AI Article Synopsis

  • Aspergillus fumigatus is a common fungal pathogen that spreads through asexual spores called conidia, which are critical for its survival and infection process.
  • The study identifies a new protein regulator named MybA that is found in the nucleus and is essential for the maturation and viability of conidia by influencing key regulatory genes.
  • Deleting the mybA gene significantly decreases the number and survival of conidia, reducing the fungus's virulence in experimental models, indicating MybA's importance in A. fumigatus propagation and pathogenicity.

Article Abstract

Aspergillus fumigatus, a ubiquitous human fungal pathogen, produces asexual spores (conidia), which are the main mode of propagation, survival and infection of this human pathogen. In this study, we present the molecular characterization of a novel regulator of conidiogenesis and conidial survival called MybA because the predicted protein contains a Myb DNA binding motif. Cellular localization of the MybA::Gfp fusion and immunoprecipitation of the MybA::Gfp or MybA::3xHa protein showed that MybA is localized to the nucleus. RNA sequencing data and a uidA reporter assay indicated that the MybA protein functions upstream of wetA, vosA and velB, the key regulators involved in conidial maturation. The deletion of mybA resulted in a very significant reduction in the number and viability of conidia. As a consequence, the ΔmybA strain has a reduced virulence in an experimental murine model of aspergillosis. RNA-sequencing and biochemical studies of the ΔmybA strain suggested that MybA protein controls the expression of enzymes involved in trehalose biosynthesis as well as other cell wall and membrane-associated proteins and ROS scavenging enzymes. In summary, MybA protein is a new key regulator of conidiogenesis and conidial maturation and survival, and plays a crucial role in propagation and virulence of A. fumigatus.

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Source
http://dx.doi.org/10.1111/mmi.13744DOI Listing

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