Dynamic crosstalk between Tspan4+ macrophage subsets and MSCs via migrasomes orchestrates fracture repair
Siyu Zhang, Mengci Wang, Abudurexiti Kutibiding, Dandan Liu, Tuersunnayi Manafu, Wen Zhao, Yi Yang

TL;DR
This study reveals how specific macrophage subsets communicate with MSCs via migrasomes to enhance fracture healing.
Contribution
The study identifies migrasomes as a novel conduit for macrophage-MSC communication during fracture repair.
Findings
Macrophages are categorized into Tspan4+Lyve1+ and Tspan4+Mpeg1+ subsets during fracture healing.
Migrasomes derived from Tspan4+Mpeg1+ macrophages enhance MSC migration and osteogenic priming via IL-1β and AMPK activation.
Abstract
The cell - cell communication between macrophages and mesenchymal stromal/stem cells (MSCs) holds pivotal importance in the fracture healing process. Considering the intricate nature of the in vivo bone regeneration microenvironment, elucidating the changes in different macrophage subsets within this microenvironment, as well as the cell - cell communication between these subsets and MSCs, is essential for the differentiation, recruitment, and regulation of MSCs. This study was designed to investigate the interactions between diverse macrophage subsets and MSCs during the fracture healing period. Single - cell sequencing was utilized to analyze the expression of Tspan4+, Lyve1+, and Mpeg1+ in macrophages during fracture healing, along with the cell - interaction signals with MSCs. It was demonstrated that the cell - interaction signal transduction might be linked to migrasomes. Scratch…
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Taxonomy
TopicsExtracellular vesicles in disease · Immune cells in cancer · Bone fractures and treatments
