The most frequent DCLRE1C (ARTEMIS) mutations are based on homologous recombination events.

[omenn syndrome]

The nuclease ARTEMIS is an essential factor of V (D )J recombination during lymphocyte development and in the repair of DNA double -strand breaks (DSB ) by the nonhomologous end joining (NHEJ ) pathway . Patients with mutations in the DCLRE 1 C gene , which encodes ARTEMIS , suffer from radiosensitive B (-/low ) T (-/low ) severe combined immunodeficiency (SCID ) or radiosensitive Omenn syndrome . To date , causative DCLRE 1 C mutations inherited as a recessive trait have been reported in 49 patients . In this study , molecular diagnoses of 29 novel patients presenting with the phenotype of B (-/low ) SCID revealed mutations in the DCLRE 1 C gene . In total , 13 different mutated DCLRE 1 C alleles were detected , nine of which have not been described before . By far the most frequent mutations (59 %) were gross deletions of exons 1 -3 or exons 1 -4 due to a homologous recombination of the wild-type DCLRE 1 C gene with a pseudo-DCLRE 1 C gene located 61 .2 kb 5 ' to the DCLRE 1 C start codon . Fine mapping of the recombination intervals revealed private mutations in most cases . MEIG 1 , a gene encoding a protein that is essential for spermatogenesis in mice , is lost by the gross deletions . Functional analyses on patients ' fibroblasts demonstrated that the corresponding alleles carry null mutations of the DCLRE 1 C gene .