精神分裂症模型大鼠前额叶皮质PKA 和内皮细胞趋化因子-5 的表达变化
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(武汉市优抚医院,武汉 430023)

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R-33

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Expression of protein kinase A and endothelial cell chemokine-5 in the prefrontal cortex of rats with schizophrenia
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(Wuhan Youfu Hospital, Wuhan 43002, China)

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    摘要:

    目的 通过建立精神分裂症大鼠模型,观察病理损伤和前额叶皮质PKA 和内皮细胞趋化因子-5 表达变化,阐明其神经损伤机制,为指导临床治疗提供参考依据?方法 实验分随机分为2 组:对照组(为正常饲养大鼠,皮下注射生理盐水, n =15)和诱导组(每日腹腔注射苯丙胺0. 5 mg/ kg,建立精神分裂症模型, n = 15),通过苏木精-伊红染色检测大鼠前额叶神经细胞核固缩情况;采用Sams-Dodd 刻板行为评分系统和旷场实验检测大鼠精神分裂模型;通过RT-qRCR 检测PKA 和CCL5 mRNA 的表达量;通过酶联免疫吸附试验试剂盒法检测实验大鼠中PKA 和CCL5 蛋白水平含量;通过蛋白质免疫印迹检测IL-1α?IL-1β 和IL-17 蛋白表达水平?结果 与对照组(0. 85±0. 14)相比,诱导组大鼠的刻板评分(2. 38±0. 26)增高,旷场实验诱导组(326. 58±15. 47)较对照组(198. 55±12. 58)升高( P <0. 05);与对照组相比,诱导组大鼠PKA 和CCL5 mRNA 表达量升高( P <0. 05);诱导组PKA(4. 21±1. 05)mmol/ g 和CCL5(3. 76±0. 51) mmol/ g 含量较对照组(2. 46±0. 67) mmol/ g 和(1. 35±0. 24) mmol/ g 高( P <0. 05);白细胞介素促炎因子(IL-1α?IL-1β?IL-17)的蛋白表达上,诱导组(2. 85±0. 35)?(2. 15±0. 27)?(2. 16±0. 32)较对照组(1. 02±0. 17)?(0. 94±0. 13)?(1. 05±0. 25)上升( P <0. 05);诱导组较对照组细胞阳性率占比高,前额叶椎体细胞大量核固缩,胞浆嗜伊红染色增强( P <0. 05)?结论 精神分裂症大鼠模型前额叶皮质PKA 和内皮细胞CCL5 表达增加,诱发认知障碍?

    Abstract:

    Objective By establishing a schizophrenic rat model, to observe the changes in protein kinase A (PKA) and chemokine-5 (CCL5) expression in the prefrontal cortex, to clarify the mechanism of neurological injury, and to provide a reference for guiding clinical treatment. Methods The experimental rats were randomly divided into two groups: the control group (received subcutaneous injection of normal saline, n = 15) and the schizophrenia model group (received daily intraperitoneal injection of amphetamine at 0. 5 mg/ kg to establish a model of schizophrenia, n = 15). Nuclear pyknosis of the prefrontal neurons was detected by pathological observation using hematoxylin-eosin staining. The rat model of schizophrenia was verified by the Sams-Dodd stereotype behavior scoring system and open field test. The expression levels of PKA and CCL5 mRNA were detected by quantitative reverse transcription polymerase chain. The levels of PKA and CCL5 protein in experimental rats were detected by enzyme-linked immunosorbent assay. The interleukin (IL)- 1α, IL-1β, and IL-17 protein expression levels were detected by western blotting. Results The stereotypic behavior score was higher in the schizophrenia model group than control group (2. 38±0. 26 vs. 0. 85±0. 14, respectively), and the open field test score was higher in the schizophrenia model group than control group (326. 58± 15. 47 vs. 198. 55± 12. 58, respectively) ( P <0. 05). The expressions of PKA and CCL5 mRNA were higher in the schizophrenia model group than control group ( P <0. 05). The PKA and CCL5 contents were higher in the schizophrenia model group (4. 21±1. 05 and 3. 76±0. 51 mmol/ g, respectively) than in the control group (2. 46±0. 67 and 1. 35±0. 24 mmol/ g, respectively) ( P < 0. 05). The protein expressions of the pro-inflammatory factors IL-1α, IL-1β, and IL-17 were higher in the schizophrenia model group (2. 85±0. 35, 2. 15±0. 27, and 2. 16±0. 32, respectively) than control group (1. 02±0. 17, 0. 94±0. 13, and 1. 05±0. 25, respectively) ( P <0. 05). The schizophrenia model group had a higher proportion of positive cells than the control group, and the anterior frontal pyramidal cells showed more nuclear pyknosis and cytoplasmic eosinophilia. Red staining was enhanced in the schizophrenia model group ( P <0. 05). Conclusions The expressions of PKA and CCL5 in the prefrontal cortex are higher in rats with than without schizophrenia and induce cognitive impairment.

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万争艳,李宁,向玲玲,陈莹,梅红彬,董红霞.精神分裂症模型大鼠前额叶皮质PKA 和内皮细胞趋化因子-5 的表达变化[J].中国比较医学杂志,2019,29(10):92~97.

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  • 收稿日期:2019-01-31
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  • 在线发布日期: 2019-11-07
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