Analysis of the correlation between the dose exposure intensity and apatinib in advanced gastric cancer: a retrospective cohort study.

IF 3.5 3区医学 Q2 ONCOLOGY Frontiers in Oncology Pub Date : 2025-02-05 eCollection Date: 2025-01-01 DOI:10.3389/fonc.2025.1470462

Xiao Ma, Lan Gao, Siying Che, Chaofeng Tao

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Abstract

Background: Apatinib is a small molecule anti-angiogenesis targeted drug that has demonstrated significant efficacy as a late-line treatment in advanced gastric cancer in phase 3 clinical trials. This study amid to evaluate the correlation between dose exposure intensity and efficacy and safety of apatinib in the treatment of advanced gastric cancer.

Methods: We conducted an observational, retrospective cohort study of patients with advanced gastric cancer who received apatinib targeted therapy in Beijing Friendship Hospital affiliated to Capital Medical University between June 1, 2018, and June 30, 2021. Dose exposure intensity (DEI) was defined as the product of dose and continuous medication time. Patients were assigned to high-dose exposure intensity (HDEI) and low-dose exposure intensity (LDEI) cohorts. The primary endpoint was progression-free survival (PFS), and the secondary endpoints were overall survival (OS) and safety. The relationship between HDEI and LDEI and clinical outcomes was analyzed by using the Kaplan-Meier curve and χ² test.

Results: 61 patients were enrolled and assigned into two retrospective cohorts. The median PFS (mPFS) were 6.50 months (95% confidence interval (CI) [4.80-9.20]) and 4.10 months (95% CI [3.70-5.20]), and the median OS (mOS) were 10.70 months (95% CI [9.20-18.50]) and 7.50 months (95% CI [6.80-9.30]) for the HDEI and LDEI cohorts, respectively. The mPFS were 5.85 months (95% CI [5.00-7.00]) and 4.60 months (95% CI [4.10-5.90]), and mOS were 9.60 months (95% CI [9.10-12.40]) and 7.60 months (95% CI [7.20-10.20]) the for the 250 mg cohort and 500 mg cohorts. The mPFS were 6.65 months (95% CI [5.90-9.20]) and 4.10 months (95% CI [3.90-5.20]), and the mOS were 11.20 months (95% CI [9.20-18.50]) and 7.60 months (95% CI [7.20-9.60])for the long medication time and short medication time cohorts, respectively. The most common TRAEs of any grade were hypertension, proteinuria, and neutrophil count decreased. The incidence of grade 3-4 adverse reactions in the 500 mg cohort was higher than the 250 mg cohort (P=0.0016).

Conclusion: The efficacy of apatinib in advanced gastric cancer was significantly positively correlated with dose exposure intensity, and HDEI can prolong PFS and OS. Early application of low-dose apatinib (250 mg/d) can improve patients' tolerability, and the adverse reactions are controllable.

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晚期胃癌患者剂量暴露强度与阿帕替尼相关性的回顾性队列研究。

背景：阿帕替尼是一种小分子抗血管生成靶向药物，在3期临床试验中作为晚期胃癌的晚期治疗显示出显著的疗效。本研究旨在评价阿帕替尼治疗晚期胃癌的剂量暴露强度与疗效和安全性的相关性。方法：对2018年6月1日至2021年6月30日在首都医科大学附属北京友谊医院接受阿帕替尼靶向治疗的晚期胃癌患者进行观察性、回顾性队列研究。剂量暴露强度（DEI）定义为剂量与连续给药时间的乘积。患者被分配到高剂量暴露强度（HDEI）和低剂量暴露强度（LDEI）队列。主要终点是无进展生存期（PFS），次要终点是总生存期（OS）和安全性。采用Kaplan-Meier曲线和χ2检验分析HDEI、LDEI与临床结局的关系。结果：61例患者被纳入两个回顾性队列。HDEI和LDEI组的中位PFS （mPFS）分别为6.50个月（95%可信区间[4.80-9.20]）和4.10个月（95% CI[3.70-5.20]），中位OS （mOS）分别为10.70个月（95% CI[9.20-18.50]）和7.50个月（95% CI[6.80-9.30]）。250 mg组和500 mg组的mPFS分别为5.85个月（95% CI[5.00-7.00]）和4.60个月（95% CI [4.10-5.90]）， mOS分别为9.60个月（95% CI[9.10-12.40]）和7.60个月（95% CI[7.20-10.20]）。较长用药时间组和较短用药时间组的最短生存期分别为6.65个月（95% CI[5.90-9.20]）和4.10个月（95% CI[3.90-5.20]），最长生存期分别为11.20个月（95% CI[9.20-18.50]）和7.60个月（95% CI[7.20-9.60]）。最常见的trae是高血压、蛋白尿和中性粒细胞计数减少。500 mg组3-4级不良反应发生率高于250 mg组（P=0.0016）。结论：阿帕替尼治疗晚期胃癌的疗效与剂量暴露强度显著正相关，HDEI可延长PFS和OS。早期应用小剂量阿帕替尼（250mg /d）可提高患者耐受性，不良反应可控。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Frontiers in Oncology Biochemistry, Genetics and Molecular Biology-Cancer Research

CiteScore

6.20

自引率

10.60%

发文量

6641

审稿时长

14 weeks

期刊介绍： Cancer Imaging and Diagnosis is dedicated to the publication of results from clinical and research studies applied to cancer diagnosis and treatment. The section aims to publish studies from the entire field of cancer imaging: results from routine use of clinical imaging in both radiology and nuclear medicine, results from clinical trials, experimental molecular imaging in humans and small animals, research on new contrast agents in CT, MRI, ultrasound, publication of new technical applications and processing algorithms to improve the standardization of quantitative imaging and image guided interventions for the diagnosis and treatment of cancer.