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IL-1β RAGE and FABP4: targeting the dynamic trio in metabolic inflammation and related pathologies

机译:IL-1βRAGE和FABP4:靶向代谢炎症和相关病理学中的动态三重奏

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摘要

Within the past decade, inflammatory and lipid mediators, such as IL-1β, FABP4 and RAGE, have emerged as important contributors to metabolic dysfunction. As growing experimental and clinical evidence continues to tie obesity-induced chronic inflammation with dysregulated lipid, insulin signaling and related pathologies, IL-1β, FABP4 and RAGE each are being independently implicated as culprits in these events. There are also convincing data that molecular pathways driven by these molecules are interconnected in exacerbating metabolic consequences of obesity. This article highlights the roles of IL-1β, FABP4 and RAGE in normal physiology as well as focusing specifically on their contribution to inflammation, insulin resistance, atherosclerosis, Type 2 diabetes and cancer. Studies implicating the interconnection between these pathways, current and emerging therapeutics, and their use as potential biomarkers are also discussed. Evidence of impact of IL-1β, FABP4 and RAGE pathways on severity of metabolic dysfunction underlines the strong links between inflammatory events, lipid metabolism and insulin regulation, and offers new intriguing approaches for future therapies of obesity-driven pathologies.
机译:在过去的十年中,炎症和脂质介质(例如IL-1β,FABP4和RAGE)已成为代谢功能异常的重要因素。随着越来越多的实验和临床证据继续将肥胖引起的慢性炎症与脂质失调,胰岛素信号传导和相关病理联系在一起,IL-1β,FABP4和RAGE各自独立地被认为是这些事件的罪魁祸首。也有令人信服的数据,由这些分子驱动的分子途径相互联系,加剧了肥胖症的代谢后果。本文重点介绍了IL-1β,FABP4和RAGE在正常生理中的作用,并特别关注了它们对炎症,胰岛素抵抗,动脉粥样硬化,2型糖尿病和癌症的贡献。还讨论了涉及这些途径,当前和新兴治疗方法之间的相互联系的研究,以及它们作为潜在生物标志物的用途。 IL-1β,FABP4和RAGE途径对代谢功能障碍严重程度的影响的证据强调了炎症事件,脂质代谢和胰岛素调节之间的紧密联系,并为肥胖症驱动的病理学的未来治疗提供了新的有趣方法。

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