Literature DB >> 10647186

The three-dimensional structure of the HRDC domain and implications for the Werner and Bloom syndrome proteins.

Z Liu1, M J Macias, M J Bottomley, G Stier, J P Linge, M Nilges, P Bork, M Sattler.   

Abstract

BACKGROUND: The HRDC (helicase and RNaseD C-terminal) domain is found at the C terminus of many RecQ helicases, including the human Werner and Bloom syndrome proteins. RecQ helicases have been shown to unwind DNA in an ATP-dependent manner. However, the specific functional roles of these proteins in DNA recombination and replication are not known. An HRDC domain exists in both of the human RecQ homologues that are implicated in human disease and may have an important role in their function.
RESULTS: We have determined the three-dimensional structure of the HRDC domain in the Saccharomyces cerevisiae RecQ helicase Sgs1p by nuclear magnetic resonance (NMR) spectroscopy. The structure resembles auxiliary domains in bacterial DNA helicases and other proteins that interact with nucleic acids. We show that a positively charged region on the surface of the Sgs1p HRDC domain can interact with DNA. Structural similarities to bacterial DNA helicases suggest that the HRDC domain functions as an auxiliary domain in RecQ helicases. Homology models of the Werner and Bloom HRDC domains show different surface properties when compared with Sgs1p.
CONCLUSIONS: The HRDC domain represents a structural scaffold that resembles auxiliary domains in proteins that are involved in nucleic acid metabolism. In Sgs1p, the HRDC domain could modulate the helicase function via auxiliary contacts to DNA. However, in the Werner and Bloom syndrome helicases the HRDC domain may have a role in their functional differences by mediating diverse molecular interactions.

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Year:  1999        PMID: 10647186     DOI: 10.1016/s0969-2126(00)88346-x

Source DB:  PubMed          Journal:  Structure        ISSN: 0969-2126            Impact factor:   5.006


  58 in total

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2.  Topography for independent binding of alpha-helical and PPII-helical ligands to a peroxisomal SH3 domain.

Authors:  Alice Douangamath; Fabian V Filipp; André T J Klein; Phil Barnett; Peijian Zou; Tineke Voorn-Brouwer; M Cristina Vega; Olga M Mayans; Michael Sattler; Ben Distel; Matthias Wilmanns
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3.  Domain mapping of Escherichia coli RecQ defines the roles of conserved N- and C-terminal regions in the RecQ family.

Authors:  Douglas A Bernstein; James L Keck
Journal:  Nucleic Acids Res       Date:  2003-06-01       Impact factor: 16.971

4.  Structural and functional homology between the RNAP(I) subunits A14/A43 and the archaeal RNAP subunits E/F.

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5.  Contribution of domain structure to the RNA 3' end processing and degradation functions of the nuclear exosome subunit Rrp6p.

Authors:  Seasson Phillips; J Scott Butler
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6.  Analysis of the unwinding activity of the dimeric RECQ1 helicase in the presence of human replication protein A.

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Review 7.  RecQ helicases; at the crossroad of genome replication, repair, and recombination.

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Journal:  Mol Biol Rep       Date:  2011-09-23       Impact factor: 2.316

8.  Influence of chemical shift tolerances on NMR structure calculations using ARIA protocols for assigning NOE data.

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Review 9.  Developing master keys to brain pathology, cancer and aging from the structural biology of proteins controlling reactive oxygen species and DNA repair.

Authors:  J J P Perry; L Fan; J A Tainer
Journal:  Neuroscience       Date:  2006-12-15       Impact factor: 3.590

10.  High-resolution structure of the E.coli RecQ helicase catalytic core.

Authors:  Douglas A Bernstein; Morgan C Zittel; James L Keck
Journal:  EMBO J       Date:  2003-10-01       Impact factor: 11.598

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