DNA double-strand break repair and development

被引:40
作者
Phillips, E. R.
McKinnon, P. J.
机构
[1] St Jude Childrens Hosp, Dept Genet & Tumor Cell Biol, Memphis, TN 38105 USA
[2] Univ Tennessee, Ctr Hlth Sci, Memphis, TN 38163 USA
来源
ONCOGENE | 2007年 / 26卷 / 56期
关键词
DNA repair; double-strand breaks; ATM; NHEJ; development;
D O I
10.1038/sj.onc.1210877
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Normal development of an organism requires the ability to respond to DNA damage. A particularly deleterious lesion is a DNA double-strand break (DSB). The cellular response to DNA DSBs occurs via an integrated sensing and signaling network that maintains genomic stability. The outcomes of defective DNA DSB repair are related to the developmental stage of an organism, and often show striking tissue specificity. Many human diseases are associated with deficiencies in DNA DSB repair and can be characterized by neuropathology, immune deficiency, growth retardation or predisposition to cancer. This review will focus on the requirements of the DNA DSB response that function to maintain homeostasis during mammalian development.
引用
收藏
页码:7799 / 7808
页数:10
相关论文
共 147 条
[81]   MDC1 maintains genomic stability by participating in the amplification of ATM-dependent DNA damage signals [J].
Lou, ZK ;
Minter-Dykhouse, K ;
Franco, S ;
Gostissa, M ;
Rivera, MA ;
Celeste, A ;
Manis, JP ;
van Deursen, J ;
Nussenzweig, A ;
Paull, TT ;
Alt, FW ;
Chen, JJ .
MOLECULAR CELL, 2006, 21 (02) :187-200
[82]   MDC1 is coupled to activated CHK2 in mammalian DNA damage response pathways [J].
Lou, ZK ;
Minter-Dykhouse, K ;
Wu, XL ;
Chen, JJ .
NATURE, 2003, 421 (6926) :957-961
[83]   Development of mammary adenocarcinomas by tissue-specific knockout of Brca2 in mice [J].
Ludwig, T ;
Fisher, P ;
Murty, V ;
Efstratiadis, A .
ONCOGENE, 2001, 20 (30) :3937-3948
[84]   ATM and ATR substrate analysis reveals extensive protein networks responsive to DNA damage [J].
Matsuoka, Shuhei ;
Ballif, Bryan A. ;
Smogorzewska, Agata ;
McDonald, E. Robert, III ;
Hurov, Kristen E. ;
Luo, Ji ;
Bakalarski, Corey E. ;
Zhao, Zhenming ;
Solimini, Nicole ;
Lerenthal, Yaniv ;
Shiloh, Yosef ;
Gygi, Steven P. ;
Elledge, Stephen J. .
SCIENCE, 2007, 316 (5828) :1160-1166
[85]   ATM-dependent phosphorylation of Mdm2 on serine 395: role in p53 activation by DNA damage [J].
Maya, R ;
Balass, M ;
Kim, ST ;
Shkedy, D ;
Leal, JFM ;
Shifman, O ;
Moas, M ;
Buschmann, T ;
Ronai, Z ;
Shiloh, Y ;
Kastan, MB ;
Katzir, E ;
Oren, M .
GENES & DEVELOPMENT, 2001, 15 (09) :1067-1077
[86]   DNA strand break repair and human genetic disease [J].
McKinnon, Peter J. ;
Caldecott, Keith W. .
ANNUAL REVIEW OF GENOMICS AND HUMAN GENETICS, 2007, 8 :37-55
[87]   ATAXIA-TELANGIECTASIA - AN INHERITED DISORDER OF IONIZING-RADIATION SENSITIVITY IN MAN - PROGRESS IN THE ELUCIDATION OF THE UNDERLYING BIOCHEMICAL DEFECT [J].
MCKINNON, PJ .
HUMAN GENETICS, 1987, 75 (03) :197-208
[88]   ATM and ataxia telangiectasia - Second in Molecular Medicine Review Series [J].
McKinnon, PJ .
EMBO REPORTS, 2004, 5 (08) :772-776
[89]   Rad54 and DNA Ligase IV cooperate to maintain mammalian chromatid stability [J].
Mills, KD ;
Ferguson, DO ;
Essers, J ;
Eckersdorff, M ;
Kanaar, R ;
Alt, FW .
GENES & DEVELOPMENT, 2004, 18 (11) :1283-1292
[90]   Artemis, a novel DNA double-strand break repair/V(D)J recombination protein, is mutated in human severe combined immune deficiency [J].
Moshous, D ;
Callebaut, I ;
de Chasseval, R ;
Corneo, B ;
Cavazzana-Calvo, M ;
Le Deist, F ;
Tezcan, I ;
Sanal, O ;
Bertrand, Y ;
Philippe, N ;
Fischer, A ;
de Villartay, JP .
CELL, 2001, 105 (02) :177-186
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