A function retained by the common mutant CLN3 protein is responsible for the late onset of juvenile neuronal ceroid lipofuscinosis

Claudia Kitzmüller¹, Rebecca L. Haines¹^,2, Sandra Codlin¹, Daniel F. Cutler¹^,3^,4 and Sara E. Mole¹^,2^,5^,*

¹ MRC Laboratory for Molecular Cell Biology ² Department of Biology ³ MRC Cell Biology Unit ⁴ Department of Biochemistry and Molecular Biology ⁵ General and Adolescent Paediatric Unit, UCL Institute of Child Health, University College London, UK

^* To whom correspondence should be addressed: MRC Laboratory for Molecular Cell Biology, University College London Gower Street, London WC1E 6BT, UK. Tel: +44 2076797257; Fax: +44 2076797805; Email: s.mole{at}ucl.ac.uk

Received September 19, 2007; Revised September 19, 2007; Accepted October 11, 2007

The neuronal ceroid lipofuscinoses (NCLs) are common neurodegenerativedisorders of childhood and are classified as lysosomal storagediseases since affected cells exhibit lysosomes containing ceroidand lipofuscin-like material. CLN3 is the most widely conservedNCL gene, suggesting that it has a basic eukaryotic cell function;its loss might be expected to cause the earliest onset and/ormost severe disease. However, mutations in CLN3 are linked tojuvenile NCL (JNCL), the latest onset and mildest form of NCLin children. We sought to explain this paradox. Almost all patientswith JNCL are homozygous or heterozygous for an intragenic 1kb deletion within CLN3, hitherto presumed to be a null mutation.We hypothesized that the 1 kb mutation may allow CLN3 residualfunction. We confirmed the presence of CLN3 transcripts in JNCLpatient cells. When RNA silencing was used to deplete thesetranscripts in cells from JNCL patients, the lysosomes significantlyincreased in size, confirming the presence of functional proteinin these cells. Consistently, overexpression of mutant CLN3transcript caused lysosomes to decrease in size. We modelledthe JNCL mutant transcripts and those corresponding to mousemodels for Cln3 in Schizosaccharomyces pombe and confirmed thatmost transcripts retained significant function as we predicted.Therefore, we concluded that the common mutant CLN3 proteindoes indeed retain significant function and that JNCL is a mutation-specificdisease phenotype. This finding has important consequences forrecognition and diagnosis of disease caused by mutations inCLN3 and for the development of therapy for JNCL.

Add to CiteULike CiteULike Add to Connotea Connotea Add to Del.icio.us Del.icio.us What's this?

This article has been cited by other articles:

C.-H. Chan, H. M. Mitchison, and D. A. Pearce
Transcript and in silico analysis of CLN3 in juvenile neuronal ceroid lipofuscinosis and associated mouse models
Hum. Mol. Genet., November 1, 2008; 17(21): 3332 - 3339.
[Abstract] [Full Text] [PDF]

S. Codlin, R. L. Haines, J. Jemima, E. Burden, and S. E. Mole
btn1 affects cytokinesis and cell-wall deposition by independent mechanisms, one of which is linked to dysregulation of vacuole pH
J. Cell Sci., September 1, 2008; 121(17): 2860 - 2870.
[Abstract] [Full Text] [PDF]

				S. Codlin, R. L. Haines, J. Jemima, E. Burden, and S. E. Mole btn1 affects cytokinesis and cell-wall deposition by independent mechanisms, one of which is linked to dysregulation of vacuole pH J. Cell Sci., September 1, 2008; 121(17): 2860 - 2870. [Abstract] [Full Text] [PDF]

Human Molecular Genetics

A function retained by the common mutant CLN3 protein is responsible for the late onset of juvenile neuronal ceroid lipofuscinosis