Morse G D, Portmore A C, Marder V, Plank C, Olson J, Taylor C, Bonnez W, Reichman R C
University of Rochester AIDS Clinical Trials Unit, New York.
Antimicrob Agents Chemother. 1992 Oct;36(10):2245-52. doi: 10.1128/AAC.36.10.2245.
Pharmacokinetic and coagulation studies were carried out over a 12-week period with 11 asymptomatic hemophilia patients with human immunodeficiency virus infection receiving zidovudine (ZDV). The patients received 300 mg every 4 h while awake (the accepted dose at the time of this study); consecutive 24-h intravenous (i.v.) and 12-h oral pharmacokinetic studies were conducted at weeks 1, 6, and 12. Coagulation studies were conducted at weeks 0, 4, 8, and 12. The numbers of units of factors VIII and IX and cryoprecipitate transfused during the 12-week periods before, during, and after ZDV treatment were recorded. Following i.v. and oral ZDV administration, the concentration in plasma declined rapidly over the first 4 h, and in some patients, ZDV was still detectable at 4 to 10 h. The i.v. total clearances (means +/- standard deviations) were 14.9 +/- 7.3, 11.2 +/- 3.7, and 15.1 +/- 4.7 ml/min/kg of body weight. The i.v. distribution volumes were 1.08 +/- 0.5, 1.0 +/- 0.4, and 1.65 +/- 1.4 liters/kg. The bioavailabilities were 0.54 +/- 0.22, 0.46 +/- 0.19, and 0.59 +/- 0.13 at weeks 1, 6, and 12, respectively. The pattern of ZDV-glucuronide (GZDV) disposition was similar to that of ZDV, and the peak plasma GZDV-to-ZDV ratio was higher after oral dosing, consistent with first-pass metabolism. In some individuals, up to 33% of an i.v. dose was excreted unchanged. At weeks 6 and 12, greater than 300 mg of total ZDV (GZDV plus ZDV) was recovered in the urine of some patients, suggesting tissue redistribution. Concentration in plasma after oral ZDV administration were variable, both within and between patients. The von Willebrand antigen level consistently decreased throughout the study but was not accompanied by a parallel change in ristocetin cofactor A activity, and no clinical adverse effects on coagulation were noted. This study demonstrates that ZDV can be used in hemophilia patients without worsening of their bleeding tendencies. The clinical significance of decreased ZDV clearance and the prolonged terminal elimination phase of ZDV will require further study with patients receiving chronic ZDV.
对11名感染人类免疫缺陷病毒的无症状血友病患者进行了为期12周的药代动力学和凝血研究,这些患者正在接受齐多夫定(ZDV)治疗。患者在清醒时每4小时接受300毫克(本研究当时的公认剂量);在第1、6和12周进行了连续24小时静脉内(i.v.)和12小时口服药代动力学研究。在第0、4、8和12周进行了凝血研究。记录了ZDV治疗前、治疗期间和治疗后12周内输注的凝血因子VIII和IX的单位数以及冷沉淀的情况。静脉内和口服ZDV给药后,血浆浓度在最初4小时内迅速下降,在一些患者中,4至10小时仍可检测到ZDV。静脉内总清除率(平均值±标准差)分别为14.9±7.3、11.2±3.7和15.1±4.7毫升/分钟/千克体重。静脉内分布容积分别为1.08±0.5、1.0±0.4和1.65±1.4升/千克。在第1、6和12周时的生物利用度分别为0.54±0.22、0.46±0.19和0.59±0.13。ZDV-葡萄糖醛酸苷(GZDV)的处置模式与ZDV相似,口服给药后血浆中GZDV与ZDV的峰值比值更高,这与首过代谢一致。在一些个体中,高达33%的静脉内剂量以原形排泄。在第6和12周时,一些患者尿液中回收的ZDV总量(GZDV加ZDV)超过300毫克,提示组织再分布。口服ZDV给药后患者体内和患者之间的血浆浓度均存在差异。在整个研究过程中,血管性血友病因子抗原水平持续下降,但瑞斯托霉素辅因子A活性没有相应变化,并且未观察到对凝血有临床不良影响表明。本研究表明,ZDV可用于血友病患者,而不会使其出血倾向恶化。ZDV清除率降低和ZDV终末消除期延长的临床意义需要在接受长期ZDV治疗的患者中进一步研究。
