[慢性乙型肝炎和非酒精性脂肪性肝病小鼠模型的建立及观察]。

中华实验和临床病毒学杂志 Pub Date : 2013-10-01

Lu Lu, Yin-Lan Liu, Wen-Jun Yang, Jing Liu, Yan Luo, Zhen-Jie Zhuang, Jian-Yu Chen, Dong-Xue Bian, Yun-Hao Xun, Jun-Ping Shi

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摘要

目的:建立慢性乙型肝炎病毒(HBV)合并非酒精性脂肪性肝病(NAFLD)小鼠模型。方法:取100只4周龄HBV转基因BALB/c小鼠，雌雄各一半。然后选出70只小鼠作为一组饲喂高脂饲料，其余小鼠饲喂正常饲料。在第16周末，随机杀死10只高脂小鼠，建立肝组织及血清学检测靶点鉴定模型。然后将小鼠分为模型组和对照组，每组30只。饲料模型组加高脂饲料、对照组加正常饲料、正常组加正常饲料至第72周(含前16周)。每组小鼠分别于第24、48、72周末处死10只，全自动生化仪检测血清ALT、AST、TC、TG、FBG，荧光定量PCR法检测HBV-DNA，化学发光法检测HBsAg, HE染色后肝脏活检评价组织学变化，观察小鼠模型动态进化。结果:(1)饲喂高脂饲料16周后，小鼠体重、血清ALT、AST、TC、TG、FBG及血液生化指标升高，HBV- dna阳性，肝脏HE染色明显出现大泡性脂肪变性肝细胞及小叶内淋巴细胞浸润，NAFLD活性评分(NAS)接近NASH，慢性HBV携带NAFLD小鼠模型建立成功。(2)模型组各时期TC、TG值均高于对照组和正常组。(3)第24周、第72周，各组HBV-DNA值与其他两组比较，差异均有统计学意义(P < 0.05)。(4)第48、72周，各组NAS与其他两组比较差异均有统计学意义(P < 0.05)。结论:(1)高脂饲料喂养HBV转基因小鼠，可建立慢性HBV携带NAFLD小鼠模型。(2) NAFLD在一定程度上加速了HBV携带小鼠的肝脏病变。

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[Model building-up and observation on the mouse carried chronic hepatitis B and nonalcoholic fatty liver disease].

Objective: Establish the model of mouse with chronic hepatitis B virus (HBV) and nonalcoholic fatty liver disease (NAFLD).

Methods: Take 100 HBV transgenic, BALB/c mice of 4 weeks old, with each gender half. Then pick out 70 mice in one group to feed high-fat feed and the rest to feed normal feed. At the end of week 16, random kill 10 mice of high-fat, then liver tissue and serological detection target identification model is established in this paper. After that, divide the mice into model group and comparison group with 30 mice in each group. Feed model group with high-fat feed, comparison group with normal feed and normal group with normal feed till week 72 (including previous 16 weeks). Kill 10 mice of each group at the end of week 24, 48 and 72 respectively, fully automatic biochemical instrument detection of serum ALT, AST, TC, TG, FBG, fluorescence quantitative PCR method to detect HBV-DNA, chemiluminescence detection of HBsAg, liver biopsy after HE staining to evaluate histology change, observe mice model of dynamic evolution.

Results: (1) Feed high fat feed after 16 weeks, mice's weight, serum ALT, AST, TC, TG, FBG and blood biochemical indicators increased, HBV-DNA positive, liver HE staining obviously big blister fatty degeneration of liver cells and within the lobule lymphocytes infiltration, NAFLD activity score (NAS) getting close to NASH, the model of chronic HBV carries with NAFLD mouse built successfully. (2) The TC and TG values of model group in each period were higher than that of comparison group and normal group. (3) In week 24 and 72, HBV-DNA values of each group are obvious different from the other two groups and the difference can be applied to statistical significance (P < 0.05). (4) In week 48 and 72, NAS of each group are obvious different from the other two groups and the difference can be applied to statistical significance (P < 0.05).

Conclusions: (1) Chronic HBV carries with NAFLD mice model can be established by HBV transgenic mice fed by high fat feed. (2) NAFLD accelerates the liver disease of the mice carrying HBV to some extent.

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中华实验和临床病毒学杂志

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4549