Mao Zhongping Lily, Stalker Dennis, Keirns James
Impax Laboratories, Hayward, California, USA.
Clin Ther. 2009 Jul;31(7):1542-50. doi: 10.1016/j.clinthera.2009.07.011.
Conivaptan is a nonpeptide vasopressin V(1A)/V(2)-receptor antagonist that produces a controlled increase in serum sodium concentration in hospitalized patients with euvolemic or hyper-volemic hyponatremia.
This study evaluated the pharmacokinetics of conivaptan in patients with euvolemic or hypervolemic hyponatremia and with or without underlying congestive heart failure who were participating in an efficacy and tolerability clinical trial.
Data from an open-label, multicenter study were used to evaluate the pharmacokinetics of conivaptan in hyponatremic patients. Patients received a 20-mg loading dose intravenously over 30 minutes, followed by a continuous 4-day infusion of 20 or 40 mg/d. In the entire cohort, plasma conivaptan concentrations were determined at baseline, at the end of the loading dose (0.5 hour), at 24 hours, on days 3 and 4, and at the follow-up visit on day 11. A subset of patients at 2 study sites (the "pharmacokineticrich" subset) provided additional samples for pharmacokinetic analysis on day 1 at 1, 4, and 24 hours; on day 2 at 24 hours; and on day 5 at 1, 2, 7, 12, and 24 hours.
Plasma conivaptan concentrations were evaluated in 31 patients who received conivaptan 20 mg/d (mean [SD] age, 73.1 [14.3] years; weight, 68.1 [17.2] kg; 71.0% female; 87.1% white, 9.7% black, 3.2% other) and 172 patients who received co-nivaptan 40 mg/d (mean [SD] age, 71.5 [14.4] years; weight, 65.6 [15.9] kg; 64.0% female; 90.1% white, 6.4% black, 3.5% other). The pharmacokinetic-rich subset included 8 patients who received conivap-tan 20 mg/d (mean [SD] age, 76.3 [12.4] years; weight, 71.5 [14.7] kg; 87.5% female; 100% white) and 8 who received conivaptan 40 mg/d (mean [SD] age, 78.3 [7.9] years; weight, 71.3 [15.6] kg; 37.5% female; 100% white). In the overall patient group, plasma conivaptan concentrations were the highest after the 30-minute (C(0.5h)) loading dose (mean [SD] C(0.5h) = 733 [323] and 701 [343] ng/mL with conivap-tan 20 and 40 mg/d, respectively) and then declined during day 1 to concentrations (C(24h)) (mean [SD] C(24h) = 84 [78] and 215 [129] ng/mL with conivaptan 20 and 40 mg/d, respectively) that were maintained by the continuous infusion of 20 or 40 mg/d. At the end of infusion (96 hours), the mean (SD) plasma conivaptan concentrations were 176 (196) and 308 (321) ng/mL for conivaptan 20 and 40 mg/d, respectively. A ratio of 1.75 indicated near dose proportionality; however, interpatient variability was evident. No apparent differences in plasma conivaptan concentrations measured at 0.5 or 96 hours were observed between patients with euvolemic or hypervolemic hypona-tremia or between patients with or without congestive heart failure. In the pharmacokinetic-rich subset, for conivaptan 20 and 40 mg/d, respectively, conivaptan clearance was 18.7 and 9.5 L/h, the elimination t1/2 was 5.3 and 10.2 hours, and exposure to conivaptan in terms of AUC(infinity) was 6996 and 30,771 ng . h/mL.
The results of this study suggest that the pharmacokinetics of conivaptan 20 and 40 mg/d do not differ by volume status or the presence or absence of congestive heart failure.
考尼伐坦是一种非肽类血管加压素V(1A)/V(2)受体拮抗剂,可使等容性或高容性低钠血症住院患者的血清钠浓度得到可控性升高。
本研究评估了考尼伐坦在参与一项疗效和耐受性临床试验的等容性或高容性低钠血症患者(无论有无潜在充血性心力衰竭)中的药代动力学。
来自一项开放标签、多中心研究的数据用于评估考尼伐坦在低钠血症患者中的药代动力学。患者在30分钟内静脉给予20mg负荷剂量,随后连续4天输注20或40mg/d。在整个队列中,于基线、负荷剂量结束时(0.5小时)、24小时、第3天和第4天以及第11天的随访时测定血浆考尼伐坦浓度。2个研究地点的一部分患者(“药代动力学丰富”亚组)在第1天的1、4和24小时;第2天的24小时;以及第5天的1、2、7、12和24小时提供额外的样本用于药代动力学分析。
对31例接受20mg/d考尼伐坦的患者(平均[标准差]年龄,73.1[14.3]岁;体重,68.1[17.2]kg;71.0%为女性;87.1%为白人,9.7%为黑人,3.2%为其他种族)和172例接受40mg/d考尼伐坦的患者(平均[标准差]年龄,71.5[14.4]岁;体重,65.6[15.9]kg;64.0%为女性;9
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