Institute of Cardiovascular and Metabolic Research, School of Biological Sciences, University of Reading, Reading, Berkshire, United Kingdom.
Am J Physiol Heart Circ Physiol. 2013 May 15;304(10):H1302-13. doi: 10.1152/ajpheart.00004.2013. Epub 2013 Mar 15.
Prolonged hemodynamic load as a result of hypertension eventually leads to maladaptive cardiac adaptation and heart failure. The signaling pathways that underlie these changes are still poorly understood. The adaptive response to mechanical load is mediated by mechanosensors that convert the mechanical stimuli into a biological response. We examined the effect of cyclic mechanical stretch on myocyte adaptation using neonatal rat ventricular myocytes with 10% (adaptive) or 20% (maladaptive) maximum strain at 1 Hz for 48 h to mimic in vivo mechanical stress. Cells were also treated with and without nitro-L-arginine methyl ester (L-NAME), a general nitric oxide synthase (NOS) inhibitor to suppress NO production. Maladaptive 20% mechanical stretch led to a significant loss of intact sarcomeres that were rescued by L-NAME (P < 0.05; n ≥ 5 cultures). We hypothesized that the mechanism was through NO-induced alteration of myocyte gene expression. L-NAME upregulated the mechanosensing proteins muscle LIM protein (MLP; by 100%; P < 0.05; n = 5 cultures) and lipoma preferred partner (LPP), a novel cardiac protein (by 80%; P < 0.05; n = 4 cultures). L-NAME also significantly altered the subcellular localization of LPP and MLP in a manner that favored growth and adaptation. These findings suggest that NO participates in stretch-mediated adaptation. The use of isoform selective NOS inhibitors indicated a complex interaction between inducible NOS and neuronal NOS isoforms regulate gene expression. LPP knockdown by small intefering RNA led to formation of α-actinin aggregates and Z bodies showing that myofibrillogenesis was impaired. There was an upregulation of E3 ubiquitin ligase (MUL1) by 75% (P < 0.05; n = 5 cultures). This indicates that NO contributes to stretch-mediated adaptation via the upregulation of proteins associated with mechansensing and myofibrillogenesis, thereby presenting potential therapeutic targets during the progression of heart failure.
长期的高血压导致的血流动力学负荷最终导致适应性心脏适应和心力衰竭。这些变化背后的信号通路仍知之甚少。机械负荷的适应性反应是由机械感受器介导的,机械感受器将机械刺激转化为生物反应。我们使用 10%(适应性)或 20%(适应性不良)最大应变的新生大鼠心室肌细胞,以 1 Hz 进行 48 小时的周期性机械拉伸,模拟体内机械应激,研究机械拉伸对心肌细胞适应性的影响。细胞还分别用和不用硝基-L-精氨酸甲酯(L-NAME)处理,L-NAME 是一种通用的一氧化氮合酶(NOS)抑制剂,可抑制 NO 的产生。适应性不良的 20%机械拉伸导致完整的肌节明显丧失,L-NAME 可挽救这一损失(P < 0.05;n ≥ 5 个培养物)。我们假设机制是通过 NO 诱导的心肌细胞基因表达改变。L-NAME 上调了机械感受器蛋白肌肉 LIM 蛋白(MLP;增加 100%;P < 0.05;n = 5 个培养物)和脂联素首选伴侣(LPP),一种新型的心脏蛋白(增加 80%;P < 0.05;n = 4 个培养物)。L-NAME 还显著改变了 LPP 和 MLP 的亚细胞定位,有利于生长和适应。这些发现表明,NO 参与了拉伸介导的适应。同工酶选择性 NOS 抑制剂的使用表明,诱导型 NOS 和神经元 NOS 同工酶之间存在复杂的相互作用,调节基因表达。通过小干扰 RNA 敲低 LPP 导致肌联蛋白聚集体和 Z 体的形成,表明肌原纤维发生受损。E3 泛素连接酶(MUL1)上调 75%(P < 0.05;n = 5 个培养物)。这表明,NO 通过上调与机械感受器和肌原纤维发生相关的蛋白质来促进拉伸介导的适应,从而为心力衰竭进展过程中的治疗靶点提供了潜在的可能性。
