拓扑工程超分子环脂纳米颗粒：用于吸入联合治疗的定制递送系统

IF 14.4 1区化学 Q1 CHEMISTRY, MULTIDISCIPLINARY

Journal of the American Chemical Society Pub Date : 2025-04-28 DOI:10.1021/jacs.5c03033

Meiqi Cheng, Zheng Jiao, Jiaqi Lei, Mengyao Li, Kai Yang, Shaolong Qi, Xinyang Yu, Yangfan Wang, Li-Tang Yan, Guocan Yu

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引用次数: 0

摘要

脂质纳米颗粒（LNPs）在核酸疗法和疫苗的开发中显示出巨大的潜力；然而，内体逃逸效率和生理稳定性不理想，阻碍了其临床应用。在此，我们设计并合成了一种新颖的拓扑工程环糊精核脂质（环脂），具有7个叔胺基，7个仲胺基和14个疏水烷基尾，以制备双组分超分子环脂纳米颗粒（CNPs）。得益于其锥形结构，环脂促进了内体膜从片层期过渡到不稳定的六方II期，从而促进了膜的不稳定和CNPs的内体逃逸。此外，高密度的可电离位点增强了CNPs与RNA的结合能力，多条疏水烷基链增强了CNPs的稳定性，从而保证了其体内循环的稳定性。有趣的是，环脂的空腔使吡非尼酮（PFD，一种抗纤维化药物）通过宿主-客体相互作用被包封，为协同治疗提供了一种很有前景的策略。合理优化CNPs的成分和理化性质可显著提高黏液的渗透能力，从而提高其在肺部的生物利用度，避免对其他器官产生不良的副作用。利用其实现生理稳定性、粘液渗透和内体逃逸的特殊能力，靶向热休克蛋白47 （siHsp47）和PFD的siRNA由CNPs （CNPs@siHsp47/PFD）共同递送，用于治疗肺纤维化。CNPs@siHsp47/PFD协同缓解肺纤维化，达到与健康小鼠相当的治疗结果，突出了CNPs作为下一代药物和基因联合治疗的传递平台的突出潜力。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Topologically Engineered Supramolecular Cyclolipid Nanoparticles: A Custom-Tailored Delivery System for Inhaled Combination Therapy

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Topologically Engineered Supramolecular Cyclolipid Nanoparticles: A Custom-Tailored Delivery System for Inhaled Combination Therapy

Lipid nanoparticles (LNPs) have shown promising potential in the development of nucleic acid therapeutics and vaccines; however, unsatisfactory endosomal escape efficiency and physiological stability hinder their clinical applications. Herein, we design and synthesize a novel topologically engineered cyclodextrin-cored lipid (cyclolipid) featuring seven tertiary amine groups, seven secondary amine groups, and 14 hydrophobic alkyl tails to fabricate two-component supramolecular cyclolipid nanoparticles (CNPs). Benefiting from its cone-shaped structure, the cyclolipid facilitates the transition of endosomal membranes from the lamellar phase to the unstable hexagonal II phase, thereby promoting membrane destabilization and endosomal escape of CNPs. Additionally, the high density of ionizable sites enhances the binding capacity with RNA, while multiple hydrophobic alkyl chains strengthen the stability of CNPs, thus guaranteeing the in vivo circulation stability. Interestingly, the cavity of the cyclolipid enables the encapsulation of pirfenidone (PFD, an antifibrotic drug) through host–guest interactions, offering a promising strategy for synergistic therapy. Rationally optimizing the components and physicochemical properties of CNPs dramatically promotes mucus penetration capability, thereby enhancing their bioavailability in the lungs and avoiding unwanted side effects toward other organs. Leveraging their exceptional ability for achieving physiological stability, mucus penetration, and endosomal escape, siRNA targeting heat shock protein 47 (siHsp47) and PFD are codelivered by CNPs (CNPs@siHsp47/PFD) for the treatment of pulmonary fibrosis. CNPs@siHsp47/PFD synergistically alleviates pulmonary fibrosis, achieving therapeutic outcomes comparable to those of healthy mice, highlighting the outstanding potential of CNPs as the next-generation delivery platform for drug and gene combination therapy.

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来源期刊

Journal of the American Chemical Society 化学-化学综合

CiteScore

24.40

自引率

6.00%

发文量

2398

审稿时长

1.6 months

期刊介绍： The flagship journal of the American Chemical Society, known as the Journal of the American Chemical Society (JACS), has been a prestigious publication since its establishment in 1879. It holds a preeminent position in the field of chemistry and related interdisciplinary sciences. JACS is committed to disseminating cutting-edge research papers, covering a wide range of topics, and encompasses approximately 19,000 pages of Articles, Communications, and Perspectives annually. With a weekly publication frequency, JACS plays a vital role in advancing the field of chemistry by providing essential research.