Antibody-antibiotic conjugate targeted therapy for orthopedic implant-associated intracellular S. aureus infections

金黄色葡萄球菌 微生物学 万古霉素 抗生素 体内 细胞内 细胞内寄生虫 生物膜 免疫系统 生物 化学 免疫学 细菌 生物化学 遗传学 生物技术
作者
Leilei Qin,Ning Hu,Yanhao Zhang,Jianye Yang,Liqun Zhao,Xiaokai Zhang,Yun Yang,Jinyong Zhang,Yinshuang Zou,Keyu Wei,Chen Zhao,Yujian Li,Hao Zeng,Wei Huang,Quanming Zou
出处
期刊:Journal of Advanced Research [Elsevier BV]
卷期号:65: 239-255 被引量:8
标识
DOI:10.1016/j.jare.2023.12.001
摘要

Treating orthopedic implant-associated infections, especially those caused by Staphylococcus aureus (S. aureus), remains a significant challenge. S. aureus has the ability to invade host cells, enabling it to evade both antibiotics and immune responses during infection, which may result in clinical treatment failures. Therefore, it is critical to identify the host cell type of implant-associated intracellular S. aureus infections and to develop a strategy for highly targeted delivery of antibiotics to the host cells. Introduced an antibody-antibiotic conjugate (AAC) for the targeted elimination of intracellular S. aureus. The AAC comprises of a human monoclonal antibody (M0662) directly recognizes the surface antigen of S. aureus, Staphylococcus protein A, which is conjugated with vancomycin through cathepsin-sensitive linkers that are cleavable in the proteolytic environment of the intracellular phagolysosome. AAC, vancomycin and vancomycin combined with AAC were used in vitro intracellular infection and mice implant infection models. We then tested the effect of AAC in vivo and in vivo by fluorescence imaging, in vivo imaging, bacterial quantitative analysis and bacterial biofilm imaging. In vitro, it was observed that AAC captured extracellular S. aureus and co-entered the cells, and subsequently released vancomycin to induce rapid elimination of intracellular S. aureus. In the implant infection model, AAC significantly improved the bactericidal effect of vancomycin. Scanning electron microscopy showed that the application of AAC effectively blocked the formation of bacterial biofilm. Further histochemical and micro-CT analysis showed AAC significantly reduced the level of bone marrow density (BMD) and bone volume fraction (BV/TV) reduction caused by bacterial infection in the distal femur of mice compared to vancomycin treatment alone. The application of AAC in an implant infection model showed that it significantly improved the bactericidal effects of vancomycin and effectively blocked the formation of bacterial biofilms, without apparent toxicity to the host.
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