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具有卓越多酶活性和近红外二区响应性的新型铜基单原子纳米酶用于对抗深部组织感染

Alternative Copper-Based Single-Atom Nanozyme with Superior Multienzyme Activities and NIR-II Responsiveness to Fight against Deep Tissue Infections.

作者信息

Bai Jiaxiang, Feng Yonghai, Li Wenming, Cheng Zerui, Rosenholm Jessica M, Yang Huilin, Pan Guoqing, Zhang Hongbo, Geng Dechun

机构信息

Department of Orthopedic Surgery, Orthopedic Institute, The First Affiliated Hospital, Medical College, Soochow University, Suzhou, Jiangsu 215006, P. R. China.

Institute for Advanced Materials, School of Materials Science and Engineering, Jiangsu University, Zhenjiang, Jiangsu 212013, P. R. China.

出版信息

Research (Wash D C). 2023;6:0031. doi: 10.34133/research.0031. Epub 2023 Jan 13.

Abstract

Nanozymes are considered to represent a new era of antibacterial agents, while their antibacterial efficiency is limited by the increasing tissue depth of infection. To address this issue, here, we report a copper and silk fibroin (Cu-SF) complex strategy to synthesize alternative copper single-atom nanozymes (SAzymes) with atomically dispersed copper sites anchored on ultrathin 2D porous N-doped carbon nanosheets (CuN -CNS) and tunable N coordination numbers in the CuN sites ( = 2 or 4). The CuN -CNS SAzymes inherently possess triple peroxidase (POD)-, catalase (CAT)-, and oxidase (OXD)-like activities, facilitating the conversion of HO and O into reactive oxygen species (ROS) through parallel POD- and OXD-like or cascaded CAT- and OXD-like reactions. Compared to CuN-CNS, tailoring the N coordination number from 2 to 4 endows the SAzyme (CuN-CNS) with higher multienzyme activities due to its superior electron structure and lower energy barrier. Meanwhile, CuN -CNS display strong absorption in the second near-infrared (NIR-II) biowindow with deeper tissue penetration, offering NIR-II-responsive enhanced ROS generation and photothermal treatment in deep tissues. The in vitro and in vivo results demonstrate that the optimal CuN-CNS can effectively inhibit multidrug-resistant bacteria and eliminate stubborn biofilms, thus exhibiting high therapeutic efficacy in both superficial skin wound and deep implant-related biofilm infections.

摘要

纳米酶被认为代表了抗菌剂的新时代,但其抗菌效率受到感染组织深度增加的限制。为了解决这个问题,在此我们报告一种铜与丝素蛋白(Cu-SF)复合策略,以合成替代性的铜单原子纳米酶(SAzymes),其具有锚定在超薄二维多孔氮掺杂碳纳米片(CuN-CNS)上的原子分散铜位点以及CuN位点中可调节的N配位数(=2或4)。CuN-CNS SAzymes固有地具有三重类过氧化物酶(POD)、类过氧化氢酶(CAT)和类氧化酶(OXD)活性,通过平行的类POD和类OXD反应或级联的类CAT和类OXD反应促进HO和O转化为活性氧(ROS)。与CuN-CNS相比,将N配位数从2调整为4使SAzyme(CuN-CNS)具有更高的多酶活性,这归因于其优越的电子结构和更低的能垒。同时,CuN-CNS在具有更深组织穿透性的第二近红外(NIR-II)生物窗口中表现出强烈吸收,在深部组织中提供NIR-II响应增强的ROS生成和光热治疗。体外和体内结果表明,最佳的CuN-CNS能够有效抑制多重耐药细菌并消除顽固生物膜,从而在浅表皮肤伤口和深部植入相关生物膜感染中均表现出高治疗效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6926/10076008/c1f516b2d8e3/research.0031.fig.001.jpg

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