Alnaim Lamya, Abou Alsoud Nermeen, Zaghloul Iman, Al-Jaser May
Department of Clinical Pharmacy, College of Pharmacy, Science & Medical Studies Department for Women Students, King Saud University, PO Box 22452, Riyadh 11495, Saudi Arabia.
Int J Antimicrob Agents. 2007 Jun;29(6):728-32. doi: 10.1016/j.ijantimicag.2007.01.013. Epub 2007 Mar 21.
Pentavalent antimony (Sb(V)) compounds are the drugs of choice for the treatment of all forms of leishmaniasis. For 20 years there has been an interest in antifungal azoles for treating leishmaniasis, with variable success. In the current study, we examined the effects of co-administration of fluconazole (FLZ) on the pharmacokinetics and pharmacodynamics of Sb(V) in cutaneous leishmaniasis-infected hamsters. Hamsters were divided into four groups. All hamsters were injected with 0.1 mL of 1x10(8)promastigotes/mL into the right foot on Day 1. Treatment was started 5 days after the infection. The antimony group received 80 mg/kg/day of Pentostam intramuscularly whilst the FLZ group received FLZ 20 mg/kg/day orally for 14 days. The combination group received both Pentostam and FLZ at the above mentioned doses for 14 days. Animals in the control group received no treatment. The infected footpads were measured on Days 1 and 14. A pharmacokinetic study was conducted on Days 1 and 14 of treatment, representing single- and multiple-dose pharmacokinetics, respectively. Blood samples were collected at different time intervals up to 24h. Sb(V) was determined using flameless atomic absorption spectrophotometry. Pharmacokinetic parameters were calculated using a non-compartmental analysis. In the single-dose study, there was no statistically significant difference in any of the pharmacokinetic parameters of Sb(V) when given alone or with FLZ. However, on Day 14 a significant increase in peak plasma concentration (C(max)) (three-fold) and area under the concentration-time curve (AUC) (four-fold) of antimony was observed when Sb(V) was co-administered with FLZ. A statistically significant prolongation of the terminal half-life from 1.63 to 8.67 h (P<0.05) was also observed. A significant reduction in clearance was detected. However, FLZ had no effect on the pharmacodynamics of Sb(V) as measured by footpad sizes. In conclusion, FLZ did not improve the therapeutic effect of Sb(V) when given concomitantly despite the significant increase in blood concentration and prolongation of the elimination half-life of Sb(V).
五价锑(Sb(V))化合物是治疗所有类型利什曼病的首选药物。二十年来,人们一直对使用抗真菌唑类药物治疗利什曼病感兴趣,但疗效不一。在本研究中,我们检测了联用氟康唑(FLZ)对皮肤利什曼病感染仓鼠体内Sb(V)的药代动力学和药效学的影响。仓鼠被分为四组。所有仓鼠在第1天右足注射0.1 mL含1×10(8)前鞭毛体/mL的溶液。感染后5天开始治疗。锑剂组肌肉注射80 mg/kg/天的喷他脒,而氟康唑组口服20 mg/kg/天的氟康唑,持续14天。联合用药组按上述剂量同时给予喷他脒和氟康唑,持续14天。对照组动物不接受治疗。在第1天和第14天测量感染的足垫。在治疗的第1天和第14天进行药代动力学研究,分别代表单剂量和多剂量药代动力学。在长达24小时的不同时间间隔采集血样。使用无火焰原子吸收分光光度法测定Sb(V)。使用非房室分析计算药代动力学参数。在单剂量研究中,单独给予或与氟康唑联用Sb(V)时,其任何药代动力学参数均无统计学显著差异。然而,在第14天,当Sb(V)与氟康唑联用时,观察到锑的血浆峰浓度(C(max))显著增加(三倍),浓度-时间曲线下面积(AUC)显著增加(四倍)。还观察到终末半衰期从1.63小时显著延长至8.67小时(P<0.05)。检测到清除率显著降低。然而,就足垫大小而言,氟康唑对Sb(V)的药效学没有影响。总之,尽管Sb(V)的血药浓度显著增加且消除半衰期延长,但联用氟康唑时并未改善Sb(V)的治疗效果。
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