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Specific uptake and interactions of peptide nucleic acid derivatives with biomimetic membranes

Year: 2012

Journal: RSC Adv., 2012,2, 4703-4712, 20120618

Authors: Tanmaya Joshi 1, Gilles Gasser 2, Lisandra L. Martin 1 and Leone Spiccia 1,3

Last authors: Leone Spiccia

Organizations: 1. School of Chemistry,Monash University, Clayton, Australia 2. Institute of Inorganic Chemistry,University of Zurich,Winterthurerstrasse 190, Zurich, Switzerland 3. ARC Centre of Excellence for Electromaterials Science,Monash University, Clayton, Australia

Country: Australia, Switzerland

There is a growing interest in understanding the uptake mechanism of metal-containing peptide nucleic acid (PNA) bioconjugates into living cells. In this study, quartz crystal microbalance with dissipation monitoring (QCM-D) has been used to explore the membrane specific uptake and interactions of PNA/peptide/Ru(II) conjugates. For all lipid compositions, the unmodified PNA oligomer and its Ru(II) conjugate were found to traverse freely across the membrane in a trans-membrane manner, causing no significant changes in the membrane structure. The nuclear localised signal peptide (NLS) conjugated sequences showed membrane specific activities. In model mammalian and bacterial-mimetic membranes, rapid trans-membrane insertion was observed followed by a concentration dependent disruption and irreversible structural changes to the membrane system. The variations in the magnitude of the structural changes and in their tendency to facilitate disruption are ascribed to hydrophobicity, the cationic charge introduced on modification of the original PNA backbone as well as the physical state of the model membrane used.