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强致癌应激诱导大鼠肝 GST-P 阳性的癌前细胞:起始的生理机制。

Strong carcinogenic stress response induction of preneoplastic cells positive for GST-P in the rat liver: Physiological mechanism for initiation.

机构信息

Department of Biomedical Sciences, Hirosaki University, Graduate School of Health Sciences, Hon-Cho 66-1, Hirosaki 036-8564, Japan.

出版信息

Life Sci. 2018 May 1;200:42-48. doi: 10.1016/j.lfs.2018.02.041. Epub 2018 Mar 2.

DOI:10.1016/j.lfs.2018.02.041
PMID:29501922
Abstract

AIMS

To identify experimental conditions that induce preneoplastic cells positive for glutathione S-transferase P-form (GST-P) in the rat liver by new approaches, and analysis of the mechanism of cancer initiation based on the findings.

MAIN METHODS

The experimental protocols employed to induce GST-P preneoplastic cells in rat liver were as follows. Protocol 1: adult rats were fed basal diet containing 2-acetylaminofluorene (AAF, 0.02% by wt) and high concentrations of N-acetyl-l-cysteine (0.5%) over 10 weeks. Protocol 2: rats were subjected to partial hepatectomy (2/3PH), followed by an AAF (0.04%) diet for two more weeks. Vibratome-prepared liver sections were then immunostained for GST-P.

KEY FINDINGS

GST-P was inducible in the rat liver in response to the strong carcinogenic stress by AAF in the two experimental protocols. When examined immunocytochemically with vibratome sections, the biliary tracts of hepatocytes, GST-P single hepatocytes and foci were heavily positive for the marker enzyme in addition to ordinary cytosolic staining of preneoplastic cell populations. The biliary tracts of hepatocytes were severely injured, and the excretory portions of GST-P single hepatocytes were significantly injured.

SIGNIFICANCE

The cytotoxic action of AAF that give rise to the GST-P single hepatocytes was suggested to be an injury to the excretory pump(s) and the duct of hepatocytes. A new physiological mechanism was hypothesized for the induction of preneoplastic cell populations in the rat liver instead of a genetic mechanism.

摘要

目的

通过新方法鉴定诱导大鼠肝内谷胱甘肽 S-转移酶 P 形(GST-P)阳性的癌前细胞的实验条件,并根据研究结果分析癌症发生的机制。

方法

诱导大鼠肝 GST-P 癌前细胞的实验方案如下。方案 1:成年大鼠喂食含 2-乙酰氨基芴(AAF,按重量计 0.02%)和高浓度 N-乙酰-L-半胱氨酸(0.5%)的基础饮食 10 周。方案 2:大鼠行部分肝切除术(2/3PH),再用 AAF(0.04%)饮食喂养 2 周。然后用振动切片机制备肝切片,并用 GST-P 进行免疫染色。

主要发现

在这两个实验方案中,AAF 的强烈致癌应激可诱导大鼠肝内 GST-P 的诱导。用振动切片机检查免疫细胞化学时,除了普通的癌前细胞群体的细胞质染色外,胆管、GST-P 单个肝细胞和灶的标记酶均强烈阳性。胆管的肝细胞严重受损,GST-P 单个肝细胞的排泄部分明显受损。

意义

AAF 引起 GST-P 单个肝细胞的细胞毒性作用提示其对排泄泵和胆管的损伤。假设了一种新的生理机制来诱导大鼠肝内的癌前细胞群体,而不是遗传机制。

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