Abstract
Viruses have evolved membrane-restructuring mechanisms for sustaining entry into cells, genome replication and release from host cells. Picornavirus 2B, a non-structural protein required for effective viral replication, functions as a potent intracellular pore-forming toxin by altering the permeability of cellular endomembranes. Two consecutive hydrophobic regions have been identified in 2B protein that could function as an “-helix-turn--helix” hairpin membraneanchor. A peptide derived from the first transmembrane domain comprised a “one-helix” 2B version that possesses the intrinsic pore-forming activity required to directly and effectively permeabilize the cell plasma membrane. Moreover, this miniaturized form is capable of translocating through the plasma membrane of culture cells and to target mitochondria. These evidences suggest that viroporins constitute a new source of membrane-active sequences, worth exploring as potential leads for the development of bioactive peptides, and/or as targets for the development of antiviral compounds.
Keywords: Enterovirus 2B, viroporins, peptide-lipid interactions, pore-forming peptides, peptide-targeting to mitochondria.
Current Protein & Peptide Science
Title:Membrane-Active Peptides Derived from Picornavirus 2B Viroporin
Volume: 13 Issue: 7
Author(s): Silvia Sanchez-Martinez, Vanesa Madan, Luis Carrasco and Jose L. Nieva
Affiliation:
Keywords: Enterovirus 2B, viroporins, peptide-lipid interactions, pore-forming peptides, peptide-targeting to mitochondria.
Abstract: Viruses have evolved membrane-restructuring mechanisms for sustaining entry into cells, genome replication and release from host cells. Picornavirus 2B, a non-structural protein required for effective viral replication, functions as a potent intracellular pore-forming toxin by altering the permeability of cellular endomembranes. Two consecutive hydrophobic regions have been identified in 2B protein that could function as an “-helix-turn--helix” hairpin membraneanchor. A peptide derived from the first transmembrane domain comprised a “one-helix” 2B version that possesses the intrinsic pore-forming activity required to directly and effectively permeabilize the cell plasma membrane. Moreover, this miniaturized form is capable of translocating through the plasma membrane of culture cells and to target mitochondria. These evidences suggest that viroporins constitute a new source of membrane-active sequences, worth exploring as potential leads for the development of bioactive peptides, and/or as targets for the development of antiviral compounds.
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Cite this article as:
Sanchez-Martinez Silvia, Madan Vanesa, Carrasco Luis and Nieva L. Jose, Membrane-Active Peptides Derived from Picornavirus 2B Viroporin, Current Protein & Peptide Science 2012; 13 (7) . https://dx.doi.org/10.2174/138920312804142165
DOI https://dx.doi.org/10.2174/138920312804142165 |
Print ISSN 1389-2037 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-5550 |
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