ROS‐Responsive Poly(α‐l‐lysine)‐Based Nanoparticles Loaded with Doxycycline Combat Oxidative Stress and Bacterial Infection

Author:

Wang Yuanchao1,Li Ying1,Liu Wen1,Li Chen2,Duo Xinghong2,Meng Xiangyan3,Feng Yakai145ORCID

Affiliation:

1. School of Chemical Engineering and Technology Tianjin University Yaguan Road 135 Tianjin 300350 P. R. China

2. School of Chemistry and Chemical Engineering Qinghai University for Nationalities Bayizhonglu 3 Xining Qinghai 810007 P. R. China

3. Institute of Disaster and Emergency Medicine Tianjin University Weijin Road 92 Tianjin 300072 P. R. China

4. Frontiers Science Center for Synthetic Biology Tianjin University Weijin Road 92 Tianjin 300072 P. R. China

5. Key Laboratory of Systems Bioengineering (Ministry of Education) Tianjin University Weijin Road 92 Tianjin 300072 P. R. China

Abstract

AbstractBacterial pneumonia is one of the major threats in clinical practice, and the reactive oxygen species (ROS) generated at the infection site can exacerbate the damage. Currently, conventional antibiotic therapies have low utilization, and their excessive use can result in substantial toxicity. Nanocarrier systems provide an ideal approach for treating bacterial infection by facilitating more efficient utilization of antibiotics. In this study, the ROS‐responsive amphiphilic nanoparticles (NPs) are developed and used to encapsulate the antibiotic doxycycline (DOXY) to achieve antibacterial and antioxidant functionalities. The NPs are prepared from poly(α‐l‐lysine) (α‐PLL) and phenylboronic acid pinacol ester simultaneously conjugated carbonyldiimidazole (abbreviated as CDIPB). The phenylboronic acid ester groups on CDIPB could react with excessive ROS to suppress oxidative damage at the infection site. The ROS‐responsive degradation of CDIPB also facilitates the rapid release of internal DOXY, effectively killing the accumulated bacteria. Additionally, in vitro cell experiments demonstrate the good biocompatibility of the NPs. These results suggest that the ROS‐responsive amphiphilic nanoparticles can serve as a novel nanoplatform for the treatment of bacterial pneumonia.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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