Difference between revisions of "Phosphatase Subfamily DSP23"

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(Domain)
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=== Domain ===
 
=== Domain ===
Laforin has two domains: carbohydrate-binding module and phosphatase domain. The carbohydrate-binding module targets laforin to Lafora inclusion bodies <cite>Wang02, Ganesh04</cite>. The phosphatase domain can directly dephosphorylates glycogen <cite>Worby06, Gentry07</cite>.
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DSP23 has a single domain, the phosphatase domain. Actually, it is the shortest within DSP family.
[http://www.omim.org/allelicVariant/607566 Epilepsy-caused mutations] are found on both domains.
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=== Function ===
 
=== Function ===

Revision as of 19:48, 2 March 2015

Phosphatase Classification: Fold CC1: Superfamily CC1: Family DSP: Subfamily DSP23

summary...

Evolution

DSP23 is found in metazoan but lost in nematodes and most arthropods (unpublished data from gOrtholog) has a single member in human, DUSP23.

Domain

DSP23 has a single domain, the phosphatase domain. Actually, it is the shortest within DSP family.

Function

Laforin is a glucan phosphatase [1, 2].

laforin is also a phosphatase of muscle glycogen synthase (GS1) in polyglucosan bodies (PBs). In Lafora disease (LD), the deficiency of either laforin or E3 ligase malin causes massive accumulation of less-branched glycogen inclusions, known as Lafora bodies, also called polyglucosan bodies (PBs), in several types of cells including neurons. Once GS1-synthesized polyglucosan accumulates into PBs, laforin recruits malin to the PBs where laforin dephosphorylates, and malin degrades the GS1 in concert with GPBB and AGL1, resulting in a breakdown of polyglucosan [3]. Laforin also dephosphorylates Ser 9 of Glycogen synthase kinase 3 [4].

Laforin also as an adaptor protein involved in several physiological pathways [5]. For instance, the complex of laforin and malin modules protein phosphatase 1 regulatory subunit PPP1R3D via ubiquitination [6]. See [5] for details.

Links

Human DUSP23 page in Phosphatome.Net database.

References

  1. []