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微生物群衍生的致肥胖物δ-戊基甜菜碱在哺乳动物体内羟基化为同型肉碱,一种五碳肉碱类似物。

Mammalian hydroxylation of microbiome-derived obesogen, delta-valerobetaine, to homocarnitine, a 5-carbon carnitine analog.

作者信息

Weinberg Jaclyn, Liu Ken H, Lee Choon-Myung, Crandall William J, Cuevas André R, Druzak Samuel A, Morgan Edward T, Jarrell Zachery R, Ortlund Eric A, Martin Greg S, Singer Grant, Strobel Frederick H, Go Young-Mi, Jones Dean P

机构信息

Division of Pulmonary, Allergy, Critical Care and Sleep Medicine, Department of Medicine, Emory University School of Medicine, Atlanta, Georgia, USA.

Department of Biochemistry, Department of Medicine, Emory University, Atlanta, Georgia, USA.

出版信息

J Biol Chem. 2025 Jan;301(1):108074. doi: 10.1016/j.jbc.2024.108074. Epub 2024 Dec 13.

Abstract

The recently discovered microbiome-generated obesogen, δ-valerobetaine (5-(trimethylammonio)pentanoate), is a 5-carbon structural analog of the carnitine precursor, γ-butyrobetaine. Here, we report that δ-valerobetaine is enzymatically hydroxylated by mammalian γ-butyrobetaine dioxygenase (BBOX) to form 3-hydroxy-5-(trimethylammonio)pentanoate, a 5-carbon analog of carnitine, which we term homocarnitine. Homocarnitine production by human liver extracts depends upon the required BBOX cofactors, 2-oxoglutarate, Fe, and ascorbate. Molecular dynamics simulations show successful docking of δ-valerobetaine and homocarnitine to BBOX, pharmacological inhibition of BBOX prevents homocarnitine production, and transfection of a liver cell line with BBOX substantially increases production. Furthermore, an in vivo isotope tracer study shows the conversion of C-trimethyllysine to C-δ-valerobetaine then C-homocarnitine in mice, confirming the in vivo production of homocarnitine. Functional assays show that carnitine palmitoyltransferase acylates homocarnitine to acyl-homocarnitine, analogous to the reactions for the carnitine shuttle. Studies of mouse tissues and human plasma show widespread distribution of homocarnitine and fatty acyl-homocarnitines. The respective structural similarities of homocarnitine and acyl-homocarnitines to carnitine and acyl-carnitines indicate that homocarnitine could impact multiple sites of carnitine distribution and activity, potentially mediating microbiome-associated obesity and metabolic disorders.

摘要

最近发现的由微生物群产生的致肥胖物δ-戊基甜菜碱(5-(三甲基铵基)戊酸)是肉碱前体γ-丁酰甜菜碱的一种5碳结构类似物。在此,我们报告δ-戊基甜菜碱被哺乳动物γ-丁酰甜菜碱双加氧酶(BBOX)酶促羟基化,形成3-羟基-5-(三甲基铵基)戊酸,一种肉碱的5碳类似物,我们将其称为高肉碱。人肝提取物产生高肉碱取决于所需的BBOX辅因子、2-氧代戊二酸、铁和抗坏血酸。分子动力学模拟显示δ-戊基甜菜碱和高肉碱成功对接至BBOX,对BBOX的药理学抑制可阻止高肉碱的产生,而用BBOX转染肝细胞系可大幅增加其产生。此外,一项体内同位素示踪研究表明,小鼠体内C-三甲基赖氨酸转化为C-δ-戊基甜菜碱,然后转化为C-高肉碱,证实了高肉碱在体内的产生。功能测定表明,肉碱棕榈酰转移酶将高肉碱酰化为酰基高肉碱,类似于肉碱穿梭的反应。对小鼠组织和人血浆的研究表明,高肉碱和脂肪酰基高肉碱广泛分布。高肉碱和酰基高肉碱与肉碱和酰基肉碱各自的结构相似性表明,高肉碱可能影响肉碱分布和活性的多个位点,潜在地介导与微生物群相关的肥胖和代谢紊乱。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a0ce/11773067/c96d986be940/gr1.jpg

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