| Literature DB >> 31718942 |
Antonio Lupia1, Selena Mimmi2, Enrico Iaccino2, Domenico Maisano2, Federica Moraca3, Carmine Talarico4, Eleonora Vecchio2, Giuseppe Fiume2, Francesco Ortuso5, Giuseppe Scala2, Ileana Quinto6, Stefano Alcaro7.
Abstract
Identification of epitopes recognized by tumour B cells could provide insights into the molecular mechanisms of B cell tumorigenesis through aberrant B cell receptor (BCR) signalling. Here, we analysed the structure of eleven peptides binders of BCRs expressed in Chronic Lymphocytic Leukemia (CLL) patients in order to identify the chemical features required for cross-reactive binding to different CLL clonotypes. Four cross-reactive (CR) and seven no-cross-reactive (NCR) peptides were analysed by means of GRID molecular interaction fields, ligand-based pharmacophore and 3D-QSAR approaches. Based on pharmacophore model, two peptides were generated by specific amino acids substitutions of the parental NCR peptides; these new peptides resumed the common chemical features of CR peptides and bound the CLL BCR clonotypes recognized by CR peptides and parental NCR peptides. Thus, our computational approach guided the pharmacophore modelling of CR peptides. In perspective, peptide binders of CLL BCR clonotypes could represent a powerful tool for computational modelling of epitopes recognized by tumour B cells clones.Entities:
Keywords: B cell receptor; CLL; GRID-Pharmacophore; LB-3D-QSAR; Peptides; Phage display
Mesh:
Substances:
Year: 2019 PMID: 31718942 DOI: 10.1016/j.ejmech.2019.111838
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514