, 化疗, 晚期胃癌, 免疫抑制

Abstract:

Background and purpose: Despite the significant advancements that have been made in the treatment of gastric cancer, there are still problems such as poor prognosis and low five-year survival rate in advanced gastric cancer. Therefore, exploring effective treatment options remains a key focus of clinical research. As a new type of immune checkpoint inhibitor, the clinical efficacy and safety of pembrolizumab still need to be confirmed by extensive research. Therefore, this study conducted regression analysis of the effect of pembrolizumab combined with XELOX regimen in the treatment of advanced gastric cancer, providing a reference for clinical treatment. Methods: Clinical data of patients with advanced gastric cancer who were admitted to Shanxi Province Cancer Hospital from March 2020 to August 2022 were retrospectively collected. Inclusion criteria: patients with HER2-negative, untreated advanced gastric cancer or adenocarcinoma of the esophagogastric junction, confirmed by clinical histopathological examination and meeting relevant diagnostic criteria; TNM stage Ⅳ; age ≥20 years; expected survival ≥6 months; no severe organ damage before treatment; Karnofsky score >60; patients with complete clinical data. Exclusion criteria: patients with concurrent major organ dysfunction; hypothyroidism or hyperthyroidism; blood or coagulation disorders; autoimmune diseases; lactating or pregnant women; individuals with mental illnesses or a history of mental illness; those with concurrent other malignancies; those with severe liver or kidney dysfunction; patients with incomplete clinical data. Based on the inclusion and exclusion criteria, 91 patients with advanced gastric cancer were selected. Among them, 45 received XELOX regimen treatment (control group), and 46 received pembrolizumab combined with XELOX regimen treatment (observation group). After establishing the database, one patient in the observation group was found to have logical errors in their treatment information and was therefore excluded. Ultimately, 90 patients were included in the study, with 45 in each of the control and observation groups. The efficacy, median overall survival (OS), median progression-free survival (PFS), toxic side effects, improvement in quality of life, and levels of carcinoembryonic antigen (CEA), carbohydrate antigen 19-9 (CA19-9), Escherichia coli, Bifidobacterium and Lactobacillus before and after treatment were compared between the two groups. This study was approved by the ethics committee of Shanxi Province Cancer Hospital (ethics number: KY2023081). Results: After treatment, the proportion of progressive disease (PD) in the observation group was 20.0% (9/45), which was lower than that in the control group (40.0%, 18/45). However, there was no significant difference between the two groups in proportion of stable disease (SD), complete response (CR) and partial response (PR) (P>0.05). The improvement rate of quality of life in the observation group after treatment was 60.0% (27/45), which was higher than that in the control group, with a rate of 37.8% (17/45) (P<0.05). The median OS and PFS in the observation group were longer compared with the control group (P<0.05). After treatment, the levels of CEA and CA19-9 in peripheral blood of the observation group were lower compared with the control group (P<0.05). After treatment, the number of Escherichia coli was lower in the observation group than in the control group, while the numbers of Bifidobacterium and Lactobacillus were higher (P<0.05). There was no significant difference in the incidence of nausea and vomiting, diarrhea, leukopenia, rash, liver function damage between the two groups (P > 0.05). Conclusion: The combination of pembrolizumab and XELOX regimen can regulate the expression levels of tumor markers in patients with advanced gastric cancer, prevent disease progression, improve patient quality of life, and help maintain intestinal microecology balance.

Key words: Pembrolizumab, XELOX regimen, Chemotherapy, Advanced gastric cancer, Immunosuppression

中图分类号:

R735.2

冯惠枝, 柳婧美, 卜晓倩. 帕博利珠单抗联合XELOX方案治疗晚期胃癌的回顾性研究[J]. 中国癌症杂志, 2024, 34(11): 1028-1035.

FENG Huizhi, LIU Jingmei, BU Xiaoqian. A retrospective study of pembrolizumab combined with XELOX regimen in the treatment of advanced gastric cancer[J]. China Oncology, 2024, 34(11): 1028-1035.

