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Bile Acid Diarrhea: Prevalence Pathogenesis and Therapy

机译:胆汁酸腹泻:流行发病机理和治疗。

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摘要

Bile acid diarrhea (BAD) is usually seen in patients with ileal Crohn’s disease or ileal resection. However, 25% to 50% of patients with functional diarrhea or diarrhea-predominant irritable bowel syndrome (IBS-D) also have evidence of BAD. It is estimated that 1% of the population may have BAD. The causes of BAD include a deficiency in fibroblast growth factor 19 (FGF-19), a hormone produced in enterocytes that regulates hepatic bile acid (BA) synthesis. Other potential causes include genetic variations that affect the proteins involved in BA enterohepatic circulation and synthesis or in the TGR5 receptor that mediates the actions of BA in colonic secretion and motility. BAs enhance mucosal permeability, induce water and electrolyte secretion, and accelerate colonic transit partly by stimulating propulsive high-amplitude colonic contractions. There is an increased proportion of primary BAs in the stool of patients with IBS-D, and some changes in the fecal microbiome have been described. There are several methods of diagnosing BAD, such as 75selenium homotaurocholic acid test retention, serum C4, FGF-19, and fecal BA measurement; presently, therapeutic trials with BA sequestrants are most commonly used for diagnosis. Management involves the use of BA sequestrants including cholestyramine, colestipol, and colesevelam. FXR agonists such as obeticholic acid constitute a promising new approach to treating BAD.
机译:回肠克罗恩病或回肠切除术的患者通常会出现胆汁酸腹泻(BAD)。但是,功能性腹泻或以腹泻为主的肠易激综合征(IBS-D)的患者中,有25%至50%也有BAD的证据。据估计,人口的1%可能患有BAD。 BAD的原因包括成纤维细胞生长因子19(FGF-19)的缺乏,成纤维细胞生长因子19是在肠细胞中产生的一种激素,可调节肝胆汁酸(BA)的合成。其他潜在原因包括影响BA肝肠循环和合成或TGR5受体的蛋白质的遗传变异,这些蛋白质介导BA在结肠分泌和运动中的作用。 BAs通过刺激推进性高振幅结肠收缩来提高粘膜通透性,诱导水和电解质分泌并部分加速结肠转运。 IBS-D患者粪便中原发性BA的比例增加,并且已描述了粪便微生物组的一些变化。诊断BAD的方法有几种,例如 75 硒高牛磺胆酸测试保留率,血清C4,FGF-19和粪便BA测量。目前,BA多价螯合剂的治疗试验最常用于诊断。管理涉及BA螯合剂的使用,包括胆甾醇胺,考来替泊和colesevelam。 FXR激动剂(如奥贝胆酸)构成了治疗BAD的有前途的新方法。

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