Virginia G. Piper Cancer Center Clinical Trials at Scottsdale Healthcare/TGen, 10510 N 92nd St, Ste 200, Scottsdale, AZ 85258, USA.
Invest New Drugs. 2013 Feb;31(1):136-44. doi: 10.1007/s10637-012-9815-9. Epub 2012 Apr 11.
This phase I study aims at assessing the safety and tolerability of LY2603618, a selective inhibitor of Checkpoint Kinase 1, in combination with pemetrexed and determining the maximum tolerable dose and the pharmacokinetic parameters.
This was an open-label, multicenter, dose-escalation study in patients with advanced solid tumors. Increasing doses of LY2603618 (40-195 mg/m(2)) were combined with 500 mg/m(2) of pemetrexed. LY2603618 was administered on Days 1 and 9 and pemetrexed on Day 8 in a 28-day cycle. For all subsequent 21-day cycles, pemetrexed was administered on Day 1 and LY2603618 on Day 2. Antitumor activity was evaluated as per Response Evaluation Criteria in Solid Tumors 1.0.
A total of 31 patients were enrolled into six cohorts (three at 40 mg/m(2) over 4.5-hour infusion, 1-hour infusion in subsequent cohorts: three each at 40 mg/m(2), 70 mg/m(2), and 195 mg/m(2); 13 at 105 mg/m(2); six at 150 mg/m(2)). Four patients experienced a dose-limiting toxicity: diarrhea (105 mg/m(2)); reversible infusion-related reaction (150 mg/m(2)); thrombocytopenia (195 mg/m(2)); and fatigue (195 mg/m(2)). The maximum tolerated dose was defined as 150 mg/m(2). The pharmacokinetic data demonstrated that the exposure of LY2603618 increased in a dose-dependent manner, displayed a suitable half-life for maintaining required human exposures while minimizing the intra- and inter-cycle accumulation, and was unaffected by the pemetrexed administration. The pharmacokinetic-defined biologically efficacious dose was achieved at doses ≥105 mg/m(2).
LY2603618 administered approximately 24 h after pemetrexed showed acceptable safety and pharmacokinetic profiles.
本 I 期研究旨在评估选择性细胞周期检查点激酶 1 抑制剂 LY2603618 联合培美曲塞的安全性和耐受性,并确定最大耐受剂量和药代动力学参数。
这是一项在晚期实体瘤患者中进行的开放性、多中心、剂量递增研究。递增剂量的 LY2603618(40-195mg/m²)联合培美曲塞 500mg/m²。LY2603618 于第 1 天和第 9 天给药,培美曲塞于第 8 天给药,每 28 天为一个周期。所有后续的 21 天周期中,培美曲塞于第 1 天给药,LY2603618 于第 2 天给药。按照实体瘤反应评价标准 1.0 评价抗肿瘤活性。
共招募了 31 名患者进入 6 个队列(3 名在 4.5 小时输注时接受 40mg/m²,随后的 1 小时输注时每个队列各有 3 名患者接受 40mg/m²、70mg/m²和 195mg/m²;13 名患者接受 105mg/m²;6 名患者接受 150mg/m²)。4 名患者发生剂量限制毒性:腹泻(105mg/m²);可逆的输注相关反应(150mg/m²);血小板减少症(195mg/m²);疲劳(195mg/m²)。最大耐受剂量定义为 150mg/m²。药代动力学数据表明,LY2603618 的暴露量呈剂量依赖性增加,半衰期适合维持所需的人体暴露量,同时最小化了周期内和周期间的蓄积,并且不受培美曲塞给药的影响。在剂量≥105mg/m²时达到了药代动力学定义的生物有效剂量。
LY2603618 在培美曲塞给药后约 24 小时给药显示出可接受的安全性和药代动力学特征。
