Guang'anmen Hospital, China Academy of Chinese Medical Science, Beijing, 100053, China.
Xiyuan Hospital, China Academy of Chinese Medical Science, Beijing, 100091, China.
J Ethnopharmacol. 2025 Jan 30;337(Pt 1):118738. doi: 10.1016/j.jep.2024.118738. Epub 2024 Aug 31.
Dehydrocorydaline (DHC), an active component of Corydalis yanhusuo (Y.H. Chou & Chun C. Hsu) W.T. Wang ex Z.Y. Su & C.Y. Wu (Papaveraceae), exhibits protective and pain-relieving effects on coronary heart disease, but the underlying mechanism still remains unknown.
Network pharmacology and experimental validation both in vivo and in vitro were applied to assess whether DHC can treat myocardial ischemia-reperfusion injury (MIRI) by regulating the forkhead box O (FoxO) signalling pathway to inhibit apoptosis.
DHC and MIRI targets were retrieved from various databases. Molecular docking and microscale thermophoresis (MST) determined potential binding affinity. An in vivo mouse model of MIRI was established by ligating the left anterior descending coronary artery. C57BL/6N mice were divided into sham, MIRI, and DHC (intraperitoneal injection of 5 mg/kg DHC) groups. Haematoxylin and eosin, Masson, and immunohistochemical stainings verified DHC treatment effects and the involved signalling pathways. In vitro, H9c2 cells were incubated with DHC and underwent hypoxia/reoxygenation. TUNEL, JC-1, and reactive oxygen species stainings and western blots were used to explore the protective effects of DHC and the underlying mechanisms.
Venny analysis identified 120 common targets from 121 DHC and 23,354 MIRI targets. DHC exhibited high affinity for CCND1, CDK2, and MDM2 (<-7 kcal/mol). In vivo, DHC attenuated decreases in left ventricular ejection fraction and fractional shortening, reduced infarct sizes, and decreased cTnI and lactate dehydrogenase levels. In vitro, DHC alleviated apoptosis and oxidative stress in the hypoxia/reoxygenation model by attenuating ΔΨm disruption; reducing the production of reactive oxygen species; upregulating Bax and CCND1 via the FoxO signalling pathway, as well as cleaved-caspase 8; downregulating the apoptosis-associated proteins Bcl-2, Bid, cleaved-caspase 3, and cleaved-caspase 9; and promoting the phosphorylation of FOXO1A and MDM2.
By upregulating the FoxO signaling pathway to inhibit apoptosis, DHC exerts a cardioprotective effect, which could serve as a potential therapeutic option for MIRI.
延胡索乙素(DHC)是罂粟科紫堇属植物延胡索(Y.H. Chou 和 Chun C. Hsu)W.T. Wang ex Z.Y. Su 和 C.Y. Wu 的一种活性成分,具有保护和缓解冠心病的作用,但作用机制尚不清楚。
应用网络药理学和体内外实验评估 DHC 是否通过调节叉头框 O(FoxO)信号通路抑制细胞凋亡来治疗心肌缺血再灌注损伤(MIRI)。
从各种数据库中检索 DHC 和 MIRI 靶点。分子对接和微量热泳(MST)确定潜在的结合亲和力。通过结扎左前降支冠状动脉建立 MIRI 小鼠模型。将 C57BL/6N 小鼠分为假手术、MIRI 和 DHC(腹腔注射 5mg/kg DHC)组。苏木精和伊红、Masson 和免疫组织化学染色验证 DHC 治疗效果和涉及的信号通路。在体外,用 DHC 孵育 H9c2 细胞并进行缺氧/复氧。TUNEL、JC-1 和活性氧染色和 Western blot 用于探讨 DHC 的保护作用及其潜在机制。
Venny 分析从 121 个 DHC 和 23354 个 MIRI 靶点中确定了 120 个共同靶点。DHC 与 CCND1、CDK2 和 MDM2 具有高亲和力(<-7kcal/mol)。体内,DHC 减轻左心室射血分数和缩短分数的降低,减少梗死面积,降低 cTnI 和乳酸脱氢酶水平。在体外,DHC 通过减轻 ΔΨm 破坏、减少活性氧的产生、上调 FoxO 信号通路以及 Bax 和 CCND1,下调凋亡相关蛋白 Bcl-2、Bid、cleaved-caspase 3 和 cleaved-caspase 9,促进 FOXO1A 和 MDM2 的磷酸化,从而减轻缺氧/复氧模型中的细胞凋亡和氧化应激。
DHC 通过上调 FoxO 信号通路抑制细胞凋亡发挥心脏保护作用,可作为 MIRI 的潜在治疗选择。
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