Relative Immunogenicity in Mice of Different Regions of the Human IgG

Abstract

Monoclonal mouse antibodies to human IgG myeloma proteins were produced and characterized by determining their binding to a series of different purified myeloma proteins. Two types of immunization schedules were used. When the same myeloma protein was used for priming and boosting the mouse, all determinants of the molecule were effectively immunogenic. Of the 353 clones originating from these experiments 42% secreted anti-F_v antibodies, 57% anti-C_H antibodies, and 0.85% anti-C_L, antibodies. In another schedule only the C_L and C_H regions were the same in priming and boosting; 270 anti-C_H (94%), 18 anti-C_L (16%), and no anti-F_v hybridomas were found. Our results indicate that a unit mass of the F_v region was 1.3 times more antigenic than a unit mass of the C_H region. A unit mass of the C_H region was nearly five times more antigenic than a unit mass of the C_L domain when the antigenicity of the F_v region had been excluded. When the antigenicity of the F_v region had not been excluded, a unit mass of the C_H region was about twenty times more antigenic than a unit mass of the C_L domain. The data suggest that an antigenic competition was taking place between different parts of the molecule and that the strongly antigenic region (F_v) was more efficient in competing out the nearest neighbour (C_L) than in competing out other parts of the molecule.