Translational Medicine Federation of Strasbourg (FMTS), CRBS, University of Strasbourg, Team 3072 "Mitochondria, Oxidative Stress and Muscle Protection", 1 Rue Eugène Boeckel, CS 60026, CEDEX 67084 Strasbourg, France.
Physiology and Functional Exploration Unit, University Hospital of Strasbourg, 1 Place de l'Hôpital, CEDEX 67091 Strasbourg, France.
Int J Mol Sci. 2023 May 31;24(11):9572. doi: 10.3390/ijms24119572.
Pulmonary arterial hypertension (PAH) is a rare disease characterized by pulmonary vascular remodeling leading to right heart failure and death. To date, despite the three therapeutic approaches targeting the three major endothelial dysfunction pathways based on the prostacyclin, nitric oxide/cyclic guanosine monophosphate, and endothelin pathways, PAH remains a serious disease. As such, new targets and therapeutic agents are needed. Mitochondrial metabolic dysfunction is one of the mechanisms involved in PAH pathogenesis in part through the induction of a Warburg metabolic state of enhanced glycolysis but also through the upregulation of glutaminolysis, tricarboxylic cycle and electron transport chain dysfunction, dysregulation of fatty acid oxidation or mitochondrial dynamics alterations. The aim of this review is to shed light on the main mitochondrial metabolic pathways involved in PAH and to provide an update on the resulting interesting potential therapeutic perspectives.
肺动脉高压(PAH)是一种罕见的疾病,其特征是肺血管重构导致右心衰竭和死亡。迄今为止,尽管有三种针对前列环素、一氧化氮/环鸟苷酸和内皮素途径的三种主要内皮功能障碍途径的治疗方法,但 PAH 仍然是一种严重的疾病。因此,需要新的靶点和治疗药物。线粒体代谢功能障碍是 PAH 发病机制之一,部分原因是诱导增强糖酵解的瓦伯格代谢状态,但也通过上调谷氨酰胺分解代谢、三羧酸循环和电子传递链功能障碍、脂肪酸氧化失调或线粒体动力学改变。本文旨在阐明参与 PAH 的主要线粒体代谢途径,并提供最新的有趣的潜在治疗前景。
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