O82 A phase 1 dose escalation study of PRS-343, a HER2/4–1BB bispecific molecule, in patients with HER2-positive malignancies

S. Piha-Paul, J. Bendell, A. Tolcher, S. Hurvitz, A. Patnaik, R. Shroff, P. Pohlmann, M. Zettl, N. Hahn, A. Krishnamurthy, M. Duerr, J. Mei, K. Aviano, R. Yusuf, L. Matis, S. Olwill, I. Bruns, G. Ku
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引用次数: 20

Abstract

Background Anticalin® proteins are recombinantly engineered human proteins based on lipocalins. PRS-343 is a first-in-class bispecific antibody-Anticalin fusion protein targeting the oncogenic tumor antigen HER2 and the costimulatory immune receptor 4-1BB on T and other immune cells. Here, we report the results of a phase 1 single-agent dose escalation trial in patients with HER2+ solid tumors. Methods PRS-343 has been evaluated in sequential dose cohorts from 0.0005 to 8 mg/kg i.v. Doses were administered Q3W and the 8 mg/kg dose was also given Q2W. An accelerated titration design was utilized for the initial dose escalation followed by a modified 3+3 design and the option to back-fill cohorts. Dose-limiting toxicities (DLTs) were reported during the first cycle of each schedule. The primary study objectives include the safety profile and RP2D of PRS-343. Secondary objectives include ORR and DCR, PD biomarker response and PK profile. PD response was assessed in tumor biopsies (CD8+ T cell IHC) pre- and post- PRS-343 treatment. Results 51 patients (median age 61.2 years, 61% female, 82% caucasian, 57% with more than three lines of prior therapy) with a variety of solid tumor indications [gastric/GEJ (n=19); BC (n=12); gynecological cancer (n=6); CRC (n=5); BTC (n=4); UC (n=2); melanoma, pancreatic and salivary duct (n=1 each)] have been treated with PRS-343. Based on pharmacokinetic analyses and observed kinetics of the CD8+ T cell expansion post-treatment, the low end of the active dose range is considered 2.5 mg/kg. 19 patients treated at active dose levels before the data cut-off on 09-06-2019 were evaluable for response [DCR 58% (11% confirmed PR) as per RECIST 1.1]. At the active doses, we observed significant and pronounced post-treatment expansion of CD8+ T cells particularly in the tumor nests, consistent with the MoA of PRS-343, while there was no increase in the doses below 2.5 mg/kg. The post-treatment expansion of CD8+ T cells was more pronounced in patients with a confirmed PR or prolonged SD. PRS-343 was very well tolerated, with no SAEs reported. The most frequent TRAEs were fatigue (9%), chills (6%) and diarrhea (5%) of mild to moderate severity. None qualified as a DLT. Conclusions PRS-343 is the first molecule of its kind to demonstrate encouraging evidence of safety and clinical benefit with a correlative PD effect in a heavily pre-treated population. These initial data suggest that PRS-343, the first 4-1BB bispecific to enter clinical development, merits further investigation in clinical trials. Trial Registration NCT03330561
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rs -343是一种HER2/4-1BB双特异性分子,用于her2阳性恶性肿瘤患者的1期剂量递增研究
antialin®蛋白是基于脂钙蛋白的重组工程人蛋白。PRS-343是一种一流的双特异性抗体-抗alin融合蛋白,靶向T细胞和其他免疫细胞上的致癌肿瘤抗原HER2和共刺激免疫受体4-1BB。在这里,我们报告了HER2+实体瘤患者的1期单药剂量递增试验的结果。方法采用0.0005 ~ 8mg /kg静脉给药的序贯剂量队列对PRS-343进行评价,每次给药3w,每次给药8mg /kg。初始剂量递增采用加速滴定设计,随后采用改良的3+3设计,并可选择回填队列。在每个方案的第一个周期报告剂量限制性毒性(dlt)。主要研究目标包括PRS-343的安全性和RP2D。次要目标包括ORR和DCR, PD生物标志物反应和PK谱。通过肿瘤活检(CD8+ T细胞免疫组化)评估PRS-343治疗前后的PD反应。结果51例患者(中位年龄61.2岁,61%为女性,82%为白种人,57%既往接受过3种以上治疗)具有多种实体瘤适应症[胃/GEJ (n=19);公元前(n = 12);妇科癌症(n=6);CRC (n = 5);BTC (n = 4);加州大学(n = 2);黑色素瘤、胰腺和唾液管(各1例)]均已接受PRS-343治疗。根据药代动力学分析和观察到的治疗后CD8+ T细胞扩增动力学,活性剂量范围的低端被认为是2.5 mg/kg。在2019年6月9日截止数据之前,19名患者接受了活性剂量水平的治疗,可评估疗效[DCR为58%(11%确认PR),根据RECIST 1.1]。在活性剂量下,我们观察到CD8+ T细胞在治疗后明显扩增,特别是在肿瘤巢中,这与PRS-343的MoA一致,而低于2.5 mg/kg的剂量没有增加。治疗后CD8+ T细胞扩增在确诊的PR或延长的SD患者中更为明显。PRS-343的耐受性非常好,没有报告急性呼吸道感染。最常见的TRAEs是轻度至中度的疲劳(9%)、寒战(6%)和腹泻(5%)。没有人符合DLT的资格。结论:PRS-343是首个在重度预处理人群中显示出安全性和临床益处的分子。这些初步数据表明,PRS-343是首个进入临床开发的4-1BB双特异性药物,值得在临床试验中进一步研究。试验注册编号NCT03330561
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