Design and synthesis of truncated EGF-A peptides that restore LDL-R recycling in the presence of PCSK9 in vitro.

Authors :: Schroeder CI
Swedberg JE
Withka JM
Rosengren KJ
Akcan M
Clayton DJ
Daly NL
Cheneval O
Borzilleri KA
Griffor M
Stock I
Colless B
Walsh P
Sunderland P
Reyes A
Dullea R
Ammirati M
Liu S
McClure KF
Tu M
Bhattacharya SK
Liras S
Price DA
Craik DJ
Source :: Chemistry & biology [Chem Biol] 2014 Feb 20; Vol. 21 (2), pp. 284-94. Date of Electronic Publication: 2014 Jan 16.
Publication Year :: 2014
Abstract: Disrupting the binding interaction between proprotein convertase (PCSK9) and the epidermal growth factor-like domain A (EGF-A domain) in the low-density lipoprotein receptor (LDL-R) is a promising strategy to promote LDL-R recycling and thereby lower circulating cholesterol levels. In this study, truncated 26 amino acid EGF-A analogs were designed and synthesized, and their structures were analyzed in solution and in complex with PCSK9. The most potent peptide had an increased binding affinity for PCSK9 (KD = 0.6 μM) compared with wild-type EGF-A (KD = 1.2 μM), and the ability to increase LDL-R recycling in the presence of PCSK9 in a cell-based assay.<br /> (Copyright © 2014 Elsevier Ltd. All rights reserved.)

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