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结核分枝杆菌哺乳动物细胞入侵(Mce)1 复合物对鼠巨噬细胞转录和炎症反应的调节。

Modulation of transcriptional and inflammatory responses in murine macrophages by the Mycobacterium tuberculosis mammalian cell entry (Mce) 1 complex.

机构信息

Section of Microbiology and Immunology, the Gade Institute, University of Bergen, Bergen, Norway.

出版信息

PLoS One. 2011;6(10):e26295. doi: 10.1371/journal.pone.0026295. Epub 2011 Oct 24.

Abstract

The outcome of many infections depends on the initial interactions between agent and host. Aiming at elucidating the effect of the M. tuberculosis Mce1 protein complex on host transcriptional and immunological responses to infection with M. tuberculosis, RNA from murine macrophages at 15, 30, 60 min, 4 and 10 hrs post-infection with M. tuberculosis H37Rv or Δ-mce1 H37Rv was analyzed by whole-genome microarrays and RT-QPCR. Immunological responses were measured using a 23-plex cytokine assay. Compared to uninfected controls, 524 versus 64 genes were up-regulated by 15 min post H37Rv- and Δ-mce1 H37Rv-infection, respectively. By 15 min post-H37Rv infection, a decline of 17 cytokines combined with up-regulation of Ccl24 (26.5-fold), Clec4a2 (23.2-fold) and Pparγ (10.5-fold) indicated an anti-inflammatory response initiated by IL-13. Down-regulation of Il13ra1 combined with up-regulation of Il12b (30.2-fold), suggested switch to a pro-inflammatory response by 4 hrs post H37Rv-infection. Whereas no significant change in cytokine concentration or transcription was observed during the first hour post Δ-mce1 H37Rv-infection, a significant decline of IL-1b, IL-9, IL-13, Eotaxin and GM-CSF combined with increased transcription of Il12b (25.1-fold) and Inb1 (17.9-fold) by 4 hrs, indicated a pro-inflammatory response. The balance between pro-and anti-inflammatory responses during the early stages of infection may have significant bearing on outcome.

摘要

许多感染的结果取决于病原体和宿主之间的初始相互作用。为了阐明结核分枝杆菌 Mce1 蛋白复合物对宿主感染结核分枝杆菌后转录和免疫反应的影响,用全基因组微阵列和 RT-QPCR 分析了感染结核分枝杆菌 H37Rv 或Δ-mce1 H37Rv 后 15、30、60 分钟、4 和 10 小时的鼠巨噬细胞的 RNA。用 23 重细胞因子检测试剂盒测定免疫反应。与未感染对照相比,H37Rv 和Δ-mce1 H37Rv 感染后 15 分钟分别有 524 个和 64 个基因上调。H37Rv 感染后 15 分钟,17 种细胞因子的浓度下降,同时 Ccl24(26.5 倍)、Clec4a2(23.2 倍)和 Pparγ(10.5 倍)上调,表明 IL-13 启动了抗炎反应。Il13ra1 下调,同时 Il12b 上调(30.2 倍),表明 4 小时后感染 H37Rv 后转为促炎反应。而在感染Δ-mce1 H37Rv 后第一小时内,细胞因子浓度或转录没有明显变化,但在 4 小时时,IL-1b、IL-9、IL-13、Eotaxin 和 GM-CSF 的浓度下降,同时 Il12b(25.1 倍)和 Inb1(17.9 倍)转录上调,表明存在促炎反应。感染早期促炎和抗炎反应之间的平衡可能对结果有重大影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f57/3200323/fe908cf2914e/pone.0026295.g001.jpg

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