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The'lipid raft' microdomain proteins reggie-I and reggie-2 (flotillins) are scaffolds for protein interaction and signalling

机译:'lipid Raft'Microdomain蛋白reggie-I和Reggie-2(甘蓝虫)是用于蛋白质相互作用和信号传导的支架

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Reggie-1 and reggie-2 are two evolutionarily highly conserved proteins which are up-regulated in retinal ganglion cells during regeneration of lesioned axons in the goldfish optic nerve.They are located at the cytoplasmic face of the plasma membrane and are considered to be 'lipid raft' constituents due to their insolubility in Triton X-100 and presence in the 'floating fractions'; hence they were independently named flotillins.According to our current view,the reggies subserve functions as protein scaffolds which form microdomains in neurons,lymphocytes and many other cell types across species as distant as flies and humans.These microdomains are of a surprisingly constant size of <=0.1 mum in all cell types,whereas the distance between them is variable.The microdomains co-ordinate signal transduction of specific cell-surface proteins and especially of GPI (glycosylphosphatidylinositol)-anchored proteins into the cell,as is demonstrated for PrP~c (cellular prion protein) in T-lymphocytes.These cells possess a pre-formed reggie cap scaffold consisting of densely packed reggie microdomains.PrP~c is targeted to the lymphocyte reggie cap when activated by antibody cross-linking,and induces a distinct Ca~(2+) signal.In developing zebrafish,reggies become concentrated in neurons and axon tracts,and their absence,after morpholino antisense RNA-knockdown,results in deformed embryos with reduced brains.Likewise,defects in Drosophila eye morphogenesis occur upon reggie overexpression in mutant flies.The defects observed in the organism,as well as in single cells in culture,indicate a mor-phogenetic function of the reggies,with emphasis on the nervous system.This complies with their role as scaffolds for the formation of multiprotein complexes involved in signalling across the plasma membrane.
机译:Reggie-1和Reggie-2是两种进化高度保守的蛋白质,在金鱼视神经中的损伤轴突再生期间在视网膜神经节细胞中调节上调。它们位于质膜的细胞质面上,被认为是'脂质筏'成分由于它们在Triton X-100中的不溶性和“浮馏分”中的存在;因此,他们独立地命名为弗罗汀。根据我们目前的观点,该项目的用作蛋白质支架,其在神经元,淋巴细胞和许多物种中形成微滴的蛋白质支架,如遥远的苍蝇和人类。的微摩检是令人惊讶的恒定概率<= 0.1妈妈在所有细胞类型,而它们之间的距离是特别的GPI(糖基)锚定蛋白进入细胞特异性细胞表面蛋白和微区variable.The坐标的信号转导,如证明了朊病毒〜 C(细胞朊病毒蛋白)在T淋巴细胞中。这些细胞具有预先形成的reggie帽支架,其由密集包装的reggie微摩擦组成。通过抗体交联激活时,PRP〜C靶向淋巴细胞reggie帽,并诱导截然不同CA〜(2+)信号。在开发斑马鱼中,Reggies浓缩于神经元和轴突,而缺席,在吗啉代反义RNA敲低后,结果具有降低的大脑的RMED胚胎。突变体中的曲粒细胞过表达对果蝇过表达发生的缺陷。在生物体中观察到的缺陷,以及在培养中的单细胞中,表明了区域的MOR-mhocecodic功能,重点是神经系统。这符合其作为支架的作用,用于形成涉及在血浆膜上的信号传导中的多素蛋白复合物。

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