Different Mismatch Repair Deficiencies All Have the Same Effects on Somatic Hypermutation: Intact Primary Mechanism Accompanied by Secondary Modifications

doi:10.1084/jem.190.1.21

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Different Mismatch Repair Deficiencies All Have the Same Effects on Somatic Hypermutation: Intact Primary Mechanism Accompanied by Secondary Modifications

Nayun Kim^a, Grazyna Bozek^b, James C. Lo^b, and Ursula Storb^b
^a From the Department of Biochemistry and Molecular Biology, University of Chicago, Chicago, Illinois 60637
^b From the Department of Molecular Genetics and Cell Biology, University of Chicago, Chicago, Illinois 60637

Correspondence to: James C. Lo

Somatic hypermutation of Ig genes is probably dependent on transcriptionof the target gene via a mutator factor associated with theRNA polymerase (Storb, U., E.L. Klotz, J. Hackett, Jr., K. Kage,G. Bozek, and T.E. Martin. 1998. J. Exp. Med. 188:689–698).It is also probable that some form of DNA repair is involvedin the mutation process. It was shown that the nucleotide excisionrepair proteins were not required, nor were mismatch repair(MMR) proteins. However, certain changes in mutation patternsand frequency of point mutations were observed in Msh2 (MutShomologue) and Pms2 (MutL homologue) MMR-deficient mice (forreview see Kim, N., and U. Storb. 1998. J. Exp. Med. 187:1729–1733).These data were obtained from endogenous immunoglobulin (Ig)genes and were presumably influenced by selection of B cellswhose Ig genes had undergone certain mutations. In this study,we have analyzed somatic hypermutation in two MutL types ofMMR deficiencies, Pms2 and Mlh1. The mutation target was a nonselectableIg- ${kappa}$ gene with an artificial insert in the V region. We foundthat both Pms2- and Mlh1-deficient mice can somatically hypermutatethe Ig test gene at approximately twofold reduced frequencies.Furthermore, highly mutated sequences are almost absent. Togetherwith the finding of genome instability in the germinal centerB cells, these observations support the conclusion, previouslyreached for Msh2 mice, that MMR-deficient B cells undergoingsomatic hypermutation have a short life span. Pms2- and Mlh1-deficientmice also resemble Msh2-deficient mice with respect to preferentialtargeting of G and C nucleotides. Thus, it appears that thedifferent MMR proteins do not have unique functions with respectto somatic hypermutation. Several intrinsic characteristicsof somatic hypermutation remain unaltered in the MMR-deficientmice: a preference for targeting A over T, a strand bias, mutationalhot spots, and hypermutability of the artificial insert areall seen in the unselectable Ig gene. This implies that theMMR proteins are not required for and most likely are not involvedin the primary step of introducing the mutations. Instead, theyare recruited to repair certain somatic point mutations, presumablysoon after these are created.

Key Words: DNA mismatch repair, immunoglobulin genes, somatic hypermutation,transgenic mice

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