对新辅助治疗失败的局部晚期食管鳞癌患者进行基于S-1的同步化放疗加尼莫妥珠单抗治疗:一项真实世界的前瞻性研究。

IF 4.4 4区 医学 Q2 ONCOLOGY
Cancer Biology & Therapy Pub Date : 2024-12-31 Epub Date: 2024-10-27 DOI:10.1080/15384047.2024.2417464
Xin Wang, Guojie Feng, Xiongtao Yang, Nuo Yu, Ziyu Zheng, Jiao Li, Xiaozheng Kang, Xiankai Chen, Ruixiang Zhang, Yong Li, Zhen Wang, Lei Deng, Tao Zhang, Wenyang Liu, Jianyang Wang, Wenqing Wang, Qinfu Feng, Zefen Xiao, Zongmei Zhou, Nan Bi, Yin Li, Jianjun Qin
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引用次数: 0

摘要

目的:这项前瞻性研究在真实世界环境中调查了基于S-1加尼莫妥珠单抗(S-1-Nimo)的同步化学放疗(CCRT)在新辅助化疗或化学免疫治疗失败的局部晚期食管鳞状细胞癌(LA-ESCC)患者中的可行性和安全性:新辅助化疗或化疗免疫治疗失败的局部晚期食管鳞癌(LA-ESCC)患者入组,接受为期4周的S-1-Nimo方案放疗(40 Gy,20次/分,每周5天)、S-1化疗和尼莫妥珠单抗治疗。然后,在手术评估后,被评估为可切除疾病的患者接受手术治疗;不可切除疾病的患者在接受S-1-尼莫治疗的同时继续接受确定性放疗(50-60 Gy,分25-30次,每周5天)。主要终点是无事件生存期(EFS):结果:64 名患者接受了治疗和评估。中位随访时间为 23.2 个月。中位无事件生存期为 9.6 个月(95% 置信区间 [CI],7.1-14.0),估计 2 年无事件生存率为 24.2%。中位总生存期(OS)和预计2年OS率分别为13.4个月(95% CI,10.3-17.5)和31.2%。12例患者接受了手术治疗,手术转化率为18.8%,R0切除率为100.0%。亚组分析发现,与接受CCRT治疗的患者相比,接受根治性手术的患者的EFS和OS明显延长(中位EFS,未达8.7个月 vs. 8.7个月;p = .0117;中位OS,24.9个月 vs. 10.6个月;p = .0205)。64名患者中,3级不良事件主要包括放射性食管炎(4.7%)、贫血(1.6%)和血小板减少(1.6%):该研究表明,在新辅助化疗或化疗免疫治疗失败的LA-ESCC患者中,基于S-1-尼莫的CCRT具有合理的疗效和良好的安全性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
S-1-based concurrent chemoradiotherapy plus nimotuzumab in patients with locally advanced esophageal squamous cell carcinoma who failed neoadjuvant therapy: a real-world prospective study.

Purpose: This prospective study in a real-world setting investigated the feasibility and safety of S-1 plus nimotuzumab (S-1-Nimo) based concurrent chemoradiotherapy (CCRT) in locally advanced esophageal squamous cell carcinoma (LA-ESCC) patients who failed to neoadjuvant chemotherapy or chemoimmunotherapy.

Methods: LA-ESCC patients who failed to converse to resectable disease after neoadjuvant chemotherapy or chemoimmunotherapy were enrolled to receive the 4-week S-1-Nimo regimen of radiotherapy (40 Gy in 20 fractions, 5 days per week), S-1 chemotherapy, and nimotuzumab. Then, after surgical assessments, patients evaluated as resectable disease received surgery; patients with unresectable disease continued to receive definitive radiotherapy (50-60 Gy in 25-30 fractions, 5 days per week) concurrently with S-1-Nimo. The primary endpoint was event-free survival (EFS).

Results: Sixty-four patients were enrolled and evaluated. The median follow-up time was 23.2 months. Median EFS was 9.6 (95% confidence interval [CI], 7.1-14.0) months, with an estimated 2-year EFS rate of 24.2%. The median overall survival (OS) and the estimated OS rate at 2 years were 13.4 (95% CI, 10.3-17.5) months and 31.2%, respectively. Twelve underwent surgery, with a surgical conversion rate of 18.8% and an R0 resection rate of 100.0%. Subgroup analysis identified the significantly prolonged EFS and OS in patients who experienced radical surgery (median EFS, not reached vs. 8.7 months; p = .0117. median OS, 24.9 vs. 10.6 months; p = .0205) as compared to those treated with CCRT. Of 64 patients, grade 3 adverse events mainly included radiation esophagitis (4.7%), anemia (1.6%), and thrombocytopenia (1.6%).

Conclusion: The study demonstrated the reasonable efficacy and promising safety of the S-1-Nimo-based CCRT in LA-ESCC patients with failure to neoadjuvant chemotherapy or chemoimmunotherapy.

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来源期刊
Cancer Biology & Therapy
Cancer Biology & Therapy 医学-肿瘤学
CiteScore
7.00
自引率
0.00%
发文量
60
审稿时长
2.3 months
期刊介绍: Cancer, the second leading cause of death, is a heterogenous group of over 100 diseases. Cancer is characterized by disordered and deregulated cellular and stromal proliferation accompanied by reduced cell death with the ability to survive under stresses of nutrient and growth factor deprivation, hypoxia, and loss of cell-to-cell contacts. At the molecular level, cancer is a genetic disease that develops due to the accumulation of mutations over time in somatic cells. The phenotype includes genomic instability and chromosomal aneuploidy that allows for acceleration of genetic change. Malignant transformation and tumor progression of any cell requires immortalization, loss of checkpoint control, deregulation of growth, and survival. A tremendous amount has been learned about the numerous cellular and molecular genetic changes and the host-tumor interactions that accompany tumor development and progression. It is the goal of the field of Molecular Oncology to use this knowledge to understand cancer pathogenesis and drug action, as well as to develop more effective diagnostic and therapeutic strategies for cancer. This includes preventative strategies as well as approaches to treat metastases. With the availability of the human genome sequence and genomic and proteomic approaches, a wealth of tools and resources are generating even more information. The challenge will be to make biological sense out of the information, to develop appropriate models and hypotheses and to translate information for the clinicians and the benefit of their patients. Cancer Biology & Therapy aims to publish original research on the molecular basis of cancer, including articles with translational relevance to diagnosis or therapy. We will include timely reviews covering the broad scope of the journal. The journal will also publish op-ed pieces and meeting reports of interest. The goal is to foster communication and rapid exchange of information through timely publication of important results using traditional as well as electronic formats. The journal and the outstanding Editorial Board will strive to maintain the highest standards for excellence in all activities to generate a valuable resource.
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