Supramolecular prodrug inspiried by the Rhizoma Coptidis - Fructus Mume herbal pair alleviated inflammatory diseases by inhibiting pyroptosis.

Journal of pharmaceutical analysis Pub Date : 2025-02-01 Epub Date: 2024-07-31 DOI:10.1016/j.jpha.2024.101056
Wenhui Qian, Bei Zhang, Ming Gao, Yuting Wang, Jiachen Shen, Dongbing Liang, Chao Wang, Wei Wei, Xing Pan, Qiuying Yan, Dongdong Sun, Dong Zhu, Haibo Cheng
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Abstract

Sustained inflammatory responses are closely related to various severe diseases, and inhibiting the excessive activation of inflammasomes and pyroptosis has significant implications for clinical treatment. Natural products have garnered considerable concern for the treatment of inflammation. Huanglian-Wumei decoction (HLWMD) is a classic prescription used for treating inflammatory diseases, but the necessity of their combination and the exact underlying anti-inflammatory mechanism have not yet been elucidated. Inspired by the supramolecular self-assembly strategy and natural drug compatibility theory, we successfully obtained berberine (BBR)-chlorogenic acid (CGA) supramolecular (BCS), which is an herbal pair from HLWMD. Using a series of characterization methods, we confirmed the self-assembly mechanism of BCS. BBR and CGA were self-assembled and stacked into amphiphilic spherical supramolecules in a 2:1 molar ratio, driven by electrostatic interactions, hydrophobic interactions, and π-π stacking; the hydrophilic fragments of CGA were outside, and the hydrophobic fragments of BBR were inside. This stacking pattern significantly improved the anti-inflammatory performance of BCS compared with that of single free molecules. Compared with free molecules, BCS significantly attenuated the release of multiple inflammatory mediators and lipopolysaccharide (LPS)-induced pyroptosis. Its anti-inflammatory mechanism is closely related to the inhibition of intracellular nuclear factor-kappaB (NF-κB) p65 phosphorylation and the noncanonical pyroptosis signalling pathway mediated by caspase-11.

以黄连-乌梅对为灵感的超分子前药通过抑制焦亡来减轻炎性疾病。
持续的炎症反应与各种严重疾病密切相关,抑制炎性小体的过度激活和焦亡对临床治疗具有重要意义。天然产物在治疗炎症方面引起了相当大的关注。黄连乌梅汤是治疗炎性疾病的经典方剂,但其联用的必要性及确切的抗炎机制尚不清楚。受超分子自组装策略和天然药物相容性理论的启发,我们成功地获得了小檗碱(BBR)-绿原酸(CGA)超分子(BCS),这是一个来自HLWMD的草药对。通过一系列表征方法,我们证实了BCS的自组装机制。在静电相互作用、疏水相互作用和π-π堆叠的驱动下,BBR和CGA以2:1的摩尔比自组装并堆叠成两亲性球形超分子;CGA的亲水片段在外侧,BBR的疏水片段在内侧。与单一自由分子相比,这种堆叠模式显著提高了BCS的抗炎性能。与游离分子相比,BCS可显著减少多种炎症介质的释放和脂多糖(LPS)诱导的焦亡。其抗炎机制与抑制细胞内核因子-κB (NF-κB) p65磷酸化及caspase-11介导的非典型焦亡信号通路密切相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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