熊去氧胆酸通过促进肠上皮细胞迁移来防止肠道屏障破坏,其机制与 EGFR 和 COX-2 有关。
Ursodeoxycholic acid protects against intestinal barrier breakdown by promoting enterocyte migration via EGFR- and COX-2-dependent mechanisms.
机构信息
Department of Pediatric Surgery, Children's Hospital Los Angeles , Los Angeles, California.
Department of Pediatrics and Biochemistry and Molecular Biology, Children's Hospital Los Angeles , Los Angeles, California.
出版信息
Am J Physiol Gastrointest Liver Physiol. 2018 Aug 1;315(2):G259-G271. doi: 10.1152/ajpgi.00354.2017. Epub 2018 Apr 19.
The intestinal barrier is often disrupted in disease states, and intestinal barrier failure leads to sepsis. Ursodeoxycholic acid (UDCA) is a bile acid that may protect the intestinal barrier. We hypothesized that UDCA would protect the intestinal epithelium in injury models. To test this hypothesis, we utilized an in vitro wound-healing assay and a mouse model of intestinal barrier injury. We found that UDCA stimulates intestinal epithelial cell migration in vitro, and this migration was blocked by inhibition of cyclooxygenase 2 (COX-2), epidermal growth factor receptor (EGFR), or ERK. Furthermore, UDCA stimulated both COX-2 induction and EGFR phosphorylation. In vivo UDCA protected the intestinal barrier from LPS-induced injury as measured by FITC dextran leakage into the serum. Using 5-bromo-2'-deoxyuridine and 5-ethynyl-2'-deoxyuridine injections, we found that UDCA stimulated intestinal epithelial cell migration in these animals. These effects were blocked with either administration of Rofecoxib, a COX-2 inhibitor, or in EGFR-dominant negative Velvet mice, wherein UDCA had no effect on LPS-induced injury. Finally, we found increased COX-2 and phosphorylated ERK levels in LPS animals also treated with UDCA. Taken together, these data suggest that UDCA can stimulate intestinal epithelial cell migration and protect against acute intestinal injury via an EGFR- and COX-2-dependent mechanism. UDCA may be an effective treatment to prevent the early onset of gut-origin sepsis. NEW & NOTEWORTHY In this study, we show that the secondary bile acid ursodeoxycholic acid stimulates intestinal epithelial cell migration after cellular injury and also protects the intestinal barrier in an acute rodent injury model, neither of which has been previously reported. These effects are dependent on epidermal growth factor receptor activation and downstream cyclooxygenase 2 upregulation in the small intestine. This provides a potential treatment for acute, gut-origin sepsis as seen in diseases such as necrotizing enterocolitis.
肠道屏障在疾病状态下经常被破坏,而肠道屏障衰竭会导致败血症。熊去氧胆酸(UDCA)是一种可能保护肠道屏障的胆酸。我们假设 UDCA 会在损伤模型中保护肠道上皮细胞。为了验证这一假设,我们利用体外伤口愈合测定法和肠道屏障损伤的小鼠模型进行了实验。我们发现 UDCA 刺激体外肠道上皮细胞迁移,这种迁移被环氧化酶 2(COX-2)、表皮生长因子受体(EGFR)或 ERK 的抑制所阻断。此外,UDCA 刺激 COX-2 诱导和 EGFR 磷酸化。体内实验中,UDCA 通过将 FITC 葡聚糖漏入血清中来保护肠道屏障免受 LPS 诱导的损伤。通过 5-溴-2'-脱氧尿苷和 5-乙炔基-2'-脱氧尿苷注射,我们发现 UDCA 刺激这些动物的肠道上皮细胞迁移。这些作用被 COX-2 抑制剂罗非考昔或 EGFR 显性负 Velvet 小鼠的给药所阻断,在这些动物中,UDCA 对 LPS 诱导的损伤没有影响。最后,我们发现 LPS 动物的 COX-2 和磷酸化 ERK 水平也增加,而 UDCA 处理后这些水平增加。总之,这些数据表明 UDCA 可以通过 EGFR 和 COX-2 依赖性机制刺激肠道上皮细胞迁移并防止急性肠道损伤。UDCA 可能是预防肠道来源性败血症早期发生的有效治疗方法。
新的和值得注意的是
在这项研究中,我们表明,次级胆汁酸熊去氧胆酸在细胞损伤后刺激肠道上皮细胞迁移,并且在急性啮齿动物损伤模型中也保护肠道屏障,这两者以前都没有报道过。这些作用依赖于小肠中表皮生长因子受体的激活和下游环氧化酶 2 的上调。这为急性、肠道来源的败血症提供了一种潜在的治疗方法,如坏死性小肠结肠炎等疾病中所见。
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