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An ARL3-UNC119-RP2 GTPase cycle targets myristoylated NPHP3 to the primary cilium.

机译:ARL3-UNC119-RP2 GTPase循环将肉豆蔻酰化的NPHP3靶向初级纤毛。

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摘要

The membrane of the primary cilium is a highly specialized compartment that organizes proteins to achieve spatially ordered signaling. Disrupting ciliary organization leads to diseases called ciliopathies, with phenotypes ranging from retinal degeneration and cystic kidneys to neural tube defects. How proteins are selectively transported to and organized in the primary cilium remains unclear. Using a proteomic approach, we identified the ARL3 effector UNC119 as a binding partner of the myristoylated ciliopathy protein nephrocystin-3 (NPHP3). We mapped UNC119 binding to the N-terminal 200 residues of NPHP3 and found the interaction requires myristoylation. Creating directed mutants predicted from a structural model of the UNC119-myristate complex, we identified highly conserved phenylalanines within a hydrophobic beta sandwich to be essential for myristate binding. Furthermore, we found that binding of ARL3-GTP serves to release myristoylated cargo from UNC119. Finally, we showed that ARL3, UNC119b (but not UNC119a), and the ARL3 GAP Retinitis Pigmentosa 2 (RP2) are required for NPHP3 ciliary targeting and that targeting requires UNC119b myristoyl-binding activity. Our results uncover a selective, membrane targeting GTPase cycle that delivers myristoylated proteins to the ciliary membrane and suggest that other myristoylated proteins may be similarly targeted to specialized membrane domains.
机译:初级纤毛的膜是高度专门化的区室,其组织蛋白质以实现空间有序的信号传导。破坏性睫状组织导致称为纤毛病的疾病,其表型范围从视网膜变性和囊性肾脏到神经管缺陷。蛋白质如何选择性地转运至初级纤毛并在初级纤毛中组织尚不清楚。使用蛋白质组学方法,我们确定了ARL3效应子UNC119是肉豆蔻酰化纤毛病蛋白nephrocystin-3(NPHP3)的结合伴侣。我们将UNC119结合定位到NPHP3的N末端200个残基,发现相互作用需要肉豆蔻酰化。创建从UNC119-肉豆蔻酸酯复合物的结构模型预测的定向突变体,我们发现疏水性β三明治中高度保守的苯丙氨酸对于肉豆蔻酸酯的结合至关重要。此外,我们发现结合ARL3-GTP可以从UNC119释放肉豆蔻酰化的货物。最后,我们显示NPHP3纤毛靶向需要ARL3,UNC119b(而不是UNC119a)和ARL3 GAP色素性视网膜炎2(RP2),并且靶向需要UNC119b肉豆蔻酰结合活性。我们的结果揭示了选择性的,靶向膜的GTPase循环,该循环将肉豆蔻酰化的蛋白质递送至睫状膜,提示其他肉豆蔻酰化的蛋白质可能类似地靶向特定的膜结构域。

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