图/表 6

表1

表2

表3

表4

表5

表6

参考文献 25

[1]	YASUDA T, WANG Y A. Gastric cancer immunosuppressive microenvironment heterogeneity: implications for therapy development[J]. Trends Cancer, 2024, 10(7): 627-642. doi: 10.1016/j.trecan.2024.03.008 pmid: 38600020
[2]	HOU W T, ZHAO Y Q, ZHU H. Predictive biomarkers for immunotherapy in gastric cancer: current status and emerging prospects[J]. Int J Mol Sci, 2023, 24(20): 15321.
[3]	XU J M, JIANG H P, PAN Y Y, et al. Sintilimab plus chemotherapy for unresectable gastric or gastroesophageal junction cancer: the ORIENT-16 randomized clinical trial[J]. JAMA, 2023, 330(21): 2064-2074. doi: 10.1001/jama.2023.19918 pmid: 38051328
[4]	LING Q, HUANG S T, YU T H, et al. Optimal timing of surgery for gastric cancer after neoadjuvant chemotherapy: a systematic review and meta-analysis[J]. World J Surg Oncol, 2023, 21(1): 377. doi: 10.1186/s12957-023-03251-y pmid: 38037067
[5]	YARCHOAN M, GANE E J, MARRON T U, et al. Personalized neoantigen vaccine and pembrolizumab in advanced hepatocellular carcinoma: a phase 1/2 trial[J]. Nat Med, 2024, 30(4): 1044-1053. doi: 10.1038/s41591-024-02894-y pmid: 38584166
[6]	WADDELL T, VERHEIJ M, ALLUM W, et al. Gastric cancer: ESMO-ESSO-ESTRO clinical practice guidelines for diagnosis, treatment and follow-up[J]. Radiother Oncol, 2014, 110(1): 189-194. doi: 10.1016/j.radonc.2013.09.015 pmid: 24636158
[7]	STEDMAN M R, WATFORD D J, CHERTOW G M, et al. Karnofsky performance score-failure to thrive as a frailty proxy?[J]. Transplant Direct, 2021, 7(7): e708. doi: 10.1097/TXD.0000000000001164 pmid: 34124344
[8]	张萍, 艾斌. 实体瘤免疫治疗疗效评价标准[J]. 国际肿瘤学杂志, 2016, 43(11): 848-851.
	ZHANG P, AI B. Efficacy evaluation criteria for immunotherapy in solid tumors[J]. J Int Oncol, 2016, 43(11): 848-851.
[9]	朱春荣, 熊峰, 朱彦博, 等. 贝伐单抗联合FOLFOX4或FOLFIRI方案治疗晚期结直肠癌的临床观察[J]. 江苏医药, 2012, 38(19): 2306-2307.
	ZHU C R, XIONG F, ZHU Y B, et al. Clinical observation of bevacizumab combined with FOLFOX4 or FOLFIRI regimen in the treatment of advanced colorectal cancer[J]. Remote Sens Technol Appl, 2012, 38(19): 2306-2307.
[10]	BANTA K L, XU X Z, CHITRE A S, et al. Mechanistic convergence of the TIGIT and PD-1 inhibitory pathways necessitates co-blockade to optimize anti-tumor CD8⁺ T cell responses[J]. Immunity, 2022, 55(3): 512-526.e9.
[11]	SHITARA K, ÖZGÜROĞLU M, BANG Y J, et al. Pembrolizumab versus paclitaxel for previously treated, advanced gastric or gastro-oesophageal junction cancer (KEYNOTE-061): a randomised, open-label, controlled, phase 3 trial[J]. Lancet, 2018, 392(10142): 123-133. doi: S0140-6736(18)31257-1 pmid: 29880231
[12]	王俊松, 吕秀鹏. 卡培他滨、奥沙利铂联合帕博利珠单抗对进展期胃癌的疗效及安全性[J]. 实用药物与临床, 2022, 25(3): 217-220.
	WANG J S, (LÜ/LV/LU/LYU) X P. Safety and efficacy of capecitabine, oxaliplatin combined with pembrolizumab in advanced gastric cancer[J]. Pract Pharm Clin Remedies, 2022, 25(3): 217-220.
[13]	李璐璐, 黄然欣, 张蓉, 等. 信迪利单抗联合白蛋白紫杉醇对晚期胃癌血清肿瘤标志物水平及免疫功能的影响[J]. 临床和实验医学杂志, 2023, 22(22): 2384-2387.
