不可切除的局部晚期或转移性胰腺癌一线化疗方案的比较:系统综述和贝叶斯网络荟萃分析

Luca Mastrantoni, Marta Chiaravalli, Alexia Spring, Viria Beccia, Armando Di Bello, Cinzia Bagalà, Maria Bensi, Diletta Barone, Giovanni Trovato, Giulia Caira, Giulia Giordano, Emilio Bria, Giampaolo Tortora, Lisa Salvatore
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引用次数: 0

摘要

背景在晚期胰腺导管腺癌(PDAC)中,一线化疗是标准的治疗方法。由于缺乏头对头比较的临床试验,我们进行了这项系统综述和网络荟萃分析,以比较 PDAC 治疗方案的疗效和毒性。我们纳入了 2000 年 1 月 1 日之后发表的 2-3 期随机对照试验,这些试验评估了既往未经治疗、无法切除、局部晚期或转移性 PDAC 患者的一线治疗方法。主要评估终点为无进展生存期和总生存期。摘要数据摘自已发表的报告。采用偏差信息标准来选择随机效应或固定效应模型。采用贝叶斯方法估算了带有 95% 可信区间的危险比 (HR)。使用 Cochrane Risk of Bias 2(RoB 2)工具对偏倚风险进行评估,并将研究划分为低偏倚风险、部分偏倚风险或高偏倚风险。证据质量采用建议分级评估、发展和评价方法进行评估。本系统综述和网络荟萃分析已在 PROSPERO 注册,注册号为 CRD42023450330。研究结果共筛选出 6050 条记录,79 项随机对照试验(22 168 例患者)被纳入分析。吉西他滨是最常见的对比治疗药物(79 项试验中有 50 项[63%]),并被视为参照治疗药物。采用固定效应模型对主要结果进行分析。关于无进展生存期(71项试验,19 479名患者),最有效的治疗方法是吉西他滨+纳布-紫杉醇交替亚叶酸、氟尿嘧啶和奥沙利铂([FOLFOX] HR 0-32,95%可信区间0-22-0-47)、顺铂、纳布-紫杉醇、卡培他滨和吉西他滨([PAXG] 0-35、0-22-0-55),以及脂质体伊立替康与氟尿嘧啶、亮菌素和奥沙利铂联合治疗([NALIRIFOX] 0-43,0-34-0-54)、其次是氟尿嘧啶、亮菌素、伊立替康和奥沙利铂([FOLFIRINOX] 0-55,0-47-0-65)和吉西他滨加纳布紫杉醇(0-62,0-54-0-72)。在总生存期方面也观察到了类似的结果(79 项试验,22 104 例患者):PAXG(HR为0-40,95%可信区间为0-25-0-65)、吉西他滨加纳布-紫杉醇交替FOLFOX(0-46,0-32-0-66)和NALIRIFOX(0-56,0-45-0-70)获益最大,其次是FOLFIRINOX(0-66,0-56-0-78)和吉西他滨加纳布-紫杉醇(0-67,0-59-0-77)。总体偏倚风险较低。我们的研究结果表明,对于能够耐受NALIRIFOX和FOLFIRINOX治疗方案的患者来说,NALIRIFOX和FOLFIRINOX是首选方案,吉西他滨加纳布紫杉醇仍是可行的替代方案,尤其是对于不适合三联疗法的患者。三期随机对照试验将对同时或连续使用四联疗法进行研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparison of first-line chemotherapy regimens in unresectable locally advanced or metastatic pancreatic cancer: a systematic review and Bayesian network meta-analysis

Background

In advanced pancreatic ductal adenocarcinoma (PDAC), first-line chemotherapy is the standard of care. Due to the absence of head-to-head comparisons in clinical trials, we performed this systematic review and network meta-analysis to compare treatment options for PDAC in terms of their efficacy and toxicity.

Methods

PubMed, the Cochrane Central Register of Controlled Trials, Embase, and oncological meetings websites were searched until Nov 15, 2023. We included phase 2–3 randomised controlled trials published after Jan 1, 2000, evaluating first-line treatments in patients with previously untreated, unresectable, locally advanced or metastatic PDAC. Primary endpoints assessed were progression-free survival and overall survival. Summary data were extracted from published reports. The deviance information criterion was used to choose between a random-effects or fixed-effects model. Hazard ratios (HRs) with 95% credible intervals were estimated using a Bayesian approach. The risk of bias was evaluated using the Cochrane Risk of Bias 2 (RoB 2) tool and studies were graded as low, some concerns, or high risk of bias. The quality of evidence was evaluated using the Grading of Recommendations Assessment, Development, and Evaluation approach. This systematic review and network meta-analysis is registered with PROSPERO, CRD42023450330.

Findings

6050 records were screened and 79 randomised controlled trials (22 168 patients) were included in the analysis. Gemcitabine was the most frequent comparator (in 50 [63%] of 79 trials) and was considered as the reference treatment. A fixed-effect model was used to analyse the primary outcomes. Regarding progression-free survival (71 trials, 19 479 patients), the most effective treatments were gemcitabine plus nab-paclitaxel alternating folinic acid, fluorouracil, and oxaliplatin ([FOLFOX] HR 0·32, 95% credible interval 0·22–0·47), cisplatin, nab-paclitaxel, capecitabine, and gemcitabine ([PAXG] 0·35, 0·22–0·55), and liposomal irinotecan in combination with fluorouracil, leucovorin, and oxaliplatin ([NALIRIFOX] 0·43, 0·34–0·54), followed by fluorouracil, leucovorin, irinotecan, and oxaliplatin ([FOLFIRINOX] 0·55, 0·47–0·65) and gemcitabine plus nab-paclitaxel (0·62, 0·54–0·72). Similar results were observed for overall survival (79 trials, 22 104 patients): PAXG (HR 0·40, 95% credible interval 0·25–0·65), gemcitabine plus nab-paclitaxel alternating FOLFOX (0·46, 0·32–0·66), and NALIRIFOX (0·56, 0·45–0·70) had the highest benefit, followed by FOLFIRINOX (0·66, 0·56–0·78) and gemcitabine plus nab-paclitaxel (0·67, 0·59–0·77). The overall risk of bias was low to some concerns. Certainty of evidence was low.

Interpretation

Our findings suggest that NALIRIFOX and FOLFIRINOX should be the preferred options for patients who can tolerate these regimens, with gemcitabine plus nab-paclitaxel remaining a viable alternative, particularly in patients unfit for triplet therapy. Phase 3 randomised controlled trials investigating concomitant or sequential quadruplets are warranted.

Funding

None.
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