Safety and Tolerability of Berzosertib, an Ataxia-Telangiectasia-Related Inhibitor, and Veliparib, an Oral Poly (ADP-ribose) Polymerase Inhibitor, in Combination With Cisplatin in Patients With Refractory Solid Tumors.

IF 5.6 2区医学 Q1 ONCOLOGY

JCO precision oncology Pub Date : 2025-07-01 Epub Date: 2025-07-16 DOI:10.1200/PO-25-00055

Geraldine O'Sullivan Coyne, Khanh T Do, Shivaani Kummar, Sarina Piha-Paul, Lawrence Rubinstein, Robert Kinders, Ralph E Parchment, Deborah Wilsker, Katherine Ferry-Galow, Brandon Miller, Naoko Takebe, Lamin Juwara, Mary Jane Ong, Ashley Bruns, Murielle Hogu, Abdul Rafeh Naqash, Arjun Mittra, Andrea Regier Voth, James H Doroshow, Alice P Chen

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Abstract

Purpose: We conducted a phase I trial of the combination of cisplatin with the ataxia-telangiectasia-related protein kinase inhibitor berzosertib and the poly (ADP-ribose) polymerase inhibitor (PARPi) veliparib, with the objective of creating a DNA damage response (DDR)-impaired, BRCA null-like phenotype to potentiate the antitumor activity of cisplatin.

Patients and methods: In this open label, 3 + 3 trial design, cisplatin and berzosertib were administered intravenously on day 1 (D1) and D8, and D2 and D9, respectively, together with twice-daily oral veliparib on D1-D3 and D8-D10 in 21-day cycles. Previous platinum and PARPi therapy were permitted. A pharmacodynamic study compared tumor nuclear DDR biomarker response on C1D1 and C1D9 at the combination maximum tolerated dose (MTD).

Results: Fifty-three patients enrolled with 46 evaluable for response (41 with measurable disease). The MTD and recommended phase II dose (RP2D) were determined to be cisplatin 40 mg/m² once daily on D1/D8, berzosertib 210 mg/m² once daily on D2/D9, and veliparib 200 mg twice a day on D1-D3 and D8-D10. Three patients achieved confirmed partial responses (PRs; 3/41, 7.3%); two patients experienced unconfirmed PRs. Median time on study was four cycles (range, 1-25), and 35 patients (66.0%) required at least one dose reduction. The most common grade 3/4 adverse events were myelosuppressive (anemia [37.7%], thrombocytopenia [32.1%], leukopenia [24.5%], neutropenia [22.6%], lymphopenia [20.8%]); no new safety signals were observed. Adding berzosertib to veliparib/cisplatin increased the frequency of RAD51-positive tumor cells in BRCA-wildtype biopsy specimens.

Conclusion: This combination shows antitumor activity, including in patients with and without homologous recombination-compromised tumors and those previously treated with platinum. Adding berzosertib further increases the DDR response elicited by combination cisplatin/veliparib treatment in BRCA-wildtype patients, indicating increased replication stress at the RP2D/MTD.

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难治性实体瘤患者与口服聚（adp -核糖）聚合酶抑制剂Veliparib联合顺铂的安全性和耐受性

目的：我们进行了顺铂与失联性毛细血管扩张相关蛋白激酶抑制剂berzosertib和聚（adp -核糖）聚合酶抑制剂（PARPi） veliparib联合的I期试验，目的是创建DNA损伤反应（DDR）受损的BRCA样表型，以增强顺铂的抗肿瘤活性。患者和方法：在这个开放标签的3 + 3试验设计中，顺铂和berzosertib分别在第1天（D1）和第8天，第D2和第9天静脉注射，同时在D1- d3和D8- d10每天两次口服veliparib，每21天一个周期。先前的铂和PARPi治疗是允许的。一项药效学研究比较了C1D1和C1D9在联合最大耐受剂量（MTD）下肿瘤核DDR生物标志物的反应。结果：入组53例患者，46例可评估缓解（41例可测量疾病）。MTD和推荐II期剂量（RP2D）确定为顺铂40 mg/m2， D1/D8每日1次，berzosertib 210 mg/m2， D2/D9每日1次，veliparib 200 mg， D1- d3和D8- d10每日2次。3例患者获得了部分缓解(PRs；3/41, 7.3%);2例患者出现未经证实的pr。研究的中位时间为4个周期（范围，1-25），35名患者（66.0%）需要至少减少一次剂量。最常见的3/4级不良事件为骨髓抑制性（贫血[37.7%]、血小板减少[32.1%]、白细胞减少[24.5%]、中性粒细胞减少[22.6%]、淋巴细胞减少[20.8%]）；没有观察到新的安全信号。在veliparib/cisplatin中加入berzosertib增加了brca野生型活检标本中rad51阳性肿瘤细胞的频率。结论：该组合具有抗肿瘤活性，包括同源重组受损肿瘤患者和非同源重组受损肿瘤患者以及先前接受过铂治疗的患者。在brca野生型患者中，加入根瑟替尼进一步增加了顺铂/维利帕尼联合治疗引起的DDR反应，表明RP2D/MTD的复制应激增加。

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