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国家教育部博士点基金(20130096110011)

作品数:4 被引量:13H指数:2
相关作者:廖红刘媛陈明明方吟荃李晨辉更多>>
相关机构:中国药科大学更多>>
发文基金:国家教育部博士点基金国家自然科学基金江苏省自然科学基金更多>>
相关领域:医药卫生更多>>

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神经营养因子低亲和力受体p75NTR的表达及新药开发被引量:1
2015年
p75NTR作为神经营养因子低亲和力受体,可与各种配体和细胞内因子相互作用后对神经系统产生促存活或致凋亡的不同效应;同时,作为肿瘤坏死因子受体超家族的一员,其在细胞凋亡和神经再生中发挥重要作用。p75NTR的表达与其多潜能性之间密切相关,因此,了解p75NTR在各种类型细胞及损伤或疾病状态下的表达,有助于对其功能或潜在作用进行更深入的研究。本文主要对p75NTR的表达进行综述,并探讨目前靶向作用于p75NTR药物的研究和开发。
倪婕刘高翔廖红
关键词:神经营养因子受体P75NTR神经退行性疾病药物靶点
Quercetin promotes neurite growth through enhancing intracellular cAMP level and GAP-43 expression被引量:5
2015年
The present study was designed to investigate the role of quercetin on neurite growth in N1E-115 cells and the underlying mechanisms. Quercetin was evaluated for its effects on cell numbers of neurites, neurite length, intracellular cAMP content, and Gap-43 expression in N1E-115 cells in vitro by use of microscopy, LANCE? cAMP 384 kit, and Western blot analysis, respectively. Our results showed that quercetin could increase the neurite length in a concentration-dependent manner, but had no effect on the numbers of cells. Quercetin significantly increased the expression of cellular cAMP in a time- and concentration-dependent manner. The Gap-43 expression was up-regulated in a time-dependent manner. In conclusion, quercetin could promote neurite growth through increasing the intracellular c AMP level and Gap-43 expression.
CHEN Ming-MingYIN Zhi-QiZHANG Lu-YongLIAO Hong
关键词:调剂学
脑卒中康复治疗的研究进展被引量:6
2016年
每年世界范围内中风的首次发患者数约为1960万,经过急性期救治后幸存的中风患者70%~80%患有残疾,严重影响其日常生活活动及适应社会生活的能力[1-2]。脑卒中后,机体神经功能受损,在恢复期神经系统会进行一定程度的自我修复,但是不足以使机体的神经功能恢复到正常水平,从而造成神经功能障碍。研究脑卒中神经功能恢复的病理机制及治疗方法,对改善中风患者预后、提高生活质量具有十分重要的意义。本文对近年来相关研究进展综述如下。
刘媛李晨辉方吟荃陈明明廖红
关键词:脑卒中神经功能
Screening of natural compounds with neuronal differentiation promoting effects in a cell-based model被引量:1
2015年
The purpose of this study was to establish a drug screening method for small molecules extracted from traditional Chinese medicines(TCM) that have neuronal differentiation promoting effects, using P19 embryonic carcinoma cell as a cell-based model. First, the constructed plasmid(p Tα1-Luc) was transfected into P19 cells to establish a screening model. Second, several TCMs were screened using the established model and all-trans-retinoic acid as a positive control. Finally, the underlying molecular mechanism was explored using immunofluorescence staining, q T-PCR, and Western blot analysis. Our results indicated that the drug screen model was established successfully and that both honokiol and hyperoside induced P19 differentiation into neurons, with the possible molecular mechanism being modulating the Wnt signaling pathway. In conclusion, the drug screening model developed in the present study provides a rapid, cell-based screening platform for identifying natural compounds with neuronal differentiation effects.
CHEN TaoWANG JuanLIU MeiZHANG Lu-YongLIAO Hong
关键词:SCREENINGMODELNEURONALP19EMBRYONIC
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