Antibacterial and Antitumorigenic Properties of Microcin E492, a Pore- Forming Bacteriocin | Bentham Science
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Current Pharmaceutical Biotechnology

Editor-in-Chief

ISSN (Print): 1389-2010
ISSN (Online): 1873-4316

Antibacterial and Antitumorigenic Properties of Microcin E492, a Pore- Forming Bacteriocin

Author(s): R. Lagos, M. Tello, G. Mercado, V. Garcia and O. Monasterio

Volume 10, Issue 1, 2009

Page: [74 - 85] Pages: 12

DOI: 10.2174/138920109787048643

Price: $65

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Abstract

Microcins are a family of low-molecular weight bacteriocins produced and secreted by Gram-negative bacteria. This review is focused on microcin E492, a pore-forming bacteriocin produced by Klebsiella pneumoniae RYC492 that exerts its antibacterial action on related strains. The steps necessary for the production of active microcin E492 involve post-translational modification with a catechol-type siderophore at the C-terminal and proteolytic processing during export to the extracellular space. This bacteriocin has a modular structure, with a toxic domain at the N-terminal and an uptake domain at the C-terminal of the mature protein. The mechanism by which the C-terminal of microcin E492 is recognized by catecholate siderophore receptors is called the “Trojan horse” strategy, because the C-terminal structure mimics essential bacterial elements, which are recognized by the respective receptors and translocated across the outer membrane to exert antibacterial action. The C-terminal uptake module can be exchanged and used with other toxic domains. Microcin E492 also has a cytotoxic effect on malignant human cell lines. The cytotoxic mechanism is through apoptosis, a desired mechanism for cancer therapy. The ability of microcin E492 to form amyloid-like fibrils constitutes a property that can be exploited in the formulation of this bacteriocin as an antitumoral agent, because these fibrils can behave as stable depots to ensure the sustained release of a biologically active molecule. Alternatively, live bacteria can be used as a continuous source of microcin E492 production in specific tumors.

Keywords: Microcin E492, channel-forming bacteriocin, antitumoral bacteriocin, amyloid-like fibrils, salmochelin, siderophore- peptide, cancer therapy

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