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全球上皮细胞转录反应揭示化脓性链球菌Fas调节因子活性与细菌侵袭性的关联。

Global epithelial cell transcriptional responses reveal Streptococcus pyogenes Fas regulator activity association with bacterial aggressiveness.

作者信息

Klenk Michael, Koczan Dirk, Guthke Reinhard, Nakata Masanobu, Thiesen Hans-Jürgen, Podbielski Andreas, Kreikemeyer Bernd

机构信息

Institute of Medical Microbiology, Virology and Hygiene, Rostock, Germany.

出版信息

Cell Microbiol. 2005 Sep;7(9):1237-50. doi: 10.1111/j.1462-5822.2005.00548.x.

DOI:10.1111/j.1462-5822.2005.00548.x
PMID:16098212
Abstract

The bacterial human pathogen Streptococcus pyogenes (group A streptococci, GAS) is able to adhere to, internalize into and cross-talk on multiple levels with its host cells. To gain insight into the Fas function in pathogenesis we used Affymetrix human genome DNA-arrays to measure temporal and global transcriptional responses of HEp-2 cells infected with M49 S. pyogenes wild-type bacteria and DeltafasX, an isogenic S. pyogenes two-component-signal-transduction system mutant. A modified stringent statistical analysis method identified a total of 86 HEp-2 cell genes as differentially transcribed upon infection over the investigated time course. Increased expression of genes encoding proteins involved in GAS host cell adherence and internalization (fibronectin, integrin-alpha5) was found as a common response. In contrast to earlier reports investigating other GAS serotype strains, Ras superfamily and RhoA pathways are exploited by M49 GAS, suggesting serotype specific interactions with the host cell cytoskeleton. Despite transcriptional induction, secreted IL-8 levels of deltafasX mutant infected cells were below those of non-infected cells, indicating an absence of Fas expression could be important for GAS tissue colonization and long-term intracellular persistence. Oppositely, activity of the S. pyogenes Fas-system apparently promotes high adherence and internalization rates, massive cytokine gene transcription and cytokine release, host cell apoptosis via a caspase-2 activation pathway, and cytotoxicity. Thus, the S. pyogenes Fas two-component signal transduction system could be involved in local tissue destruction and general bacterial aggressiveness towards host cells.

摘要

人类病原菌化脓性链球菌(A组链球菌,GAS)能够与宿主细胞在多个层面上发生黏附、内化并相互作用。为深入了解Fas在发病机制中的作用,我们使用Affymetrix人类基因组DNA芯片来检测感染M49化脓性链球菌野生型细菌和同源的化脓性链球菌双组分信号转导系统突变体DeltafasX的HEp-2细胞的时间和全局转录反应。一种改进的严格统计分析方法在研究的时间进程中确定了总共86个HEp-2细胞基因在感染后发生差异转录。发现编码参与GAS宿主细胞黏附和内化的蛋白质(纤连蛋白、整合素α5)的基因表达增加是一种常见反应。与早期研究其他GAS血清型菌株的报道相反,M49 GAS利用Ras超家族和RhoA途径,表明与宿主细胞细胞骨架存在血清型特异性相互作用。尽管有转录诱导,但感染deltafasX突变体细胞的分泌型IL-8水平低于未感染细胞,这表明缺乏Fas表达可能对GAS组织定植和长期细胞内持续存在很重要。相反,化脓性链球菌Fas系统的活性显然促进了高黏附率和内化率、大量细胞因子基因转录和细胞因子释放、通过半胱天冬酶-2激活途径导致的宿主细胞凋亡以及细胞毒性。因此,化脓性链球菌Fas双组分信号转导系统可能参与局部组织破坏和细菌对宿主细胞的总体侵袭性。

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