基于A53T转基因小鼠注射α-突触核蛋白纤维加速建立帕金森病模型
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广西医科大学基础医学院转化医学研究中心,长寿与老年相关疾病教育部重点实验室,神经科学研究所广西脑科学研究重点实验室

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国家自然科学基金项目(面上项目,重点项目,重大项目)


Accelerated establishment of a Parkinson's disease model through α-syn PFF injection in A53T transgenic mice
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Center for?Translational?Medicine,Key?Laboratory?of?Longevity?and?Aging-related?Diseases,Ministry?of?Education,Institute?of?Neuroscience?and?Guangxi?Key?Laboratory?of?Brain?Science,School?of?Basic?Medical?Sciences,Guangxi?Medical?University

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The National Natural Science Foundation of China (General Program, Key Program, Major Research Plan)

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    摘要:

    目的 通过在A53T转基因小鼠脑内注射α-突触核蛋白预形成纤维(α-syn PFF),促进帕金森病病理改变的快速出现,从而加快帕金森病小鼠模型的建立。方法 选择C57BL/6J背景的α-Syn A53T转基因小鼠作为模型组,同系C57小鼠为对照组,通过脑立体定位技术将α-syn PFF注射至小鼠双侧纹状体内。造模后,通过旷场实验评估小鼠的自主活动能力和焦虑行为;转棒、抓力及爬杆实验测定其运动协调性和四肢肌张力;埋藏食物实验评价小鼠的嗅觉功能;通过免疫组织化学染色法探究小鼠脑内炎症和α-syn病理发生。结果 与对照组比较,模型组小鼠α-syn PFF脑内注射后1月旷场实验中运动距离增加;转棒、抓力与爬杆实验无统计学差异;埋藏食物实验中寻找食物时间增加。造模后2月模型组旷场实验中运动距离减少;转棒、抓力与爬杆实验中运动协调能力以及肌张力减弱;埋藏食物实验中寻找食物时间增加。模型组小鼠黑质、皮层、海马体的磷酸化α-synuclein增加;小胶质细胞增加,路易小体沉积;黑质多巴胺能神经元显著减少。结论 A53T小鼠脑内注射α-syn PFF后更快出现嗅觉功能受损及运动功能障碍;并产生明显的病理改变,表现为α-synuclein/LBs于黑质、皮层、海马体聚集,黑质多巴胺能神经元丢失。可作为一种快速建立的α-突触核蛋白相关帕金森病的动物模型。

    Abstract:

    Objective Intracranial injection of α-synuclein preformed fibrils (α-syn PFF)in A53T transgenic mice accelerates the onset of Parkinson"s disease pathology, facilitating the rapid establishment of a Parkinson’s disease mouse model. Methods C57BL/6J background α-Syn A53T transgenic mice were selected as the model group, with isogenic C57 mice as the control group. α-Syn PFF was injected into the bilateral striatum using stereotactic brain injection. After modeling, the open field test was used to assess spontaneous activity and anxiety-like behavior, while the rotarod, grip strength, and pole tests evaluated motor coordination and limb muscle tone. The buried food test was conducted to assess olfactory function.Immunohistochemical staining was performed to investigate neuroinflammation and α-syn pathology in the mouse brain. Results Compared to the control group, One month after α-syn PFF injection, model mice showed increased locomotion in the open-field test, with no significant differences in the rotarod, grip strength, or pole tests, but prolonged food-seeking time. By two months, locomotion decreased, motor coordination and muscle tone weakened, and food-seeking time further increased. Phosphorylated α-synuclein levels were elevated in the substantia nigra, cortex, and hippocampus, with microglial activation, Lewy body deposition, and significant dopaminergic neuron loss in the substantia nigra. Conclusions A53T mice developed olfactory dysfunction and motor impairments more rapidly after α-syn PFF injection. Significant pathological changes were observed, including the aggregation of α-synuclein/LBs in the substantia nigra, cortex, and hippocampus, and the loss of dopaminergic neurons in the substantia nigra. This model can serve as a rapidly established animal model for α-synucleinopathy-related Parkinson"s disease.

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  • 收稿日期:2025-03-24
  • 最后修改日期:2025-05-22
  • 录用日期:2025-06-18
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