短链脂肪酸和多发性硬化症的肠道炎症:微生物产物对女性敏感性的调节?

Q1 Medicine Auto-Immunity Highlights Pub Date : 2021-04-07 DOI:10.1186/s13317-021-00149-1
Anouck Becker, Mosab Abuazab, Andreas Schwiertz, Silke Walter, Klaus C Faßbender, Mathias Fousse, Marcus M Unger
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引用次数: 9

摘要

背景:多发性硬化症(MS)是一种自身免疫介导的中枢神经系统疾病。实验数据表明肠道菌群和微生物产物如短链脂肪酸(SCFAs)在MS发病机制中的作用。最近的一项临床研究报告了MS患者口服丙酸短链脂肪酸后的有益效果(由免疫调节机制介导)。基于现有证据,我们研究了多发性硬化症中SCFAs和粪便炎症标志物钙保护蛋白是否发生改变。方法:76名受试者(41名复发-缓解型多发性硬化症患者和35名年龄匹配的对照组)在本病例对照研究中进行了调查。所有受试者均按照既定临床量表进行临床评估,并提供粪便样本用于定量分析粪便SCFA和粪便钙保护蛋白浓度。将MS患者和对照组的粪便标志物进行比较,并分析其与人口学和临床参数的关联。结果:两组粪便钙保护蛋白中位浓度均在正常范围内,无组间差异。与健康受试者相比,MS患者的粪便SCFA浓度没有显著降低。与男性受试者相比,女性受试者的SCFA浓度显著降低。结论:在我们的MS患者队列中,我们没有发现活动性肠道炎症的证据。然而,绝大多数被调查的MS患者正在接受免疫治疗,这可能会影响结果测量。粪便中SCFA浓度的性别相关差异可能至少部分解释了MS中女性的优势,需要包括drug-naïve MS患者在内的大规模纵向研究来确定SCFA在MS中的作用,并区分疾病内在效应和治疗方案引起的效应。
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Short-chain fatty acids and intestinal inflammation in multiple sclerosis: modulation of female susceptibility by microbial products?

Background: Multiple Sclerosis (MS) is an autoimmune-mediated disease of the central nervous system. Experimental data suggest a role of intestinal microbiota and microbial products such as short-chain fatty acids (SCFAs) in the pathogenesis of MS. A recent clinical study reported beneficial effects (mediated by immunomodulatory mechanisms) after oral administration of the SCFA propionate in MS patients. Based on available evidence, we investigated whether SCFAs and the fecal inflammation marker calprotectin are altered in MS.

Methods: 76 subjects (41 patients with relapsing-remitting MS and 35 age-matched controls) were investigated in this case-control study. All subjects underwent clinical assessment with established clinical scales and provided fecal samples for a quantitative analysis of fecal SCFA and fecal calprotectin concentrations. Fecal markers were compared between MS patients and controls, and were analyzed for an association with demographic as well as clinical parameters.

Results: Median fecal calprotectin concentrations were within normal range in both groups without any group-specific differences. Fecal SCFA concentrations showed a non-significant reduction in MS patients compared to healthy subjects. Female subjects showed significantly reduced SCFA concentrations compared to male subjects.

Conclusions: In our cohort of MS patients, we found no evidence of an active intestinal inflammation. Yet, the vast majority of the investigated MS patients was under immunotherapy which might have affected the outcome measures. The sex-associated difference in fecal SCFA concentrations might at least partially explain female predominance in MS. Large-scale longitudinal studies including drug-naïve MS patients are required to determine the role of SCFAs in MS and to distinguish between disease-immanent effects and those caused by the therapeutic regime.

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