| Literature DB >> 30880002 |
Ambra Villani1, Jørgen Benjaminsen1, Christian Moritz2, Katrin Henke3, Jonas Hartmann1, Nils Norlin2, Kerstin Richter2, Nicole L Schieber2, Tilman Franke4, Yannick Schwab2, Francesca Peri5.
Abstract
Phagocytic immune cells such as microglia can engulf and process pathogens and dying cells with high efficiency while still maintaining their dynamic behavior and morphology. Effective intracellular processing of ingested cells is likely to be crucial for microglial function, but the underlying cellular mechanisms are poorly understood. Using both living fish embryos and mammalian macrophages, we show that processing depends on the shrinkage and packaging of phagosomes into a unique cellular compartment, the gastrosome, with distinct molecular and ultra-structural characteristics. Loss of the transporter Slc37a2 blocks phagosomal shrinkage, resulting in the expansion of the gastrosome and the dramatic bloating of the cell. This, in turn, affects the ability of microglia to phagocytose and migrate toward brain injuries. Thus, this work identifies a conserved crucial step in the phagocytic pathway of immune cells and provides a potential entry point for manipulating their behavior in development and disease.Entities:
Keywords: apoptotic cell clearance; brain development; efferocytosis; macrophage; microglia; neuronal cell death; neuronal immunity; phagocytosis; slc37a2; zebrafish
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Year: 2019 PMID: 30880002 DOI: 10.1016/j.devcel.2019.02.014
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270