CLRN1 Mutations Cause Nonsyndromic Retinitis Pigmentosa
Objective
To describe the mutations in the CLRN1 gene in patients from 2 consanguineous Pakistani families diagnosed with autosomal recessive retinitis pigmentosa (arRP).
Design
Case-series study.
Participants
Affected and unaffected individuals of 2 consanguineous Pakistani families and 90 unaffected controls from the same population. Informed consent was obtained from participants and the protocol was approved by a local institutional review board.
Methods
Patients of 2 consanguineous families were genotyped with single-nucleotide polymorphism microarrays for genome-wide linkage analysis. The search for potential candidate genes within the 8-Mb overlapping homozygous region in these families revealed the presence of CLRN1, a gene previously known to cause Usher's syndrome type III (USH3), which was analyzed by direct sequence analysis. The clinical diagnosis was based on the presence of night blindness, fundoscopic findings, and electroretinography (ERG) results. Additionally, pure tone audiometry was performed to rule out Usher's syndrome.
Main Outcome Measures
Fundoscopy, single-nucleotide polymorphism microarray, DNA sequence analysis, ERG, and audiometry.
Results
Sequencing of CLRN1 revealed novel missense mutations (p.Pro31Leu and p.Leu154Trp) segregating in 2 families. Analysis of fundus photographs indicated attenuation of the retinal vessels, and bone spicule pigmentation in the periphery of the retina. The ERG responses were indicative of a rod–cone pattern of the disease. Audiometric assessment revealed no hearing impairment, thereby excluding Usher's syndrome. Subcellular localization studies demonstrated the retention of the mutant proteins in the endoplasmic reticulum, whereas the wild-type protein was mainly present at the cell membrane.
Conclusions
The RP-associated mutations p.Pro31Leu and p.Leu154Trp may represent hypomorphic mutations, because the substituted amino acids located in the transmembrane domains remain polar, whereas more severe changes have been detected in patients with USH3. These data indicate that mutations in CLRN1 are associated not only with USH3, but also with nonsyndromic arRP.
Financial Disclosure(s)
The authors have no proprietary or commercial interest in any of the materials discussed in this article.
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Manuscript no. 2010-1055.
M.I.K. and F.F.J.K. contributed equally to this manuscript.
Financial Disclosure(s): The authors have no proprietary or commercial interest in any of the materials discussed in this article.
Supported by grant no. 530 awarded (to R.Q.) by the Higher Education Commission of Pakistan and a core grant from the Shifa College of Medicine. This study was also supported by the Foundation Fighting Blindness USA (BR-GE-0507-0381-RAD to A.I.d.H.), Stichting Nederlands Oogheelkundig Onderzoek, the Stichting Nelly Reef Fund, and the Stichting ter Verbetering van het Lot der Blinden (to F.P.M.C). None of the authors have any financial or conflicting interest to disclose.
PII: S0161-6420(10)01168-1
doi:10.1016/j.ophtha.2010.10.047
© 2011 American Academy of Ophthalmology. Published by Elsevier Inc. All rights reserved.
