Functional Characterization of the GNAT Family Histone Acetyltransferase Elp3 and GcnE in .

Post-translational modifications of chromatin structure by histone acetyltransferase (HATs) play a pivotal role in the regulation of gene expression and diverse biological processes. However, the function of GNAT family HATs, especially Elp3, in the opportunistic human pathogenic fungus is largely unknown. To investigate the roles of the GNAT family HATs Elp3 and GcnE in the , we have generated and characterized individual null Δ and Δ mutants. The radial growth of fungal colonies was significantly decreased by the loss of or , and the number of asexual spores (conidia) in the Δ mutant was significantly reduced. Moreover, the mRNA levels of the key asexual development regulators were also significantly low in the Δ mutant compared to wild type (WT). Whereas both the Δ and Δ mutants were markedly impaired in the formation of adherent biofilms, the Δ mutant showed a complete loss of surface structure and of intercellular matrix. The Δ mutant responded differently to oxidative stressors and showed significant susceptibility to triazole antifungal agents. Furthermore, Elp3 and GcnE function oppositely in the production of secondary metabolites, and the Δ mutant showed attenuated virulence. In conclusion, Elp3 and GcnE are associated with diverse biological processes and can be potential targets for controlling the pathogenic fungus.