Umehara Ken-ichi, Wada Kouichi, Noguchi Kiyoshi, Iwatsubo Takafumi, Usui Takashi, Kamimura Hidetaka
Drug Metabolism Research Laboratories, Drug Discovery Research, Astellas Pharma Inc., 1-8, Azusawa 1-chome, Itabashi-ku, Tokyo 174-8511, Japan.
Drug Metab Dispos. 2009 Jul;37(7):1427-33. doi: 10.1124/dmd.108.026385. Epub 2009 Apr 9.
(-)-N-{2-[(R)-3-(6,7-Dimethoxy-1,2,3,4-tetrahydroisoquinoline-2-carbonyl)piperidino]ethyl}-4-fluorobenzamide (YM758), a novel "funny" If current channel (If channel) inhibitor, is developed as a treatment for stable angina and atrial fibrillation. In this study, the pharmacokinetic/pharmacodynamic (PK/PD) relationship after intravenous administration of YM758 to tachycardia-induced dogs was investigated and described based on the simplified compartment model. The PK of YM758 in dogs did not differ between the nontreated and tachycardia-induced groups. A drug-induced reduction in heart rate (HR) was clearly observed, and the half-life of the duration of the effect (approximately 4.0 h) was longer than that of the plasma concentration of the unchanged drug. The fitting and simulation procedure from the PK/PD relationship between the time profiles for YM758 plasma concentration and HR reduction had an ECe(50) value (YM758 concentration in the effective compartment resulting in a 50% decrease of the maximum effect) of 6.0 ng/ml, which did not agree with the results of the in vitro experiment using right atria isolated from guinea pigs (EC(30), 70.4 ng/ml). In addition, in the in vitro experiments, YM758 metabolites had a weak inhibitory effect, if any, on the spontaneous beat rate of the right atria from guinea pigs. These data, along with the previous finding that YM758 and its metabolites are eliminated rapidly from rat hearts, indicate that the duration of the pharmacological effect of YM758 (compared with the rapid elimination of the plasma drug concentration) may be the result of strong binding and/or slower dissociation of YM758 in the If channel. Such PK/PD analyses allow the pharmacological profiles of many drugs, especially cardiovascular drugs, to be more readily understood and better predicted during the clinical stages.
(-)-N-{2-[(R)-3-(6,7-二甲氧基-1,2,3,4-四氢异喹啉-2-羰基)哌啶基]乙基}-4-氟苯甲酰胺(YM758)是一种新型的“超极化激活的环核苷酸门控阳离子通道”(If通道)抑制剂,被开发用于治疗稳定型心绞痛和心房颤动。在本研究中,基于简化房室模型,研究并描述了静脉注射YM758给心动过速诱导犬后的药代动力学/药效学(PK/PD)关系。YM758在犬体内的药代动力学在未治疗组和心动过速诱导组之间没有差异。明显观察到药物诱导的心率(HR)降低,且效应持续时间的半衰期(约4.0小时)长于原形药物的血浆浓度半衰期。从YM758血浆浓度和HR降低的时间曲线之间的PK/PD关系进行拟合和模拟的过程得出,有效浓度(ECe(50))值(有效房室中导致最大效应降低50%的YM758浓度)为6.0 ng/ml,这与使用豚鼠离体右心房进行的体外实验结果(EC(30),70.4 ng/ml)不一致。此外,在体外实验中,YM758代谢产物对豚鼠右心房的自发搏动率即使有抑制作用也很微弱。这些数据,连同之前发现的YM758及其代谢产物从大鼠心脏中快速消除的结果,表明YM758药理作用的持续时间(与血浆药物浓度的快速消除相比)可能是YM758在If通道中强烈结合和/或解离较慢的结果。这种PK/PD分析使许多药物,尤其是心血管药物的药理特征在临床阶段更容易被理解和更好地预测。
