Department of Pulmonary and Critical Care Medicine, The Affiliated Hospital of Inner Mongolia Medical University, Hohhot, China.
State Key Laboratory of Respiratory Disease, National Clinical Research Center for Respiratory Disease, Guangdong Key Laboratory of Vascular Disease, Guangzhou Institute of Respiratory Health, The First Affiliated Hospital of Guangzhou Medical University, Guangzhou, China.
Am J Physiol Cell Physiol. 2023 Oct 1;325(4):C1058-C1072. doi: 10.1152/ajpcell.00286.2023. Epub 2023 Sep 4.
Previous studies have reported the beneficial role of Aloperine (ALO), an active vasodilator purified from the seeds and leaves of the herbal plant L., on experimental pulmonary hypertension (PH); however, detailed mechanisms remain unclear. In this study, monocrotaline-induced PH (MCT-PH) rat model and primarily cultured rat distal pulmonary arterial smooth muscle cells (PASMCs) were used to investigate the mechanisms of ALO on experimental PH, pulmonary vascular remodeling, and excessive proliferation of PASMCs. Results showed that first, ALO significantly prevented the disease development of MCT-PH by inhibiting right ventricular systolic pressure (RVSP) and right ventricular hypertrophy indexed by the Fulton Index, normalizing the pulmonary arterials (PAs) remodeling and improving the right ventricular function indexed by transthoracic echocardiography. ALO inhibited the excessive proliferation of both PAs and PASMCs. Then, isometric tension measurements showed vasodilation of ALO on precontracted PAs isolated from both control and MCT-PH rats via activating the KCNQ channel, which was blocked by specific KCNQ potassium channel inhibitor linopirdine. Moreover, by using immunofluorescence staining and nuclear/cytosol fractionation, we further observed that ALO significantly enhanced the PPARγ nuclear translocation and activation in PASMCs. Transcriptome analyses also revealed activated PPARγ signaling and suppressed calcium regulatory pathway in lungs from MCT-PH rats treated with ALO. In summary, ALO could attenuate MCT-PH through both transient vasodilation of PAs and chronic activation of PPARγ signaling pathway, which exerted antiproliferative roles on PASMCs and remodeled PAs. Aloperine attenuates monocrotaline-induced pulmonary hypertension (MCT-PH) in rats by inhibiting the pulmonary vascular remodeling and proliferation of pulmonary arterial smooth muscle cells (PASMCs). In mechanism, Aloperine not only exerts a transient KCNQ-dependent vasodilation in precontracted pulmonary arteries (PAs) from both control and MCT-PH rats but also activates PPARγ nuclear translocation and signaling transduction in PASMCs, which chronically inhibits the calcium regulatory pathway and proliferation of PASMCs.
先前的研究报告表明,从草药 种子和叶子中纯化出的活性血管扩张剂阿罗品(ALO)对实验性肺动脉高压(PH)具有有益作用;然而,详细的机制仍不清楚。在这项研究中,使用野百合碱诱导的 PH(MCT-PH)大鼠模型和原代培养的大鼠远端肺动脉平滑肌细胞(PASMCs)来研究 ALO 对实验性 PH、肺血管重构和 PASMCs 过度增殖的作用机制。结果表明,首先,ALO 通过抑制右心室收缩压(RVSP)和富尔顿指数(Fulton Index)指数化的右心室肥厚,使肺动脉(PAs)重构正常化,并改善经胸超声心动图指数化的右心室功能,显著预防 MCT-PH 的疾病发展。ALO 抑制了 PAs 和 PASMCs 的过度增殖。然后,等长张力测量显示,ALO 对来自对照和 MCT-PH 大鼠的预收缩 PAs 具有血管扩张作用,这是通过激活 KCNQ 通道实现的,而特定的 KCNQ 钾通道抑制剂林诺吡啶则阻断了这一作用。此外,通过免疫荧光染色和核/胞浆分离,我们进一步观察到 ALO 显著增强了 PASMCs 中 PPARγ 的核易位和激活。转录组分析还揭示了 ALO 处理的 MCT-PH 大鼠肺中激活的 PPARγ 信号通路和抑制的钙调节途径。总之,ALO 通过 PAs 的短暂血管扩张和慢性激活 PPARγ 信号通路来减轻 MCT-PH,对 PASMCs 发挥抗增殖作用,并重塑 PAs。阿罗品通过抑制肺血管重构和肺动脉平滑肌细胞(PASMCs)增殖来减轻野百合碱诱导的肺动脉高压(MCT-PH)。在机制上,阿罗品不仅在来自对照和 MCT-PH 大鼠的预收缩肺动脉(PAs)中发挥短暂的 KCNQ 依赖性血管扩张作用,还在 PASMCs 中激活 PPARγ 核易位和信号转导,慢性抑制 PASMCs 的钙调节途径和增殖。
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