Factors Determining Drug Residence in Skin during Transdermal Absorption : Studies on β-Blocking Agents
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概要
- 論文の詳細を見る
The factors determining drug residence in skin during penetraiton across rat abdominal skin were investigated using five β-blocking agents with different lipophilicities as model drugs in vivo and in vitro. The amount of β-blocking agent in the skin at steady state correlated well with lipophilicity. The distribution of β-blocking agents to the stratum corneum and the contribution of intercellular lipids in the stratum corneum to their skin distribution were also correlated with their lipophilicity, suggesting that the stratum corneum, especially intercellular lipids in the stratum corneum, wound be responsible for the residence of β-blocking agents in the skin. Furthermore, cholesterol-3-sulfate, palmitic acid, stearic acid and oleic acid were found to interact with the β-blocking agents, which are cationized under the physiological condition, and were assumed to play an important role in the skin accumulation. On the other hand, the binding to keratinocyte was so small that keratinocyte might have little effect on the skin accumulation of the β-blocking agents. Drug transport from the stratum corneum to viable skin was suggested to be regulated by the lipophilicity of these agents. To investigate the residence of these drugs in viable skin, in vitro transport studies using stripped skin were performed. The transport rate constant across viable skin to receptor cells (k_<23>) was inversely correlated with the lipophilicity of the drugs. The elimination rate constants from viable skin (k_<vs>) obtained in the in vivo study were much smaller than the values of k_<23> obtained in the in vitro study, and they were inversely correlated with the binding to cytosol components of viable skin but not the lipophilicity. The viable skin-to-muscle concentration ratio of these drugs, obtained at the β-phase of the plasma concentration-time curve after intravenous administration, was also inversely correlated with the binding to the cytosol components of viable skin. These results suggest that k_<vs> reflects the transport from viable skin to muscle rather than to blood circulation and that the binding of drugs to cytosol components in viable skin would be one of the important factors determining the residence in viable skin.
- 公益社団法人日本薬学会の論文
- 1998-11-15
著者
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HIGAKI KAZUTAKA
Faculty of Pharmaceutical Sciences, Kyoto University
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Nakayama Kazuki
Faculty Of Pharmaceutical Sciences Okayama University
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KIMURA TOSHIKIRO
Faculty of Pharmaceutical Sciences, Kyoto University
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KUROSAKI YUJI
Faculty of Pharmaceutical Sciences, Kyoto University
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YAGI Shigenori
Faculty of Pharmaceutical Sciences, Okayama University
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Yagi Shintaro
Tonen Corporation
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Yagi S
Faculty Of Pharmaceutical Sciences Okayama University
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Yagi Shigenori
Faculty Of Pharmaceutical Sciences Okayama University
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Kimura Toshikiro
Faculty Of Pharmaceutical Sciences Kyoto University
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Kurosaki Yuji
Department Of Clinical Pharmaceutical Science Faculty Of Pharmaceutical Sciences Okayama University
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Kurosaki Yuji
Faculty Of Pharmaceutical Sciences Okayama University
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Kurosaki Yuji
Faculty Of Pharmaceutical Sciences Kyoto University
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Higaki Kazutaka
Faculty Of Pharmaceutical Sciences Okayama University
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