Lee Sylvia M, Hamid Omid, Jotte Robert, Zakharia Yousef, Medina Theresa, Gillespie-Twardy Amanda, Mehmi Inderjit, Chandra Sunandana, Watson Graham, Ward Patrick, Chaney Marya, Lu Hailing, Berndt Jason, O'Connor Brian P, Rathi Kapil, Shaikh Eeman, Cowey Charles Lance
Fred Hutchinson Cancer Center, Seattle, Washington.
The Angeles Clinic and Research Institute, A Cedars-Sinai Affiliate, Los Angeles, California.
Clin Cancer Res. 2025 Mar 3;31(5):848-859. doi: 10.1158/1078-0432.CCR-24-1478.
Brentuximab vedotin (BV) is hypothesized to selectively deplete T regulatory cells that express CD30 and resensitize tumors to anti-PD-1 therapy. This study evaluated responses to BV + pembrolizumab after PD-1 therapy and explored corresponding biomarkers.
A total of 55 patients with metastatic non-small cell lung cancer and 58 patients with metastatic cutaneous melanoma received ≥1 dose of BV + pembrolizumab. Patients had received a median of 2.0 prior lines of systemic therapies (range, 1-7). The primary endpoint was confirmed objective response rate (ORR). Exploratory endpoints included overall survival (OS) and biomarker analysis in blood and tumor.
For the secondary refractory metastatic non-small cell lung cancer cohort (RECIST v1.1), the ORR was 14%, median progression-free survival (PFS) was 5.85 months, and median OS was 14.4 months. For the secondary refractory metastatic cutaneous melanoma cohort (immune RECIST), the ORR was 24%, median PFS was 4.44 months, and median OS was 21.9 months. Overall, the median duration of OS follow-up was 17.2 months (95% confidence interval, 14.62-22.87). No new safety signals were identified. No treatment-related grade 5 toxicity was seen. Longitudinal immune phenotyping in peripheral blood demonstrated a transient decrease in T regulatory cells. Paired tumor biopsies from baseline and cycle 3 day 1 showed a trend of increased CD8 T-cell infiltration, especially in responding patients.
BV + pembrolizumab in solid tumor malignancies resulted in clinically meaningful, durable responses with encouraging OS and PFS rates supportive of the immunomodulatory activity of this combination. Stronger antitumor activity was observed in secondary refractory cohorts. The safety profile of this combination was consistent with the individual drug risk profiles.
本研究假设,维布妥昔单抗(BV)可选择性清除表达CD30的调节性T细胞,并使肿瘤对抗程序性死亡蛋白1(PD-1)疗法重新敏感。本研究评估了在接受PD-1治疗后使用BV+帕博利珠单抗的疗效,并探索了相应的生物标志物。
共有55例转移性非小细胞肺癌患者和58例转移性皮肤黑色素瘤患者接受了≥1剂BV+帕博利珠单抗治疗。患者此前接受全身治疗的中位数为2.0线(范围1-7线)。主要终点为确认的客观缓解率(ORR)。探索性终点包括总生存期(OS)以及血液和肿瘤中的生物标志物分析。
对于二线难治性转移性非小细胞肺癌队列(根据实体瘤疗效评价标准第1.1版),ORR为14%,中位无进展生存期(PFS)为5.85个月,中位OS为14.4个月。对于二线难治性转移性皮肤黑色素瘤队列(根据免疫相关疗效评价标准),ORR为24%,中位PFS为4.44个月,中位OS为21.9个月。总体而言,OS随访的中位持续时间为17.2个月(95%置信区间为14.62-22.87)。未发现新的安全信号。未观察到与治疗相关的5级毒性反应。外周血的纵向免疫表型分析显示调节性T细胞短暂减少。基线和第3周期第1天的配对肿瘤活检显示CD8 T细胞浸润有增加趋势,尤其是在有反应的患者中。
在实体瘤恶性肿瘤中,BV+帕博利珠单抗产生了具有临床意义的持久反应,OS和PFS率令人鼓舞,支持了该联合疗法的免疫调节活性。在二线难治性队列中观察到更强的抗肿瘤活性。该联合疗法的安全性与各药物的风险特征一致。
