How Does It Kill?: Understanding the Candidacidal Mechanism of Salivary Histatin 5

Author:

Puri Sumant1,Edgerton Mira1

Affiliation:

1. Department of Oral Biology, School of Dental Medicine, University at Buffalo, Buffalo, New York, USA

Abstract

ABSTRACT Histatins are salivary cationic peptides that provide the first line of defense against oral candidiasis caused by Candida albicans . This minireview presents a critical evaluation of our knowledge of the candidacidal mechanism of histatin 5 (Hst 5). Hst 5 is the most potent among all histatin family members with regard to its antifungal activity. The mode of action of Hst 5 has been a subject of intense debate. Unlike other classical host innate immune proteins, pore formation or membrane lysis by Hst 5 has largely been disproven, and it is now known that all targets of Hst 5 are intracellular. Hst 5 binds C. albicans cell wall proteins (Ssa1/2) and glycans and is taken up by the cells through fungal polyamine transporters in an energy-dependent manner. Once inside the fungal cells, Hst 5 may affect mitochondrial functions and cause oxidative stress; however, the ultimate cause of cell death is by volume dysregulation and ion imbalance triggered by osmotic stress. Besides these diverse targets, a novel mechanism based on the metal binding abilities of Hst 5 is discussed. Finally, translational approaches for Hst 5, based on peptide design and synergy with other known drugs, are considered a step forward for bench-to-bed application of Hst 5.

Publisher

American Society for Microbiology

Subject

Molecular Biology,General Medicine,Microbiology

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