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MDT-28/PLIN-1 mediates lipid droplet-microtubule interaction via DLC-1 in Caenorhabditis elegans

机译:MDT-28 / PLIN-1通过DLC-1在Caenorhabditis elegans中介导脂质液滴 - 微管相互作用

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Ectopic lipid accumulation in lipid droplets (LD) has been linked to many metabolic diseases. In this study, DHS-3::GFP was used as a LD marker in C. elegans and a forward genetic screen was carried out to find novel LD regulators. There were 140 mutant alleles identified which were divided into four phenotypic categories: enlarged, aggregated, aggregated and small, and decreased. After genetic mapping, mutations in three known LD regulatory genes (maoc-1, dhs-28, daf-22) and a peroxisome-related gene (acox-3) were found to enlarge LDs, demonstrating the reliability of using DHS-3 as a living marker. In the screen, the cytoskeleton protein C27H5.2 was found to be involved in LD aggregation, as was the LD resident/structure-like protein, MDT-28/PLIN-1. Using yeast two-hybrid screening and pull-down assays, MDT-28/PLIN-1 was found to bind to DLC-1 (dynein light chain). Fluorescence imaging confirmed that MDT-28/PLIN-1 mediated the interaction between DHS-3 labeled LDs and DLC-1 labeled microtubules. Furthermore, MDT-28/PLIN-1 was directly bound to DLC-1 through its amino acids 1-210 and 275-415. Taken together, our results suggest that MDT-28/PLIN-1 is involved in the regulation of LD distribution through its interaction with microtubule-related proteins.
机译:脂质液滴(LD)中的异位脂质积累已与许多代谢疾病联系起来。在这项研究中,DHS-3 :: GFP用作C.杆杆线虫的LD标记,并进行了前进遗传筛选,寻找新型LD调节器。鉴定有140个突变等位基因,分为四种表型类别:扩大,汇总,汇总和小,减少。在遗传映射之后,发现三种已知的LD调节基因(MAOC-1,DHS-28,DAF-22)和过氧化物组相关基因(ACOX-3)中的突变扩大LD,证明了使用DHS-3的可靠性生活标记。在筛选中,发现细胞骨架蛋白C27H5.2参与LD聚集,如LD居民/结构样蛋白,MDT-28 / PLIN-1。使用酵母双杂交筛选和下拉测定,发现MDT-28 / PLIN-1与DLC-1(Dynein轻链)结合。荧光成像证实,MDT-28 / PLIN-1介导DHS-3标记的LDS和DLC-1标记的微管之间的相互作用。此外,MDT-28 / PLIN-1通过其氨基酸1-210和275-415直接与DLC-1结合。我们的结果表明,MDT-28 / PLIN-1通过其与微管相关蛋白质的相互作用参与LD分布的调节。

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