一项针对日本实体瘤患者的西妥昔单抗药代动力学的I期单剂量递增和每周固定剂量研究。
A phase I escalating single-dose and weekly fixed-dose study of cetuximab pharmacokinetics in Japanese patients with solid tumors.
作者信息
Shirao Kuniaki, Yoshino Takayuki, Boku Narikazu, Kato Ken, Hamaguchi Tetsuya, Yasui Hisateru, Yamamoto Nobuyuki, Tanigawara Yusuke, Nolting Arno, Yoshino Shinichiro
机构信息
Division of Gastrointestinal Oncology, National Cancer Center Hospital, Tokyo, Japan.
出版信息
Cancer Chemother Pharmacol. 2009 Aug;64(3):557-64. doi: 10.1007/s00280-008-0904-6. Epub 2009 Jan 24.
PURPOSE
Cetuximab is a therapeutic immunoglobulin G1 monoclonal antibody that recognizes the epidermal growth factor receptor (EGFR). This phase I dose-escalation study was designed to assess the safety and pharmacokinetics (PK) of cetuximab in Japanese patients with EGFR-expressing, advanced, solid tumors and also to look for evidence of antitumor efficacy.
PATIENTS AND METHODS
Thirty patients were enrolled in the study; 29 with colorectal adenocarcinomas and one with an adenocarcinoma of the lung. Patients received an initial/weekly infusion of cetuximab at dose levels of 100/100 (dose level 1), 250/250 (dose level 2), 400/250 (dose level 3), 500/250 (dose level 4) or 400/250 (dose level 5) mg/m(2), for 7 or more weeks, with an interval between the initial and second infusion of 1 (dose level 5 representing the standard regimen) or 2 weeks (dose levels 1-4 of the non-standard regimens).
RESULTS
No dose-limiting toxicities (DLTs) were observed during the evaluation period. All patients had at least one adverse event (AE). The most common cetuximab-related AEs were skin toxicity (93% of patients), including acneiform dermatitis (83% of patients). Two patients experienced cetuximab-related grade 3 AEs of skin toxicity and diarrhea after DLT evaluation. C (max) and AUC(0-infinity) after the initial infusion showed dose-proportional increases. Mean total body clearance (CL) values decreased with dose at the lower dose levels. At doses of >or=400 mg/m(2), CL values appeared to level off. Mean trough concentrations for dose level 5 were constant from week 4 (day 29) onward. Two patients (8%) achieved partial response (at 100/100 mg/m(2)). The overall disease control rate (partial response + stable disease) was 58%.
CONCLUSION
The current study demonstrated that cetuximab PK and safety profiles are similar between Japanese and non-Japanese patient populations. It would appear that the standard dose of an initial 2-h infusion of 400 mg/m(2) followed thereafter by weekly 1-h infusions of 250 mg/m(2) for non-Japanese patients is feasible for future clinical studies in Japanese patients.
目的
西妥昔单抗是一种治疗性免疫球蛋白G1单克隆抗体,可识别表皮生长因子受体(EGFR)。本I期剂量递增研究旨在评估西妥昔单抗在表达EGFR的日本晚期实体瘤患者中的安全性和药代动力学(PK),并寻找抗肿瘤疗效的证据。
患者和方法
30名患者入组本研究;29例为结肠腺癌患者,1例为肺腺癌患者。患者接受初始/每周一次的西妥昔单抗静脉输注,剂量水平分别为100/100(剂量水平1)、250/250(剂量水平2)、400/250(剂量水平3)、500/250(剂量水平4)或400/250(剂量水平5)mg/m²,持续7周或更长时间,初始输注与第二次输注之间的间隔为1周(剂量水平5代表标准方案)或2周(剂量水平1 - 4为非标准方案)。
结果
在评估期内未观察到剂量限制性毒性(DLT)。所有患者至少发生一次不良事件(AE)。与西妥昔单抗相关的最常见AE是皮肤毒性(93%的患者),包括痤疮样皮炎(83%的患者)。两名患者在DLT评估后出现与西妥昔单抗相关的3级皮肤毒性和腹泻AE。初始输注后的C(max)和AUC(0 - ∞)呈剂量比例增加。在较低剂量水平时,平均全身清除率(CL)值随剂量降低。在剂量≥400 mg/m²时,CL值似乎趋于平稳。剂量水平5的平均谷浓度从第4周(第29天)起保持恒定。两名患者(8%)达到部分缓解(剂量为100/100 mg/m²)。总体疾病控制率(部分缓解 + 病情稳定)为58%。
结论
当前研究表明,日本和非日本患者群体中西妥昔单抗的PK和安全性特征相似。对于日本患者未来的临床研究而言,非日本患者初始2小时输注400 mg/m²、随后每周1小时输注250 mg/m²的标准剂量似乎是可行的。
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