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Mining Exosomal Genes for Pancreatic Cancer Targets

机译:挖掘胰腺癌靶标的外泌体基因

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Background: Exosomes, cell-derived vesicles encompassing lipids, DNA, proteins coding genes and noncoding RNAs (ncRNAs) are present in diverse body fluids. They offer novel biomarker and drug therapy potential for diverse diseases, including cancer. Materials and Methods: Using gene ontology, exosomal genes database and GeneCards metadata analysis tools, a database of cancer-associated protein coding genes and ncRNAs (n=2,777) was established. Variant analysis, expression profiling and pathway mapping were used to identify putative pancreatic cancer exosomal gene candidates. Results: Five hundred and seventy-five protein-coding genes, 26 RNA genes and one pseudogene directly associated with pancreatic cancer were identified in the study. Nine open reading frames (ORFs) encompassing enzymes, apoptosis and transcriptional regulators, and secreted factors and five cDNAs (enzymes) emerged from the analysis. Among the ncRNA class, 26 microRNAs (miRs), one pseudogene, one long noncoding RNA (LNC) and one antisense gene were identified. Furthermore, 22 exosome-associated protein-coding targets (a cytokine, enzymes, membrane glycoproteins, receptors, and a transporter) emerged as putative leads for pancreatic cancer therapy. Seven of these protein-coding targets are FDA-approved and the drugs-based on these could provide repurposing opportunities for pancreatic cancer. Conclusion: The database of exosomal genes established in this study provides a framework for developing novel biomarkers and drug therapy targets for pancreatic cancer.
机译:背景:外来体,细胞衍生的囊泡,包括脂质,DNA,编码基因的蛋白质和非编码RNA(ncRNA),存在于各种体液中。它们为包括癌症在内的多种疾病提供了新颖的生物标志物和药物治疗潜力。材料与方法:利用基因本体论,外泌体基因数据库和GeneCards元数据分析工具,建立了与癌症相关的蛋白质编码基因和ncRNA(n = 2,777)的数据库。变异分析,表达谱和途径作图被用来确定推定的胰腺癌外泌体基因候选者。结果:确定了与胰腺癌直接相关的575个蛋白质编码基因,26个RNA基因和1个假基因。分析发现了9个开放阅读框(ORF),其中包含酶,凋亡和转录调节因子,以及分泌因子和5个cDNA(酶)。在ncRNA类中,鉴定出26种microRNA(miR),一种假基因,一种长非编码RNA(LNC)和一种反义基因。此外,出现了22种与外泌体相关的蛋白质编码靶标(细胞因子,酶,膜糖蛋白,受体和转运蛋白)作为胰腺癌治疗的推定先导。这些蛋白质编码靶标中有七个是FDA批准的,基于这些靶标的药物可以为胰腺癌的再利用提供机会。结论:本研究建立的外泌体基因数据库为开发新型生物标志物和胰腺癌药物治疗靶标提供了框架。

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