Nuclear organization in DNA end processing: Telomeres vs double-strand breaks |
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| Affiliation: | 1. Department of Laboratory Medicine and Pathobiology, Faculty of Medicine, University of Toronto, 661 University Avenue, Toronto, ONT, M5G 1M1, Canada;2. Canada Research Chairs Program, Faculty of Medicine, University of Toronto, 1 King’s College Circle, Toronto, ONT, M5S 1A8, Canada |
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| Abstract: | Many proteins ligands are shared between double-strand breaks and natural chromosomal ends or telomeres. The structural similarity of the 3’ overhang, and the efficiency of cellular DNA end degradation machineries, highlight the need for mechanisms that resect selectively to promote or restrict recombination events. Here we examine the means used by eukaryotic cells to suppress resection at telomeres, target telomerase to short telomeres, and process broken ends for appropriate repair. Not only molecular ligands, but the spatial sequestration of telomeres and damage likely ensure that these two very similar structures have very distinct outcomes with respect to the DNA damage response and repair. |
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| Keywords: | Double-strand break repair Telomeres DNA damage response Nuclear organization Nuclear pores SUN domain proteins |
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