| Literature DB >> 33556079 |
Sandrine Le Noir1, Amélie Bonaud1, Bastien Hervé2, Audrey Baylet1, François Boyer1, Sandrine Lecardeur1, Zeliha Oruc1, Christophe Sirac1, Michel Cogné1,3.
Abstract
DNA lesions inflicted by activation-induced deaminase (AID) instrumentally initiate the processes reshaping immunoglobulin genes in mature B-cells, from local somatic hypermutation (SHM) to junctions of distant breaks during class switch recombination (CSR). It remains incompletely understood how these divergent outcomes of AID attacks are differentially and temporally focused, with CSR strictly occurring in the Ig heavy chain (IgH) locus while SHM concentrates on rearranged V(D)J regions in the IgH and Ig light chain loci. In the IgH locus, disruption of either the 3'Regulatory Region (3'RR) super-enhancer or of switch (S) regions preceding constant genes, profoundly affects CSR. Reciprocally, we now examined if these elements are sufficient to induce CSR in a synthetic locus based on the Igκ locus backbone. Addition of a surrogate "core 3'RR" (c3'RR) and of a pair of transcribed and spliced Switch regions, together with a reporter system for "κ-CSR" yielded a switchable Igκ locus. While the c3'RR stimulated SHM at S regions, it also lowered the local SHM threshold necessary for switch recombination to occur. The 3'RR thus both helps recruit AID to initiate DNA lesions, but then also promotes their resolution through long-distance synapses and recombination following double-strand breaks.Entities:
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Year: 2021 PMID: 33556079 PMCID: PMC7869978 DOI: 10.1371/journal.pgen.1009288
Source DB: PubMed Journal: PLoS Genet ISSN: 1553-7390 Impact factor: 5.917