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Differential protein-protein interactions of LRRK1 and LRRK2 indicate roles in distinct cellular signaling pathways.

机译：LRRK1和LRRK2的差异蛋白质-蛋白质相互作用表明在不同的细胞信号通路中的作用。

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Genetic studies show that LRRK2, and not its closest paralogue LRRK1, is linked to Parkinson's disease. To gain insight into the molecular and cellular basis of this discrepancy, we searched for LRRK1- and LRRK2-specific cellular processes by identifying their distinct interacting proteins. A protein microarray-based interaction screen was performed with recombinant 3xFlag-LRRK1 and 3xFlag-LRRK2 and, in parallel, co-immunoprecipitation followed by mass spectrometry was performed from SH-SY5Y neuroblastoma cell lines stably expressing 3xFlag-LRRK1 or 3xFlag-LRRK2. We identified a set of LRRK1- and LRRK2-specific as well as common interactors. One of our most prominent findings was that both screens pointed to epidermal growth factor receptor (EGF-R) as a LRRK1-specific interactor, while 14-3-3 proteins were LRRK2-specific. This is consistent with phosphosite mapping of LRRK1, revealing phosphosites outside of 14-3-3 consensus binding motifs. To assess the functional relevance of these interactions, SH-SY5Y-LRRK1 and -LRRK2 cell lines were treated with LRRK2 kinase inhibitors that disrupt 14-3-3 binding, or with EGF, an EGF-R agonist. Redistribution of LRRK2, not LRRK1, from diffuse cytoplasmic to filamentous aggregates was observed after inhibitor treatment. Similarly, EGF induced translocation of LRRK1, but not of LRRK2, to endosomes. Our study confirms that LRRK1 and LRRK2 can carry out distinct functions by interacting with different cellular proteins. LRRK1 and LRRK2 (leucine-rich repeat kinase) interaction partners were identified by two different protein-protein interaction screens. These confirmed epidermal growth factor receptor (EGR-R) as a LRRK1-specific interactor, while 14-3-3 proteins were LRRK2-specific. Functional analysis of these interactions and the pathways they mediate shows that LRRK1 and LRRK2 signaling do not intersect, reflective of the differential role of both LRRKs in Parkinson's disease.

机译：遗传研究表明，LRRK2，而不是其最接近的旁系同源物LRRK1，与帕金森氏病有关。为了深入了解这种差异的分子和细胞基础，我们通过鉴定它们的独特相互作用蛋白来搜索LRRK1和LRRK2特异性细胞过程。用重组3xFlag-LRRK1和3xFlag-LRRK2进行基于蛋白质微阵列的相互作用筛选，同时，从稳定表达3xFlag-LRRK1或3xFlag-LRRK2的SH-SY5Y神经母细胞瘤细胞系中进行免疫共沉淀和质谱。我们确定了一组LRRK1和LRRK2特定以及常见的相互作用者。我们最突出的发现之一是，这两次筛选均指出表皮生长因子受体（EGF-R）是LRRK1特异性的相互作用物，而14-3-3蛋白是LRRK2特异性的。这与LRRK1的磷酸位点定位一致，揭示了14-3-3共有结合基序之外的磷酸位点。为了评估这些相互作用的功能相关性，用破坏14-3-3结合的LRRK2激酶抑制剂或EGF（一种EGF-R激动剂）处理了SH-SY5Y-LRRK1和-LRRK2细胞系。抑制剂处理后，观察到LRRK2而非LRRK1从弥散的细胞质重新分布到丝状聚集体。同样，EGF诱导LRRK1而不是LRRK2易位到内体。我们的研究证实，LRRK1和LRRK2通过与不同的细胞蛋白相互作用可以执行不同的功能。 LRRK1和LRRK2（富含亮氨酸的重复激酶）相互作用伙伴是通过两个不同的蛋白相互作用筛选确定的。这些证实了表皮生长因子受体（EGR-R）是LRRK1特异性的相互作用物，而14-3-3蛋白是LRRK2特异性的。对这些相互作用及其介导途径的功能分析表明，LRRK1和LRRK2信号不相交，反映了两种LRRK在帕金森氏病中的不同作用。

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Reyniers L; Del Giudice MG; Civiero L; Belluzzi E; Lobbestael E; Beilina A; Arrigoni G; Derua R; Waelkens E; Li Y; Crosio C; Iaccarino C; Cookson MR; Baekelandt V; Greggio E; Taymans JM;
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年度 2014
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专利

1. Differential protein-protein interactions of LRRK1 and LRRK2 indicate roles in distinct celluar signaling pathways [J] . Reyniers Lauran, Del Giudice Maria Grazia, Civiero Laura, Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry . 2014,第2期

机译：LRRK1和LRRK2的差异蛋白质-蛋白质相互作用表明在不同的细胞信号通路中的作用
2. Interaction of cellular prion and stress-inducible protein 1 promotes neuritogenesis and neuroprotection by distinct signaling pathways. [J] . Lopes MH, Hajj GN, Muras AG, The Journal of Neuroscience: The Official Journal of the Society for Neuroscience . 2005,第49期

机译：细胞病毒和应激诱导蛋白1的相互作用通过不同的信号通路促进神经形成和神经保护。
3. Uncovering the diversity of redox proteoforms and their significance in cellular signaling and protein-protein interactions [J] . Griesser Eva, Barayeu Uladzimir, Flemmig Joerg, Free Radical Biology and Medicine: The Official Journal of the Oxygen Society . 2018,第期

机译：揭开氧化还原蛋白质血管的多样性及其在细胞信号传导和蛋白质 - 蛋白质相互作用中的意义
4. Computational prediction of protein-protein interactions in sphingolipid signaling network [C] . Gungormez Y., Ozkirimli Olmez E., Ulgen K.O. Biomedical Engineering Meeting, 2009. BIYOMUT 2009 . 2009

机译：鞘脂信号网络中蛋白质相互作用的计算预测
5. Functional signatures in protein-protein interactions and their impact on signaling pathways. [D] . Liu, Yichuan. 2010

机译：蛋白质-蛋白质相互作用中的功能性特征及其对信号通路的影响。
6. Differential protein-protein interactions of LRRK1 and LRRK2 indicate roles in distinct cellular signaling pathways [O] . Lauran Reyniers, Maria Grazia Del Giudice, Laura Civiero, -1

机译：LRRK1和LRRK2的差异蛋白相互作用表明在不同的细胞信号通路中的作用
7. Differential protein-protein interactions of LRRK1 and LRRK2 indicate roles in distinct cellular signaling pathways [O] . Reyniers Lauran, Del Giudice Maria Grazia, Civiero Laura, 2014

机译：LRRK1和LRRK2的差异蛋白相互作用表明在不同的细胞信号通路中的作用

Differential protein-protein interactions of LRRK1 and LRRK2 indicate roles in distinct cellular signaling pathways.

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