AI Article Synopsis

  • Dugesia japonica planarians can eliminate various pathogenic bacteria, making them a useful model for studying innate immune resistance mechanisms.
  • Whole-transcriptome analysis and RNA interference screening revealed 18 resistance genes, including MORN2, which has human equivalents and is crucial for phagocytosis of bacteria like Mycobacterium tuberculosis.
  • MORN2 works by recruiting the autophagy protein LC3 to bacteria-containing phagosomes, aiding their maturation into degradative compartments, thus highlighting the significance of this flatworm in understanding immune processes.

Article Abstract

Dugesia japonica planarian flatworms are naturally exposed to various microbes but typically survive this challenge. We show that planarians eliminate bacteria pathogenic to Homo sapiens, Caenorhabditis elegans, and/or Drosophila melanogaster and thus represent a model to identify innate resistance mechanisms. Whole-transcriptome analysis coupled with RNAi screening of worms infected with Staphylococcus aureus or Legionella pneumophila identified 18 resistance genes with nine human orthologs, of which we examined the function of MORN2. Human MORN2 facilitates phagocytosis-mediated restriction of Mycobacterium tuberculosis, L. pneumophila, and S. aureus in macrophages. MORN2 promotes the recruitment of LC3, an autophagy protein also involved in phagocytosis, to M. tuberculosis-containing phagosomes and subsequent maturation to degradative phagolysosomes. MORN2-driven trafficking of M. tuberculosis to single-membrane, LC3-positive compartments requires autophagy-related proteins Atg5 and Beclin-1, but not Ulk-1 and Atg13, highlighting the importance of MORN2 in LC3-associated phagocytosis. These findings underscore the value of studying planarian defenses to identify immune factors.

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Source
http://dx.doi.org/10.1016/j.chom.2014.08.002DOI Listing

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