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The heparin-binding protein interactome in pancreatic diseases

机译:肝素结合蛋白相互作用组在胰腺疾病中的作用

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Background: The cellular microenvironment plays an important role in the regulation of homoeostasis and is a source of potential biomarkers and drug targets. In a genome-wide analysis the extracellular proteins that bind to heparin (HBPs) have been shown to form highly modular and interconnected extracellular protein regulatory networks. Using a systems biology approach, we have investigated the role of HBP networks in the normal pancreas and pancreatic digestive diseases. Methods: Lists of mRNAs encoding for HBPs associated with the normal pancreas (NP), acute pancreatitis (AP), chronic pancreatitis (CP) and pancreatic ductal adenocarcinoma (PDAC) were obtained using public databases and publications. Networks of the putative protein interactomes derived from mRNA expression data of HBPs were built and analysed using cluster analysis, gene ontology term enrichment and canonical pathways analysis. Results: The extracellular heparin-binding putative protein interactomes in the pancreas were better connected than their non heparin-binding counterparts, having higher clustering coefficients in the normal pancreas (0.273), acute pancreatitis (0.457), chronic pancreatitis (0.329) and pancreatic ductal adenocarcinoma (0.269). 'Hepatic Fibrosis/Hepatic Stellate Cell Activation' appears to be a significant canonical pathway in pancreatic homoeostasis in health and disease with a large number of important HBPs. Conclusions: Our analyses clearly demonstrate that HBPs form disease-specific and highly connected networks that can be explored for potential biomarkers and as collective drug targets via the modification of heparin binding properties.
机译:背景:细胞微环境在同稳态的调节中起着重要作用,并且是潜在生物标志物和药物靶标的来源。在全基因组分析中,已证明与肝素(HBP)结合的细胞外蛋白可形成高度模块化且相互连接的细胞外蛋白调节网络。使用系统生物学方法,我们研究了HBP网络在正常胰腺和胰腺消化系统疾病中的作用。方法:使用公共数据库和出版物获得编码与正常胰腺(NP),急性胰腺炎(AP),慢性胰腺炎(CP)和胰腺导管腺癌(PDAC)相关的HBP的mRNA清单。利用聚类分析,基因本体术语富集和规范途径分析,建立并分析了从HBPs mRNA表达数据推定的蛋白质相互作用组网络。结果:与非肝素结合对应物相比,胰腺中细胞外结合肝素的假定蛋白质相互作用体连接性更好,在正常胰腺(0.273),急性胰腺炎(0.457),慢性胰腺炎(0.329)和胰管中的聚集系数更高腺癌(0.269)。 “肝纤维化/星状肝细胞活化”似乎是具有大量重要HBP的健康和疾病中胰腺稳态的重要经典途径。结论:我们的分析清楚地表明,HBPs形成了疾病特异性和高度相关的网络,可以通过修饰肝素结合特性来探索潜在的生物标志物和作为集体药物靶点。

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