通过抑制羟柠檬酸酸/RPS6KA1/FoxO1 信号轴减少 MCE 抑制，从而减轻 HFD 诱导的肥胖。

Inhibition of the RPS6KA1/FoxO1 signaling axis by hydroxycitric acid attenuates HFD-induced obesity through MCE suppression.

机构信息

College of Pharmacy and Research Institute of Pharmaceutical Sciences, Woosuk University, Wanju 55338, Republic of Korea.

Department of Biological Sciences, College of Natural Science, Seoul National University, Seoul 08826, South Korea; Nexus Institute of Research and Innovation (NIRI), Kathmandu, Nepal.

出版信息

Phytomedicine. 2024 Jun;128:155551. doi: 10.1016/j.phymed.2024.155551. Epub 2024 Mar 20.

DOI:10.1016/j.phymed.2024.155551

PMID:38569293

Abstract

BACKGROUND

Because obesity is associated with a hyperplasia-mediated increase in adipose tissue, inhibiting cell proliferation during mitotic clonal expansion (MCE) is a leading strategy for preventing obesity. Although (-)-hydroxycitric acid (HCA) is used to control obesity, the molecular mechanisms underlying its effects on MCE are poorly understood.

PURPOSE

This study aimed to investigate the potential effects of HCA on MCE and underlying molecular mechanisms affecting adipogenesis and obesity improvements.

METHODS

Preadipocyte cell line, 3T3-L1, were treated with HCA; oil red O, cell proliferation, cell cycle, and related alterations in signaling pathways were examined. High-fat diet (HFD)-fed mice were administered HCA for 12 weeks; body and adipose tissues weights were evaluated, and the regulation of signaling pathways in epidydimal white adipose tissue were examined in vivo.

RESULTS

Here, we report that during MCE, HCA attenuates the proliferation of the preadipocyte cell line, 3T3-L1, by arresting the cell cycle at the G/G phase. In addition, HCA markedly inhibits Forkhead Box O1 (FoxO1) phosphorylation, thereby inducing the expression of cyclin-dependent kinase inhibitor 1B and suppressing the levels of cyclin-dependent kinase 2, cyclin E1, proliferating cell nuclear antigen, and phosphorylated retinoblastoma. Importantly, we found that ribosomal protein S6 kinase A1 (RPS6KA1) influences HCA-mediated inactivation of FoxO1 and its nuclear exclusion. An animal model of obesity revealed that HCA reduced high-fat diet-induced obesity by suppressing adipocyte numbers as well as epididymal and mesenteric white adipose tissue mass, which is attributed to the regulation of RPS6KA1, FoxO1, CDKN1B and PCNA that had been consistently identified in vitro.

CONCLUSIONS

These findings provide novel insights into the mechanism by which HCA regulates adipogenesis and highlight the RPS6KA1/FoxO1 signaling axis as a therapeutic target for obesity.

摘要

背景

由于肥胖与脂肪组织的增生有关，因此在有丝分裂克隆扩张（MCE）期间抑制细胞增殖是预防肥胖的主要策略。尽管（-）-羟基柠檬酸（HCA）被用于控制肥胖，但人们对其对 MCE 的影响的分子机制知之甚少。

目的

本研究旨在探讨 HCA 对 MCE 的潜在影响及其影响脂肪生成和肥胖改善的潜在分子机制。

方法

用 HCA 处理前脂肪细胞系 3T3-L1；用油红 O、细胞增殖、细胞周期和相关信号通路改变进行检测。用 HCA 处理高脂肪饮食（HFD）喂养的小鼠 12 周；评估体重和脂肪组织重量，并在体内检测附睾白色脂肪组织中信号通路的调节。

结果

在这里，我们报告说在 MCE 期间，HCA 通过将细胞周期阻滞在 G1/G0 期来减弱前脂肪细胞系 3T3-L1 的增殖。此外，HCA 显著抑制叉头框 O1（FoxO1）的磷酸化，从而诱导细胞周期蛋白依赖性激酶抑制剂 1B 的表达，并抑制细胞周期蛋白依赖性激酶 2、细胞周期蛋白 E1、增殖细胞核抗原和磷酸化视网膜母细胞瘤的水平。重要的是，我们发现核糖体蛋白 S6 激酶 A1（RPS6KA1）影响 HCA 介导的 FoxO1 失活及其核排除。肥胖动物模型表明，HCA 通过抑制脂肪细胞数量以及附睾和肠系膜白色脂肪组织的质量来减轻高脂肪饮食引起的肥胖，这归因于 RPS6KA1、FoxO1、CDKN1B 和 PCNA 的调节，这些在体外得到了一致的鉴定。