AI Article Synopsis
- Fungal infections lead to more deaths globally than malaria, prompting research into new antifungal compounds.
- The compound NGx04 targets the lipid transfer protein Sec14p in fungi, which is vital for their pathogenicity, particularly in Cryptococcus neoformans.
- NGx04 and its analogues demonstrate significant effectiveness against various strains of C. neoformans, including those resistant to fluconazole, highlighting NGx04 as a promising new antifungal agent.
Article Abstract
Invasive infections by fungal pathogens cause more deaths than malaria worldwide. We found the ergoline compound NGx04 in an antifungal screen, with selectivity over mammalian cells. High-resolution chemogenomics identified the lipid transfer protein Sec14p as the target of NGx04 and compound-resistant mutations in Sec14p define compound-target interactions in the substrate binding pocket of the protein. Beyond its essential lipid transfer function in a variety of pathogenic fungi, Sec14p is also involved in secretion of virulence determinants essential for the pathogenicity of fungi such as Cryptococcus neoformans, making Sec14p an attractive antifungal target. Consistent with this dual function, we demonstrate that NGx04 inhibits the growth of two clinical isolates of C. neoformans and that NGx04-related compounds have equal and even higher potency against C. neoformans. Furthermore NGx04 analogues showed fungicidal activity against a fluconazole resistant C. neoformans strain. In summary, we present genetic evidence that NGx04 inhibits fungal Sec14p and initial data supporting NGx04 as a novel antifungal starting point.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5147771 | PMC |
| http://dx.doi.org/10.1371/journal.pgen.1006374 | DOI Listing |
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