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微管上的动力蛋白-动力蛋白激活蛋白复合物结构显示串联衔接蛋白结合。

Structure of dynein-dynactin on microtubules shows tandem adaptor binding.

机构信息

Division of Structural Studies, Medical Research Council Laboratory of Molecular Biology, Cambridge, UK.

出版信息

Nature. 2022 Oct;610(7930):212-216. doi: 10.1038/s41586-022-05186-y. Epub 2022 Sep 7.

Abstract

Cytoplasmic dynein is a microtubule motor that is activated by its cofactor dynactin and a coiled-coil cargo adaptor. Up to two dynein dimers can be recruited per dynactin, and interactions between them affect their combined motile behaviour. Different coiled-coil adaptors are linked to different cargos, and some share motifs known to contact sites on dynein and dynactin. There is limited structural information on how the resulting complex interacts with microtubules and how adaptors are recruited. Here we develop a cryo-electron microscopy processing pipeline to solve the high-resolution structure of dynein-dynactin and the adaptor BICDR1 bound to microtubules. This reveals the asymmetric interactions between neighbouring dynein motor domains and how they relate to motile behaviour. We found that two adaptors occupy the complex. Both adaptors make similar interactions with the dyneins but diverge in their contacts with each other and dynactin. Our structure has implications for the stability and stoichiometry of motor recruitment by cargos.

摘要

细胞质动力蛋白是一种微管马达,它通过其辅助因子动力蛋白和卷曲螺旋货物衔接器而被激活。每个动力蛋白可以招募多达两个动力蛋白二聚体,它们之间的相互作用影响它们的联合运动行为。不同的卷曲螺旋衔接器与不同的货物相连,其中一些衔接器具有与动力蛋白和动力蛋白衔接蛋白上的接触位点已知的基序。关于由此产生的复合物与微管的相互作用以及衔接器如何被招募的结构信息有限。在这里,我们开发了一种低温电子显微镜处理管道来解决与微管结合的动力蛋白-动力蛋白衔接蛋白和衔接蛋白 BICDR1 的高分辨率结构。这揭示了相邻动力蛋白马达结构域之间的不对称相互作用,以及它们与运动行为的关系。我们发现两个衔接器占据了复合物。两个衔接器与动力蛋白都有相似的相互作用,但与彼此和动力蛋白衔接蛋白的接触不同。我们的结构对货物通过马达募集的稳定性和化学计量学有影响。

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