全球Fxr缺乏对实验性急性胰腺炎的影响及人类急性胰腺炎中FXR基因座的遗传变异
Impact of global Fxr deficiency on experimental acute pancreatitis and genetic variation in the FXR locus in human acute pancreatitis.
作者信息
Nijmeijer Rian M, Schaap Frank G, Smits Alexander J J, Kremer Andreas E, Akkermans Louis M A, Kroese Alfons B A, Rijkers Ger T, Schipper Marguerite E I, Verheem André, Wijmenga Cisca, Gooszen Hein G, van Erpecum Karel J
机构信息
Department of Surgery, University Medical Center Utrecht, Utrecht, the Netherlands.
Tytgat Institute for Liver and Intestinal Research, Academic Medical Center, Amsterdam, the Netherlands; Department of General Surgery, Maastricht University, Maastricht, The Netherlands.
出版信息
PLoS One. 2014 Dec 3;9(12):e114393. doi: 10.1371/journal.pone.0114393. eCollection 2014.
BACKGROUND
Infectious complications often occur in acute pancreatitis, related to impaired intestinal barrier function, with prolonged disease course and even mortality as a result. The bile salt nuclear receptor farnesoid X receptor (FXR), which is expressed in the ileum, liver and other organs including the pancreas, exhibits anti-inflammatory effects by inhibiting NF-κB activation and is implicated in maintaining intestinal barrier integrity and preventing bacterial overgrowth and translocation. Here we explore, with the aid of complementary animal and human experiments, the potential role of FXR in acute pancreatitis.
METHODS
Experimental acute pancreatitis was induced using the CCK-analogue cerulein in wild-type and Fxr-/- mice. Severity of acute pancreatitis was assessed using histology and a semi-quantitative scoring system. Ileal permeability was analyzed in vitro by Ussing chambers and an in vivo permeability assay. Gene expression of Fxr and Fxr target genes was studied by quantitative RT-PCR. Serum FGF19 levels were determined by ELISA in acute pancreatitis patients and healthy volunteers. A genetic association study in 387 acute pancreatitis patients and 853 controls was performed using 9 tagging single nucleotide polymorphisms (SNPs) covering the complete FXR gene and two additional functional SNPs.
RESULTS
In wild-type mice with acute pancreatitis, ileal transepithelial resistance was reduced and ileal mRNA expression of Fxr target genes Fgf15, SHP, and IBABP was decreased. Nevertheless, Fxr-/- mice did not exhibit a more severe acute pancreatitis than wild-type mice. In patients with acute pancreatitis, FGF19 levels were lower than in controls. However, there were no associations of FXR SNPs or haplotypes with susceptibility to acute pancreatitis, or its course, outcome or etiology.
CONCLUSION
We found no evidence for a major role of FXR in acute human or murine pancreatitis. The observed altered Fxr activity during the course of disease may be a secondary phenomenon.
背景
感染性并发症在急性胰腺炎中经常发生,这与肠屏障功能受损有关,会导致病程延长甚至死亡。胆汁盐核受体法尼醇X受体(FXR)在回肠、肝脏以及包括胰腺在内的其他器官中表达,通过抑制NF-κB激活发挥抗炎作用,并参与维持肠屏障完整性以及防止细菌过度生长和移位。在此,我们借助互补的动物和人体实验,探究FXR在急性胰腺炎中的潜在作用。
方法
使用CCK类似物雨蛙肽在野生型和Fxr基因敲除小鼠中诱导实验性急性胰腺炎。采用组织学和半定量评分系统评估急性胰腺炎的严重程度。通过尤斯灌流小室体外分析回肠通透性,并进行体内通透性测定。采用定量RT-PCR研究Fxr及其靶基因的基因表达。通过酶联免疫吸附测定法(ELISA)测定急性胰腺炎患者和健康志愿者的血清FGF19水平。使用涵盖整个FXR基因的9个标签单核苷酸多态性(SNP)以及另外两个功能性SNP,对387例急性胰腺炎患者和853例对照进行基因关联研究。
结果
在患有急性胰腺炎的野生型小鼠中,回肠跨上皮电阻降低,Fxr靶基因Fgf15、SHP和IBABP的回肠mRNA表达下降。然而,Fxr基因敲除小鼠并未表现出比野生型小鼠更严重的急性胰腺炎。在急性胰腺炎患者中,FGF19水平低于对照组。但是,FXR SNP或单倍型与急性胰腺炎的易感性、病程、结局或病因均无关联。
结论
我们没有发现证据表明FXR在人类或小鼠急性胰腺炎中起主要作用。在疾病过程中观察到的Fxr活性改变可能是一种继发现象。
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