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MicroRNAs as disease progression biomarkers and therapeutic targets in experimental autoimmune encephalomyelitis model of multiple sclerosis 被引量:10
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作者 Bridget Martinez Philip V.Peplow 《Neural Regeneration Research》 SCIE CAS CSCD 2020年第10期1831-1837,共7页
Multiple sclerosis is an autoimmune neurodegenerative disease of the central nervous system characterized by pronounced inflammatory infiltrates entering the brain,spinal cord and optic nerve leading to demyelination.... Multiple sclerosis is an autoimmune neurodegenerative disease of the central nervous system characterized by pronounced inflammatory infiltrates entering the brain,spinal cord and optic nerve leading to demyelination.Focal demyelination is associated with relapsing-remitting multiple sclerosis,while progressive forms of the disease show axonal degeneration and neuronal loss.The tests currently used in the clinical diagnosis and management of multiple sclerosis have limitations due to specificity and sensitivity.MicroRNAs(miRNAs)are dysregulated in many diseases and disorders including demyelinating and neuroinflammatory diseases.A review of recent studies with the experimental autoimmune encephalomyelitis animal model(mostly female mice 6–12 weeks of age)has confirmed miRNAs as biomarkers of experimental autoimmune encephalomyelitis disease and importantly at the pre-onset(asymptomatic)stage when assessed in blood plasma and urine exosomes,and spinal cord tissue.The expression of certain miRNAs was also dysregulated at the onset and peak of disease in blood plasma and urine exosomes,brain and spinal cord tissue,and at the post-peak(chronic)stage of experimental autoimmune encephalomyelitis disease in spinal cord tissue.Therapies using miRNA mimics or inhibitors were found to delay the induction and alleviate the severity of experimental autoimmune encephalomyelitis disease.Interestingly,experimental autoimmune encephalomyelitis disease severity was reduced by overexpression of miR-146a,miR-23b,miR-497,miR-26a,and miR-20b,or by suppression of miR-182,miR-181c,miR-223,miR-155,and miR-873.Further studies are warranted on determining more fully miRNA profiles in blood plasma and urine exosomes of experimental autoimmune encephalomyelitis animals since they could serve as biomarkers of asymptomatic multiple sclerosis and disease course.Additionally,studies should be performed with male mice of a similar age,and with aged male and female mice. 展开更多
关键词 animal model blood plasma blood serum brain tissue disease biomarkers experimental autoimmune encephalomyelitis MICRORNAS multiple sclerosis spinal cord therapeutic targets urine exosomes
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改良蟾蜍毁脑和脊髓方法的效果评价 被引量:2
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作者 朱延河 孟凯 +5 位作者 史小莲 王涛 张莉 郭媛 苟玮 胡浩 《西安交通大学学报(医学版)》 CAS CSCD 北大核心 2020年第1期128-130,共3页
目的完善传统教学中使用探针捣毁蟾蜍脑组织和脊髓实验操作技术中的相关内容。方法在传统教学操作内容基础上,增加探针进入颅腔的进针距离和捣毁脑组织及脊髓的易于体会的具体手感标志。按班级对学生进行随机分组,比较常规组和改良组学... 目的完善传统教学中使用探针捣毁蟾蜍脑组织和脊髓实验操作技术中的相关内容。方法在传统教学操作内容基础上,增加探针进入颅腔的进针距离和捣毁脑组织及脊髓的易于体会的具体手感标志。按班级对学生进行随机分组,比较常规组和改良组学生首次及第2次操作成功率和花费时间。结果改良组学生捣毁蟾蜍脑组织和脊髓成功率高(首次成功率93.2%vs.72.3%;第2次成功率97.7%vs.85.1%),而且花费时间少[首次操作时间(311.7±89.3)s vs.(511.6±171.1)s;第2次操作时间(161.3±63.5)s vs.(266.0±98.2)s],两组学生的第1、2次成功率和操作时间差异均有统计学意义(P<0.05)。结论传统教学的捣毁蟾蜍脑组织和脊髓内容经过完善后,易于被学生掌握,成功率高,用时少,更符合3R原则,便于教学推广应用。 展开更多
关键词 蟾蜍 捣毁 脑组织 脊髓
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一种直接破坏蟾蜍(蛙)脑和脊髓的新方法 被引量:1
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作者 常燕琴 高洪波 +3 位作者 王兴宇 应康 王立军 宋芳 《包头医学院学报》 CAS 2021年第11期104-106,共3页
破坏蟾蜍(蛙)脑和脊髓方法是机能实验学课程中常用的基本实验操作技能之一,其传统法是通过枕骨大孔先后破坏脑和脊髓组织达到处死蟾蜍(蛙)目的,此种方法很大程度上凭感觉和经验才能一次成功,对于初学者来说,往往一次成功率很低。本文介... 破坏蟾蜍(蛙)脑和脊髓方法是机能实验学课程中常用的基本实验操作技能之一,其传统法是通过枕骨大孔先后破坏脑和脊髓组织达到处死蟾蜍(蛙)目的,此种方法很大程度上凭感觉和经验才能一次成功,对于初学者来说,往往一次成功率很低。本文介绍的直接法可一次性直接将脑和脊髓完全破坏,简单易行,成功率高,适于教学中推广应用。 展开更多
关键词 机能实验 破坏脑和脊髓 处死蟾蜍(青蛙)
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