Department of Cardiovascular and Metabolic Sciences, Cleveland Clinic, 9500 Euclid Avenue, M/S ND50, Cleveland, OH, 44195, USA.
Proteomics Research Core Services, Lerner Research Institute, Cleveland Clinic, Cleveland, OH, 44195, USA.
Pflugers Arch. 2021 Mar;473(3):461-475. doi: 10.1007/s00424-021-02514-5. Epub 2021 Jan 16.
Atrial fibrillation (AF) is strongly associated with risk of stroke and heart failure. AF promotes atrial remodeling that increases risk of stroke due to left atrial thrombogenesis, and increases energy demand to support high rate electrical activity and muscle contraction. While many transcriptomic studies have assessed AF-related changes in mRNA abundance, fewer studies have assessed proteomic changes. We performed a proteomic analysis on left atrial appendage (LAA) tissues from 12 patients with a history of AF undergoing elective surgery; atrial rhythm was documented at time of surgery. Proteomic analysis was performed using liquid chromatography with mass spectrometry (LC/MS-MS). Data-dependent analysis identified 3090 unique proteins, with 408 differentially expressed between sinus rhythm and AF. Ingenuity Pathway Analysis of differentially expressed proteins identified mitochondrial dysfunction, oxidative phosphorylation, and sirtuin signaling among the most affected pathways. Increased abundance of electron transport chain (ETC) proteins in AF was accompanied by decreased expression of ETC complex assembly factors, tricarboxylic acid cycle proteins, and other key metabolic modulators. Discordant changes were also evident in the contractile unit with both up and downregulation of key components. Similar pathways were affected in a comparison of patients with a history of persistent vs. paroxysmal AF, presenting for surgery in sinus rhythm. Together, these data suggest that while the LAA attempts to meet the energetic demands of AF, an uncoordinated response may reduce ATP availability, contribute to tissue contractile and electrophysiologic heterogeneity, and promote a progression of AF from paroxysmal episodes to development of a substrate amenable to persistent arrhythmia.
心房颤动(AF)与中风和心力衰竭的风险密切相关。AF 可促进左心房血栓形成,增加中风风险,并增加能量需求以支持高心率电活动和肌肉收缩,从而导致心房重构。虽然许多转录组研究已经评估了与 AF 相关的 mRNA 丰度变化,但研究蛋白质组变化的研究较少。我们对 12 例因 AF 而接受择期手术的患者的左心耳(LAA)组织进行了蛋白质组分析;手术时记录了心房节律。使用液相色谱-质谱联用(LC/MS-MS)进行蛋白质组分析。数据依赖性分析确定了 3090 种独特的蛋白质,其中窦性节律和 AF 之间有 408 种差异表达。差异表达蛋白的 IPA 分析确定了线粒体功能障碍、氧化磷酸化和 Sirtuin 信号转导是受影响最严重的途径之一。AF 中电子传递链(ETC)蛋白的丰度增加伴随着 ETC 复合物组装因子、三羧酸循环蛋白和其他关键代谢调节剂的表达降低。收缩单位也出现了明显的不协调变化,关键成分既有上调也有下调。在窦性节律下接受手术的持续性 AF 与阵发性 AF 患者的比较中,也存在相似的途径受到影响。这些数据表明,尽管 LAA 试图满足 AF 的能量需求,但不协调的反应可能会降低 ATP 可用性,导致组织收缩和电生理异质性,并促进 AF 从阵发性发作向易于持续性心律失常的基质发展。