Smad3在坏死性小肠结肠炎狭窄中的表达及其可能的作用。

IF 0.8 4区医学 Q4 PEDIATRICS World Journal of Pediatric Surgery Pub Date : 2022-01-01 DOI:10.1136/wjps-2021-000289

Rui Chen, Chengjie Lv, Xiaoxia Zhao, Dong Ma, Dengming Lai, Yun Zhao, Luyin Zhang, Jinfa Tou

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Quantitative PCR, western blotting, and ELISA were used to detect the changes in transforming growth factor-β1 (TGF-β1), NF-κB, tumor necrosis factor-α (TNF-α), vascular endothelial growth factor (VEGF), and zonula occludens-1 (ZO-1) messenger RNA (mRNA) and protein expressions in IEC-6 cells. CCK8 kit and Transwell cellular migration were used to detect cell proliferation and migration. Changes in epithelial-mesenchymal transition (EMT) markers (E-cadherin and vimentin) in IEC-6 cells were detected by immunofluorescence technique.Results: The results showed that Smad3 protein and NF-κB protein were overexpressed in narrow intestinal tissues and that Smad3 protein expression was positively correlated with NF-κB protein expression. After inhibiting the expression of Smad3 in IEC-6 cells, the mRNA expressions of NF-κB, TGF-β1, ZO-1, and VEGF decreased, whereas the mRNA expression of TNF-α did not significantly change. 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摘要

目的:探讨坏死性小肠结肠炎狭窄组织中Smad3蛋白的表达及其可能的作用机制。方法:采用免疫组化方法检测Smad3和核因子κB (NF-κB)蛋白在人坏死性小肠结肠炎狭窄组织中的表达特征。体外培养大鼠小肠隐窝上皮细胞IEC-6，利用siRNA技术抑制Smad3的表达。采用定量PCR、western blotting、ELISA检测IEC-6细胞中转化生长因子-β1 (TGF-β1)、NF-κB、肿瘤坏死因子-α (TNF-α)、血管内皮生长因子(VEGF)、闭塞带-1 (ZO-1)信使RNA (mRNA)及蛋白表达的变化。CCK8试剂盒和Transwell细胞迁移检测细胞增殖和迁移。免疫荧光法检测IEC-6细胞上皮间质转化(epithelial-mesenchymal transition, EMT)标志物E-cadherin和vimentin的变化。结果:结果显示Smad3蛋白和NF-κB蛋白在狭窄肠组织中过表达，且Smad3蛋白表达与NF-κB蛋白表达呈正相关。抑制Smad3在IEC-6细胞中的表达后，NF-κB、TGF-β1、ZO-1、VEGF mRNA表达量下降，TNF-α mRNA表达量无明显变化。TGF-β1、NF-κB、TNF-α蛋白在IEC-6细胞中的表达降低，ZO-1、细胞内VEGF蛋白表达升高。IEC-6细胞增殖和迁移能力下降。EMT标志物E-cadherin和vimentin蛋白表达水平及细胞外VEGF蛋白表达无显著变化。结论:我们推测Smad3蛋白在坏死性小肠结肠炎狭窄中的高表达可能促进继发性肠狭窄的发生和发展。其机制可能与调节TGF-β1、NF-κB、TNF-α、ZO-1、VEGF mRNA及蛋白表达有关。这也可能与Smad3促进上皮细胞增殖和迁移的能力有关。

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Expression and possible role of Smad3 in postnecrotizing enterocolitis stricture.

Objective: To investigate the expression of Smad3 (mothers against decapentaplegic homolog 3) protein in postnecrotizing enterocolitis stricture and its possible mechanism of action.

Methods: We used immunohistochemistry to detect the expression characteristics of Smad3 and nuclear factor kappa B (NF-κB) proteins in human postnecrotizing enterocolitis stricture. We cultured IEC-6 (crypt epithelial cells of rat small intestine) in vitro and inhibited the expression of Smad3 using siRNA technique. Quantitative PCR, western blotting, and ELISA were used to detect the changes in transforming growth factor-β1 (TGF-β1), NF-κB, tumor necrosis factor-α (TNF-α), vascular endothelial growth factor (VEGF), and zonula occludens-1 (ZO-1) messenger RNA (mRNA) and protein expressions in IEC-6 cells. CCK8 kit and Transwell cellular migration were used to detect cell proliferation and migration. Changes in epithelial-mesenchymal transition (EMT) markers (E-cadherin and vimentin) in IEC-6 cells were detected by immunofluorescence technique.

Results: The results showed that Smad3 protein and NF-κB protein were overexpressed in narrow intestinal tissues and that Smad3 protein expression was positively correlated with NF-κB protein expression. After inhibiting the expression of Smad3 in IEC-6 cells, the mRNA expressions of NF-κB, TGF-β1, ZO-1, and VEGF decreased, whereas the mRNA expression of TNF-α did not significantly change. TGF-β1, NF-κB, and TNF-α protein expressions in IEC-6 cells decreased, whereas ZO-1 and intracellular VEGF protein expressions increased. IEC-6 cell proliferation and migration capacity decreased. There was no significant change in protein expression levels of EMT markers E-cadherin and vimentin and also extracellular VEGF protein expression.

Conclusions: We suspect that the high expression of Smad3 protein in postnecrotizing enterocolitis stricture may promote the occurrence and development of secondary intestinal stenosis. The mechanism may be related to the regulation of TGF-β1, NF-κB, TNF-α, ZO-1, and VEGF mRNA and protein expression. This may also be related to the ability of Smad3 to promote epithelial cell proliferation and migration.

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