1. 通过抑制 IPEC-J2 细胞中的 MLCK 信号通路增强肠上皮屏障功能并减轻肠毒素诱导的炎症反应。

1 Enhances Intestinal Epithelial Barrier Function and Alleviates the Inflammatory Response Induced by Enterotoxigenic Suppressing the MLCK Signaling Pathway in IPEC-J2 Cells.

机构信息

State Key Laboratory of Livestock and Poultry Breeding, Ministry of Agriculture Key Laboratory of Animal Nutrition and Feed Science in South China, Guangdong Key Laboratory of Animal Breeding and Nutrition, Maoming Branch, Guangdong Laboratory for Lingnan Modern Agriculture, Institute of Animal Science, Guangdong Academy of Agricultural Sciences, Guangzhou, China.

College of Animal Sciences and Technology, Zhongkai University of Agriculture and Engineering, Guangzhou, China.

出版信息

Front Immunol. 2022 Jul 14;13:897395. doi: 10.3389/fimmu.2022.897395. eCollection 2022.

DOI:10.3389/fimmu.2022.897395

PMID:35911699

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9331657/

Abstract

Intestinal epithelial barrier injury disrupts immune homeostasis and leads to many intestinal disorders. () strains can influence immune system development and intestinal function. However, the underlying mechanisms of LR1 that regulate inflammatory response and intestinal integrity are still unknown. The present study aimed to determine the effects of LR1 on the ETEC K88-induced intestinal epithelial injury on the inflammatory response, intestinal epithelial barrier function, and the MLCK signal pathway and its underlying mechanism. Here, we showed that the 1 × 10 cfu/ml LR1 treatment for 4 h dramatically decreased interleukin-8 (IL-8) and IL-6 expression. Then, the data indicated that the 1 × 10 cfu/ml ETEC K88 treatment for 4 h dramatically enhanced IL-8, IL-6, and tumor necrosis factor-α (TNF-α) expression. Furthermore, scanning electron microscope (SEM) data indicated that pretreatment with LR1 inhibited the ETEC K88 that adhered on IPEC-J2 and alleviated the scratch injury of IPEC J2 cells. Moreover, LR1 pretreatment significantly reversed the declined transepithelial electrical resistance (TER) and tight junction protein level, and enhanced the induction by ETEC K88 treatment. Additionally, LR1 pretreatment dramatically declined IL-8, IL-17A, IL-6, and TNF-α levels compared with the ETEC K88 group. Then, ETEC K88-treated IPEC-J2 cells had a higher level of myosin light-chain kinase (MLCK), higher MLC levels, and a lower Rho-associated kinase (ROCK) level than the control group, while LR1 pretreatment significantly declined the MLCK and MLC expression and enhanced ROCK level in the ETEC K88-challenged IPEC-J2 cells. Mechanistically, depletion of MLCK significantly declined MLC expression in IPEC-J2 challenged with compared to the si NC+ETEC K88 group. On the other hand, the TER of the si MLCK+ETEC K88 group was higher and the FD4 flux in the si MLCK+ETEC K88 group was lower compared with the si NC+ETEC K88 group. In addition, depletion of MLCK significantly enhanced Claudin-1 level and declined IL-8 and TNF-α levels in IPEC-J2 pretreated with LR1 followed by challenging with ETEC K88. In conclusion, our work indicated that LR1 can decline inflammatory response and improve intestinal epithelial barrier function through suppressing the MLCK signal pathway in the ETEC K88-challenged IPEC-J2.

摘要

肠上皮屏障损伤破坏免疫稳态，导致许多肠道疾病。（）菌株可以影响免疫系统的发育和肠道功能。然而，LR1 调节炎症反应和肠道完整性的潜在机制尚不清楚。本研究旨在确定 LR1 对 ETEC K88 诱导的肠上皮损伤对炎症反应、肠上皮屏障功能和 MLCK 信号通路及其潜在机制的影响。在这里，我们表明，1×10cfu/ml LR1 处理 4 小时可显著降低白细胞介素-8（IL-8）和白细胞介素-6（IL-6）的表达。然后，数据表明，1×10cfu/ml ETEC K88 处理 4 小时可显著增强 IL-8、IL-6 和肿瘤坏死因子-α（TNF-α）的表达。此外，扫描电子显微镜（SEM）数据表明，LR1 预处理可抑制 ETEC K88 黏附在 IPEC-J2 上，并减轻 IPEC J2 细胞的划痕损伤。此外，LR1 预处理可显著逆转 ETEC K88 处理后跨上皮电阻（TER）和紧密连接蛋白水平的下降，并增强 ETEC K88 处理的诱导作用。此外，LR1 预处理可显著降低 ETEC K88 组的白细胞介素-8（IL-8）、白细胞介素-17A（IL-17A）、白细胞介素-6（IL-6）和肿瘤坏死因子-α（TNF-α）水平。然后，与对照组相比，ETEC K88 处理的 IPEC-J2 细胞中肌球蛋白轻链激酶（MLCK）水平更高，MLC 水平更高，Rho 相关激酶（ROCK）水平更低，而 LR1 预处理可显著降低 ETEC K88 处理的 IPEC-J2 细胞中 MLCK 和 MLC 的表达，并增强 ROCK 水平。在机制上，与 siNC+ETEC K88 组相比，MLCK 耗竭可显著降低 IPCE-J2 细胞中与相比的 MLC 表达。另一方面，与 siNC+ETEC K88 组相比，siMLCK+ETEC K88 组的 TER 更高，siMLCK+ETEC K88 组的 FD4 通量更低。此外，与 siNC+ETEC K88 组相比，siMLCK+LR1 预处理后再用 ETEC K88 处理可显著增强 IPEC-J2 中的 Claudin-1 水平，并降低 IL-8 和 TNF-α 水平。总之，我们的工作表明，LR1 可以通过抑制 ETEC K88 challenged IPEC-J2 中的 MLCK 信号通路来降低炎症反应和改善肠上皮屏障功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/573a/9331657/1dcfcbe30b75/fimmu-13-897395-g001.jpg

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1. 通过抑制 IPEC-J2 细胞中的 MLCK 信号通路增强肠上皮屏障功能并减轻肠毒素诱导的炎症反应。

1 Enhances Intestinal Epithelial Barrier Function and Alleviates the Inflammatory Response Induced by Enterotoxigenic Suppressing the MLCK Signaling Pathway in IPEC-J2 Cells.

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