4.7 Article

A Novel Function of TLR2 and MyD88 in the Regulation of Leukocyte Cell Migration Behavior During Wounding in Zebrafish Larvae

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出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fcell.2021.624571

关键词

TLR2; MyD88; leukocyte migration; neutrophils; macrophages; zebrafish; tail wounding

资金

  1. China Scholarship Council (CSC)
  2. NWO Vici [865.17.004]

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In this study using zebrafish larval tail-wounding model, it was found that TLR2 and MyD88 play a role in regulating neutrophil and macrophage cell migration behavior, influencing the direction of neutrophil migration away from the wound and the speed of macrophage migration towards the wound edge. This indicates the involvement of TLR2 and MyD88 in responses to tail wounding by modulating leukocyte migration behavior and speed in vivo.
Toll-like receptor (TLR) signaling via myeloid differentiation factor 88 protein (MyD88) has been indicated to be involved in the response to wounding. It remains unknown whether the putative role of MyD88 in wounding responses is due to a control of leukocyte cell migration. The aim of this study was to explore in vivo whether TLR2 and MyD88 are involved in modulating neutrophil and macrophage cell migration behavior upon zebrafish larval tail wounding. Live cell imaging of tail-wounded larvae was performed in tlr2 and myd88 mutants and their corresponding wild type siblings. In order to visualize cell migration following tissue damage, we constructed double transgenic lines with fluorescent markers for macrophages and neutrophils in all mutant and sibling zebrafish lines. Three days post fertilization (dpf), tail-wounded larvae were studied using confocal laser scanning microscopy (CLSM) to quantify the number of recruited cells at the wounding area. We found that in both tlr2(-/-) and myd88(-/-) groups the recruited neutrophil and macrophage numbers are decreased compared to their wild type sibling controls. Through analyses of neutrophil and macrophage migration patterns, we demonstrated that both tlr2 and myd88 control the migration direction of distant neutrophils upon wounding. Furthermore, in both the tlr2 and the myd88 mutants, macrophages migrated more slowly toward the wound edge. Taken together, our findings show that tlr2 and myd88 are involved in responses to tail wounding by regulating the behavior and speed of leukocyte migration in vivo.

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