Phase Ib/II trial of ibrutinib and nivolumab in patients with advanced refractory renal cell carcinoma1

IF 1.1 Q4 ONCOLOGY

Kidney Cancer Pub Date : 2021-11-07 DOI:10.3233/kca-210128

M. Parikh, Matthew E. Tenold, L. Qi, F. Lara, D. Robles, F. Meyers, P. Lara

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Abstract

Background: Although immune checkpoint inhibitor-based therapy has improved the outcomes of many patients with metastatic renal cell carcinoma (mRCC), most eventually develop disease progression. Newer agents that modulate immune response can possibly potentiate checkpoint inhibitor therapy. The ITK/ETK/BTK inhibitor ibrutinib has been reported to inhibit myeloid derived suppressor cells in preclinical models and to potentiate immunotherapy. We conducted an investigator-initiated trial of ibrutinib plus the PD1 inhibitor nivolumab in mRCC patients, particularly in those previously exposed to immune checkpoint inhibitors. Methods: Eligible patients had mRCC of any histologic subtype, completed at least one line of prior systemic therapy which could have included prior immunotherapy, and had acceptable end-organ function with ECOG performance status of 0–2. Treatment consisted of nivolumab 240 mg intravenously every 2 weeks plus ibrutinib 560 mg (dose level 0) or 420 mg (dose level -1) orally once daily. Cycle length was 28 days. Dose limiting toxicity (DLT) was defined as any Grade 3 or higher adverse event (AE) attributable to therapy. After identification of the recommended phase 2 dose (RP2D), up to 19 patients were enrolled to an expansion cohort to further evaluate toxicities and any early evidence of efficacy. The primary endpoints of the trial were establishment of RP2D and progression-free survival (PFS). Results: A total of 31 patients were enrolled, 6 to dose level 0, 7 (of which one was not evaluable for DLT) in dose level -1, and 18 in the expansion cohort. Median age was 60 years (range, 36–90), most had clear cell histology (n = 27; 87%), and most had prior immune checkpoint inhibitor therapy (n = 28; 90%). Three patients experienced one DLT each, all in dose level 0 (all Grade 3), namely elevated lipase, hypoalbuminemia, and nausea. No DLTs were seen in dose level –1 which was declared the RP2D. The most common Grade 3 or higher AEs include anemia (n = 5), lymphocyte count decrease (4), nausea (2), and hypotension (2). Of 28 patients evaluable for response, one patient (3.6%) had a complete response, 2 (7.1%) had a partial response, and 11 (39.2%) had stable disease, for an objective response rate of 10.7%(95%CI: 3.7%–27.2%) and a disease control rate of 50%(95%CI: 32.6%–67.4%). All responders had received prior immune checkpoint inhibitor therapy. Median PFS was 2.5 months (95%CI, 1.9 –4.8) while median OS was 9.1 months (95%CI, 6.6 –19.0). Conclusions: Ibrutinib at a dose of 420 mg orally once daily in combination with nivolumab 240 mg IV every 2 weeks is feasible and tolerable in mRCC patients. No unique immune-related AEs were observed. Anti-tumor activity was seen in patients previously exposed to PD-1 targeted therapy.

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伊布替尼和尼沃单抗治疗晚期难治性肾细胞癌的Ib/II期试验1

背景:尽管基于免疫检查点抑制剂的治疗已经改善了许多转移性肾细胞癌(mRCC)患者的预后，但大多数患者最终会出现疾病进展。调节免疫反应的新药物可能会增强检查点抑制剂治疗。据报道，ITK/ETK/BTK抑制剂ibrutinib在临床前模型中抑制髓系来源的抑制细胞，并增强免疫治疗。我们在mRCC患者中进行了一项研究者发起的ibrutinib加PD1抑制剂nivolumab的试验，特别是那些先前暴露于免疫检查点抑制剂的患者。方法:符合条件的患者有任何组织学亚型的mRCC，完成了至少一条既往全身治疗(可能包括既往免疫治疗)，终末器官功能可接受，ECOG表现状态为0-2。治疗包括纳武单抗240mg每2周静脉注射加伊鲁替尼560mg(剂量水平0)或420mg(剂量水平-1)每日口服一次。周期为28天。剂量限制毒性(DLT)定义为任何3级或以上的治疗不良事件(AE)。在确定推荐的2期剂量(RP2D)后，多达19名患者被纳入扩展队列，以进一步评估毒性和任何早期疗效证据。试验的主要终点是建立RP2D和无进展生存期(PFS)。结果:共有31例患者入组，6例剂量水平为0,7例剂量水平为-1(其中1例无法评估DLT)， 18例为扩展队列。中位年龄60岁(范围36-90岁)，多数细胞组织学清晰(n = 27;87%)，大多数患者既往有免疫检查点抑制剂治疗(n = 28;90%)。3例患者分别经历了一次DLT，均为剂量水平0(均为3级)，即脂肪酶升高、低白蛋白血症和恶心。剂量水平-1未见dlt，为RP2D。最常见的3级或更高级别ae包括贫血(n = 5)、淋巴细胞计数减少(4)、恶心(2)和低血压(2)。在28例可评估缓解的患者中，1例(3.6%)患者完全缓解，2例(7.1%)患者部分缓解，11例(39.2%)患者病情稳定，客观缓解率为10.7%(95%CI: 3.7%-27.2%)，疾病控制率为50%(95%CI: 32.6%-67.4%)。所有应答者先前都接受过免疫检查点抑制剂治疗。中位PFS为2.5个月(95%CI, 1.9 -4.8)，中位OS为9.1个月(95%CI, 6.6 -19.0)。结论:伊鲁替尼420 mg口服，每日一次，联合纳武单抗240 mg IV，每2周，在mRCC患者中是可行和耐受的。未观察到独特的免疫相关ae。抗肿瘤活性见于先前暴露于PD-1靶向治疗的患者。

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来源期刊

Kidney Cancer Multiple-

CiteScore

0.90

自引率

8.30%

发文量