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논문 기본 정보

자료유형
학술저널
저자정보
Min, Young-Sil (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University) Bai, Ki-Lyong (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University) Yim, Sung-Hyuk (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University) Lee, Young-Joo (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University) Song, Hyun-Ju (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University) Kim, Jin-Hak (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University) Ham, In-Hye (Department of Pharmacology, College of Pharmacy, Chung Ang University) Whang, Wan-Kyun (Department of Pharmacology, College of Pharmacy, Chung Ang University) Sohn, Uy-Dong (Department of Pharmaceutical Botany, College of Pharmacy, Chung Ang University)
저널정보
대한약학회 Archives of pharmacal research : a publication of the Pharmaceutical Society of Korea Archives of pharmacal research : a publication of the Pharmaceutical Society of Korea 제29권 제6호
발행연도
2006.1
수록면
484 - 489 (6page)

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This Study evaluated the inhibitory action of $luteolin-7-O-{\beta}-D-glucuronopyranoside$, luteolin which was isolated from Salix gilgiana leaves, and omeprazole on reflux esophagitis and gastritis in rats. Reflux esophagitis and gastritis were induced surgically and by the administration of indomethacin, respectively. The intraduodenal administration of $luteolin-7-O-{\beta}-D-glucuronopyranoside$ decreased the ulcer index, injury area, gastric volume and acid output, and increased the gastric pH compared with luteolin. $Luteolin-7-O-{\beta}-D-glucuronopyranoside$ significantly decreased the size of the gastric lesions that had been induced by exposing the gastric mucosa to indomethacin. The malondialdehyde content, which is the end product of lipid peroxidation, was increased significantly after inducing of reflux esophagitis. The malondialdehyde content was decreased by $Luteolin-7-O-{\beta}-D-glucuronopyranoside$ but not luteolin or omeprazole. $Luteolin-7-O-{\beta}-D-glucuronopyranoside$ has a more potent antioxidative effect than luteolin. $Luteolin-7-O-{\beta}-D-glucuronopyranoside$ is a promising drug for the treatment of reflux esophagitis and gastritis.

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