Abstract
Fungal pathogens have evolved diverse strategies to sense host-relevant cues and coordinate cellular responses, which enable virulence and drug resistance. Defining circuitry controlling these traits opens new opportunities for chemical diversity in therapeutics, as the cognate inhibitors are rarely explored by conventional screening approaches. This has great potential to address the pressing need for new therapeutic strategies for invasive fungal infections, which have a staggering impact on human health. To explore this approach, we focused on a leading human fungal pathogen, Candida albicans, and screened 1,280 pharmacologically active compounds to identify those that potentiate the activity of echinocandins, which are front-line therapeutics that target fungal cell wall synthesis. We identified 19 compounds that enhance activity of the echinocandin caspofungin against an echinocandin-resistant clinical isolate, with the broad-spectrum chelator DTPA demonstrating the greatest synergistic activity. We found that DTPA increases susceptibility to echinocandins via chelation of magnesium. Whole genome sequencing of mutants resistant to the combination of DTPA and caspofungin identified mutations in the histidine kinase gene NIK1 that confer resistance to the combination. Functional analyses demonstrated that DTPA activates the mitogen-activated protein kinase Hog1, and that NIK1 mutations block Hog1 activation in response to both caspofungin and DTPA. The combination has therapeutic relevance as DTPA enhanced the efficacy of caspofungin in a mouse model of echinocandin-resistant candidiasis. We found that DTPA not only reduces drug resistance but also modulates morphogenesis, a key virulence trait that is normally regulated by environmental cues. DTPA induced filamentation via depletion of zinc, in a manner that is contingent upon Ras1-PKA signaling, as well as the transcription factors Brg1 and Rob1. Thus, we establish a new mechanism by which metal chelation modulates morphogenetic circuitry and echinocandin resistance, and illuminate a novel facet to metal homeostasis at the host-pathogen interface, with broad therapeutic potential.
Highlights
Invasive fungal infections have a devastating impact on human health worldwide
Invasive fungal infections pose a serious threat to human health worldwide, with Candida albicans being a leading fungal pathogen
We established that diethylenetriamine pentaacetic acid (DTPA) acts through Nik1 to modulate Hog1 signaling and enhance echinocandin activity, and that this combination has therapeutic benefits in a murine model of candidiasis
Summary
Invasive fungal infections have a devastating impact on human health worldwide. The most vulnerable individuals are those suffering from immune deficiencies due to chemotherapy for cancer, immunosuppression for transplants of solid organs or stem cells, or infection with HIV [1]. The incidence of deadly invasive fungal infections is on the rise, in concert with the increasing use of immunosuppressive measures and invasive medical procedures [2,3]. 1.5 million people die every year from invasive fungal infections, which exceeds the death toll of malaria or tuberculosis [1]. Candida species are a leading cause of mycotic death worldwide, and account for over 85% of all hospital acquired fungal infections [2]. Candida albicans is the primary cause of systemic candidiasis with mortality rates of ~40% [4,5], even with current treatment options
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