一项关于抗激酶插入结构域受体抗体IMC-1C11用于结直肠癌肝转移患者的I期研究。

A phase I study of anti-kinase insert domain-containing receptor antibody, IMC-1C11, in patients with liver metastases from colorectal carcinoma.

作者信息

Posey James A, Ng Thian C, Yang Baolian, Khazaeli M B, Carpenter Mark D, Fox Floyd, Needle Mike, Waksal Harlan, LoBuglio Albert F

机构信息

Department of Medicine, Division of Hematology/Oncology, Comprehensive Cancer Center, University of Alabama at Birmingham, Birmingham, Alabama 35294-3300, USA.

出版信息

Clin Cancer Res. 2003 Apr;9(4):1323-32.

PMID:12684400

Abstract

PURPOSE

Angiogenesis plays an important role in colorectal cancer progression. Stimulation of vascular endothelial growth factor receptor (VEGFR), a transmembrane glycoprotein, results in endothelial mitogenesis. Within this family of receptors, VEGFR 2/kinase-insert-domain-containing receptor (KDR) appear to be principally up-regulated during tumorigenesis. A chimeric anti-KDR antibody, IMC-1C11, blocks VEGFR-KDR interaction and inhibits VEGFR-induced endothelial cell proliferation. This trial seeks to assess the safety, tolerability and feasibility of targeting an important pathway in tumorigenesis.

EXPERIMENTAL DESIGN

In a dose-escalation, single-agent study of IMC-1C11, we enrolled 14 patients with colorectal carcinoma and hepatic metastases. Safety-, pharmacokinetic-, immunogenicity-, and magnetic resonance imaging-assessed alteration of vascular effects of IMC-1C11 were evaluated in this trial. IMC-1C11 was infused weekly at 0.2 mg/kg (n = 3), 0.6 mg/kg (n = 4), 2.0 mg/kg (n = 3), and 4.0 mg/kg (n = 4) for 4 weeks, which constituted a cycle.

RESULTS

No grade-3 or -4 IMC-1C11-related toxicities were observed. Minor grade-1 bleeding events were observed in four patients [0.2 mg/kg (n = 1) and 0.6 mg/kg (n = 3)]. Each resolved quickly and required no intervention. The starting dose of IMC-1C11 was selected to achieve a C(max) of approximately 5 micro g/ml. This concentration prevented KDR phosphorylation in vitro. Pharmacokinetic analysis demonstrated that the plasma t(1/2) and C(max) were dose dependent with a plasma t(1/2) of 67 +/- 3 h at the 4-mg/kg dose level. Human antichimeric antibodies were detected in 7 of 14 patients. The antibodies to IMC-1C11 inhibited the circulation of the agent in two patients. One patient had prolonged stable disease for seven cycles (28 weeks). The mean changes in tumor-influx volume-transfer constant k(in) (min(-1)) and enhancement factor after 4 weeks of therapy were significantly decreased compared with pretreatment values in 11 patients.

CONCLUSION

IMC-1C11 was both safe and well tolerated. Drug levels of IMC-1C11 were reliably predicted. Further clinical investigation of anti-VEGFR/KDR agents is warranted.

摘要

目的

血管生成在结直肠癌进展中起重要作用。刺激血管内皮生长因子受体（VEGFR），一种跨膜糖蛋白，可导致内皮细胞有丝分裂。在这个受体家族中，VEGFR 2/含激酶插入结构域受体（KDR）在肿瘤发生过程中似乎主要上调。一种嵌合抗KDR抗体IMC-1C11可阻断VEGFR-KDR相互作用并抑制VEGFR诱导的内皮细胞增殖。本试验旨在评估靶向肿瘤发生中一条重要途径的安全性、耐受性和可行性。

实验设计

在一项IMC-1C11的剂量递增单药研究中，我们招募了14例患有结直肠癌和肝转移的患者。在本试验中评估了IMC-1C11的安全性、药代动力学、免疫原性以及磁共振成像评估的血管效应改变。IMC-1C11以0.2mg/kg（n = 3）、0.6mg/kg（n = 4）、2.0mg/kg（n = 3）和4.0mg/kg（n = 4）的剂量每周输注1次，共4周，构成一个周期。

结果

未观察到3级或4级与IMC-1C11相关的毒性反应。4例患者[0.2mg/kg（n = 1）和0.6mg/kg（n = 3）]出现轻微的1级出血事件。每次出血事件均迅速缓解，无需干预。选择IMC-1C11的起始剂量以达到约5μg/ml的C(max)。该浓度在体外可防止KDR磷酸化。药代动力学分析表明，血浆t(1/2)和C(max)呈剂量依赖性，在4mg/kg剂量水平时血浆t(1/2)为67±3小时。14例患者中有7例检测到人抗嵌合抗体。针对IMC-1C11的抗体在2例患者中抑制了该药物的循环。1例患者疾病稳定延长了7个周期（28周）。与11例患者治疗前的值相比，治疗4周后肿瘤流入体积转移常数k(in)（min(-1)）和增强因子的平均变化显著降低。