The malin-laforin complex suppresses the cellular toxicity of misfolded proteins by promoting their degradation through the ubiquitin-proteasome system

doi:10.1093/hmg/ddn398

Human Molecular Genetics Advance Access originally published online on November 25, 2008
Human Molecular Genetics 2009 18(4):688-700; doi:10.1093/hmg/ddn398

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The malin–laforin complex suppresses the cellular toxicity of misfolded proteins by promoting their degradation through the ubiquitin–proteasome system

Punitee Garyali, Pratibha Siwach, Pankaj Kumar Singh, Rajat Puri, Shuchi Mittal, Sonali Sengupta, Rashmi Parihar and Subramaniam Ganesh^*

Department of Biological Sciences and Bioengineering, Indian Institute of Technology, Kanpur 208016, India

^* To whom correspondence should be addressed. Tel: +91 5122594040; Fax: +91 5122594010; Email: sganesh{at}iitk.ac.in

Received August 16, 2008; Accepted November 19, 2008

Lafora disease (LD), a progressive form of inherited epilepsy,is associated with widespread neurodegeneration and the formationof polyglucosan bodies in the neurons. Laforin, a protein phosphatase,and malin, an E3 ubiquitin ligase, are two of the proteins thatare defective in LD. We have shown recently that laforin andmalin (referred together as LD proteins) are recruited to aggresomeupon proteasomal blockade, possibly to clear misfolded proteinsthrough the ubiquitin–proteasome system (UPS). Here wetest this possibility using a variety of cytotoxic misfoldedproteins, including the expanded polyglutamine protein, as potentialsubstrates. Laforin and malin, together with Hsp70 as a functionalcomplex, suppress the cellular toxicity of misfolded proteins,and all the three members of this complex are required for thisfunction. Laforin and malin interact with misfolded proteinsand promote their degradation through the UPS. LD proteins arerecruited to the polyglutamine aggregates and reduce the frequencyof aggregate-positive cells. Taken together, our results suggestthat the malin–laforin complex is a novel player in theneuronal response to misfolded proteins and could be potentialtherapeutic targets for neurodegenerative disorders associatedwith cytotoxic proteins.

The authors wish it to be known that, in their opinion, thefirst two authors should be regarded as joint First Authors.

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