Impact of imatinib adjuvant therapy on the postoperative prognosis of patients with non-gastric primary high-risk GIST

doi:10.3760/cma.j.cn371439-20250826-00046

Abstract

Abstract:

Objective To analyze the impact of imatinib adjuvant therapy on the postoperative prognosis of patients with non-gastric primary high-risk gastrointestinal stromal tumor （GIST）. Methods A retrospective analysis was conducted on the clinical data， postoperative treatment and survival information of 40 patients with non-gastric primary high-risk GIST admitted to Weihai Municipal Hospital Affiliated to Shandong University from January 1， 2010 to May 30， 2022. All patients underwent radical surgical resection. Patients receiving imatinib （400 mg/d） as adjuvant therapy started taking the medication 4 to 8 weeks after the surgery. Univariate and multivariate analyses of factors influencing patient prognosis were performed using the Cox proportional hazards regression model. Kaplan-Meier survival curves were plotted， and patients were stratified based on whether they completed 3-year or 5-year postoperative imatinib adjuvant therapy. Inter-group comparisons were made using the log-rank test. Results By the end of the follow-up period， among the 40 patients， 37 received adjuvant therapy， of whom 16 experienced tumor progression and 7 of these died due to tumor progression； 3 patients did not receive adjuvant therapy， and 2 of them died due to tumor progression. The 3-， 5-， and 10-year disease-free survival （DFS） rates were 79.1%， 60.0%， and 25.3%， respectively， while the 3-， 5-， and 10-year overall survival （OS） rates were 94.1%， 90.6%， and 54.1%， respectively. Univariate analysis revealed that the Ki-67 （HR=4.01， 95%CI： 1.04-15.27， P=0.048） and imatinib adjuvant therapy （HR=4.59， 95%CI： 1.05-20.23， P=0.041） were factors influencing DFS. Tumor number （HR=5.83， 95%CI： 1.06-21.93， P=0.042） and imatinib adjuvant therapy （HR=5.05， 95%CI： 1.03-24.26， P=0.044） were factors influencing OS. Multivariate analysis identified Ki-67>5% （HR=4.21， 95%CI： 1.03-20.73， P=0.046） and without postoperative imatinib adjuvant therapy （HR=6.23， 95%CI： 1.23-31.59， P=0.027） as independent risk factors for DFS. Multiple tumor numbers （HR=8.77， 95%CI： 1.40-55.01， P=0.020） and not receiving postoperative imatinib adjuvant therapy （HR=7.70， 95%CI： 1.28-46.41， P=0.026） were independent risk factors for OS. The 5-year DFS and OS rates were 46.2% and 90.0% in the group receiving postoperative imatinib adjuvant therapy for less than 3 years， compared to 90.0% and 100.0% in the group receiving therapy for more than 3 years， with statistically significant differences （χ²=8.24， P=0.004； χ²=6.34， P=0.012）. The 5-year DFS and OS rates were 55.0% and 92.2% in the group receiving postoperative imatinib adjuvant therapy for less than 5 years， compared to 100% and 100% in the group receiving therapy for more than 5 years. There was a statistically significant difference in the 5-year DFS rate between the two groups （χ²=3.94， P=0.047）， but no statistically significant difference in the 5-year OS rate （χ²=2.10， P=0.147）. Conclusions Ki-67>5%， multiple tumor numbers and without postoperative imatinib adjuvant therapy are independent risk factors affecting the postoperative prognosis of non-gastric primary high-risk GIST patients. 5-year imatinib adjuvant therapy can prolong the postoperative DFS of non-gastric primary high-risk GIST patients and improve their prognosis.

Key words: Gastrointestinal stromal tumors, Neoadjuvant therapy, Prognosis, Imatinib

Yang Song, Zheng Xiangyun, Pan Yingxue, Wang Jiaming, Zhang Huanhu. Impact of imatinib adjuvant therapy on the postoperative prognosis of patients with non-gastric primary high-risk GIST[J]. Journal of International Oncology, 2026, 53(5): 283-289.

