1qx9: Difference between revisions
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{{STRUCTURE_1qx9| PDB=1qx9 | SCENE= }} | |||
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'''Structure of a cyclic indolicidin peptide derivative with higher charge''' | '''Structure of a cyclic indolicidin peptide derivative with higher charge''' | ||
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==About this Structure== | ==About this Structure== | ||
1QX9 is a [[Single protein]] structure | 1QX9 is a [[Single protein]] structure. Full crystallographic information is available from [http://oca.weizmann.ac.il/oca-bin/ocashort?id=1QX9 OCA]. | ||
==Reference== | ==Reference== | ||
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[[Category: Powers, J P.]] | [[Category: Powers, J P.]] | ||
[[Category: Rozek, A.]] | [[Category: Rozek, A.]] | ||
[[Category: | [[Category: Beta turn]] | ||
[[Category: | [[Category: Cyclic cationic antimicrobial peptide]] | ||
''Page seeded by [http://oca.weizmann.ac.il/oca OCA ] on Sat May 3 06:48:38 2008'' | |||
''Page seeded by [http://oca.weizmann.ac.il/oca OCA ] on | |||
Revision as of 06:48, 3 May 2008
Structure of a cyclic indolicidin peptide derivative with higher charge
OverviewOverview
Indolicidin is an antimicrobial cationic peptide with broad-spectrum activity isolated from bovine neutrophils. An indolicidin analogue CP-11, ILKKWPWWPWRRK-NH(2), with improved activity against Gram-negative bacteria had increased positive charge and amphipathicity while maintaining the short length of the parent molecule. The structure of CP-11 in the presence of dodecylphosphocholine (DPC) micelles was determined using nuclear magnetic resonance spectroscopy. CP-11 was found to be an amphipathic molecule with a U-shaped backbone bringing the N- and C-termini in close proximity. On the basis of this close proximity, a cyclic disulfide-bonded peptide cycloCP-11, ICLKKWPWWPWRRCK-NH(2), was designed to stabilize the lipid-bound structure and to increase protease resistance. The three-dimensional structure of cycloCP-11 was determined under the same conditions as for the linear peptide and was found to be similar to CP-11. Both CP-11 and cycloCP-11 associated with phospholipid membranes in a similar manner as indicated by circular dichroism and fluorescence spectra. The minimal inhibitory concentrations of CP-11 and cycloCP-11 for a range of bacteria differed by no more than 2-fold, and they were nonhemolytic at concentrations up to 256 microg/mL. Cyclization was found to greatly increase protease stability. The half-life of cycloCP-11 in the presence of trypsin was increased by 4.5-fold from 4 to 18 min. More importantly, the antibacterial activity of cycloCP-11, but not that of CP-11, in the presence of trypsin was completely retained up to 90 min since the major degradation product was equally active. A structural comparison of CP-11 and cycloCP-11 revealed that the higher trypsin resistance of cycloCP-11 may be due to the more compact packing of lysine and tryptophan side chains. These findings suggest that cyclization may serve as an important strategy in the rational design of antimicrobial peptides.
About this StructureAbout this Structure
1QX9 is a Single protein structure. Full crystallographic information is available from OCA.
ReferenceReference
Structure-based design of an indolicidin peptide analogue with increased protease stability., Rozek A, Powers JP, Friedrich CL, Hancock RE, Biochemistry. 2003 Dec 9;42(48):14130-8. PMID:14640680 Page seeded by OCA on Sat May 3 06:48:38 2008