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苯溴马隆的处置与促尿酸排泄作用;羟基化而非脱溴生成苯酰马隆的证据。

Benzbromarone disposition and uricosuric action; evidence for hydroxilation instead of debromination to benzarone.

作者信息

Walter-Sack I, de Vries J X, Ittensohn A, Kohlmeier M, Weber E

机构信息

Abteilung Klinische Pharmakologie, Universität Heidelberg.

出版信息

Klin Wochenschr. 1988 Feb 15;66(4):160-6. doi: 10.1007/BF01727785.

Abstract

Benzbromarone is one of the main uricosuric drugs currently used. We determined plasma concentrations of benzbromarone, bromobenzarone, and benzarone and 24 hour uric acid excretion in ten healthy individuals following fasting application of two different non-micronised benzbromarone brands. In addition we explored the influence of adjusting urinary pH to near neutral values and of concomitant food intake. Benzbromarone was more rapidly absorbed from the test preparation than from the reference preparation; the extent of systemic availability did not differ significantly. Urinary pH adjustment had no clearcut effect, whereas food intake retarded drug absorption (even though not significant because of the variability of the data). Binding of benzbromarone to plasma proteins exceeded 99%. Bromobenzarone and benzarone were not detectable and are unlikely to be major metabolites of benzbromarone. Instead we found two other compounds suggestive of metabolites, one of them being monohydroxilated benzbromarone. The plasma concentrations of the parent compound in one subject exceeded those of the rest of the group, possibly indicating genetic differences in drug metabolism. The uricosuric effect was not related to benzbromarone plasma concentrations.

摘要

苯溴马隆是目前使用的主要促尿酸排泄药物之一。我们测定了10名健康个体在空腹服用两种不同的非微粉化苯溴马隆品牌后,血浆中苯溴马隆、溴苯酰苯酮和苯酰苯酮的浓度以及24小时尿酸排泄量。此外,我们还探讨了将尿液pH值调节至接近中性值以及同时摄入食物的影响。与参比制剂相比,受试制剂中的苯溴马隆吸收更快;全身可用性程度无显著差异。尿液pH值调节没有明确的效果,而食物摄入会延迟药物吸收(尽管由于数据的变异性不显著)。苯溴马隆与血浆蛋白的结合率超过99%。未检测到溴苯酰苯酮和苯酰苯酮,它们不太可能是苯溴马隆的主要代谢产物。相反,我们发现了另外两种提示为代谢产物的化合物,其中一种是单羟基化苯溴马隆。一名受试者中母体化合物的血浆浓度超过了组内其他受试者,这可能表明药物代谢存在遗传差异。促尿酸排泄作用与苯溴马隆血浆浓度无关。

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