Pharmacokinetic Study and Toxicity of Leukovir: A New Combined Drug for the Treatment of Multiple Sclerosis

E. Kalinichenko, I. V. Ponteleeva, M. Golubeva
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Abstract

Leukovir, an enteric-coated tablet, is the original drug product for internal use. The well-known nucleosides cladribine and ribavirin are the active ingredients of the drug product leukovir. Pharmacokinetic parameters of the drug product for the internal use of leukovir active ingredients have been es-tablished. The cladribine half-absorption period was t 1/2a = 49.5 h, C 0 = 276.4 μg/ml, C max = 6.0 μg/ml. Distribution and accumulation parameters (V d , V ss and AUC) have indicated that the drug distribution between the blood cells and blood plasma takes place in the same way, irrespective of the dosage form. Cladribine half-life period is t 1/2e = 0.62 hours. The molecule total clearance and average lifetime in the body in the case of subcutaneous drug administration are approximately the same. Ribavirin is characterized by a half-absorption period of t 1/2a = 0.71 h, C 0 = 115.6 μg/ml and C max = 75.5 μg/ml. Ribavirin total volume of distribution (V d = 1.3 l/kg) and stationary volume of distribution (V ss = 1.64 l/kg) were practically similar to leukovir when administered subcutaneously. The AUC value = 504.2 μg h/ml, which is 2.5 times less than that in the case of drug form administration. Leukovir was regarded as slightly toxic in an acute toxicity study. The risk of cumulation for this drug product is low.
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治疗多发性硬化症的新联合药物Leukovir的药代动力学研究及毒性
Leukovir是一种肠溶片,是内服的原始药物。众所周知的核苷克拉德滨和利巴韦林是药物产品白科韦的有效成分。建立了白科韦有效成分内服药品的药动学参数。cladribine半吸收期t 1/2a = 49.5 h, c0 = 276.4 μg/ml, cmax = 6.0 μg/ml。分布和积累参数(vd, vss和AUC)表明,无论何种剂型,药物在血细胞和血浆之间的分布都是相同的。Cladribine的半衰期为1/2e = 0.62小时。在皮下给药的情况下,分子总清除率和平均寿命在体内大致相同。利巴韦林的半吸收期为t1 /2a = 0.71 h, c0 = 115.6 μg/ml, cmax = 75.5 μg/ml。利巴韦林的总分布体积(vd = 1.3 l/kg)和固定分布体积(vss = 1.64 l/kg)在皮下给药时与白科韦基本相似。AUC值为504.2 μ h/ml,比给药方式的AUC值小2.5倍。在急性毒性研究中,Leukovir被认为是轻微毒性的。本品积累的风险很低。
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