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Abstract

Kinetics of distribution and adipose tissue storage as a function of lipophilicity and chemical structure. II. Benzodiazepines.

X Xie, S H Steiner and M H Bickel
Drug Metabolism and Disposition January 1991, 19 (1) 15-19;
X Xie
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S H Steiner
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M H Bickel
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Abstract

Distribution kinetics of flurazepam, medazepam, prazepam, and clobazam were determined in rats. Concentration-time curves of unchanged drugs and non-polar metabolites in plasma, adipose tissue, liver, brain, and muscle after a single iv administration were obtained using GLC/electron capture detector analysis. Pharmacokinetic parameters were calculated for plasma and tissues. Adipose tissue storage was quantified with the adipose storage index (ASI). Including data of benzodiazepines from the literature, a correlation between ASI and log P (over a range 1.6-3.8) was nonexistent and the influence of individual functional groups was not easily discernible. However, benzodiazepines with a pKa (base) within the range 1.6-6.2 were stored in adipose tissue (ASI greater than 1), whereas those with pKa greater than 7 were not (ASI less than 1). Since many other basic lipophilic drugs with pKa greater than 7 are not stored in adipose tissue, and this is likely due to lysosomal trapping in lean tissues, which requires a pKa value above 7, it is suggested that within the series of benzodiazepines, adipose tissue storage is mainly influenced by the basicity of the drugs.

 

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Drug Metabolism and Disposition
Vol. 19, Issue 1
1 Jan 1991
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Abstract

Kinetics of distribution and adipose tissue storage as a function of lipophilicity and chemical structure. II. Benzodiazepines.

X Xie, S H Steiner and M H Bickel
Drug Metabolism and Disposition January 1, 1991, 19 (1) 15-19;

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Abstract

Kinetics of distribution and adipose tissue storage as a function of lipophilicity and chemical structure. II. Benzodiazepines.

X Xie, S H Steiner and M H Bickel
Drug Metabolism and Disposition January 1, 1991, 19 (1) 15-19;
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