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Temporal transcriptome analysis suggest modulation of multiple pathways and gene network involved in cell-cell interaction during early phase of high altitude exposure

机译:时间转录组分析表明在高海拔暴露早期阶段中涉及细胞 - 细胞相互作用的多种途径和基因网络的调节

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High altitude (HA) conditions induce several physiological and molecular changes, prevalent in individuals who are unexposed to this environment. Individuals exposed towards HA hypoxia yields physiological and molecular orchestration to maintain adequate tissue oxygen delivery and supply at altitude. This study aimed to understand the temporal changes at altitude of 4,111m. Physiological parameters and transcriptome study was conducted at high altitude day 3, 7, 14 and 21. We observed changes in differentially expressed gene (DEG) at high altitude time points along with altered BP, HR, SpO 2 , mPAP. Physiological changes and unsupervised learning of DEG’s discloses high altitude day 3 as distinct time point. Gene enrichment analysis of ontologies and pathways indicate cellular dynamics and immune response involvement in early day exposure and later stable response. Major clustering of genes involved in cellular dynamics deployed into broad categories: cell-cell interaction, blood signaling, coagulation system, and cellular process. Our data reveals genes and pathways perturbed for conditions like vascular remodeling, cellular homeostasis. In this study we found the nodal point of the gene interactive network and candidate gene controlling many cellular interactive pathways VIM, CORO1A, CD37, STMN1, RHOC, PDE7B, NELL1, NRP1 and TAGLN and the most significant among them i.e. VIM gene was identified as top hub gene. This study suggests a unique physiological and molecular perturbation likely to play a critical role in high altitude associated pathophysiological condition during early exposure compared to later time points.
机译:高海拔(HA)条件诱导几种生理和分子变化,在未曝光这种环境的个体中普遍存在。暴露于HA缺氧的个体产生生理和分子编排,以保持足够的组织氧气输送和高度供应。本研究旨在了解海拔高度为4,111米的时间变化。在高海拔第3,7,14和21天进行生理参数和转录组研究。我们观察到高海拔时间点的差异表达基因(DEG)的变化以及改变的BP,HR,SPO 2,MPAP。 Deg的生理变化和无监督学习披露了高海拔第3天作为明显的时间点。本体和途径的基因富集分析表明近日暴露和后来稳定反应的蜂窝动态和免疫应答。涉及蜂窝动态的基因的主要聚类部署到广泛类别:细胞 - 细胞相互作用,血液信号,凝血系统和细胞过程。我们的数据显示出扰动的基因和途径扰动血管重塑,细胞稳态等条件。在本研究中,我们发现基因交互网络的节点和候选基因控制许多细胞交互途径Vim,Coro1a,CD37,stmn1,rhoc,pde7b,nell1,nrp1和tagln以及它们中最重要的,即Vim基因被鉴定为顶级集线器基因。本研究表明,与稍后的时间点相比,在早期暴露期间,可能在早期暴露期间在高海拔相关病理生理病症中发挥关键作用的独特生理和分子扰动。

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