Phase I study of ribociclib (CDK4/6 inhibitor) with spartalizumab (PD-1 inhibitor) with and without fulvestrant in metastatic hormone receptor-positive breast cancer or advanced ovarian cancer.

IF 10.3 1区医学 Q1 IMMUNOLOGY Journal for Immunotherapy of Cancer Pub Date : 2025-02-25 DOI:10.1136/jitc-2024-010430

Ana C Garrido-Castro, Noah Graham, Lestat R Ali, Christina Herold, Jennifer Desrosiers, Khanh Do, Heather Parsons, Tianyu Li, Shom Goel, Molly DiLullo, Eileen Wrabel, Amy J Williams, Joyce F Liu, Elizabeth A Mittendorf, Stephanie K Dougan, Nabihah Tayob, Geoffrey I Shapiro, Sara M Tolaney

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Abstract

Background: Preclinical evidence suggests that cyclin-dependent kinases 4 and 6 (CDK4/6) inhibitors enhance antitumor immunity. We conducted a phase I trial of ribociclib (CDK4/6 inhibitor) plus spartalizumab (PD-1 inhibitor) in patients with hormone receptor (HR)-positive/HER2-negative metastatic breast cancer (MBC) or advanced ovarian cancer (AOC). The combination was also evaluated with fulvestrant in MBC.

Methods: In Cohort A, ribociclib was administered on Days 1-21 (28-day cycle) starting at 400 mg, and spartalizumab at 400 mg on Day 1. Dose escalation was followed by expansion in AOC. Fulvestrant was added (Cohort B) with a safety run-in followed by expansion in MBC. Primary objectives were to determine the maximum tolerated dose (MTD) and recommended phase 2 dose (RP2D), and safety and tolerability of the combinations.

Results: 33 patients enrolled (n=18, Cohort A; n=15, Cohort B). The RP2D of ribociclib in both cohorts was 600 mg. Treatment-related adverse events in >20% of patients in either cohort were neutropenia, fatigue, anemia, thrombocytopenia, hypertransaminasemia, maculopapular rash, fatigue, and nausea. Hypertransaminasemia occurred in 66.7% (AST) and 46.7% (ALT) of patients in Cohort B, including 46.7% and 40.0%, respectively, of grade 3 or 4 events. Two confirmed partial responses were observed (13.3%) in Cohort B, in patients with low baseline serum thymidine kinase activity, coupled with an increase on-treatment. Peripheral blood flow cytometry across patients demonstrated on-target drug binding with increases in PD-1 occupancy and activated CD8⁺ T cells during treatment, irrespective of response. PD-L1-positivity, tumor-infiltrating lymphocytes, or tumor mutational burden did not correlate with progression-free survival (PFS). Several copy-number variations detected with next-generation sequencing correlated with PFS.

Conclusions: Ribociclib with spartalizumab and fulvestrant showed limited efficacy and elevated hepatotoxicity, precluding further development. Correlative analyses revealed treatment-induced immunological effects, and genomic alterations associated with PFS.

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背景：临床前证据表明，细胞周期蛋白依赖性激酶4和6（CDK4/6）抑制剂可增强抗肿瘤免疫力。我们在激素受体（HR）阳性/HER2阴性转移性乳腺癌（MBC）或晚期卵巢癌（AOC）患者中开展了一项ribociclib（CDK4/6抑制剂）联合spartalizumab（PD-1抑制剂）的I期试验。同时还评估了与氟维司群联合治疗MBC的效果：在队列A中，从第1-21天（28天周期）开始服用ribociclib，剂量为400毫克，第1天服用spartalizumab，剂量为400毫克。剂量升级后，在 AOC 中进行扩增。添加氟维司群后（B组），在MBC患者中进行安全性试运行，然后扩大治疗范围。主要目的是确定最大耐受剂量（MTD）和第二阶段推荐剂量（RP2D），以及联合用药的安全性和耐受性：33名患者入组（A组18人；B组15人）。两组患者中，ribociclib的RP2D均为600毫克。两个队列中均有超过20%的患者出现与治疗相关的不良事件，包括中性粒细胞减少、疲劳、贫血、血小板减少、高转氨酶血症、斑丘疹、疲劳和恶心。在队列 B 中，66.7%（谷草转氨酶）和 46.7%（谷丙转氨酶）的患者出现高转氨酶血症，其中分别有 46.7% 和 40.0% 的患者出现 3 级或 4 级事件。在 B 组患者中观察到 2 例证实的部分应答（13.3%），这些患者的血清胸苷激酶活性基线较低，且在治疗后有所增加。所有患者的外周血流式细胞术均显示，无论反应如何，治疗期间PD-1占据率和活化CD8+T细胞均增加，与靶向药物结合。PD-L1阳性、肿瘤浸润淋巴细胞或肿瘤突变负荷与无进展生存期（PFS）无关。下一代测序检测到的几种拷贝数变异与PFS相关：结论：Ribociclib联合spartalizumab和氟维司群的疗效有限，肝毒性升高，因此无法进一步开发。相关分析揭示了治疗引起的免疫学效应，以及与PFS相关的基因组改变。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal for Immunotherapy of Cancer Biochemistry, Genetics and Molecular Biology-Molecular Medicine

CiteScore

17.70

自引率

4.60%

发文量

522

审稿时长

18 weeks

期刊介绍： The Journal for ImmunoTherapy of Cancer (JITC) is a peer-reviewed publication that promotes scientific exchange and deepens knowledge in the constantly evolving fields of tumor immunology and cancer immunotherapy. With an open access format, JITC encourages widespread access to its findings. The journal covers a wide range of topics, spanning from basic science to translational and clinical research. Key areas of interest include tumor-host interactions, the intricate tumor microenvironment, animal models, the identification of predictive and prognostic immune biomarkers, groundbreaking pharmaceutical and cellular therapies, innovative vaccines, combination immune-based treatments, and the study of immune-related toxicity.