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单一 IgG 型白细胞介素-1 相关受体控制分化的人肠道上皮细胞中的 TLR 反应。

The single IgG IL-1-related receptor controls TLR responses in differentiated human intestinal epithelial cells.

机构信息

Division of Pediatric Gastroenterology, BC Children's Hospital, Vancouver, British Columbia V6H 3V4,Canada.

出版信息

J Immunol. 2010 Mar 1;184(5):2305-13. doi: 10.4049/jimmunol.0900021. Epub 2010 Feb 3.

Abstract

Intestinal epithelial cells (IECs) are constantly exposed to enteric microbes. Although IECs express TLRs that recognize bacterial products, the activation of these TLRs is strictly controlled through poorly understood mechanisms, producing a state of hyporesponsiveness and preventing unwanted inflammation. The single IgG IL-1-related receptor (Sigirr) is a negative regulator of TLRs that is expressed by IECs and was recently shown to inhibit experimental colitis. However, the importance of Sigirr in IEC hyporesponsiveness and its distribution within the human colon is unknown. In this study, we investigated the role of Sigirr in regulating epithelial-specific TLR responses and characterized its expression in colonic biopsy specimens. Transformed and nontransformed human IECs were cultured as monolayers. Transient gene silencing and stable overexpression of Sigirr was performed to assess innate IEC responses. Sigirr expression in human colonic biopsy specimens was examined by immunohistochemistry. Bacterial infection of IECs and exposure to flagellin transiently decreased Sigirr protein expression, concurrent with secretion of the neutrophil chemokine IL-8. Sigirr gene silencing augmented chemokine responses to bacterial flagellin, Pam3Cys, and the cytokine IL-1beta. Conversely, stable overexpression of Sigirr diminished NF-kappaB-mediated IL-8 responses to TLR ligands. We also found that Sigirr expression increased as IECs differentiated in culture. This observation was confirmed in biopsy sections, in which Sigirr expression within colonic crypts was prominent in IECs at the apex and diminished at the base. Our findings show that Sigirr broadly regulates innate responses in differentiated human IECs; therefore, it may modulate epithelial involvement in infectious and inflammatory bowel diseases.

摘要

肠上皮细胞 (IECs) 不断暴露于肠道微生物中。尽管 IECs 表达可识别细菌产物的 TLR,但这些 TLR 的激活受到机制的严格控制,导致低反应状态并防止不必要的炎症。单一 IgG 白细胞介素-1 相关受体 (Sigirr) 是 IECs 表达的 TLR 的负调节剂,最近被证明可抑制实验性结肠炎。然而,Sigirr 在 IEC 低反应性中的重要性及其在人类结肠中的分布尚不清楚。在这项研究中,我们研究了 Sigirr 在调节上皮细胞特异性 TLR 反应中的作用,并对其在结肠活检标本中的表达进行了表征。转化和非转化的人 IEC 被培养为单层。通过瞬时基因沉默和 Sigirr 的稳定过表达来评估先天 IEC 反应。通过免疫组织化学检查人结肠活检标本中的 Sigirr 表达。IEC 感染和鞭毛蛋白的短暂暴露会降低 Sigirr 蛋白表达,同时还会分泌中性粒细胞趋化因子 IL-8。Sigirr 基因沉默增强了对细菌鞭毛蛋白、Pam3Cys 和细胞因子 IL-1beta 的趋化因子反应。相反,Sigirr 的稳定过表达减弱了 TLR 配体对 NF-kappaB 介导的 IL-8 反应。我们还发现 Sigirr 的表达随着 IEC 在培养中分化而增加。这一观察结果在活检切片中得到了证实,在切片中,Sigirr 在结肠隐窝内的表达在顶端的 IEC 中很明显,而在底部则减少。我们的发现表明 Sigirr 广泛调节分化的人 IEC 中的先天反应;因此,它可能调节上皮细胞在感染性和炎症性肠病中的参与。

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