Propionate attenuates atherosclerosis by immune-dependent regulation of intestinal cholesterol metabolism

医学 内科学 载脂蛋白E 载脂蛋白B 内分泌学 胆固醇 安慰剂 ABCA1 免疫系统 免疫学 运输机 生物 疾病 生物化学 病理 替代医学 基因
作者
Arash Haghikia,Friederike Zimmermann,P. A. Schumann,Andrzej Jasina,Johann Roessler,David Schmidt,Philipp Heinze,Johannes Kaisler,Vanasa Nageswaran,Annette Aigner,Uta Ceglarek,Roodline Cineus,Ahmed N. Hegazy,Emiel P. C. van der Vorst,Yvonne Döring,Christopher Strauch,Ina Nemet,Valentina Tremaroli,Chinmay Dwibedi,Nicolle Kränkel,David M. Leistner,Markus M. Heimesaat,Stefan Bereswill,Geraldine Rauch,Ute Seeland,Oliver Soehnlein,Dominik N. Müller,Ralf Gold,Fredrik Bäckhed,Stanley L. Hazen,Aiden Haghikia,Ulf Landmesser
出处
期刊:European Heart Journal [Oxford University Press]
卷期号:43 (6): 518-533 被引量:178
标识
DOI:10.1093/eurheartj/ehab644
摘要

Abstract Aims Atherosclerotic cardiovascular disease (ACVD) is a major cause of mortality and morbidity worldwide, and increased low-density lipoproteins (LDLs) play a critical role in development and progression of atherosclerosis. Here, we examined for the first time gut immunomodulatory effects of the microbiota-derived metabolite propionic acid (PA) on intestinal cholesterol metabolism. Methods and results Using both human and animal model studies, we demonstrate that treatment with PA reduces blood total and LDL cholesterol levels. In apolipoprotein E−/− (Apoe −/−) mice fed a high-fat diet (HFD), PA reduced intestinal cholesterol absorption and aortic atherosclerotic lesion area. Further, PA increased regulatory T-cell numbers and interleukin (IL)-10 levels in the intestinal microenvironment, which in turn suppressed the expression of Niemann-Pick C1-like 1 (Npc1l1), a major intestinal cholesterol transporter. Blockade of IL-10 receptor signalling attenuated the PA-related reduction in total and LDL cholesterol and augmented atherosclerotic lesion severity in the HFD-fed Apoe −/− mice. To translate these preclinical findings to humans, we conducted a randomized, double-blinded, placebo-controlled human study (clinical trial no. NCT03590496). Oral supplementation with 500 mg of PA twice daily over the course of 8 weeks significantly reduced LDL [−15.9 mg/dL (−8.1%) vs. −1.6 mg/dL (−0.5%), P = 0.016], total [−19.6 mg/dL (−7.3%) vs. −5.3 mg/dL (−1.7%), P = 0.014] and non-high-density lipoprotein cholesterol levels [PA vs. placebo: −18.9 mg/dL (−9.1%) vs. −0.6 mg/dL (−0.5%), P = 0.002] in subjects with elevated baseline LDL cholesterol levels. Conclusion Our findings reveal a novel immune-mediated pathway linking the gut microbiota-derived metabolite PA with intestinal Npc1l1 expression and cholesterol homeostasis. The results highlight the gut immune system as a potential therapeutic target to control dyslipidaemia that may introduce a new avenue for prevention of ACVDs.
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