Department of Biomedical Engineering (V.J., O.H., D.A.K.), Johns Hopkins School of Medicine, Baltimore, MD.
Division of Cardiology, Department of Medicine (V.J., A.J.F., I.M.C.S., M.M., D.A.K., S.H.), Johns Hopkins School of Medicine, Baltimore, MD.
Circulation. 2023 Jun 20;147(25):1919-1932. doi: 10.1161/CIRCULATIONAHA.123.064717. Epub 2023 May 17.
Right ventricular (RV) contractile dysfunction commonly occurs and worsens outcomes in patients with heart failure with reduced ejection fraction and pulmonary hypertension (HFrEF-PH). However, such dysfunction often goes undetected by standard clinical RV indices, raising concerns that they may not reflect aspects of underlying myocyte dysfunction. We thus sought to characterize RV myocyte contractile depression in HFrEF-PH, identify those components reflected by clinical RV indices, and uncover underlying biophysical mechanisms.
Resting, calcium-, and load-dependent mechanics were prospectively studied in permeabilized RV cardiomyocytes isolated from explanted hearts from 23 patients with HFrEF-PH undergoing cardiac transplantation and 9 organ donor controls.
Unsupervised machine learning using myocyte mechanical data with the highest variance yielded 2 HFrEF-PH subgroups that in turn mapped to patients with decompensated or compensated clinical RV function. This correspondence was driven by reduced calcium-activated isometric tension in decompensated clinical RV function, whereas surprisingly, many other major myocyte contractile measures including peak power and myocyte active stiffness were similarly depressed in both groups. Similar results were obtained when subgroups were first defined by clinical indices, and then myocyte mechanical properties in each group compared. To test the role of thick filament defects, myofibrillar structure was assessed by x-ray diffraction of muscle fibers. This revealed more myosin heads associated with the thick filament backbone in decompensated clinical RV function, but not compensated clinical RV function, as compared with controls. This corresponded to reduced myosin ATP turnover in decompensated clinical RV function myocytes, indicating less myosin in a crossbridge-ready disordered-relaxed (DRX) state. Altering DRX proportion (%DRX) affected peak calcium-activated tension in the patient groups differently, depending on their basal %DRX, highlighting potential roles for precision-guided therapeutics. Last, increasing myocyte preload (sarcomere length) increased %DRX 1.5-fold in controls but only 1.2-fold in both HFrEF-PH groups, revealing a novel mechanism for reduced myocyte active stiffness and by extension Frank-Starling reserve in human heart failure.
Although there are many RV myocyte contractile deficits in HFrEF-PH, commonly used clinical indices only detect reduced isometric calcium-stimulated force, which is related to deficits in basal and recruitable %DRX myosin. Our results support use of therapies to increase %DRX and enhance length-dependent recruitment of DRX myosin heads in such patients.
右心室(RV)收缩功能障碍在射血分数降低的心力衰竭伴肺动脉高压(HFrEF-PH)患者中很常见且会使预后恶化。然而,标准的临床 RV 指数往往无法检测到这种功能障碍,这引发了人们的担忧,即它们可能无法反映潜在的心肌细胞功能障碍。因此,我们试图描述 HFrEF-PH 中的 RV 心肌细胞收缩抑制,确定那些可以通过临床 RV 指数反映的成分,并揭示潜在的生物物理机制。
前瞻性研究了 23 例接受心脏移植的 HFrEF-PH 患者和 9 例器官捐献对照者的 RV 心肌细胞分离的通透性 RV 心肌细胞的静息、钙依赖性和负荷依赖性力学。
使用具有最高方差的心肌细胞力学数据进行无监督机器学习,得出了 2 个 HFrEF-PH 亚组,进而映射到 RV 功能失代偿或代偿的临床 RV 功能患者。这种对应关系是由失代偿临床 RV 功能中钙激活等长张力降低引起的,而令人惊讶的是,两组的许多其他主要心肌细胞收缩测量值,包括峰值功率和心肌细胞主动硬度,都同样降低。当首先根据临床指数定义亚组,然后比较每组的心肌细胞力学特性时,也得到了类似的结果。为了测试厚丝缺陷的作用,通过肌肉纤维的 X 射线衍射评估肌节结构。与对照组相比,在失代偿临床 RV 功能中,发现更多的肌球蛋白头与厚丝主干相关,但在代偿临床 RV 功能中没有。这与失代偿临床 RV 功能心肌细胞中肌球蛋白 ATP 周转率降低相对应,表明肌球蛋白处于一个交联准备好的无序松弛(DRX)状态的比例减少。改变 DRX 比例(%DRX)对患者组的峰值钙激活张力有不同的影响,这取决于它们的基础%DRX,这突出了精准治疗的潜在作用。最后,增加心肌细胞预负荷(肌节长度)使对照组的%DRX 增加了 1.5 倍,但在两组 HFrEF-PH 中仅增加了 1.2 倍,这揭示了一种新的机制,用于减少人类心力衰竭中的心肌细胞主动硬度和由此产生的 Frank-Starling 储备。
尽管 HFrEF-PH 中有许多 RV 心肌细胞收缩缺陷,但常用的临床指数仅检测到等长钙刺激力降低,这与基础和可募集的%DRX 肌球蛋白缺陷有关。我们的研究结果支持使用增加%DRX 和增强 DRX 肌球蛋白头的长度依赖性募集的治疗方法来治疗此类患者。
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