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健康与疾病中的胆汁酸代谢及信号传导:分子机制与治疗靶点

Bile acid metabolism and signaling in health and disease: molecular mechanisms and therapeutic targets.

作者信息

Fleishman Joshua S, Kumar Sunil

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy and Health Sciences, St. John's University, Queens, NY, USA.

出版信息

Signal Transduct Target Ther. 2024 Apr 26;9(1):97. doi: 10.1038/s41392-024-01811-6.

Abstract

Bile acids, once considered mere dietary surfactants, now emerge as critical modulators of macronutrient (lipid, carbohydrate, protein) metabolism and the systemic pro-inflammatory/anti-inflammatory balance. Bile acid metabolism and signaling pathways play a crucial role in protecting against, or if aberrant, inducing cardiometabolic, inflammatory, and neoplastic conditions, strongly influencing health and disease. No curative treatment exists for any bile acid influenced disease, while the most promising and well-developed bile acid therapeutic was recently rejected by the FDA. Here, we provide a bottom-up approach on bile acids, mechanistically explaining their biochemistry, physiology, and pharmacology at canonical and non-canonical receptors. Using this mechanistic model of bile acids, we explain how abnormal bile acid physiology drives disease pathogenesis, emphasizing how ceramide synthesis may serve as a unifying pathogenic feature for cardiometabolic diseases. We provide an in-depth summary on pre-existing bile acid receptor modulators, explain their shortcomings, and propose solutions for how they may be remedied. Lastly, we rationalize novel targets for further translational drug discovery and provide future perspectives. Rather than dismissing bile acid therapeutics due to recent setbacks, we believe that there is immense clinical potential and a high likelihood for the future success of bile acid therapeutics.

摘要

胆汁酸,曾经被认为仅仅是膳食表面活性剂,现在已成为常量营养素(脂质、碳水化合物、蛋白质)代谢以及全身促炎/抗炎平衡的关键调节因子。胆汁酸代谢和信号通路在预防或(如果异常)诱发心脏代谢、炎症和肿瘤性疾病方面起着关键作用,对健康和疾病有重大影响。目前尚无针对任何受胆汁酸影响疾病的治愈性治疗方法,而最有前景且研发最完善的胆汁酸疗法最近被美国食品药品监督管理局(FDA)否决。在此,我们提供一种关于胆汁酸的自下而上的方法,从机制上解释它们在经典和非经典受体处的生物化学、生理学和药理学。利用这种胆汁酸的机制模型,我们解释异常的胆汁酸生理学如何驱动疾病发病机制,强调神经酰胺合成如何可能作为心脏代谢疾病的一个统一致病特征。我们对现有的胆汁酸受体调节剂进行了深入总结,解释了它们的缺点,并提出了改进方法。最后,我们为进一步的转化药物发现合理化新靶点并提供未来展望。我们认为,不应因近期的挫折而摒弃胆汁酸疗法,胆汁酸疗法具有巨大的临床潜力,未来成功的可能性很大。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9458/11045871/5154b9a09ecd/41392_2024_1811_Fig1_HTML.jpg

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