An ATM-like gene was identified in the genome of Caenorhabditis elegans. The putative product of the gene, termed
Ce-atl-1 (C. elegans ATM-like 1) consists of 2514 amino acid residues. The C-terminal sequence, which contains a PI-3 kinase-like domain, showed good homology with the products of the gene MEC1/ESR1 from budding yeast, the
rad3+ gene of fission yeast and mammalian ATM (ataxia-telangiectasia and
rad3+ related) genes. The results of RNA-mediated interference indicated that the major phenotype associated with repression of
Ce-atl-1 was lethality (approximately 50-80%) during early embryogenesis. Among the surviving progeny, males (XO animals) arose at a high frequency (2-30%). In addition, 5% of oocyte chromosomes demonstrated aneuploidy due to a defect in pre-meiotic chromosomal segregation. Gene expression analyses indicated that
Ce-atl-1 mRNA was expressed in all larval stages and that its level increased about fivefold in the adult stage. The adult expression level was decreased in the
glp-4 mutant, which is defective in germ line proliferation.
Ce-atl-1 was strongly expressed in both the mitotic and meiotic cells of adult gonads. In summary,
Ce-atl-1 appears to be important for early embryogenesis, and loss of its function results in a defect in chromosome segregation, similar to what has been observed for AT-related proteins.