Sarich Troy C, Teng Renli, Peters Gary R, Wollbratt Maria, Homolka Robert, Svensson Mia, Eriksson Ulf G
AstraZeneca LP, Wilmington, Delaware 19850, USA.
Clin Pharmacokinet. 2003;42(5):485-92. doi: 10.2165/00003088-200342050-00006.
Ximelagatran, an oral direct thrombin inhibitor, is currently in clinical development for the prevention and treatment of thromboembolic disease. Following oral administration, ximelagatran undergoes rapid bioconversion to its active form, melagatran, via two minor intermediates. Obesity, defined as body mass index (BMI) >30 kg/m(2), is a recognised risk factor for thrombosis. There is potential for differences in the pharmacokinetics and pharmacodynamics of drugs administered to obese versus non-obese patients, and some drugs may require alternative administration strategies in obese patients.
To investigate the effect of obesity on the pharmacokinetics and pharmacodynamics of melagatran after oral administration of ximelagatran.
This was an open-label, single-dose, group-matched study in which obese subjects (BMI 32-39 kg/m(2); six male and six female; age 21-40 years) were matched by sex and age (+/-2 years) with non-obese subjects (BMI 21-26 kg/m(2); six male and six female; aged 21-39 years). Each subject received a single oral dose of ximelagatran 24mg. Blood samples for determination of plasma concentrations of melagatran and activated partial thromboplastin times (APTT; a marker of melagatran pharmacodynamics) were collected up to 12 hours after administration.
There were no statistically significant differences in the pharmacokinetic properties of melagatran between obese and non-obese subjects. Values of area under the melagatran plasma concentration-time curve, maximum plasma concentration (C(max)), time at which C(max) occurred and terminal elimination half-life were approximately 1 micromol. h/L, 0.2 micromol/L, 2 hours and 3 hours in both obese and non-obese subjects, respectively. In addition, there was no statistically significant difference between the obese and non-obese subjects in the amount of ximelagatran, melagatran or the minor intermediates ethyl-melagatran and melagatran hydroxyamidine excreted in urine. When relating the prolongation of APTT ratio to the square root of plasma concentration of melagatran and obesity status (no/yes), no statistically significant interaction between plasma concentration and obesity status was observed. Ximelagatran was well tolerated in both obese and non-obese subjects, and no bleeding events or serious adverse events occurred.
No differences in the pharmacokinetics or pharmacodynamics of melagatran were detected between obese and non-obese subjects after oral administration of ximelagatran, suggesting that dose adjustment of ximelagatran in obesity (BMI up to 39 kg/m(2)) is not necessary.
希美加群是一种口服直接凝血酶抑制剂,目前正处于预防和治疗血栓栓塞性疾病的临床开发阶段。口服给药后,希美加群通过两种次要中间体迅速生物转化为其活性形式美拉加群。肥胖定义为体重指数(BMI)>30kg/m²,是公认的血栓形成危险因素。给肥胖患者与非肥胖患者给药时,药物的药代动力学和药效学可能存在差异,一些药物在肥胖患者中可能需要采用不同的给药策略。
研究肥胖对口服希美加群后美拉加群药代动力学和药效学的影响。
这是一项开放标签、单剂量、组间匹配的研究,其中肥胖受试者(BMI 32 - 39kg/m²;6名男性和6名女性;年龄21 - 40岁)按性别和年龄(±2岁)与非肥胖受试者(BMI 21 - 26kg/m²;6名男性和6名女性;年龄21 - 39岁)进行匹配。每位受试者口服单剂量24mg希美加群。给药后长达12小时采集血样,用于测定美拉加群的血浆浓度和活化部分凝血活酶时间(APTT;美拉加群药效学的一个指标)。
肥胖和非肥胖受试者中美拉加群的药代动力学特性无统计学显著差异。美拉加群血浆浓度 - 时间曲线下面积、最大血浆浓度(C(max))、C(max)出现的时间以及末端消除半衰期的值在肥胖和非肥胖受试者中分别约为1微摩尔·小时/升、0.2微摩尔/升、2小时和3小时。此外,肥胖和非肥胖受试者尿液中排泄的希美加群、美拉加群或次要中间体乙基 - 美拉加群和美拉加群羟脒的量无统计学显著差异。当将APTT比值的延长与美拉加群血浆浓度的平方根及肥胖状态(否/是)相关联时,未观察到血浆浓度与肥胖状态之间有统计学显著的相互作用。希美加群在肥胖和非肥胖受试者中耐受性良好,未发生出血事件或严重不良事件。
口服希美加群后,肥胖和非肥胖受试者中美拉加群的药代动力学或药效学未检测到差异,这表明在肥胖(BMI高达39kg/m²)患者中无需调整希美加群的剂量。
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