慢性腹泻和消瘦综合征的HIV感染患者口服更昔洛韦生物利用度增加——一项群体药代动力学研究。
Increased oral ganciclovir bioavailability in HIV-infected patients with chronic diarrhoea and wasting syndrome--a population pharmacokinetic study.
作者信息
Mouly S, Aymard G, Tillement J P, Caulin C, Bergmann J F, Urien S
机构信息
Department of Internal Medicine, Lariboisiere Hospital, 75475 Paris Cedex 10, France.
出版信息
Br J Clin Pharmacol. 2001 Jun;51(6):557-65. doi: 10.1046/j.0306-5251.2001.01389.x.
AIMS
Despite a lack of data, the antiviral agent ganciclovir is not indicated in AIDS patients with diarrhoea because of its presumed poor oral bioavailability. To assess the effect of diarrhoea on ganciclovir intestinal absorption, we conducted a pharmacokinetic study in 42 HIV-infected patients categorized into three groups: A, HIV stage A and B (n = 15); B, AIDS stage C (n = 13); C, AIDS with chronic diarrhoea and wasting syndrome (n = 14).
METHODS
Each patient was evaluated for nutritional (body mass index, albumin, transferrin serum levels), inflammatory (haptoglobin, orosomucoid), immunological (CD4 count, plasma viral load) and intestinal (D-xylose test, faecal fat and nitrogen output, intestinal permeability) status. Ganciclovir (1 g) was administered orally to fasted patients. Six blood samples were collected over 24 h. Serum was analysed for ganciclovir by h.p.l.c. Population pharmacokinetic analysis was performed using a nonlinear mixed effects modelling program, MP2.
RESULTS
Mean intestinal permeability (lactulose/mannitol urinary ratio) was increased in group C (0.2) compared with group A (0.05) and B (0.1) patients. Drug concentration-time profiles were best described by a two-compartment model. Apparent oral clearance (CL/F) and central volume of distribution (V1/F) were influenced by clinical status (group). For groups A and B combined, final parameter estimates of CL/F and V1/F were 256 +/- 98 l h(-1) and 1320 +/- 470 l, respectively. Final parameter estimates for group C were 118 +/- 108 l h(-1) and 652 +/- 573 l for CL/F and V1/F, respectively. The 95% confidence intervals on differences between A and B combined and C were statistically significant ([ + 70, + 206] for CL/F, and [+ 314, + 1022] for V1/F). Compared with groups A and B, ganciclovir CL/F was significantly decreased in group C patients.
CONCLUSIONS
AIDS patients with diarrhoea and severe disease may benefit from ganciclovir therapy, but a dose adjustment may be required according to their digestive and immunological status.
目的
尽管缺乏相关数据,但由于推测口服生物利用度较差,抗病毒药物更昔洛韦未被用于患有腹泻的艾滋病患者。为评估腹泻对更昔洛韦肠道吸收的影响,我们对42名HIV感染患者进行了一项药代动力学研究,这些患者被分为三组:A组,HIV A期和B期(n = 15);B组,艾滋病C期(n = 13);C组,患有慢性腹泻和消瘦综合征的艾滋病患者(n = 14)。
方法
对每位患者的营养状况(体重指数、白蛋白、转铁蛋白血清水平)、炎症状态(触珠蛋白、类粘蛋白)、免疫状态(CD4计数、血浆病毒载量)和肠道状态(D-木糖试验、粪便脂肪和氮排出量、肠道通透性)进行评估。在空腹患者中口服给予更昔洛韦(1g)。在24小时内采集6份血样。通过高效液相色谱法分析血清中的更昔洛韦。使用非线性混合效应建模程序MP2进行群体药代动力学分析。
结果
与A组(0.05)和B组(0.1)患者相比,C组患者的平均肠道通透性(乳果糖/甘露醇尿比值)增加(0.2)。药物浓度-时间曲线用二室模型能得到最佳描述。表观口服清除率(CL/F)和中央分布容积(V1/F)受临床状态(分组)影响。对于A组和B组合并,CL/F和V1/F的最终参数估计值分别为256±98 l h⁻¹和1320±470 l。C组CL/F和V1/F的最终参数估计值分别为118±108 l h⁻¹和652±573 l。A组和B组合并与C组之间差异的95%置信区间具有统计学意义(CL/F为[+70,+206],V1/F为[+314,+1022])。与A组和B组相比,C组患者的更昔洛韦CL/F显著降低。
结论
患有腹泻和严重疾病的艾滋病患者可能从更昔洛韦治疗中获益,但可能需要根据其消化和免疫状态调整剂量。
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