原代培养脊髓神经元神经丝蛋白NF-H表达与免疫电镜观察

目的:研究原代培养脊髓神经元NF-H表达及免疫电镜的分布,为神经丝结构异常所致的神经疾病奠定实验基础。方法:采用神经细胞培养技术、免疫组织化学与免疫电镜技术,进行原代培养脊髓神经元的神经丝蛋白NF-H的表达,并用图像分析仪对NF-H表达进行了定量分析测定。结果:原代培养脊髓神经元中,神经丝蛋白的NF-H的表达,随细胞发育的逐渐成熟呈日趋上升趋势。免疫电镜观察可见神经丝蛋白呈电子密度高的丝絮状沉淀,均匀分布在细胞质中,在突起中呈束状排列。结论:神经丝蛋白的NF-H表达的增加,伴随着神经元的发育初期到成熟的形态结构变化,与培养时间成正相关。

NF-H在无症状颈动脉狭窄患者血清中的表达与认知功能的关系

目的:探讨无症状颈动脉狭窄患者颈动脉支架术前及术后血清神经丝蛋白重链(NF-H)表达与患者认知功能的关系。方法:入选2018年5月—2019年8月于四川省人民医院神经内科住院的40例伴有轻度认知功能损害的无症状颈动脉狭窄患者作为实验组,对照组为40例健康人群。用酶联免疫吸附试验(ELISA)法测定实验组CAS术前、术后3月血清NF-H水平以及对照组血清NF-H水平。分别在CAS术前1周、术后3个月用简易智力状态检查量表(MMSE)及蒙特利尔认知评估量表(MoCA)评价患者认知功能。比较术前、术后3月血清NF-H表达差异及患者术前及术后3个月认知功能变化。结果:实验组术前患者血清NF-H水平高于对照组(P<0.01),实验组术前MMSE评分为(26.08±1.59)分低于对照组MMSE评分(27.93±2.95)分(P<0.05),实验组术前MoCA评分明显低于对照组:(24.48±1.89)分个月vs.(27.97±1.21)分(P<0.01);与术前实验组相比,术后3个月实验组血清NF-H水平显著下降(P<0.01),这与实验组CAS术后3个月的后认知功能改善相符,实验组认知功能术前术后比较:MMSE(26.08±1.59)分vs.(27.48±1.95)分,P<0.05、MoCA(24.48±1.89)分vs.(26.83±.49)分,P<0.05;Pearson相关性分析得出,患者血清NF-H水平与患者MMSE评分及MoCA评分均呈负相关(P<0.01)。结论:无症状颈动脉狭窄患者存在不同程度的脑损伤及认知功能障碍,颈动脉支架术可有效改善颈动脉狭窄相关的认知功能损害,脑损伤标志物NF-H可能成为早期识别认知功能损害及监测颈动脉支架术后患者认知功能改变的生物学标志物。

Tropic1808在PC12细胞中的表达

目的构建稳定表达tropic1808基因的PC12细胞株,并通过观察稳定株中高分子量神经丝蛋白(NF-H)的表达以初步观察该基因的作用。方法构建重组真核表达载体pcDNA-HA-tropic1808,转染PC12细胞,经G418筛选、Westernblot鉴定。采用RT-PCR,实时PCR,Westernblot和细胞组织化学方法观察tropic1808稳定株中NF-H的表达。结果Westernblot检测表明,tropic1808基因稳定表达,RT-PCR,实时PCR,Westernblot和细胞组织化学方法均观察到NF-H在tropic1808稳定株中的表达高于空载体对照。结论Tropic1808基因可以在PC12稳定表达且NF-H在tropic1808稳定株中表达上升。

Efficacy of chitosan and sodium alginate scaffolds for repair of spinal cord injury in rats

