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两种 RNA 结合蛋白介导 miR223 从线粒体分拣到外泌体中。

Two RNA-binding proteins mediate the sorting of miR223 from mitochondria into exosomes.

机构信息

Department of Molecular and Cell Biology, Howard Hughes Medical Institute, University of California, Berkeley, United States.

出版信息

Elife. 2023 Jul 25;12:e85878. doi: 10.7554/eLife.85878.

Abstract

Fusion of multivesicular bodies (MVBs) with the plasma membrane results in the secretion of intraluminal vesicles (ILVs), or exosomes. The sorting of one exosomal cargo RNA, miR223, is facilitated by the RNA-binding protein, YBX1 (Shurtleff et al., 2016). We found that miR223 specifically binds a 'cold shock' domain (CSD) of YBX1 through a 5' proximal sequence motif UCAGU that may represent a binding site or structural feature required for sorting. Prior to sorting into exosomes, most of the cytoplasmic miR223 resides in mitochondria. An RNA-binding protein localized to the mitochondrial matrix, YBAP1, appears to serve as a negative regulator of miR223 enrichment into exosomes. miR223 levels decreased in the mitochondria and increased in exosomes after loss of YBAP1. We observed YBX1 shuttle between mitochondria and endosomes in live cells. YBX1 also partitions into P body granules in the cytoplasm (Liu et al., 2021). We propose a model in which miR223 and likely other miRNAs are stored in mitochondria and are then mobilized by YBX1 to cytoplasmic phase condensate granules for capture into invaginations in the endosome that give rise to exosomes.

摘要

多泡体(MVBs)与质膜融合导致腔内囊泡(ILVs)或外泌体的分泌。RNA 结合蛋白 YBX1 促进一种外泌体 cargo RNA(miR223)的分拣(Shurtleff 等人,2016)。我们发现 miR223 通过可能代表分拣所需的结合位点或结构特征的 5'近端序列基序 UCAGU 特异性结合 YBX1 的“冷休克”结构域(CSD)。在分拣到外泌体之前,细胞质中的大多数 miR223 都位于线粒体中。一种定位于线粒体基质的 RNA 结合蛋白 YBAP1 似乎作为 miR223 富集到外泌体的负调节剂。YBAP1 缺失后,线粒体中的 miR223 水平降低,外泌体中的 miR223 水平升高。我们观察到 YBX1 在活细胞中线粒体和内体之间穿梭。YBX1 还会在细胞质的 P 体颗粒中分配(Liu 等人,2021)。我们提出了一个模型,其中 miR223 和可能其他 miRNAs 储存在线粒体中,然后由 YBX1 动员到细胞质相凝聚物颗粒中,以便捕获到内体中的凹陷,从而产生外泌体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/deaf/10403255/e2fc96b0e527/elife-85878-fig1.jpg

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