β-glucan dependent shuttling of conidia from neutrophils to macrophages occurs during fungal infection establishment

吞噬细胞 吞噬体 烟曲霉 微生物学 生物 病菌 体内 细胞生物学 斑马鱼 巨噬细胞 体外 宿主-病原体相互作用 吞噬作用 毒力 基因 生物技术 生物化学
作者
Vahid Pazhakh,Felix Ellett,Joanne A. O’Donnell,Luke Pase,Keith E. Schulze,R. Stefan Greulich,Constantino Carlos Reyes‐Aldasoro,Ben A. Croker,Alex Andrianopoulos,Graham J. Lieschke
标识
DOI:10.1101/512228
摘要

Abstract The initial host response to fungal pathogen invasion is critical to infection establishment and outcome. However, the diversity of leukocyte-pathogen interactions is only recently being appreciated. We describe a new form of interleukocyte conidial exchange called “shuttling”. In Talaromyces marneffei and Aspergillus fumigatus zebrafish in vivo infections, live imaging demonstrated conidia initially phagocytosed by neutrophils were transferred to macrophages. Shuttling is unidirectional, not a chance event, involves alterations of phagocyte mobility, inter-cellular tethering, and phagosome transfer. Shuttling kinetics were fungal species-specific, implicating a fungal determinant. β-glucan serves as a fungal-derived signal sufficient for shuttling. Murine phagocytes also shuttled in vitro . The impact of shuttling for microbiological outcomes of in vivo infections is difficult to specifically assess experimentally, but for these two pathogens, shuttling augments initial conidial redistribution away from fungicidal neutrophils into the favourable macrophage intracellular niche. Shuttling is a frequent host/pathogen interaction contributing to fungal infection establishment patterns.
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