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Pharmacokinetics of alafosfalin, alone and in combination with cephalexin, in humans.

机译:单独或与头孢氨苄联用的阿拉福斯汀在人体内的药代动力学。

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摘要

Alafosfalin is a phosphonodipeptide with significant activity as an antibacterial agent and as a potentiator of beta-lactam antibiotics. Studies in humans showed that oral doses of 50 to 2,500 mg were well absorbed, but some metabolic hydrolysis occurred before the drug reached the general circulation. Oral bioavailability was approximately 50% and was largely independent of dose. Alafosfalin has an elimination half-life of about 60 min and does not accumulate during chronic administration. Healthy volunteers excreted intact phosphonodipeptide in the urine. The recovery was dose dependent and increase from 6 +/- 1% after 50-mg doses to 17 +/- 1% after 2,500-mg doses. This change with dose occurred because the human kidney has a small, saturable capacity for reabsorbing the phosphonopeptide. Less alafosfalin was excreted in the urine of subjects with impaired glomerular function. When alafosfalin was coadministered with cephalexin, both compounds wer absorbed, distributed, and eliminated at virtually identical rates. Oral administration of 500 mg of the phosphonodipeptide plus 250 mg of the beta-lactam antibiotic gave approximately equal concentrations of the drugs in plasma, with a fourfold excess of cephalexin in the urine. This 2:1 combination is being tested in the clinic.
机译:Alafosfalin是一种磷酸二肽,具有显着活性,可作为抗菌剂和β-内酰胺类抗生素的增强剂。对人体的研究表明,口服剂量为50至2500 mg,可以很好地吸收,但在药物进入全身循环之前会发生一些代谢水解。口服生物利用度约为50%,在很大程度上与剂量无关。 Alafosfalin的消除半衰期约为60分钟,在长期给药期间不会累积。健康的志愿者从尿液中排出了完整的磷酸二肽。恢复是剂量依赖性的,并且从50 mg剂量后的6 +/- 1%增加到2,500 mg剂量后的17 +/- 1%。发生这种剂量变化是因为人的肾脏具有小的,可饱和的再吸收膦酰肽的能力。肾小球功能受损的受试者的尿液中排泄的阿拉福斯法林较少。当阿拉福斯法林与头孢氨苄合用时,两种化合物几乎以相同的速率吸收,分布和消除。口服500毫克的膦酰二肽加上250毫克的β-内酰胺类抗生素,在血浆中的药物浓度大致相等,尿液中的头孢氨苄过量四倍。这种2:1组合正在临床中进行测试。

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  • 作者

    Allen, J G; Lees, L J;

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  • 年度 1980
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  • 正文语种 en
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