• Front Cell Infect Microbiol · Jan 2013

    Review Comparative Study

    Shared and distinct mechanisms of iron acquisition by bacterial and fungal pathogens of humans.

    • Mélissa Caza and James W Kronstad.
    • The Michael Smith Laboratories, Department of Microbiology and Immunology, University of British Columbia Vancouver, BC, Canada.
    • Front Cell Infect Microbiol. 2013 Jan 1;3:80.

    AbstractIron is the most abundant transition metal in the human body and its bioavailability is stringently controlled. In particular, iron is tightly bound to host proteins such as transferrin to maintain homeostasis, to limit potential damage caused by iron toxicity under physiological conditions and to restrict access by pathogens. Therefore, iron acquisition during infection of a human host is a challenge that must be surmounted by every successful pathogenic microorganism. Iron is essential for bacterial and fungal physiological processes such as DNA replication, transcription, metabolism, and energy generation via respiration. Hence, pathogenic bacteria and fungi have developed sophisticated strategies to gain access to iron from host sources. Indeed, siderophore production and transport, iron acquisition from heme and host iron-containing proteins such as hemoglobin and transferrin, and reduction of ferric to ferrous iron with subsequent transport are all strategies found in bacterial and fungal pathogens of humans. This review focuses on a comparison of these strategies between bacterial and fungal pathogens in the context of virulence and the iron limitation that occurs in the human body as a mechanism of innate nutritional defense.

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