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A Mighty Small Heart: The Cardiac Proteome of Adult Drosophila melanogaster

机译:一颗强大的小心脏:成人的心脏蛋白质组 果蝇

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摘要

Drosophila melanogaster is emerging as a powerful model system for the study of cardiac disease. Establishing peptide and protein maps of the Drosophila heart is central to implementation of protein network studies that will allow us to assess the hallmarks of Drosophila heart pathogenesis and gauge the degree of conservation with human disease mechanisms on a systems level. Using a gel-LC-MS/MS approach, we identified 1228 protein clusters from 145 dissected adult fly hearts. Contractile, cytostructural and mitochondrial proteins were most abundant consistent with electron micrographs of the Drosophila cardiac tube. Functional/Ontological enrichment analysis further showed that proteins involved in glycolysis, Ca2+-binding, redox, and G-protein signaling, among other processes, are also over-represented. Comparison with a mouse heart proteome revealed conservation at the level of molecular function, biological processes and cellular components. The subsisting peptidome encompassed 5169 distinct heart-associated peptides, of which 1293 (25%) had not been identified in a recent Drosophila peptide compendium. PeptideClassifier analysis was further used to map peptides to specific gene-models. 1872 peptides provide valuable information about protein isoform groups whereas a further 3112 uniquely identify specific protein isoforms and may be used as a heart-associated peptide resource for quantitative proteomic approaches based on multiple-reaction monitoring. In summary, identification of excitation-contraction protein landmarks, orthologues of proteins associated with cardiovascular defects, and conservation of protein ontologies, provides testimony to the heart-like character of the Drosophila cardiac tube and to the utility of proteomics as a complement to the power of genetics in this growing model of human heart disease.
机译:果蝇(Drosophila melanogaster)逐渐成为研究心脏病的强大模型系统。建立果蝇心脏的肽和蛋白质图谱是实施蛋白质网络研究的关键,这将使我们能够评估果蝇心脏发病机制的标志,并在系统水平上评估人类疾病机制的保守程度。使用gel-LC-MS / MS方法,我们从145个解剖的成年蝇心中鉴定了1228个蛋白簇。收缩蛋白,细胞结构蛋白和线粒体蛋白最丰富,与果蝇心管的电子显微照片一致。功能/本体富集分析进一步表明,糖酵解,Ca 2+结合,氧化还原和G蛋白信号传导等过程中涉及的蛋白质也被过度表达。与小鼠心脏蛋白质组的比较揭示了在分子功能,生物学过程和细胞成分水平上的保守性。存在的肽组包含5169种与心脏相关的独特肽,其中1293种(25%)尚未在最近的果蝇肽汇编中鉴定。进一步使用PeptideClassifier分析将肽定位到特定的基因模型。 1872个肽提供了有关蛋白质同工型的有价值的信息,而另外3112个肽可唯一识别特定的蛋白质同工型,可用作基于心脏的肽资源,用于基于多反应监测的定量蛋白质组学方法。总之,鉴定激发收缩蛋白标志物,与心血管缺陷相关的蛋白的直向同源物以及蛋白本体的保守性,为果蝇心管的心脏样特征以及蛋白质组学作为能量补充的效用提供了证据。人类心脏病的这种增长模型中的遗传学研究。

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