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首页> 外文期刊>Molecular biology of the cell >Novel fibrillar structure in the inversin compartment of primary cilia revealed by 3D single-molecule superresolution microscopy
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Novel fibrillar structure in the inversin compartment of primary cilia revealed by 3D single-molecule superresolution microscopy

机译:通过3D单分子超级化学显微镜揭示原发性纤毛的逆素盒中的新型纤维结构

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Primary cilia in many cell types contain a periaxonemal subcompartment called the inversin compartment. Four proteins have been found to assemble within the inversin compartment: INVS, ANKS6, NEK8, and NPHP3. The function of the inversin compartment is unknown, but it appears to be critical for normal development, including left-right asymmetry and renal tissue homeostasis. Here we combine superresolution imaging of human RPE1 cells, a classic model for studying primary cilia in vitro, with a genetic dissection of the protein-protein binding relationships that organize compartment assembly to develop a new structural model. We observe that INVS is the core structural determinant of a compartment composed of novel fibril-like substructures, which we identify here by three-dimensional single-molecule superresolution imaging. We find that NEK8 and ANKS6 depend on INVS for localization to these fibrillar assemblies and that ANKS6-NEK8 density within the compartment is regulated by NEK8. Together, NEK8 and ANKS6 are required downstream of INVS to localize and concentrate NPHP3 within the compartment. In the absence of these upstream components, NPHP3 is redistributed within cilia. These results provide a more detailed structure for the inversin compartment and introduce a new example of a membraneless compartment organized by protein-protein interactions.
机译:许多细胞类型中的主要纤毛包含一个称为Inversin Co.rament的Periacemal子组件。已发现四种蛋白质组合在逆脉络箱内:INV表,ANKS6,NEK8和NPHP3。逆素隔室的功能是未知的,但对于正常发育至关重要,包括左右不对称和肾组织稳态。在这里,我们将人RPE1细胞的超级化成像,一种用于在体外研究原发性纤毛的经典模型,具有组织室组件的蛋白质 - 蛋白质结合关系的遗传解剖,以开发一种新的结构模型。我们观察到Invs是由新型原纤维状亚结构组成的隔室的核心结构决定簇,其通过三维单分子超级化成像来识别。我们发现NEK8和ANKS6依赖于对这些纤维组件的定位的INV,并且隔室内的ANKS6-NEK8密度由NEK8调节。在一起,NEK8和ANKS6在INVS下游需要在隔间内定位和集中NPHP3。在没有这些上游组分的情况下,NPHP3被重新分配在纤毛内。这些结果为逆素隔室提供了更详细的结构,并引入由蛋白质 - 蛋白质相互作用组织的膜容器的新实例。

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