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循环脂肪酸的改变与多发性硬化症中的肠道微生物失调和炎症有关。

Alterations in Circulating Fatty Acid Are Associated With Gut Microbiota Dysbiosis and Inflammation in Multiple Sclerosis.

机构信息

IRCCS Fondazione Don Carlo Gnocchi, Milan, Italy.

Microbial Ecology of Health Unit, Department of Pharmacy and Biotechnology, University of Bologna, Bologna, Italy.

出版信息

Front Immunol. 2020 Jul 7;11:1390. doi: 10.3389/fimmu.2020.01390. eCollection 2020.

DOI:10.3389/fimmu.2020.01390
PMID:32733460
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7358580/
Abstract

Butyric acid (BA) is a short-chain fatty acid (SCFA) with anti-inflammatory properties, which promotes intestinal barrier function. Medium-chain fatty acids (MCFA), including caproic acid (CA), promote TH1 and TH17 differentiation, thus supporting inflammation. Since most SCFAs are absorbed in the cecum and colon, the measurement of BA in peripheral blood could provide information on the health status of the intestinal ecosystem. Additionally, given the different immunomodulatory properties of BA and CA the evaluation of their serum concentration, as well as their ratio could be as a simple and rapid biomarker of disease activity and/or treatment efficacy in MS. We evaluated serum BA and CA concentrations, immune parameters, intestinal barrier integrity and the gut microbiota composition in patients with multiple sclerosis (MS) comparing result to those obtained in healthy controls. In MS, the concentration of BA was reduced and that of CA was increased. Concurrently, the microbiota was depleted of BA producers while it was enriched in mucin-degrading, pro-inflammatory components. The reduced serum concentration of BA seen in MS patients correlated with alterations of the barrier permeability, as evidenced by the higher plasma concentrations of lipopolysaccharide and intestinal fatty acid-binding protein, and inflammation. Specifically, CA was positively associated with CD4+/IFNγ+ T lymphocytes, and the BA/CA ratio correlated positively with CD4+/CD25/Foxp3+ and negatively with CD4+/IFNγ+ T lymphocytes. The gut microbiota dysbiosis found in MS is possibly associated with alterations of the SCFA/MCFA ratio and of the intestinal barrier; this could explain the chronic inflammation that characterizes this disease. SCFA and MCFA quantification could be a simple biomarker to evaluate the efficacy of therapeutic and rehabilitation procedures in MS.

摘要

丁酸(BA)是一种具有抗炎特性的短链脂肪酸(SCFA),可促进肠道屏障功能。中链脂肪酸(MCFA),包括己酸(CA),促进 TH1 和 TH17 分化,从而支持炎症。由于大多数 SCFA 在盲肠和结肠中被吸收,因此外周血中 BA 的测量可以提供有关肠道生态系统健康状况的信息。此外,鉴于 BA 和 CA 的免疫调节特性不同,评估其血清浓度及其比值可能是 MS 疾病活动和/或治疗效果的简单快速生物标志物。我们评估了多发性硬化症(MS)患者的血清 BA 和 CA 浓度、免疫参数、肠道屏障完整性和肠道微生物群组成,并将结果与健康对照组进行了比较。在 MS 中,BA 的浓度降低,CA 的浓度增加。同时,BA 产生菌的微生物群减少,而粘蛋白降解、促炎成分丰富。MS 患者血清中 BA 浓度降低与屏障通透性改变相关,这表现为血浆中脂多糖和肠脂肪酸结合蛋白浓度升高和炎症。具体而言,CA 与 CD4+/IFNγ+T 淋巴细胞呈正相关,BA/CA 比值与 CD4+/CD25/Foxp3+呈正相关,与 CD4+/IFNγ+T 淋巴细胞呈负相关。MS 中发现的肠道微生物群失调可能与 SCFA/MCFA 比值和肠道屏障的改变有关;这可以解释该疾病的慢性炎症。SCFA 和 MCFA 的定量可能是评估 MS 治疗和康复程序疗效的简单生物标志物。

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