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A Ral guanine exchange factor-Ral pathway is conserved in Drosophila melanogaster and sheds new light on the connectivity of the Ral, Ras, and Rap pathways

机译:Ral鸟嘌呤交换因子-Ral途径在果蝇中是保守的,为Ral,Ras和Rap途径的连通性提供了新的思路

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摘要

Ras GTPases are central to many physiological and pathological signaling pathways and act via a combination of effectors. In mammals, at least three Ral exchange factors (RalGEFs) contain a Ras association domain and constitute a discrete subgroup of Ras effectors. Despite their ability to bind activated Rap as well as activated Ras, they seem to act downstream of Ras but not downstream of Rap. We have revisited the Ras/Rap-Ral connections in Drosophila melanogaster by using iterative two-hybrid screens with these three GTPases as primary baits and a subsequent genetic approach. We show that (i) the Ral-centered protein network appears to be extremely conserved in human and flies, (ii) in this network, RGL is a functional Drosophila orthologue of RalGEFs, and (iii) the RGL-Ral pathway functionally interacts with both the Ras and Rap pathways. Our data do not support the paradigmatic model where Ral is in the effector pathway of Ras. They reveal a signaling circuitry where Ral is functionally downstream of the Rap GTPase, at odds with the pathways described for mammalian cell lines. Thus, in vivo data show variations in the connectivity of pathways described for cell lines which might display only a subset of the biological possibilities.
机译:Ras GTPases对许多生理和病理信号通路至关重要,并通过多种效应子共同发挥作用。在哺乳动物中,至少三个Ral交换因子(RalGEF)包含Ras缔合域,并构成Ras效应子的离散亚组。尽管它们具有结合活化的Rap和活化的Ras的能力,但它们似乎在Ras的下游起作用,但在Rap的下游却不起作用。我们通过使用具有这三个GTPases作为主要诱饵的迭代双杂交筛选以及随后的遗传方法,重新研究了果蝇中的Ras / Rap-Ral连接。我们显示(i)以Ral为中心的蛋白质网络在人类和果蝇中似乎极为保守,(ii)在该网络中,RGL是RalGEF的功能性果蝇直系同源物,并且(iii)RGL-Ral途径在功能上与Ras和Rap通路。我们的数据不支持Ral在Ras的效应途径中的范式模型。他们揭示了一个信号传导电路,其中Ral在功能上位于Rap GTPase的下游,与描述的哺乳动物细胞系途径不同。因此,体内数据显示出针对细胞系描述的途径的连通性的变化,其可能仅显示出生物学可能性的一部分。

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