A. Colombo, M. Busnelli, S. Manzini, E. Franchi, Mariel Garcia Rivera, J. Kirwan, G. Chiesa
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At the end of the dietary treatment, atherosclerosis development was quantified at the aortic sinus, targeted plasma metabolomics was performed, and gene expression was evaluated in liver, duodenum, jejunum and ileum. With both diets, DKO mice developed much larger plaques than DKO/hA-I mice. High-choline diet increased plasma TMAO levels in both genotypes. Interestingly, a worsening of plaque development by high choline diet occurred in DKO/hA-I mice only (0.057±0.048 mm2 vs 0.0988±0.064 mm2, p<0.01). Plasma metabolomics indicated that choline supplementation, only in the presence of HDL, significantly increased the concentration of some ceramide species in addition to several markers of impaired kidney function. High-choline diet increased the hepatic gene expression of Fmo1 and Fmo2 in DKO/hA-I, whereas the expression of Scarb1 was lower in DKO/hA-I compared to DKO mice, regardless of the dietary treatment. Intestinal expression of genes involved in inflammatory response and in lipid metabolism was comparable between genotypes and was not modified by choline supplementation. In conclusion, high choline diet increased plasma TMAO concentration in both genotypes, but affected atherosclerosis development, plasma metabolome and hepatic gene expression only in high HDL mice. Intestinal gene expression was not affected neither by genotype nor by dietary choline content.","PeriodicalId":227903,"journal":{"name":"European Atherosclerosis Journal","volume":"76 1","pages":"0"},"PeriodicalIF":0.0000,"publicationDate":"2023-04-20","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Impact of dietary choline on lipid metabolism and atherosclerosis development in apoEKO mice deficient or overexpressing apolipoprotein A-I: Selected Abstract - XVI SITeCS Congress\",\"authors\":\"A. Colombo, M. Busnelli, S. 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引用次数: 0
摘要
氧化三甲胺是膳食胆碱的代谢物,被认为是一种促动脉粥样硬化分子,因为它能够干扰胆固醇的逆向运输,其中载脂蛋白a - i和高密度脂蛋白起关键作用。本研究评估了氧化三甲胺对不同apoA-I/HDL水平小鼠动脉粥样硬化的影响。小鼠apoA-I和apoE缺乏(DKO)和DKO小鼠过度表达人apoA-I (DKO/hA-I),分别以极低或高血浆HDL水平为特征,饲喂两种标准啮齿动物饮食16周,仅胆碱含量(0.09%或1.2%)不同。在饮食治疗结束时,量化主动脉窦动脉粥样硬化的发展,进行靶向血浆代谢组学研究,并评估肝脏、十二指肠、空肠和回肠的基因表达。在这两种饮食中,DKO小鼠的斑块都比DKO/ ha - 1小鼠大得多。高胆碱饮食增加了两种基因型的血浆TMAO水平。有趣的是,高胆碱饮食仅在DKO/hA-I小鼠中发生斑块发展恶化(0.057±0.048 mm2 vs 0.0988±0.064 mm2, p<0.01)。血浆代谢组学表明,仅在HDL存在的情况下,胆碱的补充显著增加了一些神经酰胺种类的浓度,以及一些肾功能受损的标志物。无论何种饮食处理,高胆碱日粮增加了DKO/ ha - 1小鼠肝脏中Fmo1和Fmo2基因的表达,而与DKO小鼠相比,DKO/ ha - 1小鼠中Scarb1的表达较低。肠道中参与炎症反应和脂质代谢的基因表达在基因型之间是相似的,并且没有被补充胆碱改变。由此可见,高胆碱饮食增加了两种基因型小鼠的血浆TMAO浓度,但仅影响高HDL小鼠的动脉粥样硬化发展、血浆代谢组和肝脏基因表达。肠道基因表达不受基因型和饲粮胆碱含量的影响。
Impact of dietary choline on lipid metabolism and atherosclerosis development in apoEKO mice deficient or overexpressing apolipoprotein A-I: Selected Abstract - XVI SITeCS Congress
TMAO, a metabolite of dietary choline, is considered a pro-atherogenic molecule for its ability to interfere with the reverse cholesterol transport, in which apolipoprotein A-I and HDL play a key role. In the present work it was evaluated how TMAO impacts on the development of atherosclerosis in mice with different levels of apoA-I/HDL. Mice deficient in both murine apoA-I and apoE (DKO) and DKO mice overexpressing human apoA-I (DKO/hA-I), characterized by extremely low or high plasma HDL levels respectively, were fed for 16 weeks two standard rodent diets, differing only in their choline content (0.09% or 1.2%). At the end of the dietary treatment, atherosclerosis development was quantified at the aortic sinus, targeted plasma metabolomics was performed, and gene expression was evaluated in liver, duodenum, jejunum and ileum. With both diets, DKO mice developed much larger plaques than DKO/hA-I mice. High-choline diet increased plasma TMAO levels in both genotypes. Interestingly, a worsening of plaque development by high choline diet occurred in DKO/hA-I mice only (0.057±0.048 mm2 vs 0.0988±0.064 mm2, p<0.01). Plasma metabolomics indicated that choline supplementation, only in the presence of HDL, significantly increased the concentration of some ceramide species in addition to several markers of impaired kidney function. High-choline diet increased the hepatic gene expression of Fmo1 and Fmo2 in DKO/hA-I, whereas the expression of Scarb1 was lower in DKO/hA-I compared to DKO mice, regardless of the dietary treatment. Intestinal expression of genes involved in inflammatory response and in lipid metabolism was comparable between genotypes and was not modified by choline supplementation. In conclusion, high choline diet increased plasma TMAO concentration in both genotypes, but affected atherosclerosis development, plasma metabolome and hepatic gene expression only in high HDL mice. Intestinal gene expression was not affected neither by genotype nor by dietary choline content.
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