	LI L L, HUANG R X, ZHANG R, et al. Effect of sintilimab combined with albumin paclitaxel on serum tumor marker levels and immune function in advanced gastric cancer[J]. J Clin Exp Med, 2023, 22(22): 2384-2387.
[14]	邵化敏, 马锦程, 杨贺才. 血清TK1、CEA、CA19-9检测对胃癌的诊断价值及与其临床病理特征的相关性研究[J]. 实用癌症杂志, 2023, 38(5): 730-733.
	SHAO H M, MA J C, YANG H C. Diagnostic value of serum TK1, CEA and CA19-9 detection on gastric cancer and their correlation with clinicopathological features of gastric cancer[J]. Pract J Cancer, 2023, 38(5): 730-733.
[15]	ZHENG L, HU F, HUANG L, et al. Association of metabolomics with PD-1 inhibitor plus chemotherapy outcomes in patients with advanced non-small-cell lung cancer[J]. J Immunother Cancer, 2024, 12(4): e008190.
[16]	AHMED A, TAIT S W G. Targeting immunogenic cell death in cancer[J]. Mol Oncol, 2020, 14(12): 2994-3006. doi: 10.1002/1878-0261.12851 pmid: 33179413
[17]	XIONG G, CHEN Z, LIU Q W, et al. CD276 regulates the immune escape of esophageal squamous cell carcinoma through CXCL1-CXCR2 induced NETs[J]. J Immunother Cancer, 2024, 12(5): e008662.
[18]	GOU M M, ZHANG Y, WANG Z K, et al. PD-1 inhibitor combined with albumin paclitaxel and apatinib as second-line treatment for patients with metastatic gastric cancer: a single-center, single-arm, phase Ⅱ study[J]. Invest New Drugs, 2024, 42(2): 171-178.
[19]	ZHANG T Q, GENG Z J, ZUO M X, et al. Camrelizumab (a PD-1 inhibitor) plus apatinib (an VEGFR-2 inhibitor) and hepatic artery infusion chemotherapy for hepatocellular carcinoma in Barcelona Clinic Liver Cancer stage C (TRIPLET): a phase Ⅱ study[J]. Signal Transduct Target Ther, 2023, 8(1): 413.
[20]	刘昭, 任玉川, 张亚鹏, 等. 信迪利单抗联合化疗对晚期胃癌患者近期疗效及血清CEA sTim-3 sLAG-3和T淋巴细胞亚群的影响[J]. 河北医学, 2024, 30(2): 335-340.
	LIU Z, REN Y C, ZHANG Y P, et al. Effects of sintilimab combined with chemotherapy on short-term efficacy and serum CEA, sTim-3 sLAG-3 and T lymphocyte subsets in patients with advanced gastric cancer[J]. Hebei Med, 2024, 30(2): 335-340.
[21]	李慧珍, 吴紫莹, 范婷婷, 等. 山西省东南部地区胃癌患者肠道菌群分布的配对病例对照研究[J]. 中国微生态学杂志, 2021, 33(8): 869-875.
	LI H Z, WU Z Y, FAN T T, et al. A paired case-control study on the distribution of intestinal flora in patients with gastric cancer in southeastern Shanxi Province[J]. Chin J Microecol, 2021, 33(8): 869-875.
[22]	PAN C L, ZHANG H W, ZHANG L Y, et al. Surgery-induced gut microbial dysbiosis promotes cognitive impairment via regulation of intestinal function and the metabolite palmitic amide[J]. Microbiome, 2023, 11(1): 248. doi: 10.1186/s40168-023-01689-6 pmid: 37936242
[23]	WANG S, XU B L, ZHANG Y Y, et al. The role of intestinal flora on tumorigenesis, progression, and the efficacy of PD-1/PD-L1 antibodies in colorectal cancer[J]. Cancer Biol Med, 2023, 21(1): 65-82.
[24]	MAGER L F, BURKHARD R, PETT N, et al. Microbiome-derived inosine modulates response to checkpoint inhibitor immunotherapy[J]. Science, 2020, 369(6510): 1481-1489. doi: 10.1126/science.abc3421 pmid: 32792462
[25]	ABDULQADIR R, ENGERS J, AL-SADI R. Role of Bifidobacterium in modulating the intestinal epithelial tight junction barrier: current knowledge and perspectives[J]. Curr Dev Nutr, 2023, 7(12): 102026.