Spinal cord injury results in the loss of motor and sensory pathways and spontaneous regeneration of adult mammalian spinal cord neurons is limited. Chitosan and sodium alginate have good biocompatibility, biodegradability, and are suitable to assist the recovery of damaged tissues, such as skin, bone and nerve. Chitosan scaffolds, sodium alginate scaffolds and chitosan-sodium alginate scaffolds were separately transplanted into rats with spinal cord hemisection. Basso-Beattie-Bresnahan locomotor rating scale scores and electrophysiological results showed that chitosan scaffolds promoted recovery of locomotor capacity and nerve transduction of the experimental rats.Sixty days after surgery, chitosan scaffolds retained the original shape of the spinal cord. Compared with sodium alginate scaffolds- and chitosan-sodium alginate scaffolds-transplanted rats, more neurofilament-H-immunoreactive cells （regenerating nerve fibers） and less glial fibrillary acidic protein-immunoreactive cells （astrocytic scar tissue） were observed at the injury site of experimental rats in chitosan scaffold-transplanted rats. Due to the fast degradation rate of sodium alginate, sodium alginate scaffolds and composite material scaffolds did not have a supporting and bridging effect on the damaged tissue. Above all, compared with sodium alginate and composite material scaffolds, chitosan had better biocompatibility, could promote the regeneration of nerve fibers and prevent the formation of scar tissue,and as such, is more suitable to help the repair of spinal cord injury.

Progesterone modulates m TOR in the hippocampus of mice after traumatic brain injury

Spinal cord injury results in the loss of motor and sensory pathways and spontaneous regeneration of adult mammalian spinal cord neurons is limited. Chitosan and sodium alginate have good biocompatibility, biodegradability, and are suitable to assist the recovery of damaged tissues, such as skin, bone and nerve. Chitosan scaffolds, sodium alginate scaffolds and chitosan-sodium alginate scaffolds were separately transplanted into rats with spinal cord hemisection. Basso-Beattie-Bresnahan locomotor rating scale scores and electrophysiological results showed that chitosan scaffolds promoted recovery of locomotor capacity and nerve transduction of the experimental rats.Sixty days after surgery, chitosan scaffolds retained the original shape of the spinal cord. Compared with sodium alginate scaffolds- and chitosan-sodium alginate scaffolds-transplanted rats, more neurofilament-H-immunoreactive cells （regenerating nerve fibers） and less glial fibrillary acidic protein-immunoreactive cells （astrocytic scar tissue） were observed at the injury site of experimental rats in chitosan scaffold-transplanted rats. Due to the fast degradation rate of sodium alginate, sodium alginate scaffolds and composite material scaffolds did not have a supporting and bridging effect on the damaged tissue. Above all, compared with sodium alginate and composite material scaffolds, chitosan had better biocompatibility, could promote the regeneration of nerve fibers and prevent the formation of scar tissue,and as such, is more suitable to help the repair of spinal cord injury.

NF-H基因参与K562/A02细胞多药耐药机制形成的研究

目的 分析K5 6 2 /A0 2细胞多药耐药性 (MDR)分子机制 ,寻找可能参与K5 6 2 /A0 2细胞耐药机制的新基因。方法 通过长期逐步增加K5 6 2细胞培养液中阿霉素 (ADM)的浓度 ,诱导出多药耐药细胞株K5 6 2 /A0 2 ,利用cDNAmicroarray比较K5 6 2和K5 6 2 /A0 2基因表达的差别 ,从中选择NF H基因进行RT PCR和免疫细胞化学验证 ,并利用反义核酸技术和细胞内ADM浓度的测定 ,进一步验证该基因与K5 6 2 /A0 2细胞多药耐药的关系。结果 通过比较发现 ,有 12个基因可能参与了K5 6 2 /A0 2细胞的耐药机制 ,其中 7个基因在K5 6 2 /A0 2中被下调 ,5个基因被上调。本研究结果显示 ,NF H基因在K5 6 2 /A0 2细胞中高表达 ,并且 ,将NF H和mdr1反义核酸同时转入K5 6 2 /A0 2细胞后 ,可明显提高细胞内ADM浓度 ,而单独转入NF H反义核酸效果不明显。结论 K5 6 2 /A0 2细胞耐药表型的形成是多因素的 ,除了P 糖蛋白 (P gp)等常见因素外 ,可能还有NF