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短期高氧暴露后大鼠器官中信号级联的时程依赖性途径激活。

Time Dependent Pathway Activation of Signalling Cascades in Rat Organs after Short-Term Hyperoxia.

机构信息

Department of Anesthesiology and Intensive Care Medicine, University Hospital of Cologne, 50937 Cologne, Germany.

Department of Anaesthesiology, St George's University Hospital, NHS Foundation Trust, London SW17 0QT, UK.

出版信息

Int J Mol Sci. 2018 Jul 4;19(7):1960. doi: 10.3390/ijms19071960.

Abstract

Administration of oxygen is one of the most common interventions in medicine. Previous research showed that differential regulated proteins could be linked to hyperoxia-associated signaling cascades in different tissues. However, it still remains unclear which signaling pathways are activated by hyperoxia. The present study analyses hyperoxia-induced protein alterations in lung, brain, and kidney tissue using a proteomic and bioinformatic approach. Pooled data of 36 Wistar rats exposed to hyperoxia were used. To identify possible hyperoxia biomarkers, and to evaluate the relationship between protein alterations in hyperoxia affected organs and blood, proteomics data from brain, lung, and kidney were analyzed. Functional network analyses (IPA, PathwaysStudio, and GENEmania) in combination with hierarchical cluster analysis (Perseus) was used to identify relevant pathways and key proteins. Data of 54 2D-gels with more than 2500 significantly regulated spots per gel were collected. Thirty-eight differentially expressed proteins were identified and consecutively analyzed by bioinformatic methods. Most differences between hyperoxia and normoxia (21 proteins up-regulated, 17 proteins down-regulated) were found immediately after hyperoxia (15 protein spots), followed by day 3 (13 spots), and day 7 (10 spots). A highly significant association with inflammation and the inflammatory response was found. Cell proliferation, oxidative stress, apoptosis and cell death as well as cellular functions were revealed to be affected. Three hours of hyperoxia resulted in significant alterations of protein expression in different organs (brain, lung, kidney) up to seven days after exposure. Further studies are required to interpret the relevance of protein alterations in signaling cascades during/after hyperoxia.

摘要

氧疗是医学中最常见的干预措施之一。之前的研究表明,差异调节蛋白可能与不同组织中与高氧相关的信号级联有关。然而,高氧激活的信号通路仍不清楚。本研究采用蛋白质组学和生物信息学方法分析了肺、脑和肾组织中高氧诱导的蛋白变化。使用了暴露于高氧的 36 只 Wistar 大鼠的汇总数据。为了鉴定可能的高氧生物标志物,并评估高氧影响器官和血液中蛋白变化之间的关系,对脑、肺和肾的蛋白质组学数据进行了分析。功能网络分析(IPA、PathwaysStudio 和 GENEmania)与层次聚类分析(Perseus)相结合,用于鉴定相关途径和关键蛋白。收集了 54 张 2D 凝胶的数据,每张凝胶的差异调节点超过 2500 个。鉴定了 38 个差异表达蛋白,并通过生物信息学方法对其进行了连续分析。高氧和常氧之间的大多数差异(21 个上调蛋白,17 个下调蛋白)在高氧后立即出现(15 个蛋白点),其次是第 3 天(13 个点)和第 7 天(10 个点)。与炎症和炎症反应有高度显著的相关性。细胞增殖、氧化应激、细胞凋亡和细胞死亡以及细胞功能均受到影响。高氧 3 小时导致暴露后 7 天内不同器官(脑、肺、肾)的蛋白表达发生显著变化。需要进一步研究来解释高氧期间/之后信号级联中蛋白变化的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f08a/6073502/ecfe0b9a3b92/ijms-19-01960-g001.jpg

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