细菌诱导的炎症性肠病差异易感小鼠模型中盲肠基因表达的特征分析

Characterization of cecal gene expression in a differentially susceptible mouse model of bacterial-induced inflammatory bowel disease.

作者信息

Myles Matthew H, Dieckgraefe Brian K, Criley Jennifer M, Franklin Craig L

机构信息

Research Animal Diagnostic Laboratory, Department of Veterinary Pathobiology, University of Missouri, Columbia, Missouri 65211, USA.

出版信息

Inflamm Bowel Dis. 2007 Jul;13(7):822-36. doi: 10.1002/ibd.20138.

DOI:10.1002/ibd.20138

PMID:17455200

Abstract

BACKGROUND

A/JCr mice develop typhlitis in response to Helicobacter hepaticus infection, whereas C57BL/6 mice coexist with this bacterium in a "commensal" relationship and do not develop disease even during prolonged colonization.

METHODS

To determine mechanisms that control this balance between responsiveness and nonresponsiveness, the mucosal response of A/JCr and C57BL/6 mice to acute H. hepaticus colonization was evaluated using genome-wide profiling. Transcription levels for a subset of gene discoveries were then evaluated longitudinally by semiquantitative real-time reverse-transcriptase polymerase chain reaction (RT-PCR) to identify changes in gene expression that occur during progression from the acute to chronic phase of colonization. To determine whether chronic mucosal inflammation in A/JCr mice was mediated through a Th1 mechanism, as was inferred from the gene expression data, mice with typhlitis were treated with neutralizing antibody targeting IL-12/23p40 or IFN-gamma and the response to treatment was determined by cecal lesion severity and transcription of disease-related genes.

RESULTS

A/JCr mice had a biphasic expression of proinflammatory genes that corresponded with the acute and chronic phases of disease. In contrast, C57BL/6 mice exhibited a less robust acute transcriptional response that waned by day 30 postinoculation. Sustained upregulation of proinflammatory signals and responsiveness to anti-IL-12/23p40 and anti-IFN-gamma antibody suggests that inflammation in A/JCr mice was mediated through a Th1 mechanism. Prolonged upregulation of SOCS3 during the acute response to colonization suggests that C57BL/6 mice maintain mucosal homeostasis, at least in part by attenuating responsiveness to cytokine signaling.

CONCLUSIONS

Collectively, these findings provide a foundation for understanding the immunological mechanisms that confer resistance or susceptibility to H. hepaticus-induced typhlitis.

摘要

背景

A/JCr小鼠在感染肝螺杆菌后会发生盲肠炎，而C57BL/6小鼠与这种细菌以“共生”关系共存，即使在长期定植期间也不会发病。

方法

为了确定控制这种反应性与无反应性之间平衡的机制，使用全基因组分析评估了A/JCr和C57BL/6小鼠对急性肝螺杆菌定植的黏膜反应。然后通过半定量实时逆转录聚合酶链反应（RT-PCR）纵向评估一部分基因发现的转录水平，以确定在从定植急性期到慢性期的进展过程中发生的基因表达变化。为了确定A/JCr小鼠的慢性黏膜炎症是否如基因表达数据所推断的那样通过Th1机制介导，对患有盲肠炎的小鼠用靶向IL-12/23p40或IFN-γ的中和抗体进行治疗，并通过盲肠病变严重程度和疾病相关基因的转录来确定治疗反应。

结果

A/JCr小鼠促炎基因有双相表达，与疾病的急性和慢性阶段相对应。相比之下，C57BL/6小鼠表现出较弱的急性转录反应，在接种后第30天减弱。促炎信号的持续上调以及对抗IL-12/23p40和抗IFN-γ抗体的反应表明，A/JCr小鼠的炎症是通过Th1机制介导的。在对定植的急性反应期间SOCS3的长期上调表明，C57BL/6小鼠至少部分通过减弱对细胞因子信号传导的反应来维持黏膜稳态。