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A peptide mimetic of an anti-CD4 monoclonal antibody by rational design.

作者信息

Casset Florence, Roux Florence, Mouchet Patrick, Bes Cedric, Chardes Thierry, Granier Claude, Mani Jean-Claude, Pugnière Martine, Laune Daniel, Pau Bernard, Kaczorek Michel, Lahana Roger, Rees Anthony

机构信息

Synt:em, Parc Scientifique Georges Besse, FR-30035 1, Ni;mes Cédex, France.

出版信息

Biochem Biophys Res Commun. 2003 Jul 18;307(1):198-205. doi: 10.1016/s0006-291x(03)01131-8.

Abstract

The development of rational methods to design 'continuous' sequence mimetics of discontinuous regions of protein sequence has, to now, been only marginally successful. This has been largely due to the difficulty of constraining the recognition elements of a mimetic structure to the relative conformational and spatial orientations present in the parent molecule. Using peptide mapping to determine 'active' antigen recognition residues, molecular modeling, and a molecular dynamics trajectory analysis, we have developed a peptide mimic of an anti-CD4 antibody, containing antigen contact residues from multiple CDRs. The design described is a 27-residue peptide formed by juxtaposition of residues from 5 CDR regions. It displays an affinity for the antigen (CD4) of 0.9nM, compared to 2nM for the parent antibody ST40. Nevertheless, the mimetic shows low biological activity in an anti-retroviral assay.

摘要

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