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SLC6A14 缺乏与肥胖、脂肪肝和代谢综合征有关,但仅在高脂肪饮食的条件下。

SLC6A14 deficiency is linked to obesity, fatty liver, and metabolic syndrome but only under conditions of a high-fat diet.

机构信息

Department of Cell Biology and Biochemistry, Texas Tech University Health Sciences Center, Lubbock, TX 79430, USA.

Department of Cell Biology and Biochemistry, Texas Tech University Health Sciences Center, Lubbock, TX 79430, USA.

出版信息

Biochim Biophys Acta Mol Basis Dis. 2021 May 1;1867(5):166087. doi: 10.1016/j.bbadis.2021.166087. Epub 2021 Jan 26.

Abstract

SLC6A14 is a Na/Cl-coupled transporter for neutral/cationic amino acids, expressed in ileum and colon. A single-nucleotide polymorphism (SNP), rs2011162 (-22,510C > G), in SLC6A14 coding for the 3'-untranslated region (3'-UTR) is associated with obesity in humans. But the impact of this polymorphism on the transporter expression and its connection to obesity are not known. Our objective was to address these issues. The impact of rs2011162 (-22,510C > G) on SLC6A14 expression was monitored using a luciferase reporter. The link between Slc6a14 and obesity was investigated in wild type and Slc6a14 mice when fed a normal diet or a high-fat diet. The obesity-associated 3'-UTR polymorphism reduced SLC6A14 expression. With a high-fat diet, Slc6a14 mice gained more weight than wild type mice. With normal diet, there was no difference between the two genotypes. The gain in body weight with the high-fat diet in Slc6a14 mice was accompanied with metabolic syndrome. With the high-fat diet, Slc6a14 mice showed increased food intake, developed fatty liver, and altered plasma amino acid profile. The high-fat diet-associated hepatic steatosis in Slc6a14 mice showed male preponderance. We conclude that the 3'-UTR SNP in SLC6A14 associated with obesity decreases the expression of SLC6A14 and that the deficiency of SLC6A14 is linked to obesity. This is supported by the findings that Slc6a14 mice develop obesity, fatty liver, and metabolic syndrome. This connection is evident only with a high-fat diet. Therefore, dietary/pharmacologic interventions that induce SLC6A14 expression in the intestinal tract might have potential for obesity prevention..

摘要

SLC6A14 是一种 Na/Cl 偶联转运体,用于转运中性/阳离子氨基酸,在回肠和结肠中表达。SLC6A14 编码 3'-非翻译区(3'-UTR)的单核苷酸多态性(SNP)rs2011162(-22,510C>G)与人类肥胖有关。但该多态性对转运体表达的影响及其与肥胖的关系尚不清楚。我们的目的是解决这些问题。使用荧光素酶报告基因监测 rs2011162(-22,510C>G)对 SLC6A14 表达的影响。在正常饮食或高脂肪饮食喂养的野生型和 Slc6a14 小鼠中,研究 Slc6a14 与肥胖的关系。与肥胖相关的 3'-UTR 多态性降低了 SLC6A14 的表达。在高脂肪饮食中,Slc6a14 小鼠比野生型小鼠体重增加更多。在正常饮食下,两种基因型之间没有差异。Slc6a14 小鼠在高脂肪饮食下体重增加伴随着代谢综合征。在高脂肪饮食中,Slc6a14 小鼠表现出摄食量增加、脂肪肝和血浆氨基酸谱改变。Slc6a14 小鼠的高脂肪饮食相关肝脂肪变性表现出雄性优势。我们得出结论,与肥胖相关的 SLC6A14 3'-UTR SNP 降低了 SLC6A14 的表达,而 SLC6A14 的缺乏与肥胖有关。这一结论得到了以下发现的支持:Slc6a14 小鼠会发生肥胖、脂肪肝和代谢综合征。只有在高脂肪饮食下才会出现这种联系。因此,诱导肠道中 SLC6A14 表达的饮食/药物干预可能具有预防肥胖的潜力。

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