The checkpoint kinase Chk2 has a key role in delaying cell cycle progression in response to DNA damage. Upon activation by low-dose ionizing radiation (IR), which occurs in an ataxia telangiectasia mutated (ATM)-dependent manner, Chk2 can phosphorylate the mitosis-inducing phosphatase Cdc25C on an inhibitory site, blocking entry into mitosis, and p53 on a regulatory site, causing G 1 arrest. Here we show that the ATMdependent activation of Chk2 by ␥-radiation requires Nbs1, the gene product involved in the Nijmegen breakage syndrome (NBS), a disorder that shares with AT a variety of phenotypic defects including chromosome fragility, radiosensitivity, and radioresistant DNA synthesis. Thus, whereas in normal cells Chk2 undergoes a time-dependent increased phosphorylation and induction of catalytic activity against Cdc25C, in NBS cells null for Nbs1 protein, Chk2 phosphorylation and activation are both defective. Importantly, these defects in NBS cells can be complemented by reintroduction of wild-type Nbs1, but neither by a carboxyterminal deletion mutant of Nbs1 at amino acid 590, unable to form a complex with and to transport Mre11 and Rad50 in the nucleus, nor by an Nbs1 mutated at Ser343 (S343A), the ATM phosphorylation site. Chk2 nuclear expression is unaffected in NBS cells, hence excluding a mislocalization as the cause of failed Chk2 activation in Nbs1-null cells. Interestingly, the impaired Chk2 function in NBS cells correlates with the inability, unlike normal cells, to stop entry into mitosis immediately after irradiation, a checkpoint abnormality that can be corrected by introduction of the wild-type but not the S343A mutant form of Nbs1. Altogether, these findings underscore the crucial role of a functional Nbs1 complex in Chk2 activation and suggest that checkpoint defects in NBS cells may result from the inability to activate Chk2.The integrity of genetic information is essential for the life and survival of cells. Genomic lesions arising spontaneously during DNA replication or in response to oxidative metabolism or exposure to radiation or chemical mutagens need to be recognized and repaired. Delay of cell cycle progression at specific checkpoints provides the time necessary to prevent replication and segregation of damaged DNA and to process lesions (reviewed in references 52 and 57). A defective or incorrect activation of the surveillance and repair systems can lead to increased mutagenesis, genomic instability, and ultimately cancer (for a review, see reference 13).The Nijmegen breakage syndrome (NBS) and ataxia telangiectasia (AT) are rare human autosomal recessive diseases (22, 51) exhibiting hypersensitivity to ionizing radiation (IR), immunodeficiency, and increased predisposition to develop cancer. NBS patients, however, do not manifest the hallmarks of AT, i.e., cerebellar ataxia and oculocutaneous telangiectasia. At the cellular level, NBS and AT patients show chromosome instability, hypersensitivity to genotoxic agents, and cell cycle checkpoints defects (1,29,30). These similarities su...
