Neethu, Puthumadathil and Poornendhu , Jayasree and K. , Santhosh Kumar and Kozhinjampara R., Mahendran (2010) Detecting the structural assembly pathway of human antimicrobial peptide pores at single-channel level. Biomaterials Science. ISSN 2047-4830
Full text not available from this repository. (Request a copy)Abstract
The pore-forming structures of an anionic human antimicrobial peptide dermcidin (DCD) in a membrane environment has not been demonstrated previously. Using single-channel electrical recordings, we characterized the structural and functional properties of the DCD peptide channel in lipid membranes. We show that a 48-residue, 8 nm long anionic DCD-1L peptide is folded in the right conformation in sodium dodecyl sulfate (SDS) that spontaneously inserts into lipid bilayers to form well-defined channels. However, the DCD-1L peptides are not properly folded in n-dodecyl-β-D-maltoside (DDM), resulting in unstable channels suggesting the significance of specific detergent in stable channel formation. Furthermore, a 25-residue cationic DCD SSL-25 peptide formed channels both in SDS and DDM micelles as the length of the peptide matches with the thickness of the membrane. Finally, we quantified the permeation of small molecules through the DCD channels in liposome assays. Accordingly, we propose a molecular model demonstrating the structural self-assembly of the DCD channels in the membrane. We suggest that an understanding of the mechanism of action of DCD peptides at single-channel resolution will lead to developing peptide-based therapeutics.
Item Type: | Article |
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Subjects: | Neuro-Bio-Physics |
Depositing User: | Central Library RGCB |
Date Deposited: | 05 Jul 2019 09:24 |
Last Modified: | 05 Jul 2019 09:24 |
URI: | http://rgcb.sciencecentral.in/id/eprint/802 |
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