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β-和α-乙酰地高辛的异构化及生物利用度(作者译)

[Isomerisation and bioavailability of beta- and alpha-acetyldigoxin (author's transl)].

作者信息

Rietbrock N, Vöhringer H F, Kuhlmann J, Maertin K

出版信息

Klin Wochenschr. 1977 Jul 1;55(13):641-6. doi: 10.1007/BF01482534.

Abstract

Bioavailability of acetylated derivatives of digoxin tablets have been studied in healthy subjects after a single oral and intravenous dose as well as during maintenance therapy. alpha-acetyldigoxin shows a lower bioavailability than beta-acetyldigoxin even if the alpha-acetylated derivative is incorporated in a matrix of aerosil (SiO2). Moreover, beta-acetyldigoxin can be transferred to alpha-acetyldigoxin in alkaline solutions. This isomerisation leads to a decrease of the bioavailability of such fixed preparations which contain beta-acetyldigoxin and the hygroscopic salts of potassium-magnesium-aspartate. A prevention of the isomerisation is attained by isolating beta-acetyldigoxin from potassium-magnesium-aspartate. The bioavailability of a such new formulation is comparable to that of beta-acetyldigoxin alone. The experiments show the bioavailability of acetylated derivatives of digoxin to be influenced by the physico-chemical properties of a drug and its preparation.

摘要

地高辛片乙酰化衍生物的生物利用度已在健康受试者单次口服和静脉给药后以及维持治疗期间进行了研究。即使α-乙酰化衍生物被掺入气相二氧化硅(SiO2)基质中,α-乙酰地高辛的生物利用度仍低于β-乙酰地高辛。此外,β-乙酰地高辛在碱性溶液中可转化为α-乙酰地高辛。这种异构化导致含有β-乙酰地高辛和天冬氨酸钾镁吸湿盐的固定制剂的生物利用度降低。通过将β-乙酰地高辛与天冬氨酸钾镁分离可防止异构化。这种新制剂的生物利用度与单独的β-乙酰地高辛相当。实验表明,地高辛乙酰化衍生物的生物利用度受药物及其制剂的物理化学性质影响。

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