Surrogate Indicators of Overall Survival in Advanced Hepatocellular Carcinoma

Hao Liu
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引用次数: 0

Abstract

For more than a decade, the targeted drug sorafenib[1, 2] has been the dominant first-line treatment for patients with advanced hepatocellular carcinoma (HCC). However, due to the low overall response rate and high drug resistance rate, many new targeted drugs have been developed, including sunitinib, brivanib, linifanib, nintedanib, dovitinib, sorafenib plus erlotinib, lenvatinib, and donafenib. On the other hand, with the increasing use of immune checkpoint inhibitors in solid tumors, several trials investigated the efficacy and safety of immune checkpoint inhibitors in advanced HCC. Among these trials, only lenvatinib and donafenib as monotherapy were non-inferior to sorafenib in overall survival in untreated advanced HCC. Most of other trials did not meet their primary end point of overall survival. However, the efficacy of the combination therapy with PD-1 or PD-L1 inhibitor plus bevacizumab (VEGF inhibitor) is amazing.[3, 4] An expert panel convened by the American Association for the Study of Liver Diseases recommended time to progression as the primary endpoint in randomized phase 2 trials and overall survival as the main endpoint to measure effectiveness in phase 3 trials.[5, 6] In real world clinical practice, subsequent antitumor therapies after tumor progression and/or therapies for concurrent liver disease can confound the assessment of clinical benefit. In the recent issue of Journal of Hepatology, on behalf of EASL, Bruix and coworkers updated the recommendations of systemic treatment of HCC.7 This review proposed that “overall survival is the sole robust endpoint to assess the benefit from any intervention in advanced HCC” and “all proposed surrogates lack adequate validation”. Here, we tried to reveal the relationship among objective response rate (ORR), median overall survival (OS) time and median progression-free survival (PFS) time by presenting them in a same curve graph. The potential relationship between PFS and OS is revealed by representing the hazard ratio (with 95% confidence interval) of PFS and OS with a forest plot. We systematically searched PubMed and EMBASE databases and analyzed phase 3 clinical trials with large sample size. A total of 11 trials about first-line systemic therapies for advanced HCC published from 2008 to 2021 were included into analysis. All these 11 trials included a group of patients treated with sorafenib. In addition, 7 trials about second-line systemic therapies published from 2015 to 2021 were also included into analysis. The control group received placebo treatment in all these 7 trials. All these 18 trials reported ORR, median PFS and OS time. The ORR according to RECIST 1.1 in the sorafenib group ranged from 0.7% to 11.9% (median 6.1%). Among patients with sorafenib therapy, the median PFS and OS time was 3.75 (range 2.8 to 5.5) and 10.4 (range 6.5 to 14.7) months, reHao-Tian Liu,2 Yu-Hong Sun,1 Zhu-Jian Deng,2 Zi-Yi Zhang,2 Da-Long Yang,2 Kun-Jun Wu2 Xiao-Bu Lan,1
晚期肝细胞癌总生存率的替代指标
十多年来,靶向药物索拉非尼[1,2]一直是晚期肝细胞癌(HCC)患者的主要一线治疗药物。然而,由于总有效率低,耐药率高,许多新的靶向药物被开发出来,包括舒尼替尼、布里伐尼、利尼法尼、尼达尼、多维替尼、索拉非尼联合厄洛替尼、lenvatinib和多纳非尼。另一方面,随着免疫检查点抑制剂在实体肿瘤中的应用越来越多,一些试验研究了免疫检查点抑制剂在晚期HCC中的疗效和安全性。在这些试验中,只有lenvatinib和donafenib单药治疗未治疗的晚期HCC的总生存率不低于sorafenib。其他大多数试验没有达到总生存期的主要终点。然而,PD-1或PD-L1抑制剂加贝伐单抗(VEGF抑制剂)联合治疗的疗效是惊人的。[3,4]由美国肝病研究协会召集的专家小组建议将进展时间作为随机2期试验的主要终点,将总生存期作为衡量3期试验有效性的主要终点。[5,6]在现实世界的临床实践中,肿瘤进展后的后续抗肿瘤治疗和/或并发肝脏疾病的治疗可能会混淆临床获益的评估。在最近一期的《国际肝病杂志》上,Bruix及其同事代表EASL更新了HCC全身治疗的建议。该综述提出,“总生存期是评估晚期HCC干预获益的唯一可靠终点”,“所有建议的替代指标都缺乏足够的验证”。在这里,我们试图揭示客观缓解率(ORR)、中位总生存期(OS)时间和中位无进展生存期(PFS)时间之间的关系,将它们呈现在同一曲线图中。通过用森林图表示PFS和OS的风险比(95%置信区间),揭示了PFS和OS之间的潜在关系。我们系统地检索了PubMed和EMBASE数据库,分析了大样本量的3期临床试验。2008年至2021年间发表的11项关于晚期HCC一线全身治疗的试验被纳入分析。所有这11项试验都包括一组接受索拉非尼治疗的患者。此外,2015年至2021年发表的7项二线全身治疗试验也被纳入分析。在这7项试验中,对照组均接受安慰剂治疗。这18项试验均报告了ORR、中位PFS和OS时间。根据RECIST 1.1,索拉非尼组的ORR范围为0.7%至11.9%(中位数为6.1%)。在接受索拉非尼治疗的患者中,中位PFS和OS时间分别为3.75个月(2.8 ~ 5.5个月)和10.4个月(6.5 ~ 14.7个月),刘浩天,孙玉红,邓竹建,张子怡,杨大龙,吴坤军,兰小步,1
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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CiteScore
5.60
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