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Stoichioproteomics reveal oxygen usage bias, key proteins and pathways in glioma

机译:Stoichioproteomics显示胶质瘤中的氧气使用偏向,关键蛋白和途径

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The five-year survival rate and therapeutic effect of malignant glioma is low. Identification of key/associated proteins and pathways in glioma is necessary for developing effective diagnosis and targeted therapy of glioma. In addition, Glioma involves hypoxia-specific microenvironment, whether hypoxia restriction influences the stoichioproteomic characteristics of expressed proteins is unknown. In this study, we analyzed the most comprehensive immunohistochemical data from 12 human glioma samples and 4 normal cell types of cerebral cortex, identified differentially expressed proteins (DEPs), and researched the oxygen contents of DEPs, highly and lowly expressed proteins. Further we located key genes on human genome to determine their locations and enriched them for key functional pathways. Our results showed that although no difference was detected on whole proteome, the average oxygen content of highly expressed proteins is 6.65% higher than that of lowly expressed proteins in glioma. A total of 1480 differentially expressed proteins were identified in glioma, including 226 up regulated proteins and 1254 down regulated proteins. The average oxygen content of up regulated proteins is 2.56% higher than that of down regulated proteins in glioma. The localization of differentially expressed genes on human genome showed that most genes were on chromosome 1 and least on Y. The up regulated proteins were significantly enriched in pathways including cell cycle, pathways in cancer, oocyte meiosis, DNA replication etc. Functional dissection of the up regulated proteins with high oxygen contents showed that 51.28% of the proteins were involved in cell cycle and cyclins. Element signature of oxygen limitation could not be detected in glioma, just as what happened in plants and microbes. Unsaved use of oxygen by the highly expressed proteins and DEPs were adapted to the fast division of glioma cells. This study can help to reveal the molecular mechanism of glioma, and provide a new approach for studies of cancer-related biomacromolecules. In addition, this study lays a foundation for application of stoichioproteomics in precision medicine.
机译:恶性神经胶质瘤的五年生存率和治疗效果低。鉴定神经胶质瘤中关键/相关蛋白和途径对于开发有效的神经胶质瘤诊断和靶向治疗是必要的。另外,神经胶质瘤涉及缺氧特异性微环境,缺氧限制是否影响表达蛋白的化学骨蛋白学特征尚不清楚。在这项研究中,我们分析了来自12个人类神经胶质瘤样本和4种正常大脑皮层正常细胞类型的最全面的免疫组化数据,鉴定了差异表达蛋白(DEP),并研究了DEPs的氧含量,高表达和低表达的蛋白质。此外,我们在人类基因组上定位了关键基因,以确定它们的位置,并丰富了它们的关键功能途径。我们的结果表明,尽管在整个蛋白质组中未检测到差异,但高表达蛋白的平均氧含量比神经胶质瘤中低表达蛋白的平均氧含量高6.65%。在神经胶质瘤中鉴定出总共1480种差异表达的蛋白,包括226种上调蛋白和1254种下调蛋白。胶质瘤中上调蛋白的平均氧含量比下调蛋白的平均氧含量高2.56%。人类基因组中差异表达基因的定位表明,大多数基因位于1号染色体上,而最少的位于Y染色体上。上调的蛋白在细胞周期,癌症,卵母细胞减数分裂,DNA复制等途径中显着富集。具有高氧含量的上调蛋白表明51.28%的蛋白与细胞周期和细胞周期蛋白有关。就像植物和微生物中发生的一样,在胶质瘤中无法检测到氧限制的元素特征。高度表达的蛋白质和DEP未利用氧气来适应神经胶质瘤细胞的快速分裂。这项研究可以帮助揭示神经胶质瘤的分子机制,并为研究与癌症有关的生物大分子提供新的方法。此外,该研究为化学计量学在精密医学中的应用奠定了基础。

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