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Dimeric quaternary structure of human laforin.

ABSTRACT: The phosphatase laforin removes phosphate groups from glycogen during biosynthetic activity. Loss-of-function mutations in the gene encoding laforin is the predominant cause of Lafora disease, a fatal form of progressive myoclonic epilepsy. Here, we used hybrid structural methods to determine the molecular architecture of human laforin. We found that laforin adopts a dimeric quaternary structure, topologically similar to the prototypical dual specificity phosphatase VH1. The interface between the laforin carbohydrate-binding module and the dual specificity phosphatase domain generates an intimate substrate-binding crevice that allows for recognition and dephosphorylation of phosphomonoesters of glucose. We identify novel molecular determinants in the laforin active site that help decipher the mechanism of glucan phosphatase activity.

SUBMITTER: Sankhala RS 

PROVIDER: S-EPMC4335197 | biostudies-literature | 2015 Feb

REPOSITORIES: biostudies-literature

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Dimeric quaternary structure of human laforin.

Sankhala Rajeshwer S RS   Koksal Adem C AC   Ho Lan L   Nitschke Felix F   Minassian Berge A BA   Cingolani Gino G  

The Journal of biological chemistry 20141223 8

The phosphatase laforin removes phosphate groups from glycogen during biosynthetic activity. Loss-of-function mutations in the gene encoding laforin is the predominant cause of Lafora disease, a fatal form of progressive myoclonic epilepsy. Here, we used hybrid structural methods to determine the molecular architecture of human laforin. We found that laforin adopts a dimeric quaternary structure, topologically similar to the prototypical dual specificity phosphatase VH1. The interface between th  ...[more]

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