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羟基氨基喹啉 1-氧化物诱导大鼠胰腺腺泡细胞病变后药物代谢潜力的改变

Altered drug metabolizing potential of acinar cell lesions induced in rat pancreas by hydroxyaminoquinoline 1-oxide.

作者信息

Moore M A, Makino T, Tsuchida S, Sato K, Ichihara A, Amelizad Z, Oesch F, Konishi Y

出版信息

Carcinogenesis. 1987 Aug;8(8):1089-94. doi: 10.1093/carcin/8.8.1089.

Abstract

Foci of atypical acinar cells observed in male rats 1 year after a single injection of hydroxyaminoquinoline 1-oxide (HAQO) were assessed immunohistochemically for altered expression of a number of enzyme forms considered to play important roles in drug metabolism. The pancreatic lesions, classified as of either basophilic or eosinophilic type on histological appearance, demonstrated distinctive patterns of altered enzyme phenotype. On the one hand, the basophilic foci composed of enlarged cells/nuclei with very prominent nucleoli were characterized by increase in GST-P, G6PD and P450 PB1 and MC2 forms. The eosinophilic type, in contrast, comprised smaller cells demonstrating elevated P450 MC1 and PB1 but not MC2, normal G6PD and strong GST-P binding limited only to a proportion of the nuclei. Both shared decreased GGT and almost total lack of GST-B positive connective tissue and ductular elements. Apparent islet cell lesions and normal islet tissue were characterized by a distinct enzyme phenotype strongly positive for all P450 species investigated. The results indicate that HAQO-induced putative preneoplastic pancreatic lesions, like equivalent carcinogen associated with focal populations in liver, kidney and ductular pancreas, demonstrate a non-random altered expression of specific drug metabolizing enzyme species.

摘要

对单次注射氧化羟氨基喹啉(HAQO)一年后的雄性大鼠体内观察到的非典型腺泡细胞灶进行免疫组织化学评估,以检测多种被认为在药物代谢中起重要作用的酶形式的表达变化。根据组织学外观分类为嗜碱性或嗜酸性类型的胰腺病变,表现出独特的酶表型改变模式。一方面,由细胞/细胞核增大且核仁非常突出组成的嗜碱性病灶,其特征是谷胱甘肽S-转移酶P(GST-P)、葡萄糖-6-磷酸脱氢酶(G6PD)以及细胞色素P450 PB1和MC2形式增加。相比之下,嗜酸性类型由较小的细胞组成,这些细胞显示细胞色素P450 MC1和PB1升高,但MC2未升高,G6PD正常,且仅部分细胞核有强烈的GST-P结合。两者均表现出γ-谷氨酰转肽酶(GGT)降低,几乎完全缺乏GST-B阳性结缔组织和导管成分。明显的胰岛细胞病变和正常胰岛组织的特征是,对于所有研究的细胞色素P450种类均表现出明显的酶表型强阳性。结果表明,HAQO诱导的假定胰腺肿瘤前病变,与肝脏、肾脏和胰腺导管中局部群体相关的等效致癌物一样,表现出特定药物代谢酶种类的非随机表达变化。

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