Higano C S, Berlin J, Gordon M, LoRusso P, Tang S, Dontabhaktuni A, Schwartz J D, Cosaert J, Mehnert J M
Departments of Medicine and Urology, University of Washington and Fred Hutchinson Cancer Research Center, Seattle, USA,
Invest New Drugs. 2015 Apr;33(2):450-62. doi: 10.1007/s10637-015-0217-7. Epub 2015 Mar 7.
Type 1 insulin-like growth factor receptor (IGF-IR) signaling is often dysregulated in cancer. Cixutumumab, a fully human IgG1 monoclonal antibody, blocks IGF-IR and inhibits downstream signaling. The current study determined the recommended dose, safety, and pharmacokinetic (PK) profile of weekly or every-2-week dosing of cixutumumab.
Two open-label, multicenter phase I studies evaluated weekly (3-15 mg/kg) or every-2-weeks (6-15 mg/kg) dosing of cixutumumab in patients with advanced solid tumors. Serial blood samples for PK were collected up to 168-336 h (day 8-15) following the first administration of cixutumumab. Efficacy was evaluated as best overall tumor response.
A total of 24 and 16 patients were enrolled in the weekly and every-2-week dosing studies, respectively. Treatment-emergent adverse events (≥10%) included hyperglycemia, fatigue, anemia, nausea, and vomiting. Severe adverse events (AE) were infrequent; one serious AE (grade 3 electrocardiogram QT prolongation) was deemed possibly cixutumumab-related (10 mg/kg every-2-weeks). One death occurred due to disease progression (6 mg/kg weekly cohort). Maximum serum concentrations increased with dose. A maximum tolerated dose was not identified; pre-determined target serum minimum concentrations (60 μg/mL) were achieved with ≥6 mg/kg weekly and ≥10 mg/kg every-2-week dosing. Cixutumumab terminal elimination half-life is approximately a week (individual range, t1/2 = 4.58-9.33 days based upon 10 mg/kg every 2 weeks). Overall, stable disease was achieved in 25% of all patients.
Cixutumumab was associated with favorable safety and PK profiles. A dosing regimen of 10 mg/kg every 2 weeks was recommended for subsequent disease-focused clinical trials.
1型胰岛素样生长因子受体(IGF-IR)信号传导在癌症中常失调。西妥昔单抗是一种全人源IgG1单克隆抗体,可阻断IGF-IR并抑制下游信号传导。本研究确定了西妥昔单抗每周或每2周给药的推荐剂量、安全性和药代动力学(PK)特征。
两项开放标签、多中心I期研究评估了西妥昔单抗在晚期实体瘤患者中每周(3-15mg/kg)或每2周(6-15mg/kg)给药的情况。在首次给予西妥昔单抗后长达168-336小时(第8-15天)采集用于PK的系列血样。疗效评估为最佳总体肿瘤反应。
每周给药和每2周给药研究分别共纳入24例和16例患者。治疗中出现的不良事件(≥10%)包括高血糖、疲劳、贫血、恶心和呕吐。严重不良事件不常见;1例严重不良事件(3级心电图QT延长)被认为可能与西妥昔单抗有关(每2周10mg/kg)。1例患者因疾病进展死亡(每周6mg/kg队列)。血清最大浓度随剂量增加。未确定最大耐受剂量;每周≥6mg/kg和每2周≥10mg/kg给药可达到预定的目标血清最低浓度(60μg/mL)。西妥昔单抗的终末消除半衰期约为一周(个体范围,基于每2周10mg/kg,t1/2 = 4.58-9.33天)。总体而言,25%的患者病情稳定。
西妥昔单抗具有良好的安全性和PK特征。推荐每2周10mg/kg的给药方案用于后续针对疾病的临床试验。
