LoRusso Patricia M, Krishnamurthi Smitha, Youssoufian Hagop, Hall Nancy, Fox Floyd, Dontabhaktuni Aruna, Grebennik Dmitri, Remick Scot
Karmanos Cancer Institute, Wayne State University, Detroit, MI, USA,
Invest New Drugs. 2014 Apr;32(2):303-11. doi: 10.1007/s10637-013-9998-8. Epub 2013 Aug 1.
IMC-18F1 (icrucumab), a human monoclonal antibody against vascular endothelial growth factor receptor-1 (VEGFR-1), potently inhibits ligand-dependent phosphorylation of VEGFR-1 and downstream signaling, making icrucumab an attractive candidate for antitumor activity.
The primary objective was to determine the safety profile and maximum tolerated dose of icrucumab in patients with advanced solid tumors that were previously unresponsive to standard therapy or for which no standard therapy was available.
In this open-label, dose-escalation, Phase 1 study, patients received icrucumab intravenously weekly at 2, 3, 6, and 12 mg/kg (Cohorts 1-4), every other week (q2w) at 15 mg/kg (Cohort 5), or every third week at 20 mg/kg (Cohort 6). Patients received icrucumab until evidence of progressive disease or other withdrawal criteria were met.
Twenty-six patients received icrucumab. The most common adverse events were fatigue, nausea, peripheral edema, anemia, dyspnea, and vomiting. No dose-limiting toxicities (DLTs) were observed in Cohorts 1-5. Two DLTs were observed in Cohort 6 (anemia and hyponatremia), and enrollment was stopped. No patient demonstrated an immunogenic response. Overall, icrucumab exhibited nonlinear pharmacokinetics at doses >6 mg/kg. Six patients (23.1 %) achieved stable disease with median duration of 11.1 weeks (range = 10.3-18.7 weeks); tumor types were thyroid, melanoma, colorectal (3 patients), and small-cell lung cancers.
Icrucumab was safely administered weekly at doses of 2-12 mg/kg and q2w at a dose of 15 mg/kg with no DLTs. Based on achievement of stable disease, icrucumab has potential for antitumor activity against advanced solid tumors.
IMC-18F1(icrucumab)是一种抗血管内皮生长因子受体-1(VEGFR-1)的人源单克隆抗体,能有效抑制VEGFR-1的配体依赖性磷酸化及下游信号传导,使icrucumab成为具有抗肿瘤活性的有吸引力的候选药物。
主要目的是确定icrucumab在先前对标准治疗无反应或无标准治疗可用的晚期实体瘤患者中的安全性及最大耐受剂量。
在这项开放标签、剂量递增的1期研究中,患者每周静脉注射icrucumab,剂量分别为2、3、6和12mg/kg(第1 - 4组),每两周(q2w)注射15mg/kg(第5组),或每三周注射20mg/kg(第6组)。患者接受icrucumab治疗,直至出现疾病进展证据或满足其他停药标准。
26例患者接受了icrucumab治疗。最常见的不良事件为疲劳、恶心、外周水肿、贫血、呼吸困难和呕吐。在第1 - 5组中未观察到剂量限制性毒性(DLT)。在第6组中观察到2例DLT(贫血和低钠血症),随后停止入组。没有患者表现出免疫原性反应。总体而言,icrucumab在剂量>6mg/kg时表现出非线性药代动力学。6例患者(23.1%)病情稳定,中位持续时间为11.1周(范围 = 10.3 - 18.7周);肿瘤类型为甲状腺癌、黑色素瘤、结直肠癌(3例)和小细胞肺癌。
icrucumab每周以2 - 12mg/kg的剂量及每两周以15mg/kg的剂量安全给药,未出现DLT。基于病情稳定的情况,icrucumab对晚期实体瘤具有抗肿瘤活性的潜力。
