PMD Browser
Detalied information of PMD entry
Entry name
A000159
Type
Artificial
Create date
2007-10-12 15:51:18
Mutated sequences
| No | Name | Length (aa) | Mutated Proteins (Name / Length / Disease name(s) / OMIM term(s)) | ||||||||||
| 1 | A000159 | 345 |
|
References
Title
Structural basis for recognition and repair of the endogenous mutagen 8-oxoguanine in DNA.
Journal name
Nature.
Publication date
2000 : (403) 859 - 866
Authors
Bruner SD, Norman DP, Verdine GL.
Affiliation
Department of Chemistry and Chemical Biology, Harvard University, Cambridge, Massachusetts 02138, USA.
Abstract
Spontaneous oxidation of guanine residues in DNA generates 8-oxoguanine (oxoG). By mispairing with adenine during replication, oxoG gives rise to a G x C --> T x A transversion, a frequent somatic mutation in human cancers. The dedicated repair pathway for oxoG centres on 8-oxoguanine DNA glycosylase (hOGG1), an enzyme that recognizes oxoG x C base pairs, catalysing expulsion of the oxoG and cleavage of the DNA backbone. Here we report the X-ray structure of the catalytic core of hOGG1 bound to oxoG x C-containing DNA at 2.1 A resolution. The structure reveals the mechanistic basis for the recognition and catalytic excision of DNA damage by hOGG1 and by other members of the enzyme superfamily to which it belongs. The structure also provides a rationale for the biochemical effects of inactivating mutations and polymorphisms in hOGG1. One known mutation, R154H, converts hOGG1 to a promutator by relaxing the specificity of the enzyme for the base opposite oxoG.
