高脂肪饮食加重氯氮平治疗小鼠胰岛β细胞毒性。

Chung-Huei Huang, Shin-Huei Fu, Samuel Hsu, Yu-Yao Huang, Szu-Tah Chen, Brend Ray-Sea Hsu
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引用次数: 5

摘要

背景:氯氮平是一种非典型抗精神病药物,在某些患者中引起葡萄糖稳态紊乱。本研究探讨氯氮平诱导β细胞毒性的机制。方法:将52只健康C57BL/6雄性小鼠随机分为4组,研究氯氮平(C、D组)和高脂饮食(B、D组)对小鼠的影响。每组随机取3只小鼠,测定第8 ~ 10天的摄食量,第11天切除胰腺进行组织学检查。各组其余10只小鼠于第8周处死,测定胰腺胰岛素含量(PIC)。结果:氯氮平给药8周小鼠PIC有降低趋势。第11天的胰腺组织学检查显示细胞凋亡改变,细胞增殖受到抑制。虽然喂食高脂肪食物的小鼠体重增加,但同时喂食氯氮平和高脂肪食物的小鼠体重增加较少,组织学恶化更严重,并且四组中PIC水平最低。结论:氯氮平可抑制小鼠胰腺β细胞凋亡,抑制细胞增殖,降低胰腺胰岛素含量。氯氮平诱导的β细胞毒性在给小鼠同时喂食高脂肪食物时进一步加重。
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High-fat diet aggravates islet beta-cell toxicity in mice treated with clozapine.

Background: Clozapine, an atypical antipsychotic drug, induces derangements in glucose homeostasis in certain patients. This study investigated the mechanisms of clozapine-induced beta-cell toxicity.

Methods: Fifty-two healthy C57BL/6 male mice were randomized into 4 groups to study the effects of clozapine (group C, D) and a high-fat diet (group B, D). Three mice from each group were randomly selected to determine the amount of food intake on days 8-10, and their pancreases were removed for histological examination on day 11. The remaining 10 mice in each group were sacrificed at the 8th week to measure pancreatic insulin content (PIC).

Results: Mice given clozapine for 8 weeks demonstrated trends of lower PIC. The histological examination of the pancreases retrieved on day 11 already revealed apoptotic changes and suppression of cell proliferation. Although mice fed high-fat chow gained weight, mice given both clozapine and a high-fat diet showed less weight gain and more severe histological deterioration, and had the lowest PIC levels of the 4 groups.

Conclusion: Pancreatic beta-cell apoptosis, suppression of cell proliferation, and trends of reduction in pancreatic insulin content were observed in mice taking clozapine. The findings of clozapine induced beta-cell toxicity were further aggravated when mice were concomitantly fed a high-fat diet.

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