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柚皮素和β-胡萝卜素可将人白色脂肪细胞转化为米色表型,并提高激素刺激的脂肪分解。

Naringenin and β-carotene convert human white adipocytes to a beige phenotype and elevate hormone- stimulated lipolysis.

机构信息

Computational Biology, Pennington Biomedical Research Center, Baton Rouge, LA, United States.

Clinical Trials, Pennington Biomedical Research Center, Baton Rouge, LA, United States.

出版信息

Front Endocrinol (Lausanne). 2023 Apr 17;14:1148954. doi: 10.3389/fendo.2023.1148954. eCollection 2023.

Abstract

INTRODUCTION

Naringenin, a peroxisome proliferator-activated receptor (PPAR) activator found in citrus fruits, upregulates markers of thermogenesis and insulin sensitivity in human adipose tissue. Our pharmacokinetics clinical trial demonstrated that naringenin is safe and bioavailable, and our case report showed that naringenin causes weight loss and improves insulin sensitivity. PPARs form heterodimers with retinoic-X-receptors (RXRs) at promoter elements of target genes. Retinoic acid is an RXR ligand metabolized from dietary carotenoids. The carotenoid β-carotene reduces adiposity and insulin resistance in clinical trials. Our goal was to examine if carotenoids strengthen the beneficial effects of naringenin on human adipocyte metabolism.

METHODS

Human preadipocytes from donors with obesity were differentiated in culture and treated with 8µM naringenin + 2µM β-carotene (NRBC) for seven days. Candidate genes involved in thermogenesis and glucose metabolism were measured as well as hormone-stimulated lipolysis.

RESULTS

We found that β-carotene acts synergistically with naringenin to boost UCP1 and glucose metabolism genes including GLUT4 and adiponectin, compared to naringenin alone. Protein levels of PPARα, PPARγ and PPARγ-coactivator-1α, key modulators of thermogenesis and insulin sensitivity, were also upregulated after treatment with NRBC. Transcriptome sequencing was conducted and the bioinformatics analyses of the data revealed that NRBC induced enzymes for several non-UCP1 pathways for energy expenditure including triglyceride cycling, creatine kinases, and Peptidase M20 Domain Containing 1 (PM20D1). A comprehensive analysis of changes in receptor expression showed that NRBC upregulated eight receptors that have been linked to lipolysis or thermogenesis including the β1-adrenergic receptor and the parathyroid hormone receptor. NRBC increased levels of triglyceride lipases and agonist-stimulated lipolysis in adipocytes. We observed that expression of RXRγ, an isoform of unknown function, was induced ten-fold after treatment with NRBC. We show that RXRγ is a coactivator bound to the immunoprecipitated PPARγ protein complex from white and beige human adipocytes.

DISCUSSION

There is a need for obesity treatments that can be administered long-term without side effects. NRBC increases the abundance and lipolytic response of multiple receptors for hormones released after exercise and cold exposure. Lipolysis provides the fuel for thermogenesis, and these observations suggest that NRBC has therapeutic potential.

摘要

简介

柚皮素是一种在柑橘类水果中发现的过氧化物酶体增殖物激活受体(PPAR)激活剂,可上调人体脂肪组织的产热和胰岛素敏感性标志物。我们的药代动力学临床试验表明,柚皮素是安全且可生物利用的,我们的病例报告表明,柚皮素可减轻体重并提高胰岛素敏感性。PPAR 与视黄酸-X 受体(RXR)在靶基因的启动子元件上形成异二聚体。视黄酸是一种由膳食类胡萝卜素代谢而来的 RXR 配体。类胡萝卜素β-胡萝卜素可在临床试验中减少肥胖和胰岛素抵抗。我们的目标是研究类胡萝卜素是否能增强柚皮素对人体脂肪细胞代谢的有益作用。

方法

从肥胖供体中分离培养的人前脂肪细胞分化后,用 8µM 柚皮素+2µM β-胡萝卜素(NRBC)处理 7 天。还测量了参与产热和葡萄糖代谢的候选基因以及激素刺激的脂肪分解。

结果

我们发现,与单独使用柚皮素相比,β-胡萝卜素与柚皮素协同作用可促进 UCP1 和葡萄糖代谢基因的表达,包括 GLUT4 和脂联素。经过 NRBC 处理后,PPARα、PPARγ 和 PPARγ 共激活因子-1α 的蛋白水平也上调,这些都是产热和胰岛素敏感性的关键调节剂。进行了转录组测序,对数据的生物信息学分析表明,NRBC 诱导了几种非 UCP1 能量消耗途径的酶,包括甘油三酯循环、肌酸激酶和肽酶 M20 结构域包含蛋白 1(PM20D1)。对受体表达变化的综合分析表明,NRBC 上调了 8 种与脂肪分解或产热相关的受体,包括β1-肾上腺素能受体和甲状旁腺激素受体。NRBC 增加了脂肪细胞中的甘油三酯脂肪酶和激动剂刺激的脂肪分解。我们观察到,NRBC 处理后 RXRγ(一种功能未知的同工型)的表达增加了十倍。我们表明,RXRγ 是从白色和米色人脂肪细胞的免疫沉淀 PPARγ 蛋白复合物中结合的共激活因子。

讨论

需要有可以长期服用而无副作用的肥胖症治疗方法。NRBC 增加了运动和冷暴露后释放的激素的多种受体的丰度和脂肪分解反应。脂肪分解为产热提供燃料,这些观察结果表明 NRBC 具有治疗潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e9b7/10153092/fe5a3c879af8/fendo-14-1148954-g001.jpg

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