Potassium dehydroandrographolide succinate regulates the MyD88/CDH13 signaling pathway to enhance vascular injury-induced pathological vascular remodeling

IF 4 2区 医学 Q1 INTEGRATIVE & COMPLEMENTARY MEDICINE Chinese Journal of Natural Medicines Pub Date : 2024-01-01 DOI:10.1016/S1875-5364(24)60562-5
Qiru GUO , Jiali LI , Zheng WANG , Xiao WU , Zhong JIN , Song ZHU , Hongfei LI , Delai ZHANG , Wangming HU , Huan XU , Lan YANG , Liangqin SHI , Yong WANG
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Abstract

Pathological vascular remodeling is a hallmark of various vascular diseases. Previous research has established the significance of andrographolide in maintaining gastric vascular homeostasis and its pivotal role in modulating endothelial barrier dysfunction, which leads to pathological vascular remodeling. Potassium dehydroandrographolide succinate (PDA), a derivative of andrographolide, has been clinically utilized in the treatment of inflammatory diseases precipitated by viral infections. This study investigates the potential of PDA in regulating pathological vascular remodeling. The effect of PDA on vascular remodeling was assessed through the complete ligation of the carotid artery in C57BL/6 mice. Experimental approaches, including rat aortic primary smooth muscle cell culture, flow cytometry, bromodeoxyuridine (BrdU) incorporation assay, Boyden chamber cell migration assay, spheroid sprouting assay, and Matrigel-based tube formation assay, were employed to evaluate the influence of PDA on the proliferation and motility of smooth muscle cells (SMCs). Molecular docking simulations and co-immunoprecipitation assays were conducted to examine protein interactions. The results revealed that PDA exacerbates vascular injury-induced pathological remodeling, as evidenced by enhanced neointima formation. PDA treatment significantly increased the proliferation and migration of SMCs. Further mechanistic studies disclosed that PDA upregulated myeloid differentiation factor 88 (MyD88) expression in SMCs and interacted with T-cadherin (CDH13). This interaction augmented proliferation, migration, and extracellular matrix deposition, culminating in pathological vascular remodeling. Our findings underscore the critical role of PDA in the regulation of pathological vascular remodeling, mediated through the MyD88/CDH13 signaling pathway.

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脱氢穿心莲内酯琥珀酸钾可调节 MyD88/CDH13 信号通路,从而增强血管损伤诱导的病理性血管重塑
病理性血管重塑是各种血管疾病的标志。以往的研究已经证实了穿心莲内酯在维持胃血管稳态方面的重要作用,以及它在调节内皮屏障功能障碍(导致病理性血管重塑)方面的关键作用。脱氢穿心莲内酯琥珀酸钾(PDA)是穿心莲内酯的一种衍生物,已被临床用于治疗由病毒感染引发的炎症性疾病。本研究探讨了 PDA 在调节病理性血管重塑方面的潜力。通过完全结扎 C57BL/6 小鼠的颈动脉来评估 PDA 对血管重塑的影响。实验方法包括大鼠主动脉原代平滑肌细胞培养、流式细胞术、溴脱氧尿苷(BrdU)掺入试验、波伊登室细胞迁移试验、球形萌发试验和基于 Matrigel 的管形成试验,以评估 PDA 对平滑肌细胞(SMC)增殖和运动的影响。研究人员还进行了分子对接模拟和共免疫沉淀试验,以检验蛋白质之间的相互作用。结果表明,PDA 会加剧血管损伤引起的病理重塑,表现为增强了新生血管的形成。PDA 能明显增加 SMC 的增殖和迁移。进一步的机理研究发现,PDA 上调了 SMC 中髓系分化因子 88(MyD88)的表达,并与 T-cadherin(CDH13)相互作用。这种相互作用增强了增殖、迁移和细胞外基质沉积,最终导致病理性血管重塑。我们的发现强调了 PDA 通过 MyD88/CDH13 信号通路在调节病理性血管重塑中的关键作用。
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来源期刊
Chinese Journal of Natural Medicines
Chinese Journal of Natural Medicines INTEGRATIVE & COMPLEMENTARY MEDICINE-PHARMACOLOGY & PHARMACY
CiteScore
7.50
自引率
4.30%
发文量
2235
期刊介绍: The Chinese Journal of Natural Medicines (CJNM), founded and sponsored in May 2003 by China Pharmaceutical University and the Chinese Pharmaceutical Association, is devoted to communication among pharmaceutical and medical scientists interested in the advancement of Traditional Chinese Medicines (TCM). CJNM publishes articles relating to a broad spectrum of bioactive natural products, leading compounds and medicines derived from Traditional Chinese Medicines (TCM). Topics covered by the journal are: Resources of Traditional Chinese Medicines; Interaction and complexity of prescription; Natural Products Chemistry (including structure modification, semi-and total synthesis, bio-transformation); Pharmacology of natural products and prescription (including pharmacokinetics and toxicology); Pharmaceutics and Analytical Methods of natural products.
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