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A family of ADP-ribosylation factor effectors that can alter membrane transport through the trans-Golgi

机译:ADP-核糖基化因子效应子家族,可改变通过反式高尔基体的膜转运

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A family of three structurally related proteins were cloned from human cDNA libraries by their ability to interact preferentially with the activated form of human ADP-ribosylation factor 3 (ARF3) in two-hybrid assays. The specific and GTP-dependent binding was later confirmed through direct protein binding of recombinant proteins. The three proteins share large (approximate to 300 residues) domains at their N termini that are 60-70% identical to each other and a shorter (73 residues) domain at their C termini with 70% homology to the C-terminal "ear" domain of gamma-adaptin. Although GGA1 is found predominantly as a soluble protein by cell fractionation, all three proteins were found to localize to the trans-Golgi network (TGN) by indirect immunofluorescence. The binding of GGAs to TGN was sensitive to brefeldin A, consistent with this being an ARF-dependent event. Thus, these proteins have been named Golgi-localizing, gamma-adaptin ear homology domain, ARF-binding proteins, or GGAs. The finding that overexpression of GGAs was sufficient to alter the distribution of markers of the TGN (TGN38 and mannose 6-phosphate receptors) led us to propose that GGAs are effecters for ARFs that function in the regulation of membrane traffic through the TGN. [References: 57]
机译:通过在两个杂交试验中与人ADP-核糖基化因子3(ARF3)的活化形式优先相互作用的能力,从人cDNA文库中克隆了三个结构相关蛋白家族。后来通过重组蛋白的直接蛋白结合证实了特异性和GTP依赖性结合。这三种蛋白质在其N末端共享大(约300个残基)结构域,彼此之间具有60-70%的同一性,在其C末端共享一个较短的(约73个残基)结构域,与C端“耳朵”具有70%的同源性-adaptin的结构域。尽管通过细胞分级分离发现GGA1主要为可溶性蛋白,但通过间接免疫荧光法发现所有这三种蛋白均位于反式高尔基网络(TGN)中。 GGA与TGN的结合对布雷菲德菌素A敏感,这与ARF依赖性事件一致。因此,这些蛋白质已被命名为高尔基体定位,γ-adaptin耳朵同源结构域,ARF结合蛋白或GGA。 GGA的过表达足以改变TGN标记(TGN38和甘露糖6磷酸受体)的分布的发现使我们提出,GGA是ARF的效应物,在通过TGN调节膜运输中起作用。 [参考:57]

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