Therapeutic effects of FGF21 mimetic bFKB1 on MASH and atherosclerosis in Ldlr−/−.Leiden mice

IF 4.4 2区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY The FASEB Journal Pub Date : 2024-10-28 DOI:10.1096/fj.202401397R

José A. Inia, Joline Attema, Christa de Ruiter, Aswin L. Menke, Martien P. M. Caspers, Lars Verschuren, Maria Wilson, Alexander Arlantico, Hans D. Brightbill, J. Wouter Jukema, Anita M. van den Hoek, Hans M. G. Princen, Mark Z. Chen, Martine C. Morrison

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Abstract

Fibroblast growth factor 21 (FGF21) is a promising target for treatment of obesity-associated diseases including metabolic dysfunction-associated steatohepatitis (MASH) and atherosclerosis. We evaluated the effects of the bispecific anti-FGF21-β klotho (KLB) agonist antibody bFKB1 in a preclinical model of MASH and atherosclerosis. Low-density lipoprotein receptor knockout (Ldlr−/−).Leiden mice received a high-fat diet for 20 weeks, followed by treatment with an isotype control antibody or bFKB1 for 12 weeks. Effects on plasma risk markers and (histo)pathology of liver, adipose tissue, and heart were evaluated alongside hepatic transcriptomics analysis. bFKB1 lowered body weight (−21%) and adipose tissue mass (−22%) without reducing food intake. The treatment also improved plasma insulin (−80%), cholesterol (−48%), triglycerides (−76%), alanine transaminase (ALT: −79%), and liver weight (−43%). Hepatic steatosis and inflammation were strongly reduced (macrovesicular steatosis −34%; microvesicular steatosis −100%; inflammation −74%) and while the total amount of fibrosis was not affected, bFKB1 did decrease new collagen formation (−49%). Correspondingly, hepatic transcriptomics and pathway analysis revealed the mechanistic background underlying these histological improvements, demonstrating broad inactivation of inflammatory and profibrotic transcriptional programs by bFKB1. In epididymal white adipose tissue, bFKB1 reduced adipocyte size (−16%) and inflammation (−52%) and induced browning, signified by increased uncoupling protein-1 (UCP1) protein expression (8.5-fold increase). In the vasculature, bFKB1 had anti-atherogenic effects, lowering total atherosclerotic lesion area (−38%). bFKB1 has strong beneficial metabolic effects associated with a reduction in hepatic steatosis, inflammation, and atherosclerosis. Analysis of new collagen formation and profibrotic transcriptional programs indicate that bFKB1 treatment may have antifibrotic potential in a longer treatment duration as well.

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FGF21 模拟物 bFKB1 对 Ldlr-/-.Leiden 小鼠 MASH 和动脉粥样硬化的治疗效果。

成纤维细胞生长因子 21（FGF21）是治疗肥胖相关疾病（包括代谢功能障碍相关性脂肪性肝炎（MASH）和动脉粥样硬化）的一个很有前景的靶点。我们评估了双特异性抗 FGF21-β klotho（KLB）激动剂抗体 bFKB1 在 MASH 和动脉粥样硬化临床前模型中的作用。低密度脂蛋白受体剔除（Ldlr-/-）.Leiden小鼠接受了20周的高脂饮食，随后接受了12周的同型对照抗体或bFKB1治疗。bFKB1 可降低体重（-21%）和脂肪组织质量（-22%），而不减少食物摄入量。治疗还改善了血浆胰岛素（-80%）、胆固醇（-48%）、甘油三酯（-76%）、丙氨酸转氨酶（ALT：-79%）和肝脏重量（-43%）。肝脏脂肪变性和炎症均显著减轻（大泡脂肪变性-34%；小泡脂肪变性-100%；炎症-74%），虽然纤维化的总量未受影响，但 bFKB1 确实减少了新胶原的形成（-49%）。相应地，肝脏转录组学和通路分析揭示了这些组织学改善的机理背景，显示了 bFKB1 对炎症和坏死转录程序的广泛失活作用。在附睾白色脂肪组织中，bFKB1 使脂肪细胞体积缩小（-16%），炎症减轻（-52%），并诱导褐变，解偶联蛋白-1（UCP1）蛋白表达增加（增加 8.5 倍）表明了这一点。在血管中，bFKB1 具有抗动脉粥样硬化的作用，降低了动脉粥样硬化病变的总面积（-38%）。对新胶原形成和脆性转录程序的分析表明，bFKB1疗法在更长的治疗时间内也可能具有抗纤维化的潜力。

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来源期刊

The FASEB Journal 生物-生化与分子生物学

CiteScore

9.20

自引率

2.10%

发文量

6243

审稿时长

3 months

期刊介绍： The FASEB Journal publishes international, transdisciplinary research covering all fields of biology at every level of organization: atomic, molecular, cell, tissue, organ, organismic and population. While the journal strives to include research that cuts across the biological sciences, it also considers submissions that lie within one field, but may have implications for other fields as well. The journal seeks to publish basic and translational research, but also welcomes reports of pre-clinical and early clinical research. In addition to research, review, and hypothesis submissions, The FASEB Journal also seeks perspectives, commentaries, book reviews, and similar content related to the life sciences in its Up Front section.