The Journal of Experimental Medicine
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Published online 20 November 2000.
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© The Rockefeller University Press, 0022-1007/2000/11/1509/ $5.00
The Journal of Experimental Medicine, Volume 192, Number 10, November 20, 2000 1509-1514

Brief Definitive Report

Somatic Hypermutation in the Absence of DNA-Dependent Protein Kinase Catalytic Subunit (DNA-Pkcs) or Recombination-Activating Gene (Rag)1 Activity

Mats Bemarka, Julian E. Salea, Hye-Jung Kimb, Claudia Berekb, Ruth A. Cosgrovea, and Michael S. Neubergera

a Medical Research Council Laboratory of Molecular Biology, Cambridge CB2 2QH, United Kingdom
b Deutsches Rheuma ForschungsZentrum, Berlin 10117, Germany
Medical Research Council Laboratory of Molecular Biology, Hills Rd., Cambridge CB2 2QH, UK.44-1223-41217844-1223-402245

Somatic hypermutation and isotype switch recombination occur in germinal center B cells, are linked to transcription, and are similarly affected by deficiency in MutS homologue (MSH)2. Class-switch recombination is abrogated by disruption of genes encoding components of the catalytic subunit of DNA-dependent protein kinase (DNA-PKcs)/Ku complex and likely involves nonhomologous end joining (NHEJ). That somatic hypermutation might also be associated with end joining is suggested by its association with the creation of deletions, duplications, and sites accessible to terminal transferase. However, a requirement for NHEJ in the mutation process has not been demonstrated. Here we show that somatic mutation in mice deficient in NHEJ can be tested by introduction of rearranged immunoglobulin and T cell receptor transgenes: the transgene combination not only permits reconstitution of peripheral lymphoid compartments but also allows formation of germinal centers, despite the wholly monoclonal nature of the lymphocyte antigen receptors in these animals. Using this strategy, we confirm that somatic hypermutation like class-switching can occur in the absence of recombination-activating gene (RAG)1 but show that the two processes differ in that hypermutation can proceed essentially unaffected by deficiency in DNA-PKcs activity.

Key Words: immunoglobulin gene • B lymphocyte • switch recombination • end-joining • mutation

M. Bemark and J.E. Sale contributed equally to this work.

© 2000 The Rockefeller University Press


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