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A Highlights from MBoC Selection: Coordination of Grp1 recruitment mechanisms by its phosphorylation

机译:来自MBOC选择的亮点:通过其磷酸化协调GRP1招生机制

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The action of guanine nucleotide exchange factors (GEFs) on the ADP-ribosylation factor (ARF) family of small GTPases initiates intracellular transport pathways. This role requires ARF GEFs to be recruited from the cytosol to intracellular membrane compartments. An ARF GEF known as General receptor for 3-phosphoinositides 1 (Grp1) is recruited to the plasma membrane through its pleckstrin homology (PH) domain that recognizes phosphatidylinositol 3,4,5-trisphosphate (PIP3). Here, we find that the phosphorylation of Grp1 induces its PH domain to recognize instead phosphatidylinositol 4-phosphate (PI4P). This phosphorylation also releases an autoinhibitory mechanism that results in the coil–coil (CC) domain of Grp1 engaging two peripheral membrane proteins of the recycling endosome. Because the combination of these actions results in Grp1 being recruited preferentially to the recycling endosome rather than to the plasma membrane, our findings reveal the complexity of recruitment mechanisms that need to be coordinated in localizing an ARF GEF to an intracellular compartment to initiate a transport pathway. Our elucidation is also remarkable for having revealed that phosphoinositide recognition by a PH domain can be switched through its phosphorylation.
机译:鸟嘌呤核苷酸交换因子(GEF)对小GTP酶的ADP-核糖基化因子(ARF)系列的作用引发了细胞内传输途径。该作用需要将ARF GEF从细胞溶溶剂募集到细胞内膜隔室。称为3-磷酸阳性1(GRP1)的ARF GEF通过其Pleckstrin同源性(pH)结构域募集到血浆膜中,识别磷脂酰肌醇3,4,5-三磷酸(PIP3)。在这里,我们发现GRP1的磷酸化诱导其pH结构域以识别磷脂酰肌醇4-磷酸酯(PI4P)。该磷酸化还释放出一种自动抑制机制,导致GRP1的线圈线圈(CC)结构域接合循环内体的两个外周膜蛋白。因为这些动作的组合导致GRP1优先募集到循环内体而不是血浆膜,所以我们的研究结果揭示了需要协调的招生机制的复杂性,以便将ARF GEF定位成细胞内隔室以启动运输途径。我们的阐明也显着,揭示了通过其磷酸化通过pH结构域通过pH结构域识别。

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