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剧烈运动可改变 LPS 刺激和未刺激全血培养物中的不同基因表达谱和途径。

Exhaustive exercise modifies different gene expression profiles and pathways in LPS-stimulated and un-stimulated whole blood cultures.

机构信息

Division of Exercise Immunology & Genetics, Institute of Clinical and Experimental Transfusion Medicine (IKET), University Hospital Tuebingen, Tuebingen, Germany; Institute of Sports Science, Eberhard Karls University, Tuebingen, Germany.

Division of Exercise Immunology & Genetics, Institute of Clinical and Experimental Transfusion Medicine (IKET), University Hospital Tuebingen, Tuebingen, Germany.

出版信息

Brain Behav Immun. 2014 Jul;39:130-41. doi: 10.1016/j.bbi.2013.10.023. Epub 2013 Oct 26.

Abstract

Exhaustive exercise can interfere with immunity, causing transient immunosuppression and infections/inflammation in athletes. We used microarray technology to analyze the gene expression profiles of whole blood in short time (1h) LPS-stimulated and un-stimulated cultures drawn before, 30min after, 3h after and 24h after a half-marathon run. Four male and 4 female athletes participated. Exercise induced differential expression of genes known to be involved in innate immunity/inflammatory response, metabolic response, DNA methylation, apoptosis and regulation of brain function. Several genes with prominent anti-inflammatory function were up-regulated in un-stimulated cultures, including ARG-1, SOCS3, DUSP-1, ORMs, IRAK3, and GJB6. Some of these genes were also strongly up-regulated in LPS-stimulated cultures (ARG-1, ORM2, and GJB6). Some genes were strongly up-regulated through exercise in LPS-stimulated cultures, but not in un-stimulated cultures (TNIP3, PLAU, and HIVEP1). There was also a row of genes, which were strongly down-regulated by exercise in LPS-stimulated cultures, notably IFN-β1 and CXCL10. Exercise also significantly changed the expression of genes (OLIG2, TMEM106B) which are known to be related to brain function and expression of which has never been documented in peripheral blood. In summary, exhaustive exercise, in addition to modifying gene expression in un-stimulated cells, could also interfere with the early gene expression response to endotoxin. There was an anti-inflammatory bias of gene regulation by exercise, including genes involved in the negative regulation of TLRs signalling. The results of the present study demonstrate that some potentially important effects of exercise can only be detected in relation to pathogen stimulation.

摘要

剧烈运动可干扰免疫功能,导致运动员出现短暂的免疫抑制和感染/炎症。我们使用微阵列技术分析了短时间(1 小时)内的全血基因表达谱,这些血液样本取自马拉松比赛前、比赛后 30 分钟、3 小时和 24 小时,分别进行了 LPS 刺激和未刺激培养。共有 4 名男性和 4 名女性运动员参与了研究。运动诱导了已知参与固有免疫/炎症反应、代谢反应、DNA 甲基化、细胞凋亡和大脑功能调节的基因的差异表达。一些具有明显抗炎功能的基因在未刺激培养物中上调,包括 ARG-1、SOCS3、DUSP-1、ORMs、IRAK3 和 GJB6。其中一些基因在 LPS 刺激培养物中也被强烈上调(ARG-1、ORM2 和 GJB6)。一些基因在 LPS 刺激培养物中通过运动强烈上调,但在未刺激培养物中没有(TNIP3、PLAU 和 HIVEP1)。还有一系列基因在 LPS 刺激培养物中被运动强烈下调,特别是 IFN-β1 和 CXCL10。运动还显著改变了 LPS 刺激培养物中基因的表达(OLIG2、TMEM106B),这些基因已知与大脑功能有关,其在外周血中的表达从未有过记录。总之,剧烈运动除了修饰未刺激细胞中的基因表达外,还可能干扰内毒素的早期基因表达反应。运动对基因调控具有抗炎偏向性,包括参与 TLRs 信号转导负调控的基因。本研究的结果表明,一些潜在的重要运动效应只能在与病原体刺激相关时才能检测到。

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