| Literature DB >> 31762965 |
Kyohei Muguruma1, Mayu Ito1, Akane Fukuda1, Satoshi Kishimoto2, Akihiro Taguchi1, Kentaro Takayama1, Atsuhiko Taniguchi1, Yuji Ito2, Yoshio Hayashi1.
Abstract
Currently, IgG-binding peptides are widely utilized as a research tool, as molecules that guide substrates to the Fc site for site-selective antibody modification, leading to preparation of a homogeneous antibody-drug conjugate. In this study, a structure-activity relationship study of an IgG-binding peptide, 15-IgBP, that is focused on its C-terminal His residue was performed in an attempt to create more potent peptides. A peptide with a substitution of His17 by 2-pyridylalanine (2-Pya) showed a good binding affinity (15-His17(2-Pya), K d = 75.7 nM). In combination with a previous result, we obtained 15-Lys8Leu/His17(2-Pya)-OH that showed a potent binding affinity (K d = 2.48 nM) and avoided three synthetic problems concerning the p-hydroxybenzyl amidation at the C-terminus, the difficulty associated with coupling at the His7 position and the racemization of 2-Pya. This journal is © The Royal Society of Chemistry 2019.Entities:
Year: 2019 PMID: 31762965 PMCID: PMC6855313 DOI: 10.1039/c9md00294d
Source DB: PubMed Journal: Medchemcomm ISSN: 2040-2503 Impact factor: 3.597