Gastroenterological Center, Yokohama City University Medical Center, 4-57 Urafune-cho, Minami-ku, Yokohama, Kanagawa, Japan.
Department of Gastroenterology, Internal Medicine, Kitasato University School of Medicine, Sagamihara, Japan.
Hepatol Int. 2024 Oct;18(5):1472-1485. doi: 10.1007/s12072-024-10680-8. Epub 2024 Jul 4.
The aims of this study were to identify clinically significant biomarkers of a response to atezolizumab plus bevacizumab (ATZ + BV) therapy and to develop target strategies against unresectable hepatocellular carcinoma (u-HCC).
We first investigated the potential of circulating tumor DNA (ctDNA) to serve as a biomarker for predicting the therapeutic outcome in 24 u-HCC patients treated with ATZ + BV therapy. Next, we analyzed levels of immune-related cytokines in blood samples from 134 u-HCC patients who received ATZ + BV. For this, serum immune-related molecules or cancer-immune cycle-related molecules that have been reported in HCC patient sera, namely CD274, LAG-3, CCL2, 4, 5, CXCL1, 9, 10, 12, 13, CX3CL1, CCR5, IFNγ and IL-6, 8 were measured using enzyme-linked immunosorbent assay.
More than 1% of variant read frequency (VRF) mutations were found in TP53, APC, PIK3CA and VHL, although with no correlation with treatment response. Among the 15 cytokines evaluated, CXCL9 and LAG-3 levels were significantly different between patients with objective response (OR), stable disease (SD), and progressive disease (PD) following ATZ + BV treatment. Receiver-operating characteristic curve analyses of CXCL9 (cut-off value: 419.1 pg/ml) and LAG-3 (cut-off value: 3736.3 pg/ml) indicated areas of 0.779 and 0.697, respectively, for differentiating PD from non-PD and OR from non-OR. In multivariate analysis of progression-free survival (PFS) and overall survival (OS), high serum CXCL9 (hazard ratio (HR) and 95% confidence interval (CI): 0.412 (0.251-0.677) (p = 0.0005) for PFS and 0.252 (0.125-0.508) (p = 0.0001) for OS), and low serum LAG-3 (HR and 95% CI 0.419 (0.249-0.705) (p = 0.0011) for PFS and 0.294 (0.140-0.617) (p = 0.0012) for OS) were independent positive predictive factors.
Although, as far as we examined, no ctDNA mutations in blood were found to be related to ATZ + BV treatment efficacy, serum CXCL9 and LAG-3 levels, which are related to the cancer-immune cycle, were associated with treatment efficacy and could be predictive markers of the efficacy of ATZ + BV treatment in HCC patients.
本研究旨在确定与阿替利珠单抗联合贝伐珠单抗(ATZ+BV)治疗应答相关的有临床意义的生物标志物,并制定针对不可切除肝细胞癌(u-HCC)的靶向策略。
我们首先在 24 例接受 ATZ+BV 治疗的 u-HCC 患者中研究了循环肿瘤 DNA(ctDNA)作为预测治疗结果的生物标志物的潜力。接下来,我们分析了 134 例接受 ATZ+BV 治疗的 u-HCC 患者的血液样本中免疫相关细胞因子的水平。为此,使用酶联免疫吸附测定法测量了已在 HCC 患者血清中报道的血清免疫相关分子或癌症免疫循环相关分子,即 CD274、LAG-3、CCL2、4、5、CXCL1、9、10、12、13、CX3CL1、CCR5、IFNγ和 IL-6、8。
在 TP53、APC、PIK3CA 和 VHL 中发现了超过 1%的变异读取频率(VRF)突变,但与治疗反应无相关性。在所评估的 15 种细胞因子中,CXCL9 和 LAG-3 水平在 ATZ+BV 治疗后出现客观缓解(OR)、疾病稳定(SD)和疾病进展(PD)的患者之间存在显著差异。对 CXCL9(截断值:419.1 pg/ml)和 LAG-3(截断值:3736.3 pg/ml)的受试者工作特征曲线分析表明,区分 PD 与非 PD 和 OR 与非 OR 的面积分别为 0.779 和 0.697。在无进展生存期(PFS)和总生存期(OS)的多变量分析中,高血清 CXCL9(风险比(HR)和 95%置信区间(CI):0.412(0.251-0.677)(p=0.0005)用于 PFS 和 0.252(0.125-0.508)(p=0.0001)用于 OS)和低血清 LAG-3(HR 和 95%CI 0.419(0.249-0.705)(p=0.0011)用于 PFS 和 0.294(0.140-0.617)(p=0.0012)用于 OS)是独立的阳性预测因素。
尽管就我们检查的结果而言,血液中的 ctDNA 突变与 ATZ+BV 治疗效果无关,但与癌症免疫循环相关的血清 CXCL9 和 LAG-3 水平与治疗效果相关,并且可能是 ATZ+BV 治疗 HCC 患者疗效的预测标志物。
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