Egyszerű nézet

dc.contributor.author Gorham RD Jr,
dc.contributor.author Forest DL,
dc.contributor.author Tamamis P,
dc.contributor.author Lopez de Victoria A,
dc.contributor.author Mazákné Kraszni, Márta
dc.date.accessioned 2014-11-16T17:45:58Z
dc.date.available 2014-11-16T17:45:58Z
dc.date.issued 2013
dc.identifier 84884385236
dc.identifier.citation pagination=96-108; journalVolume=116; journalTitle=EXPERIMENTAL EYE RESEARCH;
dc.identifier.uri http://repo.lib.semmelweis.hu//handle/123456789/539
dc.identifier.uri doi:10.1016/j.exer.2013.07.023
dc.description.abstract We have used a novel human retinal pigmented epithelial (RPE) cell-based model that mimics drusen biogenesis and the pathobiology of age-related macular degeneration to evaluate the efficacy of newly designed peptide inhibitors of the complement system. The peptides belong to the compstatin family and, compared to existing compstatin analogs, have been optimized to promote binding to their target, complement protein C3, and to enhance solubility by improving their polarity/hydrophobicity ratios. Based on analysis of molecular dynamics simulation data of peptide-C3 complexes, novel binding features were designed by introducing intermolecular salt bridge-forming arginines at the N-terminus and at position -1 of N-terminal dipeptide extensions. Our study demonstrates that the RPE cell assay has discriminatory capability for measuring the efficacy and potency of inhibitory peptides in a macular disease environment.
dc.relation.ispartof urn:issn:0014-4835
dc.title Novel compstatin family peptides inhibit complement activation by drusen-like deposits in human retinal pigmented epithelial cell cultures.
dc.type Journal Article
dc.date.updated 2014-11-16T17:44:55Z
dc.language.rfc3066 en
dc.identifier.mtmt 2476373
dc.identifier.wos 000327562500013
dc.identifier.pubmed 23954241
dc.mtmt.swordnote PMC PMC3840162


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