The Replication Focus Targeting Sequence (RFTS) Domain Is a DNA-competitive Inhibitor of Dnmt1

Structural Genomics Consortium and Department of Physiology, University of Toronto, Toronto, Ontario M5G 1L7, Canada.
Journal of Biological Chemistry (Impact Factor: 4.57). 03/2011; 286(17):15344-51. DOI: 10.1074/jbc.M110.209882
Source: PubMed


Dnmt1 (DNA methyltransferase 1) is the principal enzyme responsible for maintenance of cytosine methylation at CpG dinucleotides in the mammalian genome. The N-terminal replication focus targeting sequence (RFTS) domain of Dnmt1 has been implicated in subcellular localization, protein association, and catalytic function. However, progress in understanding its function has been limited by the lack of assays for and a structure of this domain. Here, we show that the naked DNA- and polynucleosome-binding activities of Dnmt1 are inhibited by the RFTS domain, which functions by virtue of binding the catalytic domain to the exclusion of DNA. Kinetic analysis with a fluorogenic DNA substrate established the RFTS domain as a 600-fold inhibitor of Dnmt1 enzymatic activity. The crystal structure of the RFTS domain reveals a novel fold and supports a mechanism in which an RFTS-targeted Dnmt1-binding protein, such as Uhrf1, may activate Dnmt1 for DNA binding.

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    • "In order to avoid runaway methylation , DNMT1 undergoes to several auto - inhibitory mechanisms . In particular , to keep DNMT1 inactive the RFTS domain is positioned and stabilized deep inside the catalytic domain in a task where the hemimethy - lated DNA is expected to fit , thus , masking the catalytic core of the enzyme ( Qin et al . , 2011 ; Syeda et al . , 2011 ; Bashtrykov et al . , 2014 ) . The auto - inhibitory function of the CXXC domain is more controversial . Song et al . ( 2011 ) . reported that CXXC specifically binds to unmethylated CpG , activating the CXXC - BH21 linker , which then occupies the catalytic pocket and interferes with its function . By contrast , Bashtrykov et al . ( 2"
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    • "This suggests that Uhrf1 may act to first engage a hemimethylated site which is then subsequently bound by Dnmt1, displacing Uhrf1, before the methylation reaction can occur [95]. A displacement type mechanism may be mediated through the replication foci targeting sequence (RFTS) domain in Dnmt1 that normally functions to inhibit catalytic activity [96] [97]. This is supported by reports that Uhrf1 interacts with Dnmt1 through the RFTS domain [98], and this interaction may be instrumental in relieving the autoinhibitory effect on Dnmt1, making it competent for DNA methylation . "
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    • "The function of the RFTS domain of mammalian DNMT1 has been the subject of several studies [27], [32], [39], [49]. However, the role of RFTS domains in proteins such as Raf2 in organisms like S. pombe that lack DNA methylation remains unknown. "
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