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基于杂化细胞膜囊泡伪装的光响应多效纳米武器用于铜绿假单胞菌感染肺炎和创伤的高效抗菌治疗

Photoresponsive Multirole Nanoweapon Camouflaged by Hybrid Cell Membrane Vesicles for Efficient Antibacterial Therapy of Pseudomonas aeruginosa-Infected Pneumonia and Wound.

机构信息

State Key Laboratory of Natural Medicines, Department of Pharmaceutics, School of Pharmacy, China Pharmaceutical University, Nanjing, 211198, P. R. China.

NMPA Key Laboratory for Research and Evaluation of Cosmetics, China Pharmaceutical University, Nanjing, 211198, P. R. China.

出版信息

Adv Sci (Weinh). 2024 Sep;11(35):e2403101. doi: 10.1002/advs.202403101. Epub 2024 Jul 15.

Abstract

Exploring effective antibacterial approaches for targeted treatment of pathogenic bacterial infections with reduced drug resistance is of great significance. Combinational treatment modality that leverages different therapeutic components can improve the overall effectiveness and minimize adverse effects, thus displaying considerable potential against bacterial infections. Herein, red blood cell membrane fuses with macrophage membrane to develop hybrid cell membrane shell, which further camouflages around drug-loaded liposome to fabricate biomimetic liposome (AB@LRM) for precise antibacterial therapy. Specifically, photoactive agent black phosphorus quantum dots (BPQDs) and classical antibiotics amikacin (AM) are loaded in AB@LRM to accurately target the inflammatory sites through the guidance of macrophage membrane and long residence capability of red blood cell membrane, eventually exerting efficacious antibacterial activities. Besides, due to the excellent photothermal and photodynamic properties, BPQDs act as an efficient antibacterial agent when exposed to near-infrared laser irradiation, dramatically increasing the sensitivity of bacteria to antibiotics. Consequently, the synergistic sterilizing effect produced by AB@LRM further restricts bacterial resistance. Upon laser irradiation, AB@LRM shows superior anti-inflammatory and antibacterial properties in models of P. aeruginosa-infected pneumonia and wounds. Hence, this light-activatable antibacterial nanoplatform with good biocompatibility presents great potential to advance the clinical development in the treatment of bacterial infections.

摘要

探索针对致病性细菌感染的有效抗菌方法,减少耐药性具有重要意义。联合治疗模式利用不同的治疗成分可以提高整体疗效并最小化不良反应,因此对细菌感染具有相当大的潜力。本文中,红细胞膜与巨噬细胞膜融合以开发杂交细胞膜壳,进一步将载药脂质体包裹起来,制备仿生脂质体(AB@LRM),用于精确的抗菌治疗。具体而言,光敏剂黑磷量子点(BPQDs)和经典抗生素阿米卡星(AM)被装载在 AB@LRM 中,通过巨噬细胞膜的指导和红细胞膜的长居留能力准确靶向炎症部位,最终发挥有效的抗菌作用。此外,由于具有优异的光热和光动力特性,BPQDs 在近红外激光照射下可作为有效的抗菌剂,显著提高了细菌对抗生素的敏感性。因此,AB@LRM 产生的协同杀菌作用进一步限制了细菌的耐药性。在激光照射下,AB@LRM 在铜绿假单胞菌感染性肺炎和伤口模型中表现出优异的抗炎和抗菌性能。因此,这种具有良好生物相容性的光激活抗菌纳米平台具有很大的潜力推进细菌感染治疗的临床发展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/61d8/11425291/874e6c3f5b17/ADVS-11-2403101-g006.jpg

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