Richardson Brian C, Fromme J Christopher
Department of Molecular Biology and Genetics, Weill Institute for Cell and Molecular Biology, Cornell University, Ithaca, NY, USA.
Small GTPases. 2012 Oct-Dec;3(4):240-3. doi: 10.4161/sgtp.21828. Epub 2012 Sep 20.
Members of the highly conserved Arf family of small GTPases serve as master regulators of vesicular transport. In yeast, Arf1 acts at the Golgi and trans-Golgi network (TGN) to recruit vesicular coat proteins and other effectors for both anterograde and retrograde transport. Arf1 is activated at the TGN by Sec7, the founding member of the Sec7 family of guanine nucleotide exchange factors (GEFs) and a close homolog of the human ARFGEF2 implicated in congenital defects in cerebral cortex development. Through the use of purified Sec7 in biochemical assays, we recently discovered that autoinhibition of Sec7 is relieved by stable recruitment to lipid membranes by activated Arf1. This interaction is mediated by a conserved domain proximal to, but not including, the GEF domain, creating a positive feedback loop in the activation of Arf1 at the TGN. We further demonstrated that this stable interaction with Arf1 plays a role in localizing Sec7 to the TGN. We elaborate here on the implications of these results to small GTPase-mediated cellular processes and coincidence detection models of GEF localization.
高度保守的小GTP酶Arf家族成员是囊泡运输的主要调节因子。在酵母中,Arf1在高尔基体和反式高尔基体网络(TGN)发挥作用,募集囊泡包被蛋白和其他效应因子以进行顺行和逆行运输。Arf1在TGN被Sec7激活,Sec7是鸟嘌呤核苷酸交换因子(GEF)Sec7家族的创始成员,也是与大脑皮质发育先天性缺陷有关的人类ARFGEF2的紧密同源物。通过在生化分析中使用纯化的Sec7,我们最近发现,激活的Arf1将Sec7稳定募集到脂质膜上可解除Sec7的自抑制。这种相互作用由靠近但不包括GEF结构域的保守结构域介导,在TGN处Arf1的激活中形成正反馈回路。我们进一步证明,与Arf1的这种稳定相互作用在将Sec7定位于TGN中发挥作用。我们在此详细阐述这些结果对小GTP酶介导的细胞过程以及GEF定位的巧合检测模型的影响。
