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SCI TRANSL MED:Src/c-Abl通路有望成为肌萎缩性脊髓侧索硬化症治疗药物新靶点

2017-05-25 cailingrui MedSci原创

采用取自ALS病人的运动神经元所产生的诱导性多功能干细胞(iPSCs)为实验材料,进行药物筛选。研究人员筛选了现有的药物,Src/c-Abl激酶抑制剂可以促进自噬作用,防止ALS运动神经元退行性病变

肌萎缩性脊髓侧索硬化症(ALS)是一种异质的运动神经元疾病,目前还未发现通用的药物靶点和治疗方案。在这项新的研究中,Imamura等人采用取自ALS病人的运动神经元所产生的诱导性多功能干细胞(iPSCs)为实验材料,进行药物筛选。研究人员筛选了现有的药物,实验显示Src/c-Abl激酶抑制剂可以促进自噬作用,防止ALS运动神经元退行性病变。其中一种药物更是对带有多个基因突变的ALS病人的运动神经元的存活起促进作用。

实验所用诱导性多功能干细胞(iPSCs)来自一位带有超氧化物歧化酶编码基因(SOD1)的ALS病人的运动神经元。筛选结果显示,超过一半的靶点落在了Src/c-Abl信号通路中。体外实验证明,Src/c-Abl抑制剂可以提升ALS iPSC的存活率。用siRNA敲除Src或c-Abl,同样可以防止ALS运动神经元退行性病变。其中,博舒替尼可以加快自噬作用,减少突变SOD1蛋白的错误折叠数量,改变线粒体基因表达。对TAR DNA结合蛋白编码基因(TDP-43)突变,或C9orf72基因上的串联重复导致的散发ALS或其他家族性ALS,博舒替尼同样在体外试验中表现出对神经元的存活起到促进作用。此外,博舒替尼治疗同样在带有SOD1突变的小鼠模型中,表现出了一定的积极作用。Src/c-Abl通路有望成为ALS治疗的药物新靶点。

原始出处:
Keiko Imamura, et al. The Src/c-Abl pathway is a potential therapeutic target in amyotrophic lateral sclerosis. Sci Transl Med. 24 May 2017:Vol. 9, Issue 391, eaaf3962

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    2018-01-26 bsmagic9140
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    2017-09-01 zhangxingru
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  5. 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  6. 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createdBy=eebd9606217, createdName=neizongke, createdTime=Sat May 27 00:19:00 CST 2017, time=2017-05-27, status=1, ipAttribution=), GetPortalCommentsPageByObjectIdResponse(id=1607566, encodeId=b20f160e56615, content=<a href='/topic/show?id=eb6b1145939' target=_blank style='color:#2F92EE;'>#Med#</a>, beContent=null, objectType=article, channel=null, level=null, likeNumber=53, replyNumber=0, topicName=null, topicId=null, topicList=[TopicDto(id=11459, encryptionId=eb6b1145939, topicName=Med)], attachment=null, authenticateStatus=null, createdAvatar=null, createdBy=552a19396740, createdName=ms3994565386320060, createdTime=Sat May 27 00:19:00 CST 2017, time=2017-05-27, status=1, ipAttribution=)]
    2018-01-18 chendoc252
  8. 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    2017-05-27 lsndxfj
  9. 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研究显示ALS患者队列中连续的额叶代谢障碍反映了临床和解剖学上的疾病进展的过程,从单纯ALS、伴有中间认知缺陷的ALS到ALS-FTD。伴有中间认知障碍的ALS患者在PET检查下显示独特的代谢模式。

Neurology:TBK1无效突变易引起额颞叶痴呆和肌萎缩性脊髓侧索硬化症

这项比利时临床患者队列研究发现TBK1 LOF突变是紧随C9orf72 和GRN之后,引起临床FTD的第三大常见原因,同时TBK1 LOF突变也是紧随 C9orf72之后引起临床ALS的第二大常见原因。这些发现说明FTD和ALS实际上属于一种连续的谱系疾病。

Cell Res:肌萎缩性脊髓侧索硬化症(渐冻症)转基因猪模型建立

近日,记者在中科院广州生物医药与健康研究院获悉,该院研究员赖良学与中科院遗传与发育生物学研究所教授李晓江、澳大利亚蒙纳什大学教授肖志成、南方医科大学教授姜晓丹等联合攻关,成功培育出渐冻人症模型猪。相关研究在线发表于《细胞研究》上。 渐冻人症是一种渐进和致命的神经退行性疾病,病人由于上、下运动神经元都退化和死亡并停止传送讯息到肌肉,导致肌肉逐渐萎缩,最后神经系统完全丧失控制随意运动的能力,导致病人瘫

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