Cheng Ying, Zhang Shuang, Han Liang, Wu Lin, Chen Jun, Zhao Peiyan, Sun Hongmei, Wen Guilan, Ji Yinghua, Zimina Anastasia, Shi Jianhua, Pan Zhijie, Shi Jinsheng, Wang Xicheng, Bai Yuansong, Melkadze Tamar, Pan Yueyin, Min Xuhong, Viguro Maksym, Li Xingya, Zhao Yanqiu, Yang Junquan, Makharadze Tamta, Arkania Ekaterine, Yu Haoyu, Li Jing, Yang Fang, Yang Xinyi, Ling Chen, Wang Qingyu, Shan Yongqiang, Zhu Jun
Department of Oncology, Jilin Cancer Hospital, Changchun, Jilin, P. R. China.
Department of Oncology, Xuzhou Central Hospital, Xuzhou, Jiangsu, P. R. China.
Cancer Commun (Lond). 2025 Aug;45(8):990-1009. doi: 10.1002/cac2.70032. Epub 2025 May 29.
The ASTRUM-005 study previously demonstrated a significant overall survival (OS) benefit with serplulimab (a programmed death 1 inhibitor) plus chemotherapy versus chemotherapy alone in previously untreated extensive-stage small-cell lung cancer (ES-SCLC). Here, we report updated efficacy and safety results after an extended median follow-up of 19.8 months, along with the first report on findings from exploratory biomarker analyses.
A total of 585 patients were randomized in a 2:1 ratio to receive 4.5 mg/kg serplulimab (n = 389) or placebo (n = 196) intravenously every 3 weeks, together with carboplatin and etoposide. The primary endpoint was OS. In addition, genomic profiling was performed to identify mutated genes, and quantitative serum proteome profiling was conducted to identify differentially expressed proteins (DEPs) between responders and non-responders of serplulimab plus chemotherapy. Regression analysis was subsequently used to construct a protein signature based on the DEPs. The associations between efficacy outcomes (objective response rate [ORR], OS, and progression-free survival [PFS]) and gene mutation status or DEP expression were also examined with regression analysis. Furthermore, the prognostic value of hematological parameters was evaluated.
In the intent-to-treat population, the median OS was 15.8 months in the serplulimab group versus 11.1 months in the placebo group (hazard ratio, 0.62; 95% confidence interval, 0.50-0.76; P < 0.001). We identified 181 DEPs between responders and non-responders in the serplulimab group, from which a 15-protein signature was constructed. In the serplulimab group, patients with a higher 15-protein signature score were associated with significantly longer OS and PFS. Also, patients harboring tumor-suppressor retinoblastoma-1 (RB1) mutations or mutations in Notch pathway members showed improved ORR, OS, or PFS compared with their wild-type counterparts. Baseline neutrophil-to-lymphocyte ratio (NLR) and lactate dehydrogenase (LDH) level were independent prognosticators of patients with ES-SCLC.
First-line serplulimab provided a sustained clinical benefit over placebo in patients with ES-SCLC. A 15-protein signature and mutations in RB1 or Notch pathway genes may serve as predictive biomarkers for benefits from serplulimab plus chemotherapy, while baseline NLR and LDH were independent prognosticators for ES-SCLC.
ASTRUM-005研究先前已证明,在既往未接受过治疗的广泛期小细胞肺癌(ES-SCLC)患者中,与单纯化疗相比,斯鲁利单抗(一种程序性死亡1抑制剂)联合化疗可显著延长总生存期(OS)。在此,我们报告了在中位随访期延长至19.8个月后的疗效和安全性更新结果,以及探索性生物标志物分析结果的首次报告。
总共585例患者按2:1的比例随机分组,每3周静脉注射4.5mg/kg斯鲁利单抗(n = 389)或安慰剂(n = 196),同时联合卡铂和依托泊苷。主要终点为OS。此外,进行了基因组分析以鉴定突变基因,并进行了定量血清蛋白质组分析以鉴定斯鲁利单抗联合化疗的缓解者与未缓解者之间差异表达的蛋白质(DEP)。随后使用回归分析基于DEP构建蛋白质特征。还通过回归分析研究了疗效结果(客观缓解率[ORR]、OS和无进展生存期[PFS])与基因突变状态或DEP表达之间的关联。此外,评估了血液学参数的预后价值。
在意向性治疗人群中,斯鲁利单抗组的中位OS为15.8个月,而安慰剂组为11.1个月(风险比,0.62;95%置信区间,0.50 - 0.76;P < 0.001)。我们在斯鲁利单抗组的缓解者与未缓解者之间鉴定出181个DEP,从中构建了一个包含15种蛋白质的特征。在斯鲁利单抗组中,15种蛋白质特征评分较高的患者的OS和PFS显著更长。此外,与野生型患者相比,携带肿瘤抑制基因视网膜母细胞瘤1(RB1)突变或Notch通路成员突变的患者的ORR、OS或PFS有所改善。基线中性粒细胞与淋巴细胞比值(NLR)和乳酸脱氢酶(LDH)水平是ES-SCLC患者的独立预后指标。
一线使用斯鲁利单抗为ES-SCLC患者提供了优于安慰剂的持续临床获益。一个包含15种蛋白质的特征以及RB1或Notch通路基因的突变可能作为斯鲁利单抗联合化疗获益的预测生物标志物,而基线NLR和LDH是ES-SCLC的独立预后指标。
