Intracerebral hemorrhage (ICH) is a devastating condition. Existing preclinical ICH models focus largely on striatum but neglect other brain areas such as ventricle, cortex, and hippocampus. Clinically, however, hemorrhagic strokes do occur in these other brain regions. In this study, we established mouse hemorrhagic models that utilize stereotactic injections of autologous whole blood or collagenase to produce ventricular, cortical, and hippocampal injury. We validated and characterized these models by histology, immunohistochemistry, and neurobehavioral tests. In the intraventricular hemorrhage (IVH) model, C57BL/6 mice that received unilateral ventricular injections of whole blood demonstrated bilateral ventricular hematomas, ventricular enlargement, and brain edema in the ipsilateral cortex and basal ganglia at 72 h. Unilateral injections of collagenase (150 U/ml) caused reproducible hematomas and brain edema in the frontal cortex in the cortical ICH (c-ICH) model and in the hippocampus in the hippocampal ICH (h-ICH) model. Immunostaining revealed cellular inflammation and neuronal death in the periventricular regions in the IVH brain and in the perihematomal regions in the c-ICH and h-ICH brains. Locomotor abnormalities measured with a 24-point scoring system were present in all three models, especially on days 1, 3, and 7 post-ICH. Locomotor deficits measured by the wire-hanging test were present in models of IVH and c-ICH, but not h-ICH. Interestingly, mice in the c-ICH model demonstrated emotional abnormality, as measured by the tail suspension test and forced swim test, whereas h-ICH mice exhibited memory abnormality, as measured by the novel object recognition test. All three ICH models generated reproducible brain damage, brain edema, inflammation, and consistent locomotor deficits. Additionally, the c-ICH model produced emotional deficits and the h-ICH model produced cognitive deficits. These three models closely mimic human ICH and should be useful for investigating the pathophysiology of ICH in ventricle, cortex, and hippocampus and for evaluating potential therapeutic strategies.
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机译:脑出血(ICH)是一种破坏性疾病。现有的临床前ICH模型主要关注纹状体,而忽略了其他脑部区域,如心室,皮质和海马体。然而,在临床上,出血性中风的确发生在这些其他大脑区域。在这项研究中,我们建立了小鼠出血模型,该模型利用立体定向注射自体全血或胶原酶来产生心室,皮层和海马损伤。我们通过组织学,免疫组织化学和神经行为测试验证并表征了这些模型。在脑室内出血(IVH)模型中,接受单侧心室全血注射的C57BL / 6小鼠在72 h时表现出同侧皮质和基底神经节的双侧心室血肿,心室扩大和脑水肿。单侧注射胶原酶(150 U / ml)在皮质ICH(c-ICH)模型和海马ICH(h-ICH)模型的额叶皮层中引起可再现的血肿和脑水肿。免疫染色显示,IVH脑的脑室周围区域以及c-ICH和h-ICH脑的血肿周围区域存在细胞炎症和神经元死亡。在所有三个模型中均存在使用24点评分系统测量的运动异常,尤其是在ICH后的第1、3和7天。 IVH和c-ICH模型中存在通过导线悬挂测试测量的运动缺陷,但h-ICH中没有。有趣的是,c-ICH模型中的小鼠表现出情绪异常,如通过尾部悬吊测试和强迫游泳测试所测,而h-ICH小鼠则表现出记忆异常,如通过新型物体识别测试所测。所有这三种ICH模型均产生可再现的脑损伤,脑水肿,炎症和持续的运动功能障碍。另外,c-ICH模型产生情绪缺陷,h-ICH模型产生认知缺陷。这三种模型紧密模拟人类ICH,对于研究脑室,皮层和海马中ICH的病理生理学以及评估潜在的治疗策略应该有用。
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