Institute of Clinical Chemistry and Laboratory Medicine, University Hospital Regensburg, Regensburg 93053, Germany.
Department of Internal Medicine I, Gastroenterology, Hepatology, Endocrinology, Rheumatology, and Infectious Diseases, University Hospital Regensburg, Regensburg 93053, Germany.
J Steroid Biochem Mol Biol. 2025 Jan;245:106621. doi: 10.1016/j.jsbmb.2024.106621. Epub 2024 Sep 16.
Inflammatory bowel disease (IBD) triggers chronic intestinal inflammation and is linked to primary sclerosing cholangitis (PSC). Cholesterol homeostasis, tightly regulated under normal conditions, becomes disrupted in both inflammation and chronic liver disease. We analyzed fecal and serum levels of cholesterol synthesis precursors, oxysterols, and phytosterols in 87 patients with IBD (81 for serum analysis) including patients with Crohn's disease (CD) and ulcerative colitis (UC), 11 patients with PSC, 21 patients with PSC-IBD (18 for serum analysis), and 16 healthy controls (17 for serum analysis). Cholesterol was analysed by flow injection analysis on a high-resolution hybrid quadrupole-Orbitrap mass spectrometer and further serum sterols and all fecal sterols were analysed by a gas chromatograph mass spectrometer. Serum levels of lanosterol, 7-dehydrocholesterol, 7-beta-hydroxycholesterol, 27-hydroxycholesterol, and the plant sterols campesterol, stigmasterol, and sitosterol were similar across control and patient groups. Notably, serum lathosterol was elevated in CD patients compared to those with UC, PSC, PSC-IBD, and healthy controls. All other serum and fecal sterols showed no differences between CD and UC. Cholesterol synthesis precursors in serum, serum cholesterol levels, and both serum and fecal plant sterol levels decreased with increasing IBD severity. Consequently, serum cholesterol, campesterol, sitosterol, and fecal 5-beta sitostanol and 5-alpha sitostanol were negatively correlated with C-reactive protein and fecal calprotectin. The conversion of cholesterol to coprostanol in feces was impaired in IBD, PSC, and PSC-IBD, independent of bowel inflammation severity or liver disease extent. Patients with PSC, and to a lesser extent PSC-IBD, had elevated serum plant sterol levels, positively correlating with liver disease markers. In conclusion, in patients with IBD, cholesterol biosynthetic precursors, serum cholesterol levels, and fecal plant sterols decrease with intestinal inflammation. An inverse association of serum plant sterols with intestinal inflammation was observed in patients with IBD and a direct association of serum phytosterols with liver injury in patients with PSC. The conversion of fecal cholesterol to coprostanol was impaired in all patient cohorts. IBD and PSC alter serum sterol levels differently, whereas changes in fecal sterols are not disease specific and are moderate.
炎症性肠病 (IBD) 引发慢性肠道炎症,并与原发性硬化性胆管炎 (PSC) 有关。胆固醇稳态在正常情况下受到严格调控,但在炎症和慢性肝病中都会被打破。我们分析了 87 名 IBD 患者(81 名进行血清分析)的粪便和血清胆固醇合成前体、氧化固醇和植物固醇水平,包括克罗恩病 (CD) 和溃疡性结肠炎 (UC) 患者、11 名 PSC 患者、21 名 PSC-IBD 患者(18 名进行血清分析)和 16 名健康对照者(17 名进行血清分析)。胆固醇通过高分辨率混合四极杆-轨道阱质谱仪的流动注射分析进行分析,进一步通过气相色谱质谱仪分析所有血清甾醇和所有粪便甾醇。在对照组和患者组中,血清羊毛甾醇、7-脱氢胆固醇、7-β-羟胆固醇、27-羟胆固醇以及植物甾醇菜油固醇、豆固醇和谷固醇的水平相似。值得注意的是,与 UC、PSC、PSC-IBD 和健康对照组相比,CD 患者的血清麦角固醇水平升高。所有其他血清和粪便甾醇在 CD 和 UC 之间没有差异。血清胆固醇合成前体、血清胆固醇水平以及血清和粪便植物甾醇水平均随 IBD 严重程度的增加而降低。因此,血清胆固醇、菜油固醇、谷固醇和粪便 5-β 谷甾烷醇和 5-α 谷甾烷醇与 C 反应蛋白和粪便钙卫蛋白呈负相关。粪便中胆固醇向粪甾烷醇的转化在 IBD、PSC 和 PSC-IBD 中受损,与肠道炎症严重程度或肝脏疾病范围无关。PSC 患者,尤其是 PSC-IBD 患者,血清植物甾醇水平升高,与肝脏疾病标志物呈正相关。总之,在 IBD 患者中,胆固醇生物合成前体、血清胆固醇水平和粪便植物甾醇随肠道炎症而减少。在 IBD 患者中观察到血清植物固醇与肠道炎症呈负相关,而在 PSC 患者中血清植物固醇与肝损伤呈正相关。所有患者组的粪便胆固醇向粪甾烷醇的转化都受损。IBD 和 PSC 以不同的方式改变血清甾醇水平,而粪便甾醇的变化则不是疾病特异性的,且变化程度适中。
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