解析与晚期肝癌患者接受阿替利珠单抗联合贝伐单抗治疗的临床反应相关的免疫激活肿瘤微环境。
Unraveling the immune-activated tumor microenvironment correlated with clinical response to atezolizumab plus bevacizumab in advanced HCC.
作者信息
Lim Jinyeong, Goh Myung Ji, Song Byeong Geun, Sinn Dong Hyun, Kang Wonseok, Gwak Geum-Youn, Choi Moon Seok, Lee Joon Hyeok, Cha Dong Ik, Gu Kyowon, Ha Sang Yun, Hwang Inwoo, Park Woong-Yang, Paik Yong-Han
机构信息
Department of Health Science and Technology, Samsung Advanced Institute for Health Science and Technology, Sunkyunkwan University, Seoul, South Korea.
Samsung Genome Institute, Samsung Medical Center, Seoul, South Korea.
出版信息
JHEP Rep. 2024 Dec 15;7(4):101304. doi: 10.1016/j.jhepr.2024.101304. eCollection 2025 Apr.
BACKGROUND & AIMS: Despite atezolizumab plus bevacizumab being a standard treatment for advanced hepatocellular carcinoma (HCC), a significant proportion of patients do not achieve durable benefit. This study aimed to identify predictive biomarkers for this therapy by investigating the role of immune activation within the tumor microenvironment (TME).
METHODS
We characterized the intratumoral TME of patients with advanced HCC treated with atezolizumab plus bevacizumab using single cell transcriptomics on pretreatment tumor biopsies from 12 patients. To complement and support these findings, we integrated our single cell data with publicly available bulk RNA-sequencing data from independent clinical trial cohorts.
RESULTS
Patients who responded to combination therapy with atezolizumab plus bevacizumab demonstrated an immune-activated TME, marked by enhanced cytotoxicity and a tumor-specific T cell response. These patients also exhibited an increased proportion of inflammatory cytokine-enriched tumor-associated macrophage clusters with stronger interactions with T cells, an increased population of conventional dendritic cells, and activated antigen-presenting function in tumor endothelial cells. When publicly available bulk RNA-sequencing data from independent clinical trial cohorts were analyzed, these immune activation features were associated with improved progression-free survival (median 10.8 months, 95% CI: 7.3-not reached versus 5.5 months, 95% CI: 4.0-6.7; <0.001).
CONCLUSIONS
These findings suggest that the existence of an activated immune TME before treatment is crucial for a favorable clinical response in patients with HCC treated with atezolizumab plus bevacizumab.
IMPACT AND IMPLICATIONS
Only a subset of patients with HCC benefit from combination therapy with atezolizumab plus bevacizumab, limiting its clinical utility. In this study, we used single cell RNA analysis to identify TME features associated with a clinical response to this therapy. Our findings suggest that a pre-existing immune-activated TME is crucial for predicting the response to atezolizumab plus bevacizumab. Specifically, features such as enhanced T cell cytotoxicity, inflammatory cytokine-enriched macrophage clusters, active antigen presentation in endothelial cells, and an increased presence of dendritic cells may aid patient selection and inform therapeutic strategies.
背景与目的
尽管阿替利珠单抗联合贝伐单抗是晚期肝细胞癌(HCC)的标准治疗方法,但仍有相当一部分患者未获得持久益处。本研究旨在通过调查肿瘤微环境(TME)内免疫激活的作用来确定该疗法的预测生物标志物。
方法
我们对12例接受阿替利珠单抗联合贝伐单抗治疗的晚期HCC患者的瘤内TME进行了特征分析,采用单细胞转录组学技术对治疗前肿瘤活检样本进行检测。为补充和支持这些发现,我们将单细胞数据与来自独立临床试验队列的公开可用的批量RNA测序数据进行整合。
结果
对阿替利珠单抗联合贝伐单抗联合治疗有反应的患者表现出免疫激活的TME,其特征为细胞毒性增强和肿瘤特异性T细胞反应。这些患者还表现出富含炎性细胞因子的肿瘤相关巨噬细胞簇比例增加,与T细胞的相互作用更强,传统树突状细胞数量增加,以及肿瘤内皮细胞的抗原呈递功能激活。在分析来自独立临床试验队列的公开可用批量RNA测序数据时,这些免疫激活特征与无进展生存期改善相关(中位生存期10.8个月,95%CI:7.3 - 未达到 对比 5.5个月,95%CI:4.0 - 6.7;P<0.001)。
结论
这些发现表明,治疗前存在激活的免疫TME对于接受阿替利珠单抗联合贝伐单抗治疗的HCC患者获得良好临床反应至关重要。
影响与意义
只有一部分HCC患者能从阿替利珠单抗联合贝伐单抗联合治疗中获益,限制了其临床应用。在本研究中,我们使用单细胞RNA分析来确定与该疗法临床反应相关的TME特征。我们的发现表明,预先存在的免疫激活TME对于预测对阿替利珠单抗联合贝伐单抗的反应至关重要。具体而言,诸如增强的T细胞细胞毒性、富含炎性细胞因子的巨噬细胞簇、内皮细胞中的活性抗原呈递以及树突状细胞数量增加等特征可能有助于患者选择并为治疗策略提供依据。
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