Figures/Tables 6

References 26

[1]	Wang MX, Devine C, Segaran N, et al. Current update on molecular cytogenetics, diagnosis and management of gastrointestinal stromal tumors[J]. World J Gastroenterol, 2021, 27(41): 7125-7133. DOI: 10.3748/wjg.v27.i41.7125.
[2]	Serrano C, Martín-Broto J, Asencio-Pascual JM, et al. 2023 GEIS Guidelines for gastrointestinal stromal tumors[J]. Ther Adv Med Oncol, 2023, 15: 17588359231192388. DOI: 10.1177/17588359231192388.
[3]	Nishida T, Naito Y, Takahashi T, et al. Molecular and clinicopathological features of KIT/PDGFRA wild-type gastrointestinal stromal tumors[J]. Cancer Sci, 2024, 115(3): 894-904. DOI: 10.1111/cas.16058.
[4]	Nannini M, Rizzo A, Indio V, et al. Targeted therapy in SDH-deficient GIST[J]. Ther Adv Med Oncol, 2021, 13: 17588359211023278. DOI: 10.1177/17588359211023278.
[5]	Khosroyani HM, Klug LR, Heinrich MC. TKI treatment sequencing in advanced gastrointestinal stromal tumors[J]. Drugs, 2023, 83(1): 55-73. DOI: 10.1007/s40265-022-01820-1. pmid: 36607590
[6]	中国临床肿瘤学会指南工作委员会. 中国临床肿瘤学会(CSCO)胃肠间质瘤诊疗指南2024[M]. 北京: 人民卫生出版社, 2024.
[7]	Zhang XQ, Ning L, Hu YL, et al. Prognostic factors for primary localized gastrointestinal stromal tumors after radical resection: Shandong Gastrointestinal Surgery Study Group, Study 1201[J]. Ann Surg Oncol, 2020, 27(8): 2812-2821. DOI: 10.1245/s10434-020-08244-9. pmid: 32040699
[8]	Alfagih A, AlJassim A, Alshamsan B, et al. Gastrointestinal stromal tumors: 10-year experience in Cancer Center—The Ottawa Hospital (TOH)[J]. Curr Oncol, 2022, 29(10): 7148-7157. DOI: 10.3390/curroncol29100562.
[9]	Joensuu H. KIT and PDGFRA variants and the survival of patients with gastrointestinal stromal tumor treated with adjuvant imatinib[J]. Cancers (Basel), 2023, 15(15): 3879. DOI: 10.3390/cancers15153879.
[10]	Kim Y, Lee SH. Pathologic diagnosis and molecular features of gastrointestinal stromal tumors: a mini-review[J]. Front Oncol, 2024, 14: 1487467. DOI: 10.3389/fonc.2024.1487467.
[11]	Lopez Gordo S, Bettonica C, Miró M, et al. Gastric and small intestine gist: results of 156 cases in 20 years[J]. J Gastrointest Cancer, 2022, 53(2): 451-459. DOI: 10.1007/s12029-021-00641-x.
[12]	黄镇, 张蔡羽天, 柯少波, 等. 结直肠癌患者术后预后模型的构建[J]. 国际肿瘤学杂志, 2023, 50(3): 157-163. DOI: 10.3760/cma.j.cn371439-20221123-00031.
[13]	Masucci MT, Motti ML, Minopoli M, et al. Emerging targeted therapeutic strategies to overcome imatinib resistance of gastrointestinal stromal tumors[J]. Int J Mol Sci, 2023, 24(7): 6026. DOI: 10.3390/ijms24076026.
[14]	Wang LQ, Ni ZT, Xu W, et al. Clinical characteristics and outcomes of gastrointestinal stromal tumor patients receiving surgery with or without TKI therapy: a retrospective real-world study[J]. World J Surg Oncol, 2023, 21(1): 21. DOI: 10.1186/s12957-023-02897-y. pmid: 36691015
[15]	Qu H, Xu Z, Ren Y, et al. The analysis of prognostic factors of primary small intestinal gastrointestinal stromal tumors with R0 resection: a single-center retrospective study[J]. Medicine (Baltimore), 2022, 101(25): e29487. DOI: 10.1097/MD.0000000000029487.
[16]	Wu H, Li C, Li H, et al. Clinicopathological characteristics and longterm survival of patients with synchronous multiple primary gastrointestinal stromal tumors: a propensity score matching analysis[J]. World J Gastroenterol, 2021, 27(36): 6128-6141. DOI: 10.3748/wjg.v27.i36.6128.
[17]	Chen L, Lu Y, Qian JW, et al. Clinical characteristics and prognosis of non-metastatic multiple gastrointestinal stromal tumors: a population-based study[J]. Discov Oncol, 2025, 16(1): 643. DOI: 10.1007/s12672-025-02454-x. pmid: 40304924
[18]	Joensuu H, Eriksson M, Sundby Hall K, et al. One vs Three Years of adjuvant imatinib for operable gastrointestinal stromal tumor: a randomized trial[J]. JAMA, 2012, 307(12): 1265-1272. DOI: 10.1001/jama.2012.347. pmid: 22453568
[19]	Joensuu H, Eriksson M, Sundby Hall K, et al. Survival outcomes associated with 3 years vs 1 year of adjuvant imatinib for patients with high-risk gastrointestinal stromal tumors: an analysis of a randomized clinical trial after 10-year follow-up[J]. JAMA Oncology, 2020, 6(8): 1241-1246. DOI: 10.1001/jamaoncol.2020.2091. pmid: 32469385
[20]	Raut CP, Espat NJ, Maki RG, et al. Efficacy and tolerability of 5-year adjuvant imatinib treatment for patients with resected intermediate- or high-risk primary gastrointestinal stromal tumor: the PERSIST-5 clinical trial[J]. JAMA Oncology, 2018, 4(12): e184060. DOI: 10.1001/jamaoncol.2018.4060.
[21]	蒋祈, 田红坤, 杜雨强, 等. 2004―2022年单中心高危胃肠道间质瘤的诊断与治疗(附568例报告)[J]. 中华消化外科杂志, 2024, 23(3): 398-405. DOI: 10.3760/cma.j.cn115610-20240203-00065.
[22]	王晓娜, 曹景新, 王宝贵, 等. 初诊手术治疗胃肠间质瘤临床病理特征及预后因素的真实世界研究[J]. 中华消化外科杂志, 2024, 23(8): 1080-1086. DOI: 10.3760/cma.j.cn115610-20240613-00293.
[23]	张鹏, 张军, 张波, 等. 中国胃肠间质瘤患者伊马替尼服药依从性的多中心横断面调查[J]. 中华胃肠外科杂志, 2021, 24(9): 775-782. DOI: 10.3760/cma.j.cn.441530-20210426-00174.
[24]	Joensuu H, Eriksson M, Sundby Hall K, et al. Adjuvant imatinib for high-risk GI stromal tumor: analysis of a randomized trial[J]. J Clin Oncol, 2015, 34(3): 244-250. DOI: 10.1200/JCO.2015.62.9170.
[25]	Zemła P, Stelmach A, Jabłońska B, et al. A retrospective study of postoperative outcomes in 98 patients diagnosed with gastrointestinal stromal tumor (GIST) of the upper, middle, and lower gastrointestinal tract between 2009 and 2019 at a single center in Poland[J]. Med Sci Monit, 2021, 27: e932809. DOI: 10.12659/MSM.932809.
[26]	Blay JY, Schiffler C, Bouché O, et al. A randomized study of 6 versus 3 years of adjuvant imatinib in patients with localized GIST at high risk of relapse[J]. Ann Oncol, 2024, 35(12): 1157-1168. DOI: 10.1016/j.annonc.2024.08.2343. pmid: 39241959

