Rao Yong, Su Rui, Wu Chenyan, Yang Guanyu, Fu Renquan, Wu Junjie, Liang Jinqiang, Liu Jin, Jiang Zhongping, Xu Congjun, Huang Ling
Key Laboratory of Tropical Biological Resources of Ministry of Education, School of Pharmaceutical Sciences, Hainan University, Haikou, China.
Front Pharmacol. 2024 Jan 25;15:1320040. doi: 10.3389/fphar.2024.1320040. eCollection 2024.
Obesity is one of the most prevalent diseases worldwide with less ideal approved agents in clinic. Activating the HSF1/PGC-1α axis in adipose tissues has been reported to induce thermogenesis in mice, which presents a promising therapeutic avenue for obesity treatment. The present study aimed to identified novel natural HSF1 activator and evaluated the therapeutic effects of the newly discovered compound on obesity-associated metabolic disorders and the molecular mechanisms of these effects. Our previous reported HSF1/PGC-1α activator screening system was used to identify novel natural HSF1 activator. The PGC-1α luciferase activity, immunoblot, protein nuclear-translocation, immunofluorescence, chromatin immunoprecipitation assays were used to evaluate the activity of compound HN-001 in activating HSF1. The experiments of mitochondrial number measurement, TG assay and imaging, cellular metabolic assay, gene assays, and CRISPR/Cas 9 were applied for investigating the metabolic effect of HN-001 in C3H10-T1/2 adipocytes. The anti-obesity efficacies and beneficial metabolic effects of HN-001 were evaluated by performing body and fat mass quantification, plasma chemical analysis, GTT, ITT, cold tolerance test, thermogenesis analysis. HN-001 dose- and time-dependently activated HSF1 and induced HSF1 nuclear translocation, resulting in an enhancement in binding with the gene . This improvement induced activation of adipose thermogenesis and enhancement of mitochondrial oxidation capacity, thus inhibiting adipocyte maturation. Deletion of HSF1 in adipocytes impaired mitochondrial oxidation and abolished the above beneficial metabolic effects of HN-001, including adipocyte browning induction, improvements in mitogenesis and oxidation capacity, and lipid-lowering ability. In mice, HN-001 treatment efficiently alleviated diet-induced obesity and metabolic disorders. These changes were associated with increased body temperature in mice and activation of the HSF1/PGC-1α axis in adipose tissues. UCP1 expression and mitochondrial biogenesis were increased in both white and brown adipose tissues of HN-001-treated mice. These data indicate that HN-001 may have therapeutic potential for obesity-related metabolic diseases by increasing the capacity of energy expenditure in adipose tissues through a mechanism involving the HSF1/PGC-1α axis, which shed new light on the development of novel anti-obesity agents derived from marine sources.
肥胖是全球最普遍的疾病之一,临床上可用的理想药物较少。据报道,激活脂肪组织中的热休克因子1(HSF1)/过氧化物酶体增殖物激活受体γ共激活因子1α(PGC-1α)轴可在小鼠中诱导产热,这为肥胖治疗提供了一条有前景的治疗途径。本研究旨在鉴定新型天然HSF1激活剂,并评估新发现的化合物对肥胖相关代谢紊乱的治疗效果及其作用的分子机制。我们之前报道的HSF1/PGC-1α激活剂筛选系统被用于鉴定新型天然HSF1激活剂。采用PGC-1α荧光素酶活性、免疫印迹、蛋白质核转位、免疫荧光、染色质免疫沉淀分析来评估化合物HN-001激活HSF1的活性。通过线粒体数量测量、甘油三酯测定与成像、细胞代谢分析、基因分析以及CRISPR/Cas 9实验来研究HN-001对C3H10-T1/2脂肪细胞的代谢作用。通过进行体重和脂肪量定量、血浆化学分析、葡萄糖耐量试验、胰岛素耐量试验、耐寒试验、产热分析来评估HN-001的抗肥胖功效和有益的代谢作用。HN-001剂量和时间依赖性地激活HSF1并诱导HSF1核转位,导致其与该基因的结合增强。这种改善诱导了脂肪组织产热的激活和线粒体氧化能力的增强,从而抑制脂肪细胞成熟。脂肪细胞中HSF1的缺失损害了线粒体氧化,并消除了HN-001上述有益的代谢作用,包括诱导脂肪细胞褐变、改善有丝分裂和氧化能力以及降脂能力。在小鼠中,HN-001治疗有效减轻了饮食诱导的肥胖和代谢紊乱。这些变化与小鼠体温升高以及脂肪组织中HSF1/PGC-1α轴的激活有关。在接受HN-001治疗的小鼠的白色和棕色脂肪组织中,解偶联蛋白1(UCP1)表达和线粒体生物发生均增加。这些数据表明,HN-001可能通过涉及HSF1/PGC-1α轴的机制增加脂肪组织中的能量消耗能力,从而对肥胖相关代谢疾病具有治疗潜力,这为开发新型海洋来源抗肥胖药物提供了新的思路。
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