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01121 Journal of Nara Medical Association >
Vol.51 No.6 >

このアイテムの引用には次の識別子を使用してください: http://hdl.handle.net/10564/637

タイトル: ラットにおけるコリン欠乏アミノ酸食による肝発癌に対するphenyl N-terl-butyl nitroneおよびその誘導体のおよぼす影響
その他のタイトル: EFFECTS OF PHENYL N-tert-BUTYL NITRONE AND ITS DERIVATIVES ON HEPATOCARCINOGENESIS IN RATS FED A CHOLINE-DEFICIENT, L-AMINO ACID-DEFINED DIET
著者: 榎並, 倫宣
キーワード: choline-deficient L-amino acid-defined diet
phenyl N-tert-butyl nitrone derivative
apoptosis
oxidative stress
hepatocarcinogenesis
発行日: 2000年12月31日
出版者: 奈良医学会
引用: Journal of Nara Medical Association Vol.51 No.6 p.468-482
抄録: The present study examined effects of phenyl N-tert-butyl nitrone (PBN) and its derivatives on the early phase of hepatocarcinogenesis in rats fed a choline- deficient, L-amino acid-defined (CDAA) diet. Male Wistar rats, 6 weeks old, were fed the CDAA diet for 16 weeks without or with PBN or its derivatives admixed into the diet at concentrations of 0.009, 0.045 or 0.090%, and then sacrificed. The livers were assessed for the induction of glutathione S-transferase placental form (GST-P)-positive lesions and apoptosis, proliferation and oxidative injuries in hepatocytes. The numbers of GST-P- positive lesions were decreased only by the high dose of PBN. In contrast, the lesion sizes were decreased by all of the doses of 4-OHPBN and the high doses of PBN and 3-OHPBN. PBN, 4-OHPBN and 3-OHPBN inhibited the induction of the borderline cirrhosis, enhan- ced hepatocellular apoptosis in GST-P-positive lesions, inhibited apoptosis in surrounding tissue, and reduced the induction of oxidative damage on nuclear DNA and extranuclear components of hepatocytes. In addition, 4-OHPBN inhibited proliferating activity of hepatocytes both in GST-P-positive lesions and in surrounding tissue. Neither 2-OHPBN nor 2-SPBN exerted any of the effects described above. These results indicate that PBN, 4-OHPBN and 3-OHPBN inhibit the growth of putative preneoplastic lesions induced in the livers of rats fed the CDAA diet by reducing oxidative stress and liver injury. Among these, 4-OHPBN, a major metabolite of PBN, can exert the most superior effects because of the additional inhibition of hepatocyte proliferation. In conclusion, PBN inhibits endogenous hepatocarcinogenesis in rats fed the CDAA diet depending on its metabolic activation into 4-OHPBN, through antioxidative effects and possibly by regulating the oxidative stress-related signal transduction.
URI: http://hdl.handle.net/10564/637
ISSN: 13450069
出現コレクション:Vol.51 No.6

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