4.7 Article

Loss of PIKfyve Causes Transdifferentiation of Dictyostelium Spores Into Basal Disc Cells

期刊

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fcell.2021.692473

关键词

1-phosphatidylinositol-3-phosphate 5-kinase; Atg18; Vac14; membrane scission; vesicle trafficking; cell-type specific gene expression; sporulation; Dictyostelium

资金

  1. Wellcome Trust [100293/Z/12/Z]
  2. European Research Council [742288]
  3. Japanese Society for the Promotion of Science KAKENHI [JP20K06672]
  4. BBSRC [BB/K000799/1, BB/G020426/1, BB/D013453/1] Funding Source: UKRI

向作者/读者索取更多资源

The study highlights the crucial role of PIKfyve in the fusion process of V-ATPase receptor vesicles within cells, and indicates its regulatory role in cell differentiation and gene expression.
The 1-phosphatidylinositol-3-phosphate 5-kinase PIKfyve generates PtdIns3,5P2 on late phagolysosomes, which by recruiting the scission protein Atg18, results in their fragmentation in the normal course of endosome processing. Loss of PIKfyve function causes cellular hypervacuolization in eukaryotes and organ failure in humans. We identified pikfyve as the defective gene in a Dictyostelium mutant that failed to form spores. The amoebas normally differentiated into prespore cells and initiated spore coat protein synthesis in Golgi-derived prespore vesicles. However, instead of exocytosing, the prespore vesicles fused into the single vacuole that typifies the stalk and basal disc cells that support the spores. This process was accompanied by stalk wall biosynthesis, loss of spore gene expression and overexpression of ecmB, a basal disc and stalk-specific gene, but not of the stalk-specific genes DDB_G0278745 and DDB_G0277757. Transdifferentiation of prespore into stalk-like cells was previously observed in mutants that lack early autophagy genes, like atg5, atg7, and atg9. However, while autophagy mutants specifically lacked cAMP induction of prespore gene expression, pikfyve(-) showed normal early autophagy and prespore induction, but increased in vitro induction of ecmB. Combined, the data suggest that the Dictyostelium endosomal system influences cell fate by acting on cell type specific gene expression.

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