King's BHF Centre of Research Excellence, London, UK (J.B.-B., M.F., U.M., W.-Y.L., E.E., E.D., M.H., L.E.S., B.S., R.L., F.B., A.M.S., N.C., K.T., A.M.S., M.M.).
Heart and Vascular Center, Department of Cardiology, Semmelweis University, Budapest, Hungary (T.R., L.D., B.M.).
Circulation. 2021 Dec 21;144(25):2021-2034. doi: 10.1161/CIRCULATIONAHA.121.055732. Epub 2021 Nov 22.
Remodeling of the extracellular matrix (ECM) is a hallmark of heart failure (HF). Our previous analysis of the secretome of murine cardiac fibroblasts returned ADAMTS5 (a disintegrin and metalloproteinase with thrombospondin motifs 5) as one of the most abundant proteases. ADAMTS5 cleaves chondroitin sulfate proteoglycans such as versican. The contribution of ADAMTS5 and its substrate versican to HF is unknown.
Versican remodeling was assessed in mice lacking the catalytic domain of ADAMTS5 (Adamts5). Proteomics was applied to study ECM remodeling in left ventricular samples from patients with HF, with a particular focus on the effects of common medications used for the treatment of HF.
Versican and versikine, an ADAMTS-specific versican cleavage product, accumulated in patients with ischemic HF. Versikine was also elevated in a porcine model of cardiac ischemia/reperfusion injury and in murine hearts after angiotensin II infusion. In Adamts5 mice, angiotensin II infusion resulted in an aggravated versican build-up and hyaluronic acid disarrangement, accompanied by reduced levels of integrin β1, filamin A, and connexin 43. Echocardiographic assessment of Adamts5 mice revealed a reduced ejection fraction and an impaired global longitudinal strain on angiotensin II infusion. Cardiac hypertrophy and collagen deposition were similar to littermate controls. In a proteomics analysis of a larger cohort of cardiac explants from patients with ischemic HF (n=65), the use of β-blockers was associated with a reduction in ECM deposition, with versican being among the most pronounced changes. Subsequent experiments in cardiac fibroblasts confirmed that β1-adrenergic receptor stimulation increased versican expression. Despite similar clinical characteristics, patients with HF treated with β-blockers had a distinct cardiac ECM profile.
Our results in animal models and patients suggest that ADAMTS proteases are critical for versican degradation in the heart and that versican accumulation is associated with impaired cardiac function. A comprehensive characterization of the cardiac ECM in patients with ischemic HF revealed that β-blockers may have a previously unrecognized beneficial effect on cardiac chondroitin sulfate proteoglycan content.
细胞外基质(ECM)的重塑是心力衰竭(HF)的标志。我们之前对小鼠心脏成纤维细胞分泌组的分析发现 ADAMTS5(含血栓反应蛋白基序的解整合素金属蛋白酶 5)是最丰富的蛋白酶之一。ADAMTS5 切割软骨素硫酸蛋白聚糖,如 versican。ADAMTS5 及其底物 versican 对 HF 的贡献尚不清楚。
在缺乏 ADAMTS5 催化结构域的小鼠(Adamts5)中评估 versican 重塑。应用蛋白质组学研究心力衰竭患者左心室样本中的 ECM 重塑,特别关注用于治疗 HF 的常见药物的影响。
缺血性 HF 患者的 versican 和 versikine(ADAMTS 特异性 versican 切割产物)积累。心脏缺血/再灌注损伤的猪模型和血管紧张素 II 输注后的小鼠心脏中也升高了 versikine。在 Adamts5 小鼠中,血管紧张素 II 输注导致 versican 积累加剧和透明质酸排列紊乱,同时整合素β1、细丝蛋白 A 和连接蛋白 43 水平降低。Adamts5 小鼠的超声心动图评估显示,血管紧张素 II 输注后射血分数降低,整体纵向应变受损。心脏肥大和胶原蛋白沉积与同窝对照相似。在更大队列的缺血性 HF 心脏标本的蛋白质组学分析中(n=65),β 受体阻滞剂的使用与 ECM 沉积减少相关,versican 是最明显的变化之一。随后在心脏成纤维细胞中的实验证实,β1-肾上腺素能受体刺激增加了 versican 的表达。尽管临床特征相似,但接受β受体阻滞剂治疗的 HF 患者具有独特的心脏 ECM 特征。
我们在动物模型和患者中的结果表明,ADAMTS 蛋白酶对心脏中 versican 的降解至关重要,versican 的积累与心脏功能受损有关。对缺血性 HF 患者心脏 ECM 的全面表征表明,β 受体阻滞剂可能对心脏软骨素硫酸蛋白聚糖含量具有以前未被认识到的有益作用。
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