Pediatric Autoimmune or Primary Sclerosing Cholangitis: Metronidazole Effectiveness on Biochemical Data, Bile Acid Profile, and Gut Microbiota: A Pilot Study.

Manon Karemera, Marko Verce, Martin Roumain, Giulio G Muccioli, Patrice D Cani, Amandine Everard, Xavier Stephenne, Etienne Sokal
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Abstract

Objectives: Autoimmune hepatitis and primary sclerosing cholangitis (PSC) can both be present, resulting in autoimmune sclerosing cholangitis (ASC). PSC physiopathology could be based on the cross-talk between gut microbiota and bile acids (BAs); antibiotics are an innovative therapy. This pilot study assesses metronidazole (MTZ)'s effectiveness in ASC or PSC patients according to the stage of the disease, and its effects on biochemical parameters, BA profiles, and gut microbiota.

Methods: ASC or PSC patients from Cliniques universitaires Saint-Luc's pediatric hepato-gastroenterology division were enrolled retrospectively and prospectively; both datasets were merged. MTZ was administered over at least 14 days on top of standard treatment (ursodeoxycholic acid, azathioprine, and steroids). Fecal and blood samples were collected before (T0) and at MTZ day 14 (T14). Sustained biochemical remission was defined by the reduction of transaminases (AST and ALT), gamma-glutamyl transferase (GGT), and CRP until 12 months post-MTZ.

Results: A total of 18 patients (mean age, 13.2 ± 4.5 years) were enrolled (13 ASC and 5 PSC), and divided in remission or relapse patients. CRP, AST, ALT, and GGT levels decreased post-MTZ in both groups (excepting GGT in relapse patients), with decreases between T0 and T14 being significant for AST and ALT. Relapse patients were older (P = 0.0351) and in late-disease stage, with mainly large-duct PSC (P = 0.0466). In remission patients, the mean plasma relative abundance of hydrophilic BA increased by +6.3% (P = 0.0391) after MTZ. Neither at baseline nor T14, there were significant differences in gut microbiota recorded.

Conclusion: These data are likely indicative of long-term benefits following MTZ therapy at early-stage ASC or PSC, with increased hydrophilic BA abundance. Multicenter prospective studies are needed.

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儿童自身免疫性或原发性硬化性胆管炎:甲硝唑对生化数据、胆汁酸谱和肠道微生物群的有效性:一项初步研究。
目的:自身免疫性肝炎和原发性硬化性胆管炎(PSC)均可存在,导致自身免疫性硬化性胆管炎(ASC)。PSC的生理病理可基于肠道菌群与胆汁酸(BAs)之间的相互作用;抗生素是一种创新疗法。这项初步研究评估了甲硝唑(MTZ)在ASC或PSC患者中的有效性,根据疾病的阶段,以及它对生化参数、BA谱和肠道微生物群的影响。方法:从倩碧ASC或PSC患者大学医疗Saint-Luc儿科hepato-gastroenterology部门为回顾性和前瞻性;两个数据集被合并。在标准治疗(熊去氧胆酸、硫唑嘌呤和类固醇)的基础上,给予MTZ至少14天。在T0和MTZ第14天分别采集粪便和血液样本。持续的生化缓解是通过转氨酶(AST和ALT)、γ -谷氨酰转移酶(GGT)和CRP的减少来定义的,直到mtz后12个月。结果:共纳入18例患者(平均年龄13.2±4.5岁)(ASC 13例,PSC 5例),分为缓解组和复发组。两组患者mtz后CRP、AST、ALT、GGT水平均下降(复发患者GGT除外),T0 ~ T14间AST、ALT水平下降较为显著。复发患者年龄较大(P = 0.0351),病程较晚,以大导管PSC为主(P = 0.0466)。在缓解患者中,MTZ后平均血浆亲水性BA相对丰度增加了+6.3% (P = 0.0391)。在基线和T14时,记录的肠道微生物群都没有显着差异。结论:这些数据可能表明MTZ治疗早期ASC或PSC的长期获益,亲水性BA丰度增加。需要多中心前瞻性研究。
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