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相关作者:王凯翟伟胡宏秀匡世焕赵英更多>>
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Rett综合征相关基因MeCP2敲除大鼠模型的构建及分析被引量:3
2016年
MeCP2(Methyl CpG binding protein 2)基因突变可导致Rett综合征(Rett syndrome,RTT)。目前已报道的MeCP2敲除小鼠表型与RTT病人症状存在显著差异。为探索MeCP2在脑发育中的作用及其导致RTT的机制,本研究利用CRISPR/Cas9技术构建了MeCP2基因敲除大鼠模型。通过构建靶向敲除MeCP2基因的载体,体外将Cas9 mRNA和sgRNA显微注射到SD大鼠受精卵中,在MeCP2基因exon2中造成移码突变,从而获得MeCP2基因敲除大鼠。利用测序和Westernblotting方法鉴定MeCP2敲除大鼠,并对其表型和行为学特征进行分析,发现MeCP2敲除大鼠体重降低,存在焦虑倾向和认知缺陷。本研究成功构建了MeCP2基因敲除大鼠模型,其表型类似人类RTT患者的症状,为后续MeCP2功能研究提供了更好的动物模型。
翟伟胡宏秀乐亮庄峰峰王克柱赵英王凯刘新民孙迪安王晓英匡世焕胡克平
关键词:MECP2SD大鼠模型RETT综合征
Positive effects of low dose IMPX977 on Rett syndrome related MeCP2 targeted-genes被引量:1
2019年
Objective: To investigate the effect of IMPX977 on MeCP2 targeted-genes and the feasibility of IMPX977 acting as a therapeutic candidate drug for Rett syndrome by genomewide transcription profiling.Methods: Rats' cortex of control group, IMPX977-treated low-dose group(10 mg/kg), and IMPX977-treated high-dose group(30 mg/kg) were collected and RNA was extracted from the tissues. Then, RNA was subjected to RNA-sequencing. Gene ontology(GO) and kyoto encyclopedia of genes and genomes(KEGG)were used in functional enrichment analysis of differentially expressed genes.Results: Six MeCP2 targeted-genes were identified in the low/control categories, but not in the high/control categories.Conclusion: Low-dose treatment of IMPX977(10 mg/kg) showed a positive effect on MeCP2 targeted-genes and it may serve as a drug candidate for Rett syndrome therapy with proper dosage.
Ying ZhaoLiang LeYue-qiang SongLi-xin QiHui FuXue BaiSi-guang LiXin-sheng NanKe-ping Hu
关键词:MECP2RETT
Comprehensive Evaluation on Effect of IMPX977 on Expression of Methyl-CpG-binding Protein 2 in Rats被引量:1
2017年
Objective To investigate the effect of IMPX977 on methyl-Cp G-binding protein 2(MeCP2) expression in rats. Methods Forty-eight SD rats were randomly divided into four groups: normal control group, olive oil(negative control, 5 mL/kg oil) group, and 10 mg/kg and 30 mg/kg IMPX977 administration groups. All rats were given corresponding dose of drugs each other day and administered orally for two weeks. Tissues including cortex and cerebellum were collected from rats to assay the expression of MeCP2 by quantitative RT-PCR and Western blotting. Results The IMPX977 supplement showed no significant effect on the body weight of rats. In normal rats, MeCP2 was highly expressed in cerebellum, cortex and hippocampus, and less expressed in heart, spleen and lung. In addition to male rats, compared with the control group, the expression of MeCP2 mRNA was significantly increased in cerebellum after 30 mg/kg IMPX977 treatment and contrarily, absolutely decreased in cortex of all treatment groups. Furthermore, in female rats MeCP2 mRNA was reduced in cortex of both olive oil and 30 mg/kg IMPX977 treatment groups compared with control group. Meanwhile, MeCP2 protein level was significantly elevated in cerebellum of treated male rats compared to the control group. In contrast to the control group, the expression of MeCP2 protein in both cerebellum and cortex of female rats in other three groups was increased. Conclusion IMPX977 treatment(10 mg/kg) may elevate the expression of MeCP2, which establishes experimental foundation for the further research on rat models of Rett syndrome.
Ya HuLiang LeLi-xin QiYing ZhaoHui FuChen DuanXiao-ying WangKe-ping Hu
关键词:CEREBELLUMHOMEOSTASISMECP2
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