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重组干扰素-β与齐多夫定在艾滋病患者中的代谢相互作用。

Metabolic interaction of recombinant interferon-beta and zidovudine in AIDS patients.

作者信息

Nokta M, Loh J P, Douidar S M, Ahmed A E, Pollard R B

机构信息

Department of Internal Medicine, University of Texas Medical Branch, Galveston.

出版信息

J Interferon Res. 1991 Jun;11(3):159-64. doi: 10.1089/jir.1991.11.159.

Abstract

Zidovudine (AZT), the only currently approved drug for treatment of human immunodeficiency virus (HIV) in AIDS, is known to be metabolized by mammalian systems to a variety of metabolites including 3'-azido-3'-deoxy-5'-O-glucuronide (GAZT). Interferons (IFNs) are known to alter the microsomal enzyme system responsible for the metabolism of some compounds. The aim of the present study was to investigate the effect of combination therapy of recombinant (r) IFN-beta and AZT on the rates of metabolism of AZT in AIDS patients. AZT was given orally (200 mg every 4 h) for 8 weeks prior to initiation of rIFN-beta therapy (45 X 10(6) U/day, s.c.). Serum samples from 8 patients were obtained prior to and at days 3 and 15 following initiation of rIFN-beta therapy. Serum was analyzed by high-performance liquid chromatography (HPLC) for both AZT and GAZT. The serum data were analyzed by a computer-assisted pharmacokinetics program that calculates rates of AZT metabolism. The half life for AZT was increased approximately two-fold by day 15. The rate of metabolism of AZT was diminished from 1.43 h-1 prior to IFN-beta therapy, to 0.4 h-1 and 0.05 h-1 at days 3 and 15, respectively. The volume of distribution of AZT was 2 l/kg at day 0 and increased to 3.2 and 3.5 l/kg on days 3 and 15, respectively. In conclusion, the results indicate that rIFN-beta inhibits the rate of AZT metabolism in AIDS patients.

摘要

齐多夫定(AZT)是目前唯一被批准用于治疗艾滋病患者体内人类免疫缺陷病毒(HIV)的药物,已知它在哺乳动物体内会代谢为多种代谢产物,包括3'-叠氮基-3'-脱氧-5'-O-葡萄糖醛酸苷(GAZT)。已知干扰素(IFN)会改变负责某些化合物代谢的微粒体酶系统。本研究的目的是调查重组(r)IFN-β与AZT联合治疗对艾滋病患者体内AZT代谢速率的影响。在开始rIFN-β治疗(45×10⁶U/天,皮下注射)前8周,患者口服AZT(每4小时200毫克)。在开始rIFN-β治疗前以及治疗开始后的第3天和第15天,采集8名患者的血清样本。通过高效液相色谱法(HPLC)分析血清中的AZT和GAZT。血清数据通过计算机辅助药代动力学程序进行分析,该程序可计算AZT的代谢速率。到第15天时,AZT的半衰期增加了约两倍。AZT的代谢速率从IFN-β治疗前的1.43 h⁻¹分别降至治疗第3天和第15天的0.4 h⁻¹和0.05 h⁻¹。AZT在第0天的分布容积为2升/千克,在第3天和第15天分别增加到3.2升/千克和3.5升/千克。总之,结果表明rIFN-β抑制了艾滋病患者体内AZT的代谢速率。

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