Information	Control group (n=45)	Observation group (n=45)	t/χ²/U value	P value
Gender			0.189	0.664
Male	29 (64.44)	27 (60.00)
Female	16 (35.56)	18 (40.00)
Age/year range ($\bar{x}±s$)	40-67 (55.45±5.15)	40-69 (55.67±5.33)	0.199	0.843
ASA classification			0.394	0.694
Level Ⅰ	14 (31.11)	16 (35.56)
Level Ⅱ	19 (42.22)	18 (40.00)
Level Ⅲa	12 (26.67)	11 (24.44)
Tumor location			0.411	0.938
Gastric antrum	13 (28.89)	15 (33.33)
Gastric body	10 (22.22)	11 (24.44)
Cardia	14 (31.11)	12 (26.67)
Angular notch	8 (17.78)	7 (15.56)
Transfer situation			0.284	0.868
Not transferred	8 (17.78)	10 (22.22)
Lymph node metastasis	24 (53.33)	23 (51.11)
Hematogenous metastasis	13 (28.89)	12 (26.67)

Group	Case ⁿ	CEA/(ng·mL^-1)	CA19-9/(U·mL^-1)
Before treatment
Observation group	45	15.90±3.96	56.05±5.67
Control group	45	17.11±2.87	54.89±6.81
t value		1.660	0.878
P value		0.101	0.382
After treatment
Observation group	45	5.51±0.46	18.89±3.01
Control group	45	9.98±0.71	24.75±4.15
t value		35.445	7.668
P value		<0.001	<0.001

Group	Case n	Bifidobacterium CFU/mL		Escherichia coli CFU/mL		Lactobacillus CFU/mL
Group	Case n	Before treatment	After treatment	Before treatment	After treatment	Before treatment	After treatment
Observation group	45	7.95±0.74	8.61±0.84	8.36±0.72	7.55±0.61	7.90±0.67	8.74±0.83
Control group	45	7.83±0.81	7.50±0.63	8.52±0.61	9.11±0.80	7.76±0.78	7.62±0.81
Healthy people	45	9.23±0.95		6.60±0.54		9.30±0.88
F value		38.595	7.092	129.613	10.402	53.449	6.478
P value		<0.001	<0.001	<0.001	<0.001	<0.001	<0.001

Group	Case n	Improvement	Stability	Progress
Observation group	45	27 (60.0)	14 (31.1)	4 (8.9)
Control group	45	17 (37.8)	19 (42.2)	9 (20.0)
χ² value		4.447	1.196	2.248
P value		0.035	0.274	0.134

Group	Case n	Nausea and vomiting		Leukopenia		Rash		Diarrhea		Liver function damage
Group	Case n	Ⅰ-Ⅱ	Ⅲ-Ⅳ	Ⅰ-Ⅱ	Ⅲ-Ⅳ	Ⅰ-Ⅱ	Ⅲ-Ⅳ	Ⅰ-Ⅱ	Ⅲ-Ⅳ	Ⅰ-Ⅱ	Ⅲ-Ⅳ
Observation group	45	5 (11.1)	4 (8.9)	2 (4.4)	2 (4.4)	3 (6.7)	2 (4.4)	4 (8.9)	3 (6.7)	3 (6.7)	5 (11.11)
Control group	45	8 (17.8)	6 (13.3)	5 (11.1)	6 (13.3)	8 (17.8)	5 (11.1)	8 (17.8)	5 (11.1)	9 (20.0)	8 (17.78)
U value		0.064		0.135		0.051		0.887		0.624
P value		0.949		0.893		0.960		0.375		0.533