Hydrogel delivery of lysostaphin eliminates orthopedic implant infection by and supports fracture healing.
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2018
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Abstract
Orthopedic implant infections are a significant clinical problem, with current therapies limited to surgical debridement and systemic antibiotic regimens. Lysostaphin is a bacteriolytic enzyme with high antistaphylococcal activity. We engineered a lysostaphin-delivering injectable PEG hydrogel to treat infections in bone fractures. The injectable hydrogel formulation adheres to exposed tissue and fracture surfaces, ensuring efficient, local delivery of lysostaphin. Lysostaphin encapsulation within this synthetic hydrogel maintained enzyme stability and activity. Lysostaphin-delivering hydrogels exhibited enhanced antibiofilm activity compared with soluble lysostaphin. Lysostaphin-delivering hydrogels eradicated infection and outperformed prophylactic antibiotic and soluble lysostaphin therapy in a murine model of femur fracture. Analysis of the local inflammatory response to infections treated with lysostaphin-delivering hydrogels revealed indistinguishable differences in cytokine secretion profiles compared with uninfected fractures, demonstrating clearance of bacteria and associated inflammation. Importantly, infected fractures treated with lysostaphin-delivering hydrogels fully healed by 5 wk with bone formation and mechanical properties equivalent to those of uninfected fractures, whereas fractures treated without the hydrogel carrier were equivalent to untreated infections. Finally, lysostaphin-delivering hydrogels eliminate methicillin-resistant infections, supporting this therapy as an alternative to antibiotics. These results indicate that lysostaphin-delivering hydrogels effectively eliminate orthopedic infections while simultaneously supporting fracture repair.Reference Key |
johnson2018hydrogelproceedings
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Authors | Johnson, Christopher T;Wroe, James A;Agarwal, Rachit;Martin, Karen E;Guldberg, Robert E;Donlan, Rodney M;Westblade, Lars F;García, Andrés J; |
Journal | Proceedings of the National Academy of Sciences of the United States of America |
Year | 2018 |
DOI | 10.1073/pnas.1801013115 |
URL | |
Keywords | Keywords not found |
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