因素	β值	SE值	Wald χ²值	HR值	95%CI	P值
性别
男				Ref
女	-0.48	0.64	0.56	0.62	0.18~2.17	0.455
年龄（岁）
≤60				Ref
>60	-0.32	0.49	0.43	0.73	0.28~1.89	0.512
肿瘤位置
小肠				Ref
非小肠	-0.07	0.64	0.01	0.93	0.26~3.28	0.912
肿瘤数目
单发				Ref
多发	0.88	0.78	1.27	2.40	0.52~11.05	0.260
肿瘤最大径（cm）
≤5				Ref
>5	-0.50	0.54	0.87	0.61	0.21~1.73	0.351
组织学类型
梭形细胞型				Ref
非梭形细胞型	0.62	1.06	0.34	1.86	0.23~14.90	0.559
核分裂象（个/5 mm²）
≤5				Ref
>5	0.71	0.50	1.96	2.02	0.76~5.43	0.161
Ki-67(%)
≤5				Ref
>5	1.39	0.69	4.06	4.01	1.04~15.27	0.048
CD34
阴性				Ref
阳性	-0.50	0.52	0.91	0.60	0.22~1.69	0.340
伊马替尼辅助治疗
是				Ref
否	1.52	0.74	4.15	4.59	1.05~20.23	0.041

因素	β值	SE值	Wald χ²值	HR值	95%CI	P值
性别
男				Ref
女	-3.48	3.48	1.00	0.03	0.05~28.21	0.317
年龄（岁）
≤60				Ref
>60	0.45	0.73	0.38	1.57	0.37~6.56	0.539
肿瘤位置
小肠				Ref
非小肠	0.07	1.08	<0.01	1.07	0.13~8.81	0.950
肿瘤数目
单发				Ref
多发	1.76	0.87	4.12	5.83	1.06~21.93	0.042
肿瘤最大径（cm）
≤5				Ref
>5	-0.16	0.82	0.04	0.85	0.17~4.26	0.847
组织学类型
梭形细胞型				Ref
非梭形细胞型	2.35	1.41	2.76	10.50	0.66~67.86	0.096
核分裂象（个/5mm²）
≤5				Ref
>5	0.01	0.75	<0.01	1.01	0.23~4.40	0.989
Ki-67（%）
≤5				Ref
>5	0.76	1.09	0.50	2.15	0.26~18.00	0.481
CD34
阴性				Ref
阳性	-0.03	0.83	<0.01	0.97	0.19~4.90	0.971
伊马替尼辅助治疗
是				Ref
否	1.62	0.81	4.04	5.05	1.03~24.26	0.044

因素	β值	SE值	Wald χ²值	HR值	95%CI	P值
Ki-67数（%）
≤5				Ref
>5	1.53	0.77	3.97	4.21	1.03~20.73	0.046
伊马替尼辅助治疗
是				Ref
否	1.83	0.83	4.87	6.23	1.23~31.59	0.027

因素	β值	SE值	Wald χ²值	HR值	95%CI	P值
肿瘤数目
单发				Ref
多发	2.17	0.94	5.38	8.77	1.40~55.01	0.020
伊马替尼辅助治疗
是				Ref
否	2.04	0.92	4.96	7.70	1.28~46.41	0.026