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慢性缺血时亚硝酸盐治疗的基因表达谱分析和网络分析:可能的机制和有趣的分子。

Genome expression profiling and network analysis of nitrite therapy during chronic ischemia: possible mechanisms and interesting molecules.

机构信息

Department of Pathology, LSU Health Sciences Center-Shreveport, Shreveport, LA 71130, USA.

出版信息

Nitric Oxide. 2010 Feb 15;22(2):168-79. doi: 10.1016/j.niox.2009.11.008. Epub 2009 Dec 4.

Abstract

Sodium nitrite is widely recognized to be a highly effective NO donor for the treatment of several ischemic tissue disorders. However, mechanisms by which nitrite confers cytoprotection during ischemic disorders remain largely unknown. In this study, we used genome expression profiling approaches to evaluate changes in gene expression in the hind-limb ischemia model using vehicle or sodium nitrite therapy. Sodium nitrite significantly restored ischemic tissue perfusion by day 3 post-ligation which returned to normal by day 7. Genesifter analysis of Affymetrix GeneChip data revealed a significant down-regulation of gene expression profiles at day 3, whereas gene expression profiles were predominantly up-regulated at day 7. Ingenuity network analysis of gene expression profiles at day 3 showed a strong decrease in gene expression from networks associated with immune functions such as acute inflammatory responses, antigen presentation, and humoral immune responses while networks containing increased gene expression profiles were associated with cardiovascular, skeletal, and muscle system development and function. Network analysis of day 7 gene array data revealed predominant up-regulation of genes associated with cell survival, tissue morphology, connective tissue function, skeletal and muscular system development, and lymphoid tissue structure and development. These data suggest that sodium nitrite elicits potent anti-inflammatory and pro-angiogenic gene responses at early time points which is later followed by up-regulation of genes associated with tissue repair and homeostasis.

摘要

亚硝酸钠被广泛认为是一种治疗多种缺血性组织疾病的高效一氧化氮供体。然而,亚硝酸钠在缺血性疾病中发挥细胞保护作用的机制在很大程度上尚不清楚。在这项研究中,我们使用基因表达谱分析方法评估了在使用载体或亚硝酸钠治疗的后肢缺血模型中的基因表达变化。亚硝酸钠在结扎后第 3 天显著恢复了缺血组织的灌注,到第 7 天恢复正常。Affymetrix GeneChip 数据的 Genesifter 分析显示,第 3 天的基因表达谱显著下调,而第 7 天的基因表达谱主要上调。第 3 天基因表达谱的 Ingenuity 网络分析显示,与急性炎症反应、抗原呈递和体液免疫反应等免疫功能相关的网络中的基因表达明显减少,而包含上调基因表达谱的网络则与心血管、骨骼和肌肉系统发育和功能相关。第 7 天基因芯片数据的网络分析显示,与细胞存活、组织形态、结缔组织功能、骨骼和肌肉系统发育以及淋巴组织结构和发育相关的基因上调为主。这些数据表明,亚硝酸钠在早期引发强烈的抗炎和促血管生成基因反应,随后是与组织修复和内稳态相关的基因上调。

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