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Article Dans Une Revue Biochemistry Année : 2008

Human Mismatch Repair Protein MSH6 Contains a PWWP Domain That Targets Double Stranded DNA

Résumé

The eukaryotic mismatch repair (MMR) protein MSH6 exhibits a core region structurally and functionally similar to bacterial MutS. However, it possesses an additional N-terminal region (NTR), comprising a PCNA binding motif, a large region of unknown function and a nonspecific DNA binding fragment. Yeast NTR was recently described as an extended tether between PCNA and the core of MSH6 (1). In contrast, we show that human NTR presents a globular PWWP domain in the region of unknown function. We demonstrate that this PWWP domain binds double-stranded DNA, without any preference for mismatches or nicks, whereas its apparent affinity for single-stranded DNA is about 20 times lower. The S144I mutation, which in human MSH6 causes inherited somatic defects in MMR resulting in increased development of hereditary non polyposis colorectal cancer (2), is located in the DNA binding surface of the PWWP domain. However, it only moderately affects domain stability, and it does not perturb DNA binding in Vitro.
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Dates et versions

hal-00289019 , version 1 (19-06-2008)

Identifiants

  • HAL Id : hal-00289019 , version 1

Citer

Cédric Laguri, Isabelle Duband-Goulet, Nikolas Friedrich, Marianne Axt, Pascal Belin, et al.. Human Mismatch Repair Protein MSH6 Contains a PWWP Domain That Targets Double Stranded DNA. Biochemistry, 2008, 47, pp.6199-6207. ⟨hal-00289019⟩
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