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机械化学重编程界面协调中性粒细胞杀菌活性和细胞凋亡,以预防植入物相关感染。

Mechanochemically Reprogrammed Interface Orchestrates Neutrophil Bactericidal Activity and Apoptosis for Preventing Implant-Associated Infection.

机构信息

Spine Lab, Department of Orthopedic Surgery, The First Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou, 310003, China.

Department of Orthopedics, The First Affiliated Hospital of USTC, Division of Life Sciences and Medicine, University of Science and Technology of China, Hefei, Anhui, 230001, China.

出版信息

Adv Mater. 2024 Apr;36(16):e2311855. doi: 10.1002/adma.202311855. Epub 2024 Jan 2.

Abstract

The onset of implant-associated infection (IAI) triggers a cascade of immune responses, which are initially dominated by neutrophils. Bacterial aggregate formation and hypoxic microenvironment, which occur shortly after implantation, may be two major risk factors that impair neutrophil function and lead to IAI. Here, the implant surface with phytic acid-Zn coordinated TiO nanopillar arrays (PA-Zn@TiNPs) and oxygen self-supporting CaO nanoparticles, named as CPZTs, is mechanochemically reprogrammed. The engineered CPZTs interface integrates multiple properties to inhibit the formation of nascent biofilm, encompassing antibacterial adhesion, mechanobactericidal effect, and chemobiocidal effect. Meanwhile, continuous oxygenation fuels the neutrophils with reactive oxygen species (ROS) for efficient bacterial elimination on the implant surface and inside the neutrophils. Furthermore, this surface modulation strategy accelerates neutrophil apoptosis and promotes M2 macrophage-mediated osteogenesis both in vitro and in a rat model of IAI. In conclusion, targeting neutrophils for immunomodulation is a practical and effective strategy to prevent IAI and promote bone-implant integration.

摘要

植入物相关感染 (IAI) 的发作引发了一系列免疫反应,最初主要由中性粒细胞主导。植入后不久发生的细菌聚集形成和缺氧微环境可能是两个主要的风险因素,会损害中性粒细胞的功能并导致 IAI。在这里,具有植酸-Zn 配位 TiO 纳米柱阵列 (PA-Zn@TiNPs) 和自支撑氧的 CaO 纳米颗粒的植入物表面,被命名为 CPZTs,通过机械化学方法进行了重新编程。工程 CPZTs 界面集成了多种特性来抑制新生生物膜的形成,包括抗菌粘附、机械杀菌作用和化学杀菌作用。同时,持续的供氧为中性粒细胞提供活性氧 (ROS),以有效清除植入物表面和中性粒细胞内的细菌。此外,这种表面调节策略加速了中性粒细胞的凋亡,并促进了体外和 IAI 大鼠模型中 M2 巨噬细胞介导的成骨作用。总之,针对中性粒细胞进行免疫调节是预防 IAI 和促进骨-植入物整合的一种实用且有效的策略。

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