Poly(Glu60Ala30Tyr10) (GAT)-induced IgG monoclonal antibodies cross-react with various self and non-self antigens through the complementarity determining regions. Comparison with IgM monoclonal polyreactive natural antibodies

Abstract

Previous studies have shown that the antibodies of the preimmune repertoire are able to bind to various auto‐ and xenoantigens including chemical haptens. Sequence analysis of two such murine monoclonal IgM natural autoantibodies showed that they are encoded by unmutated germ‐line variable regions of the light and heavy chain (V_x and V_H) genes which were also found in various murine immune responses, like phenyl‐oxazolone, dinitrophenyl, arsonate, phosphoryl‐choline and influenza virus hemagglutinin. These data raised the question as to whether induced antibodies possessing germ‐line sequence are also able to react with autoantigens. To study this problem, anti‐poly(Glu⁶⁰Ala³⁰Tyr¹⁰) (GAT) and anti‐alprenolol (Alp) monoclonal antibodies, carrying similar V_H and V_x genes and the same IgG₁ isotype, were examined for their capacity to react with several self and non‐self antigens. The results showed that: (a) the anti‐GAT antibodies tested reacted with different autoantigens, such as murine tubulin, actin and myosin as well as trinitrophenyl (TNP) and bovine serum albumin. Similarly, one of the anti‐Alp showed weak reactivities for myosin, DNA, actin and TNP; (b) in contrast two other anti‐Alp antibodies did not react with any of the tested antigens. Since the major differences between the oligoreactive anti‐GAT and the monoreactive anti‐Alp antibodies are in the complementarity determining regions (CDR) our results suggest that the observed cross‐reactions are mediated by hypervariable loops. Sequence comparison of these antibodies indicate a possible correlation between cross‐reactivity and the presence of aromatic and charged amino acids in the CDR.