Saturable Absorption of Glycerol in the Rat Intestine(Biopharmacy)
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概要
- 論文の詳細を見る
The permeability of glycerol, a small hydrophilic solute, across the intestinal membrane would be low, if passive diffusion restricted to the paracellular route is the principal transport mechanism as generally assumed for this class of solutes. However, in the present study using a closed loop of rat small intestine in situ, we found that the absorption of glycerol was faster than that of urea, a probe solute widely assumed to permeate exclusively via the paracellular route. This finding is inconsistent with the paracellular permeation hypothesis, which predicts that the absorption of glycerol, which is larger than urea in terms of molecular size, could not be faster than that of urea. We also found that glycerol absorption was saturable. These findings suggest the involvement of carrier-mediated transport in intestinal glycerol absorption. Glycerol absorption in the colon was also saturable, suggesting the involvement of carrier-mediated transport, although it was much slower than that in the small intestine. Carrier-mediated glycerol transport might play an important role in absorbing glycerol liberated from dietary triglyceride. It would be interesting to further examine the possibility that a carrier-mediated glycerol transport system (or systems) might be involved in drug absorption and also that it might be utilized for oral drug delivery.
- 社団法人日本薬学会の論文
- 2003-11-01
著者
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Hayashi Yoshie
Department Of Pharmacy Kyoto University Hospital Faculty Of Medicine Kyoto University
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Hayashi Yoshie
京都大学医学部附属病院 薬剤
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林 弥生
College Of Pharmacy Kinjo Gakuin University
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NAKAJIMA Aki
Graduate School of Science and Engineering, Ehime University
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Kato T
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Kato Toyonori
名古屋市立大学 薬学研究科
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Watanabe J
School Of Pharmacy Aichi Gakuin University
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INOUE Katsuhisa
Graduate School of Pharmaceutical Sciences, Nagoya City University
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YUASA Hiroaki
Graduate School of Pharmaceutical Sciences, Nagoya City University
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HAYASHI Yayoi
Graduate School of Pharmaceutical Sciences, Nagoya City University
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WATANABE Jun
College of Pharmacy, Nihon University
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HAMAMOTO Kaori
Graduate School of Pharmaceutical Sciences, Nagoya City University
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DOGU Shinya
Graduate School of Pharmaceutical Sciences, Nagoya City University
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MARUTANI Takeshi
Graduate School of Pharmaceutical Sciences, Nagoya City University
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KATO Toyonori
Graduate School of Pharmaceutical Sciences, Nagoya City University
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Kato Toyonori
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Inoue K
Gifu Pharmaceutical University
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Huang Ye
Department Of Pharmacy Kyoto University Hospital Faculty Of Medicine Kyoto University
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Dogu Shinya
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Nakajima Aki
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Yuasa H
Department Of Pharmaceutics And Drug Delivery School Of Pharmacy Tokyo University Of Pharmacy And Li
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Hayashi Yayoi
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Yuasa Hiroaki
Department Of Biopharmaceutics Graduate School Of Pharmaceutical Sciences Nagoya City University
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Yuasa Hiroaki
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Hamamoto Kaori
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Watanabe J
Department Of Pharmaceutics College Of Pharmacy Nihon University
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井上 勝央
名古屋市立大学大学院薬学研究科薬物動態制御学分野
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Hayashi Y
Life Science Laboratories Central Research Laboratories Ajinomoto Co. Inc.:pharmaceuticals Research
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Hayashi Yayoi
Department Of Biopharmaceutics Faculty Of Pharmaceutical Sciences Nagoya City University
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Marutani Takeshi
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Inoue Katsuhisa
Graduate School Of Pharmaceutical Sciences Nagoya City University
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Watanabe Jun
College Of Pharmacy Nihon University
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Dogu Shin-ya
Graduate School of Pharmaceutical Sciences, Nagoya City University
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