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Inhibition of the classical activation pathway of complement-mediated lysis by monoclonal antibodies to complement components C3c and C3d.

作者信息

Mushens R E, Bakacs T

机构信息

International Blood Group Reference Laboratory, South Western Regional Transfusion Centre, Bristol, UK.

出版信息

Transfusion. 1992 Jun;32(5):430-4. doi: 10.1046/j.1537-2995.1992.32592327716.x.

DOI:10.1046/j.1537-2995.1992.32592327716.x
PMID:1378236
Abstract

Eight epitope-mapped monoclonal antibodies (MoAbs) to complement component C3d and five to complement component C3c were investigated to determine whether they could inhibit the classical activation pathway of complement-mediated lysis (CML) by using blood group AB red cells sensitized by A or B MoAbs. Three IgM C3d MoAbs and one IgG1 C3c MoAb were able to inhibit CML in a dose-dependent manner. In the presence of excess complement, no inhibition was observed. The greatest inhibition was observed with two high-affinity IgM antibodies that were specific for epitope 1 on the C3d component. Some inhibition was observed with a high-affinity IgM antibody specific for epitope 3 of the C3d component and also with a lower-affinity IgG antibody specific for epitope 1 of the C3c component. The results indicate that some complement MoAbs have the capacity to distinguish between conformationally and/or functionally different forms of red cell-bound C3.

摘要

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