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A reconstituted mammalian APC-kinesin complex selectively transports defined packages of axonal mRNAs

机译:一个重构的哺乳动物APC-Kinesin复合体选择性地运送定义的轴突MRNA包装

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Through the asymmetric distribution of messenger RNAs (mRNAs), cells spatially regulate gene expression to create cytoplasmic domains with specialized functions. In neurons, mRNA localization is required for essential processes such as cell polarization, migration, and synaptic plasticity underlying long-term memory formation. The essential components driving cytoplasmic mRNA transport in neurons and mammalian cells are not known. We report the first reconstitution of a mammalian mRNA transport system revealing that the tumor suppressor adenomatous polyposis coli (APC) forms stable complexes with the axonally localized β-actin and β2B-tubulin mRNAs, which are linked to a kinesin-2 via the cargo adaptor KAP3. APC activates kinesin-2, and both proteins are sufficient to drive specific transport of defined mRNA packages. Guanine-rich sequences located in 3′UTRs of axonal mRNAs increase transport efficiency and balance the access of different mRNAs to the transport system. Our findings reveal a minimal set of proteins sufficient to transport mammalian mRNAs.
机译:通过信使RNA(MRNA)的不对称分布,细胞在空间上调节基因表达以产生具有专用功能的细胞质结构域。在神经元中,对于细胞偏振,迁移和突触塑性的基本方法,需要MRNA定位,包括长期记忆形成的突触件。不知道在神经元和哺乳动物细胞中驱动细胞质mRNA转运的基本组分。我们报告了哺乳动物mRNA运输系统的第一次重构揭示肿瘤抑制腺瘤性息肉(APC)与官方局部β-肌动蛋白和β2B-微管蛋白MRNA形成稳定的复合物,其通过货物适配器与Kinesin-2连接KAP3。 APC激活Kinesin-2,并且两种蛋白质足以驱动定义的mRNA包的特定传输。富含富含轴突的序列,位于轴突MRNA的3级,提高运输效率并平衡不同MRNA的进入运输系统。我们的研究结果揭示了一种足以运输哺乳动物MRNA的最小蛋白质。

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