From the Department of Cardiovascular Medicine (R.K., K.S., N.K., E.A.M., M.A.H.S., J.O., T.S., S.S., M.N., K.N., S.M., H.S.), Sendai, Japan.
Japan Society for the Promotion of Science, Tokyo, Japan (R.K.).
Circ Res. 2019 Jul 19;125(3):309-327. doi: 10.1161/CIRCRESAHA.119.315229. Epub 2019 Jun 14.
Pulmonary arterial hypertension (PAH) is characterized by enhanced proliferation of pulmonary artery smooth muscle cells (PASMCs) accompanying increased production of inflammatory factors and adaptation of the mitochondrial metabolism to a hyperproliferative state. However, all the drugs in clinical use target pulmonary vascular dilatation, which may not be effective for patients with advanced PAH.
We aimed to discover a novel drug for PAH that inhibits PASMC proliferation.
We screened 5562 compounds from original library using high-throughput screening system to discover compounds which inhibit proliferation of PASMCs from patients with PAH (PAH-PASMCs). We found that celastramycin, a benzoyl pyrrole-type compound originally found in a bacteria extract, inhibited the proliferation of PAH-PASMCs in a dose-dependent manner with relatively small effects on PASMCs from healthy donors. Then, we made 25 analogs of celastramycin and selected the lead compound, which significantly inhibited cell proliferation of PAH-PASMCs and reduced cytosolic reactive oxygen species levels. Mechanistic analysis demonstrated that celastramycin reduced the protein levels of HIF-1α (hypoxia-inducible factor 1α), which impairs aerobic metabolism, and κB (nuclear factor-κB), which induces proinflammatory signals, in PAH-PASMCs, leading to reduced secretion of inflammatory cytokine. Importantly, celastramycin treatment reduced reactive oxygen species levels in PAH-PASMCs with increased protein levels of Nrf2 (nuclear factor erythroid 2-related factor 2), a master regulator of cellular response against oxidative stress. Furthermore, celastramycin treatment improved mitochondrial energy metabolism with recovered mitochondrial network formation in PAH-PASMCs. Moreover, these celastramycin-mediated effects were regulated by ZFC3H1 (zinc finger C3H1 domain-containing protein), a binding partner of celastramycin. Finally, celastramycin treatment ameliorated pulmonary hypertension in 3 experimental animal models, accompanied by reduced inflammatory changes in the lungs.
These results indicate that celastramycin ameliorates pulmonary hypertension, reducing excessive proliferation of PAH-PASMCs with less inflammation and reactive oxygen species levels, and recovered mitochondrial energy metabolism. Thus, celastramycin is a novel drug for PAH that targets antiproliferative effects on PAH-PASMCs.
肺动脉高压(PAH)的特征是肺动脉平滑肌细胞(PASMC)的增殖增强,同时伴有炎症因子的产生增加和线粒体代谢向增殖状态的适应。然而,临床使用的所有药物都靶向肺血管扩张,对于晚期 PAH 患者可能效果不佳。
我们旨在发现一种抑制 PASMC 增殖的治疗 PAH 的新药。
我们使用高通量筛选系统从原始文库中筛选了 5562 种化合物,以发现可抑制 PAH 患者 PASMC 增殖的化合物(PAH-PASMCs)。我们发现,从细菌提取物中最初发现的苯甲酰吡咯类化合物 celastramycin 以剂量依赖性方式抑制 PAH-PASMCs 的增殖,对来自健康供体的 PASMCs 的影响相对较小。然后,我们合成了 celastramycin 的 25 种类似物,并选择了一种显著抑制 PAH-PASMCs 细胞增殖和降低胞质活性氧水平的先导化合物。机制分析表明,celastramycin 降低了缺氧诱导因子 1α(HIF-1α)的蛋白水平,HIF-1α 损害有氧代谢,核因子-κB(NF-κB)诱导促炎信号,导致炎性细胞因子分泌减少。重要的是,celastramycin 治疗可降低 PAH-PASMCs 中的活性氧水平,同时增加核因子红细胞 2 相关因子 2(Nrf2)的蛋白水平,Nrf2 是细胞对氧化应激反应的主要调节因子。此外,celastramycin 治疗改善了 PAH-PASMCs 的线粒体能量代谢,恢复了线粒体网络的形成。此外,celastramycin 介导的这些作用受 celastramycin 的结合伴侣 ZFC3H1(锌指 C3H1 结构域蛋白)调节。最后,celastramycin 治疗改善了 3 种实验动物模型的肺动脉高压,同时肺部的炎症变化减少。
这些结果表明,celastramycin 可改善肺动脉高压,减少 PAH-PASMCs 的过度增殖,减少炎症和活性氧水平,并恢复线粒体能量代谢。因此,celastramycin 是一种针对 PAH-PASMCs 抗增殖作用的治疗 PAH 的新型药物。
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