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Proximity labeling reveals novel interactomes in live Drosophila tissue

机译:邻近标记揭示了活果蝇组织中的新型患者

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Gametogenesis is dependent on intercellular communication facilitated by stable intercellular bridges connecting developing germ cells. During Drosophila oogenesis, intercellular bridges (referred to as ring canals; RCs) have a dynamic actin cytoskeleton that drives their expansion to a diameter of 10 mu m. Although multiple proteins have been identified as components of RCs, we lack a basic understanding of how RC proteins interact together to form and regulate the RC cytoskeleton. Thus, here, we optimized a procedure for proximity-dependent biotinylation in live tissue using the APEX enzyme to interrogate the RC interactome. APEX was fused to four different RC components (RC-APEX baits) and 55 unique high-confidence prey were identified. The RC-APEX baits produced almost entirely distinct interactomes that included both known RC proteins and uncharacterized proteins. A proximity ligation assay was used to validate close-proximity interactions between the RC-APEX baits and their respective prey. Furthermore, an RNA interference screen revealed functional roles for several high-confidence prey genes in RC biology. These findings highlight the utility of enzyme-catalyzed proximity labeling for protein interactome analysis in live tissue and expand our understanding of RC biology.
机译:配子发生依赖于通过连接胚芽细胞的稳定的细胞桥促进的细胞间连通。在果蝇上生期间,细胞外桥(称为环旋转; RCS)具有动态肌动蛋白细胞骨架,使其膨胀的膨胀为10μm的直径。虽然已经将多种蛋白质鉴定为RCS的组分,但我们缺乏对RC蛋白如何相互作用以形成和调节RC细胞骨架的基本理解。因此,在这里,我们优化了使用顶点酶在活组织中优化了依赖于活蛋白的过程,以询问RC互联蛋白。顶点融合到四种不同的RC组件(RC-Apex Baits)和55个独特的高信心猎物。 RC-Apex诱饵产生几乎完全独树的副术,包括已知的RC蛋白和非特征蛋白质。使用近距离连接测定来验证RC-Apex Baits及其各自的猎物之间的近距离相互作用。此外,RNA干扰筛网揭示了RC生物学中几种高置信猎物基因的功能作用。这些发现突出了酶催化的邻近标记在活组织中蛋白质互乱分析的效用,并扩大了对RC生物学的理解。

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