UR-3216: a manageable oral GPIIb/IIIa antagonist.

K. Baba, Y. Aga, T. Nakanishi, T. Motoyama, H. Ueno
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引用次数: 5

Abstract

UR-3216, a prodrug, is a novel, selective, and orally active platelet surface glycoprotein (GPIIb/IIIa) receptor antagonist. The most important property of UR-3216 is the very tight binding of its active metabolite to platelets (Ki for resting platelets is < 1 nM). UR-2992, the active form of UR-3216, binds to platelets for a long period of time, while the unbound drug is rapidly cleared. Therefore, after an initial loading dose of 0.1 mg/kg, only once daily repeated low maintenance doses of UR-3216 (< 0.05 mg/kg p.o.) are required. This regimen maintains a high level of inhibition of platelet aggregation and, due to a small peak-to-trough ratio, severe bleeding is avoided. The therapy with UR-3216 is easy to manage, because it has low peak-to-trough ratio and high efficacy (> 80% inhibition of platelet aggregation). In addition, UR-3216 does not produce excessive bleeding or thrombocytopenia and does not interact with abciximab. UR-3216 is excreted mostly in bile, so that it will not accumulate in patients with chronic renal dysfunction. UR-2316 has the following abciximab-like features: (a) its half-lives for residence on platelets, inhibition of platelets aggregation and bleeding time prolongation are 60 to 80 h, 24, and 2 h, respectively; (b) its receptor binding occupancy is similar to that of abciximab (Mab1 is inhibited and Mab2 is unaltered). In conclusion, UR-3216 is a promising, orally active GPIIb/IIIa antagonist for the treatment of cardiovascular diseases.
UR-3216:口服GPIIb/IIIa拮抗剂。
UR-3216是一种新型的、选择性的、口服活性的血小板表面糖蛋白(GPIIb/IIIa)受体拮抗剂。UR-3216最重要的特性是其活性代谢物与血小板的紧密结合(静息血小板的Ki < 1 nM)。UR-3216的活性形式UR-2992与血小板结合时间长,而未结合的药物被迅速清除。因此,在初始负荷剂量为0.1 mg/kg后,只需每天重复一次低维持剂量UR-3216 (< 0.05 mg/kg p.o.)。该方案保持了对血小板聚集的高水平抑制,并且由于峰谷比小,避免了严重出血。UR-3216治疗易于管理,峰谷比低,疗效高(抑制血小板聚集> 80%)。此外,UR-3216不会产生过多出血或血小板减少症,也不会与阿昔单抗相互作用。UR-3216主要通过胆汁排出,因此不会在慢性肾功能不全患者体内积累。UR-2316具有以下类似阿昔单抗的特点:(a)其在血小板上的停留半衰期、抑制血小板聚集的半衰期和延长出血时间的半衰期分别为60 ~ 80小时、24小时和2小时;(b)其受体结合占比与阿昔单抗相似(Mab1被抑制,而Mab2未改变)。总之,UR-3216是一种有前景的口服活性GPIIb/IIIa拮抗剂,可用于治疗心血管疾病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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