par Osbourn, J K;Earnshaw, J C;Johnson, K S;Parmentier, Marc 
;Timmermans, Vinciane ;McCafferty, J
Référence Nature biotechnology, 16, 8, page (778-781)
Publication Publié, 1998-08
;Timmermans, Vinciane ;McCafferty, JRéférence Nature biotechnology, 16, 8, page (778-781)
Publication Publié, 1998-08
Article révisé par les pairs
| Résumé : | The seven trans-membrane chemokine receptor CCR-5 is a coreceptor for macrophage tropic HIV-1 strains. CCR-5 responds to a number of chemokines, including macrophage inflammatory protein (MIP)-1 alpha. We describe the use of MIP-1 alpha in a biotin tyramine-mediated proximity selection to guide the selection of CCR-5-specific phage antibodies from a large phage display human library. Proximity based selections resulted in a population of antibodies recognizing CCR-5 on primary CD4+ lymphocytes, none of which blocked MIP-1 alpha binding to cells. The selected population of phage antibodies were subsequently used as guide molecules for a second phase of selection that was carried out in the absence of MIP-1 alpha. This generated a panel of CCR-5-binding antibodies, of which around 20% inhibited MIP-1 alpha binding to CD4+. The single chain Fvs (scFv) generated by this step-back selection procedure also inhibited MIP-1 alpha-mediated calcium signaling. |
