| Literature DB >> 25522713 |
Abstract
Biophysical and structural studies of peptide-lipid interactions, peptide topology and dynamics have changed our view on how antimicrobial peptides insert and interact with membranes. Clearly, both the peptides and the lipids are highly dynamic, change and mutually adapt their conformation, membrane penetration and detailed morphology on a local and a global level. As a consequence, the peptides and lipids can form a wide variety of supramolecular assemblies in which the more hydrophobic sequences preferentially, but not exclusively, adopt transmembrane alignments and have the potential to form oligomeric structures similar to those suggested by the transmembrane helical bundle model. In contrast, charged amphipathic sequences tend to stay intercalated at the membrane interface where they cause pronounced disruptions of the phospholipid fatty acyl packing. At increasing local or global concentrations, the peptides result in transient membrane openings, rupture and ultimately lysis. Depending on peptide-to-lipid ratio, lipid composition and environmental factors (temperature, buffer composition, ionic strength, etc.), the same peptide sequence can result in a variety of those responses. Therefore, the SMART model has been introduced to cover the full range of possibilities. With such a view in mind, novel antimicrobial compounds have been designed from amphipathic polymers, peptide mimetics, combinations of ultra-short polypeptides with hydrophobic anchors or small designer molecules.Entities:
Keywords: PGLa; alamethicin; carpet model; cecropin; equlibria; hydrophobic mismatch; local disorder; magainin; membrane macroscopic phase; membrane pore; membrane topology; peptaibol; peptide-lipid interactions; toroidal pore
Mesh:
Substances:
Year: 2014 PMID: 25522713 DOI: 10.1002/psc.2729
Source DB: PubMed Journal: J Pept Sci ISSN: 1075-2617 Impact factor: 1.905