Deletion of C2orf34, PREPL and SLC3A1 causes atypical hypotonia-cystinuria syndrome

doi:10.1136/jmg.2007.055475

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Published Online First: 30 January 2008. doi:10.1136/jmg.2007.055475
Journal of Medical Genetics 2008;45:314-318

LETTERS TO JMG

Deletion of C2orf34, PREPL and SLC3A1 causes atypical hypotonia–cystinuria syndrome

B Chabrol¹, K Martens²^,3, S Meulemans², A Cano¹, J Jaeken⁴, G Matthijs³ and J W M Creemers²

¹ Reference Center for inborn metabolic disorders, CHU de la Timone, Marseille, France
² Laboratory for Biochemical Neuroendocrinology, Center for Human Genetics, University of Leuven, Belgium
³ Laboratory for Molecular Diagnosis, Center for Human Genetics, University of Leuven, Belgium
⁴ Center for Metabolic Disease, University of Leuven, Belgium

Correspondence to:
Dr J Creemers, Center for Human Genetics, University of Leuven, Gasthuisberg O/N 6, box 602, Herestraat 49, B-3000 Leuven; john.creemers{at}med.kuleuven.be

ABSTRACT

Background: Hypotonia–cystinuria syndrome (HCS) and 2p21 deletionsyndrome are two recessive contiguous gene deletion syndromesassociated with cystinuria type I. The deletions differ in sizeand the number of genes involved. In HCS patients, only SLC3A1and PREPL are disrupted. In the 2p21 deletion syndrome, twoadditional genes (C2orf34 and PPM1B) are lost.

Objective: Clinical and molecular analysis of two siblings who presentedwith an atypical HCS phenotype.

Methods: Molecular analysis of the SLC3A1/PREPL locus was performed inthe patients using quantitative polymerase chain reaction (PCR)methods.

Results: HCS in both siblings was confirmed with the deletion screenof the SLC3A1/PREPL locus. Fine mapping of the breakpoint revealeda deletion of 77.4 kb, including three genes: SLC3A1, PREPLand C2orf34. Features not present in classical HCS were a mild/moderatemental retardation and a respiratory chain complex IV deficiencydocumented in patient 2.

Conclusions: We report the first patients with a deletion of SLC3A1, PREPLand C2orf34. They present with a phenotype intermediate betweenHCS and 2p21 deletion syndrome. These patients facilitate theelucidation of the contribution of each gene to the phenotypein the different 2p21 deletion syndromes.

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