Literature DB >> 7650481

Random mutagenesis of two complementarity determining region amino acids yields an unexpectedly high frequency of antibodies with increased affinity for both cognate antigen and autoantigen.

L P Casson1, T Manser.   

Abstract

To gain insight into the mechanism and limitations of antibody affinity maturation leading to memory B cell formation, we generated a phage display library of random mutants at heavy chain variable (V) complementarity determining region 2 positions 58 and 59 of an anti-p-azophenylarsonate (Ars) Fab. Single amino acid substitutions at these positions resulting from somatic hypermutation are recurrent products of affinity maturation in vivo. Most of the ex vivo mutants retained specificity for Ars. Among the many mutants displaying high Ars-binding activity, only one contained a position 58 and 59 amino acid combination that has been previously observed among the monoclonal antibodies (mAbs) derived from Ars-immunized mice. Affinity measurements on 14 of the ex vivo mutants with high Ars-binding activity showed that 11 had higher intrinsic affinities for Ars that the wild-type V region. However, nine of these Fabs also bound strongly to denatured DNA, a property neither displayed by the wild-type V region nor observed among the mutants characteristic of in vivo affinity maturation. These data suggest that ex vivo enhancement of mAb affinity via site-directed and random mutagenesis approaches may often lead to a reduction in antibody specificity that could complicate the use of the resulting mAbs for diagnostic and therapeutic applications. Moreover, the data are compatible with a hypothesis proposing that increased specificity for antigen, rather than affinity per se, is the driving force for formation of the memory B cell compartment.

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Year:  1995        PMID: 7650481      PMCID: PMC2192174          DOI: 10.1084/jem.182.3.743

Source DB:  PubMed          Journal:  J Exp Med        ISSN: 0022-1007            Impact factor:   14.307


  36 in total

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Review 6.  Making antibodies by phage display technology.

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7.  Residues that mediate DNA binding of autoimmune antibodies.

Authors:  M Z Radic; J Mackle; J Erikson; C Mol; W F Anderson; M Weigert
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9.  Verification of a model of a F(ab) complex with phenylarsonate by oligonucleotide-directed mutagenesis.

Authors:  S R Sompuram; J Sharon
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10.  Induction of tolerance to an IgG autoantibody.

Authors:  D Offen; L Spatz; H Escowitz; S Factor; B Diamond
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  15 in total

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4.  Construction of an artificially randomized IgNAR phage display library: screening of variable regions that bind to hen egg white lysozyme.

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5.  Autoreactivity in human IgG+ memory B cells.

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8.  Somatic hypermutation of immunoglobulin genes is independent of the Bloom's syndrome DNA helicase.

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9.  The double edged sword of the immune response: mutational analysis of a murine anti-pneumococcal, anti-DNA antibody.

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