Boucher B A, Feler C A, Dean J C, Michie D D, Tipton B K, Smith K R, Kramer R E, Young B, Parks B R, Kugler A R
Department of Clinical Pharmacy, University of Tennessee, Memphis, USA.
Pharmacotherapy. 1996 Jul-Aug;16(4):638-45.
To evaluate the safety, tolerability, and pharmacokinetic profile of fosphenytoin, a water-soluble phenytoin prodrug, after intramuscular and intravenous administration.
Open-label study of intramuscular administration, and double-blind, randomized study of intravenous administration.
Six and ten hospitals throughout the United States for the intramuscular and intravenous multicenter studies, respectively.
Neurosurgical patients who required anticonvulsant prophylaxis or treatment.
In the intramuscular study, 118 patients received loading doses ranging from 480-1500 mg phenytoin equivalents (PE) and daily maintenance doses ranging from 130-1250 mg PE for 3-14 days. In the intravenous study, 88 patients received fosphenytoin and 28 received phenytoin sodium for 3-14 days. Mean +/- SD loading doses and maintenance doses of intravenous fosphenytoin and phenytoin were 1082 +/- 299 mg PE and 411 +/- 221 mg PE, and 1082 +/- 299 mg and 422 +/- 197 mg, respectively. Trough phenytoin concentrations were measured daily in all patients.
Intramuscular fosphenytoin was safe and well tolerated, with no irritation found for 99% of all injection site evaluations. Adverse events associated with the drug occurred in 9% of patients, commonly those typical of the parent drug. For intravenous treatment, the frequency of mild irritation at the infusion site was significantly lower in the fosphenytoin group (6%) than in the phenytoin group (25%, p < 0.05). Reductions in infusion rates were required in 17% and 36% of fosphenytoin and phenytoin recipients, respectively. No significant difference was observed relative to adverse events or seizure frequency between the groups. Trough plasma phenytoin concentrations were approximately 10 micrograms/ml or greater in patients receiving at least 3 days of intramuscular and intravenous fosphenytoin. Trough phenytoin concentrations were similar between patients receiving intravenous phenytoin and fosphenytoin on all study days.
Fosphenytoin can be administered intramuscularly and intravenously in neurosurgical patients to achieve and maintain therapeutic phenytoin concentrations for up to 14 days. Both routes are safe and well tolerated. Intravenous fosphenytoin is significantly better tolerated than intravenous phenytoin sodium in this patient subset.
评估水溶性苯妥英前体药物磷苯妥英在肌肉注射和静脉注射后的安全性、耐受性及药代动力学特征。
肌肉注射为开放标签研究,静脉注射为双盲、随机研究。
分别在美国的6家医院和10家医院进行肌肉注射和静脉注射的多中心研究。
需要抗惊厥预防或治疗的神经外科患者。
在肌肉注射研究中,118例患者接受了苯妥英等效剂量480 - 1500mg的负荷剂量以及苯妥英等效剂量130 - 1250mg的每日维持剂量,持续3 - 14天。在静脉注射研究中,88例患者接受了磷苯妥英治疗,28例患者接受了苯妥英钠治疗,持续3 - 14天。静脉注射磷苯妥英和苯妥英的平均±标准差负荷剂量及维持剂量分别为1082±299mg苯妥英等效剂量和411±221mg苯妥英等效剂量,以及1082±299mg和422±197mg。所有患者每日均测定苯妥英谷浓度。
肌肉注射磷苯妥英安全且耐受性良好,在所有注射部位评估中,99%未发现刺激反应。与该药物相关的不良事件发生在9%的患者中,通常为母体药物的典型不良事件。对于静脉治疗,磷苯妥英组输液部位轻度刺激的发生率(6%)显著低于苯妥英组(25%,p < 0.05)。磷苯妥英和苯妥英接受者中分别有17%和36%需要降低输液速度。两组在不良事件或癫痫发作频率方面未观察到显著差异。接受至少3天肌肉注射和静脉注射磷苯妥英的患者,其苯妥英谷血浆浓度约为10μg/ml或更高。在所有研究日,接受静脉注射苯妥英和磷苯妥英的患者之间苯妥英谷浓度相似。
磷苯妥英可在神经外科患者中进行肌肉注射和静脉注射,以达到并维持治疗性苯妥英浓度长达14天。两种给药途径均安全且耐受性良好。在该患者亚组中,静脉注射磷苯妥英的耐受性明显优于静脉注射苯妥英钠。
