pRED Clinical Pharmacology, F Hoffmann-La Roche AG, Bldg 663/2130, 4070 Basel, Switzerland.
Clin Pharmacokinet. 2013 Jun;52(6):463-73. doi: 10.1007/s40262-013-0051-z.
Human mass balance studies and the assessment of absolute oral bioavailability (F) are usually assessed in separate studies. Intravenous microdose administration of an isotope tracer concomitant to an unlabeled oral dose is an emerging technique to assess F. We report a novel double-tracer approach implemented for tofogliflozin combining oral administration of a radiolabel tracer with concomitant intravenous administration of a stable isotope tracer. Tofogliflozin is a potent and selective sodium/glucose cotransporter 2 inhibitor for the treatment of type 2 diabetes mellitus currently in clinical development.
The objectives of the present study were to assess the systemic exposure of major circulating metabolites, excretion balance, F and contribution of renal clearance (CLR) to total clearance (CL) of tofogliflozin in healthy subjects within one study applying a novel double-tracer technique.
Six healthy male subjects received 20 mg [(12)C/(14)C]tofogliflozin (3.73 MBq) orally and a concomitant microdose of 0.1 mg [(13)C]tofogliflozin intravenously. Pharmacokinetics of tofogliflozin were determined for the oral and intravenous route; the pharmacokinetics of the metabolites M1 and M5 were determined for the oral route. Quantification of [(12)C]tofogliflozin in plasma and urine and [(13)C]tofogliflozin in plasma was performed by selective LC-MS/MS methods. For the pre-selected metabolites of tofogliflozin, M1 and M5, a validated liquid chromatography-tandem mass spectrometry (LC-MS/MS) was applied to plasma and urine samples. Total radioactivity was assessed in plasma, urine and feces. Pharmacokinetic analysis was conducted by non-compartmental methods.
The pharmacokinetics of tofogliflozin in healthy subjects were characterized by an F of 97.5 ± 12.3 %, CL of 10.0 ± 1.3 l/h and volume of distribution at steady-state (V(ss)) of 50.6 ± 6.7 l. The main route of elimination of total drug-related material was by excretion into urine (77.0 ± 4.1 % of the dose). The observed CL(R) of 25.7 ± 5.0 ml/min was higher than the product of the estimated glomerular filtration rate (eGFR) and fraction unbound in plasma (f(u)) (eGFR × f(u) 15 ml/min), indicating the presence of net active tubular secretion in the renal elimination of tofogliflozin. However, CLR contributed only 15.5 % to the CL of tofogliflozin, suggesting that reductions in CLR by renal impairment won't significantly affect systemic exposure to tofogliflozin. Tofogliflozin and its metabolite M1 were the only major circulating entities accounting for 46 ± 8.6 and 50 ± 8.2 %, respectively, of total circulating drug-related material, while the metabolite M5 was a minor circulating metabolite accounting for 3.0 ± 0.3 % of total circulating drug-related material. Both the M1 and M5 metabolites were excreted into urine and the major metabolite M1 did not exhibit active tubular secretion.
These results demonstrate the utility of the double-tracer approach to provide essential pharmacokinetic data and excretion data for drug-related material in one study at the same dosing occasion. The data obtained allowed the characterization of absorption, distribution, metabolism and excretion of tofogliflozin. Tofogliflozin exhibited highly favorable pharmacokinetic properties as demonstrated by its high F, low CL and a low V(ss. The presence of only one major circulating metabolite of tofogliflozin was unambiguously demonstrated. As a drug targeting the kidney, luminal exposure of the kidney is achieved by renal filtration and active tubular secretion.
人体质量平衡研究和绝对口服生物利用度(F)的评估通常在单独的研究中进行。在口服给予非标记药物剂量的同时静脉内给予同位素示踪剂,是一种新兴的评估 F 的技术。我们报告了一种新的双重示踪剂方法,用于评估托格列净,该方法结合了放射性标记示踪剂的口服给药和同时静脉内给予稳定同位素示踪剂。托格列净是一种用于治疗 2 型糖尿病的新型、强效和选择性钠/葡萄糖共转运蛋白 2 抑制剂,目前正在临床开发中。
本研究的目的是在一项研究中应用新的双重示踪剂技术,评估健康受试者中单药给予托格列净时主要循环代谢物的全身暴露、排泄平衡、F 和肾清除率(CLR)对托格列净总清除率(CL)的贡献。
6 名健康男性受试者口服给予 20mg [(12)C/(14)C]托格列净(3.73MBq)和同时静脉内给予 0.1mg [(13)C]托格列净。测定托格列净的口服和静脉途径药代动力学;测定代谢物 M1 和 M5 的口服途径药代动力学。通过选择性 LC-MS/MS 方法定量测定血浆和尿液中的[(12)C]托格列净和血浆中的[(13)C]托格列净。对于托格列净的预先选择的代谢物 M1 和 M5,应用经验证的液相色谱-串联质谱(LC-MS/MS)法测定血浆和尿液样本。总放射性在血浆、尿液和粪便中进行评估。采用非房室模型法进行药代动力学分析。
健康受试者中托格列净的药代动力学特征为 F 为 97.5±12.3%,CL 为 10.0±1.3l/h,稳态时分布容积(V(ss))为 50.6±6.7l。总药物相关物质的主要排泄途径是尿液排泄(占剂量的 77.0±4.1%)。观察到的 CLR(25.7±5.0ml/min)高于估计的肾小球滤过率(eGFR)和血浆中未结合分数(f(u))的乘积(eGFR×f(u)15ml/min),表明托格列净在肾脏消除中存在净主动肾小管分泌。然而,CLR 仅占托格列净 CL 的 15.5%,提示肾脏损害导致 CLR 降低不会显著影响托格列净的全身暴露。托格列净及其代谢物 M1 是唯一的主要循环实体,分别占总循环药物相关物质的 46±8.6%和 50±8.2%,而代谢物 M5 是占总循环药物相关物质 3.0±0.3%的次要循环代谢物。M1 和 M5 代谢物均被排泄到尿液中,主要代谢物 M1 未表现出主动肾小管分泌。
这些结果表明,双重示踪剂方法可在同一给药时机的一项研究中提供药物相关物质的基本药代动力学数据和排泄数据。获得的数据允许对托格列净的吸收、分布、代谢和排泄进行特征描述。托格列净表现出非常有利的药代动力学特性,表现为高 F、低 CL 和低 V(ss)。明确证明了托格列净只有一种主要的循环代谢物。作为一种靶向肾脏的药物,肾脏的腔暴露是通过肾滤过和主动肾小管分泌来实现的。
