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肠道上皮细胞对霍乱弧菌感染的转录反应。

Transcriptional responses of intestinal epithelial cells to infection with Vibrio cholerae.

作者信息

Stokes Neil R, Zhou Xin, Meltzer Stephen J, Kaper James B

机构信息

Center for Vaccine Development, University of Maryland School of Medicine, 685 West Baltimore Street, Baltimore, MD 21201, USA.

出版信息

Infect Immun. 2004 Jul;72(7):4240-8. doi: 10.1128/IAI.72.7.4240-4248.2004.

Abstract

Vibrio cholerae is a noninvasive enteric bacterium that causes the severe diarrheal disease cholera. Candidate cholera vaccines have been engineered by deleting genes encoding known virulence factors in V. cholerae; however, many of these attenuated strains were still reactogenic in human volunteers. In this study, DNA arrays were utilized to monitor the transcriptional responses of human intestinal epithelial cells (T84) to eight strains of V. cholerae, including attenuated, toxigenic, and environmental isolates. cDNA probes generated from host RNA samples were hybridized against low- and high-density gene arrays. V. cholerae induced the transcription of a variety of host genes and repressed the expression of a lower number of genes. Expression patterns were confirmed for certain genes by reverse transcriptase PCR and enzyme-linked immunosorbent assays. A core subset of genes was found to be differentially regulated in all experiments. These genes included genes involved in innate mucosal immunity, intracellular signaling, and cellular proliferation. Reactogenic vaccine strains induced greater expression of genes for certain proinflammatory cytokines than nonreactogenic strains. Wild-type and attenuated derivatives induced and repressed many genes in common, although there were differences in the transcription profiles. These results indicate that the types of host genes modulated by attenuated V. cholerae, and the extent of their induction, may mediate the symptoms seen with reactogenic cholera vaccine strains.

摘要

霍乱弧菌是一种非侵袭性肠道细菌,可引发严重的腹泻疾病霍乱。候选霍乱疫苗是通过删除霍乱弧菌中编码已知毒力因子的基因构建而成的;然而,许多这些减毒株在人类志愿者中仍具有反应原性。在本研究中,利用DNA阵列监测人类肠道上皮细胞(T84)对八株霍乱弧菌的转录反应,这些霍乱弧菌包括减毒株、产毒株和环境分离株。从宿主RNA样本生成的cDNA探针与低密度和高密度基因阵列进行杂交。霍乱弧菌诱导了多种宿主基因的转录,并抑制了较少数量基因的表达。通过逆转录PCR和酶联免疫吸附测定法对某些基因的表达模式进行了确认。发现在所有实验中都有一组核心基因受到差异调节。这些基因包括参与先天性黏膜免疫、细胞内信号传导和细胞增殖的基因。有反应原性的疫苗株比无反应原性的菌株诱导某些促炎细胞因子基因的表达更高。野生型和减毒衍生物诱导和抑制了许多共同的基因,尽管转录谱存在差异。这些结果表明,减毒霍乱弧菌调节的宿主基因类型及其诱导程度可能介导了有反应原性的霍乱疫苗株所出现的症状。

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本文引用的文献

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Human macrophage activation programs induced by bacterial pathogens.由细菌病原体诱导的人类巨噬细胞激活程序。
Proc Natl Acad Sci U S A. 2002 Feb 5;99(3):1503-8. doi: 10.1073/pnas.022649799. Epub 2002 Jan 22.

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