AI Article Synopsis
- After a tissue injury, inflammatory cells immediately respond to clear debris and manage other cells for repair, but their role can be both beneficial and detrimental.
- This study examines the use of protocells loaded with R848 to reprogram innate immune cells in zebrafish, observing significant changes in inflammatory responses during skin and skeletal repair.
- The research shows that R848-reprogrammed macrophages enhance healing outcomes by improving bactericidal activities and positively influencing processes vital for recovery, with findings also applicable to human macrophages.
Article Abstract
After tissue injury, inflammatory cells are rapidly recruited to the wound where they clear microbes and other debris, and coordinate the behaviour of other cell lineages at the repair site in both positive and negative ways. In this study, we take advantage of the translucency and genetic tractability of zebrafish to evaluate the feasibility of reprogramming innate immune cells in vivo with cargo-loaded protocells and investigate how this alters the inflammatory response in the context of skin and skeletal repair. Using live imaging, we show that protocells loaded with R848 cargo (which targets TLR7 and TLR8 signalling), are engulfed by macrophages resulting in their switching to a pro-inflammatory phenotype and altering their regulation of angiogenesis, collagen deposition and re-epithelialization during skin wound healing, as well as dampening osteoblast and osteoclast recruitment and bone mineralization during fracture repair. For infected skin wounds, R848-reprogrammed macrophages exhibited enhanced bactericidal activities leading to improved healing. We replicated our zebrafish studies in cultured human macrophages, and showed that R848-loaded protocells similarly reprogramme human cells, indicating how this strategy might be used to modulate wound inflammation in the clinic.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11385641 | PMC |
| http://dx.doi.org/10.1242/jcs.262202 | DOI Listing |
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