In developing lymphocytes, the recombination activating gene endonuclease cleaves DNA between V, D, or J coding and recombination signal (RS) sequences to form hairpin coding and blunt RS ends, which are fused to form coding and RS joins. Nonhomologous end joining (NHEJ) factors repair DNA double strand breaks including those induced during VDJ recombination. Human radiosensitive severe combined immunodeficiency results from lack of Artemis function, an NHEJ factor with in vitro endonuclease/exonuclease activities. We inactivated Artemis in murine embryonic stem (ES) cells by targeted mutation. Artemis deficiency results in impaired VDJ coding, but not RS, end joining. In addition, Artemis-deficient ES cells are sensitive to a radiomimetic drug, but less sensitive to ionizing radiation. VDJ coding joins from Artemis-deficient ES cells, which surprisingly are distinct from the highly deleted joins consistently obtained from DNA-dependent protein kinase catalytic subunit–deficient ES cells, frequently lack deletions and often display large junctional palindromes, consistent with a hairpin coding end opening defect. Strikingly, Artemis-deficient ES cells have increased chromosomal instability including telomeric fusions. Thus, Artemis appears to be required for a subset of NHEJ reactions that require end processing. Moreover, Artemis functions as a genomic caretaker, most notably in prevention of translocations and telomeric fusions. As Artemis deficiency is compatible with human life, Artemis may also suppress genomic instability in humans.
Defective DNA Repair and Increased Genomic Instability in Artemis-deficient Murine Cells
S. Rooney and J. Sekiguchi contributed equally to this work.
The online version of this article contains supplemental material.
Abbreviations used in this paper: DNA-PKcs, DNA-dependent protein kinase catalytic subunit; DSB, double strand break; ES, embryonic stem; ICL, interstrand cross-links; IR, ionizing radiation; Lig4, ligase 4; MMC, mitomycin C; NHEJ, nonhomologous end joining; P, palindromic; RS, recombination signal; RS-SCID, radiosensitive T− B− SCID; SKY, spectral karyotyping.
Sean Rooney, Frederick W. Alt, David Lombard, Scott Whitlow, Mark Eckersdorff, James Fleming, Sebastian Fugmann, David O. Ferguson, David G. Schatz, JoAnn Sekiguchi; Defective DNA Repair and Increased Genomic Instability in Artemis-deficient Murine Cells . J Exp Med 3 March 2003; 197 (5): 553–565. doi: https://doi.org/10.1084/jem.20021891
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