Tocchetti Paola, Tudone Elena, Marier Jean-Francois, Marbury Thomas C, Zomorodi Katie, Eller Mark
Gentium.
Clinical Operations, Gentium, Villa Guardia, Como, Italy.
Drug Des Devel Ther. 2016 Aug 16;10:2631-41. doi: 10.2147/DDDT.S112181. eCollection 2016.
Hepatic veno-occlusive disease, also called sinusoidal obstruction syndrome (VOD/SOS), is an unpredictable, potentially life-threatening complication of hematopoietic stem cell transplant conditioning. Severe VOD/SOS, generally associated with multiorgan dysfunction (pulmonary or renal dysfunction), may be associated with >80% mortality. Defibrotide, recently approved in the US, has demonstrated efficacy treating hepatic VOD/SOS with multiorgan dysfunction. Because renal impairment is prevalent in patients with VOD/SOS, this Phase I, open-label, two-part study in adults examined the effects of hemodialysis and severe or end-stage renal disease (ESRD) on defibrotide pharmacokinetics (PK). Part 1 compared defibrotide PK during single 6.25 mg/kg doses infused with and without dialysis. Part 2 assessed defibrotide plasma PK after multiple 6.25 mg/kg doses in nondialysis-dependent subjects with severe/ESRD versus healthy matching subjects. Among six subjects enrolled in Part 1, percent ratios of least-squares mean and 90% confidence intervals (CIs) on dialysis and nondialysis days were 109.71 (CI: 97.23, 123.78) for maximum observed plasma concentration (Cmax); 108.39 (CI: 97.85, 120.07) for area under the concentration-time curve to the time of the last quantifiable plasma concentration (AUC0-t); and 109.98 (CI: 99.39, 121.70) for AUC extrapolated to infinity (AUC0-∞). These ranges were within 80%-125%, indicating no significant effect of dialysis on defibrotide exposure/clearance. In Part 2, defibrotide exposure parameters in six subjects with severe/ESRD after multiple doses (AUC0-t, 113 µg·h/mL; AUC over dosing interval, 113 µg·h/mL; Cmax, 53.8 µg/mL) were within 5%-8% of parameters after the first dose (AUC0-t, 117 µg·h/mL; AUC0-∞, 118 µg·h/mL; Cmax, 54.9 µg/mL), indicating no accumulation. Defibrotide peak and extent of exposures in those with severe/ESRD were ~35%-37% and 50%-60% higher, respectively, versus controls, following single and multiple doses. One adverse event (vomiting, possibly drug-related) was reported. These findings support defibrotide prescribing guidance stating no dose adjustment is necessary for hemodialysis or severe/ESRD.
肝静脉闭塞病,也称为窦性阻塞综合征(VOD/SOS),是造血干细胞移植预处理中一种不可预测的、可能危及生命的并发症。严重的VOD/SOS通常与多器官功能障碍(肺或肾功能障碍)相关,死亡率可能超过80%。去纤苷最近在美国获批,已证明对伴有多器官功能障碍的肝VOD/SOS有效。由于肾功能损害在VOD/SOS患者中很常见,这项针对成人的I期开放标签两部分研究考察了血液透析以及严重或终末期肾病(ESRD)对去纤苷药代动力学(PK)的影响。第1部分比较了在有和没有透析的情况下单次输注6.25 mg/kg剂量去纤苷时的PK。第2部分评估了在未依赖透析的严重/ESRD受试者与健康对照受试者中多次给予6.25 mg/kg剂量后去纤苷的血浆PK。在第1部分纳入的6名受试者中,透析日和非透析日的最大观察血浆浓度(Cmax)的最小二乘均值百分比比值及90%置信区间(CI)为109.71(CI:97.23,123.78);至最后可定量血浆浓度时间的浓度-时间曲线下面积(AUC0-t)为108.39(CI:97.85,120.07);外推至无穷大的AUC(AUC0-∞)为109.98(CI:99.39,121.70)。这些范围在80%-125%以内,表明透析对去纤苷的暴露/清除无显著影响。在第2部分中,6名严重/ESRD受试者多次给药后的去纤苷暴露参数(AUC0-t,113 μg·h/mL;给药间隔内的AUC,113 μg·h/mL;Cmax,53.8 μg/mL)在首次给药后的参数(AUC0-t,117 μg·h/mL;AUC0-∞,118 μg·h/mL;Cmax,54.9 μg/mL)的5%-8%以内,表明无蓄积。在单次和多次给药后,严重/ESRD患者的去纤苷峰值和暴露程度分别比对照组高约35%-至37%和50%-60%。报告了1例不良事件(呕吐,可能与药物有关)。这些发现支持去纤苷的处方指南,即血液透析或严重/ESRD患者无需调整剂量。
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