Violation of the 12/23 rule of genomic V(D)J recombination is common in lymphocytes
Author(s) -
Nick Parkinson,
Matthew Roddis,
Ben Ferneyhough,
Gang Zhang,
Adam J. Marsden,
Siarhei Maslau,
Yasmin SánchezPearson,
Thomas Barthlott,
Ian R. Humphreys,
Kristin Ladell,
David A. Price,
Chris P. Ponting,
Georg A. Holländer,
Michael D. Fischer
Publication year - 2014
Publication title -
genome research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 9.556
H-Index - 297
eISSN - 1549-5469
pISSN - 1088-9051
DOI - 10.1101/gr.179770.114
Subject(s) - recombination signal sequences , v(d)j recombination , recombination , biology , genetics , gene rearrangement , gene , locus (genetics) , recombination activating gene , non allelic homologous recombination , genetic recombination
V(D)J genomic recombination joins single gene segments to encode an extensive repertoire of antigen receptor specificities in T and B lymphocytes. This process initiates with double-stranded breaks adjacent to conserved recombination signal sequences that contain either 12- or 23-nucleotide spacer regions. Only recombination between signal sequences with unequal spacers results in productive coding genes, a phenomenon known as the "12/23 rule." Here we present two novel genomic tools that allow the capture and analysis of immune locus rearrangements from whole thymic and splenic tissues using second-generation sequencing. Further, we provide strong evidence that the 12/23 rule of genomic recombination is frequently violated under physiological conditions, resulting in unanticipated hybrid recombinations in ∼10% of Tcra excision circles. Hence, we demonstrate that strict adherence to the 12/23 rule is intrinsic neither to recombination signal sequences nor to the catalytic process of recombination and propose that nonclassical excision circles are liberated during the formation of antigen receptor diversity.
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