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Fine mapping of the X-linked recessive congenital idiopathic nystagmus locus at Xq24-q26.3

Version 2 2025-03-18, 23:58
Version 1 2023-05-16, 18:23
journal contribution
posted on 2025-03-18, 23:58 authored by JE Self, S Ennis, A Collins, F Shawkat, CM Harris, David MackeyDavid Mackey, PR Hodgkins, IK Temple, XL Chen, AJ Lotery
Purpose: To refine the interval for X-linked congenital idiopathic nystagmus at Xq24-q26.3 and to evaluate a novel candidate gene (Muscleblind-like 3 gene [MBNL3]). Methods: A single pedigree with congenital idiopathic nystagmus (CIN) inherited as an X-linked recessive trait underwent detailed clinical examination including nystagmology and electrophysiological investigation in selected subjects. Following detailed phenotyping, genotyping was performed using 52 microsatellite markers spaced at an average of 5 cM along the X chromosome. Subsequent two-point and multipoint linkage analysis were performed and a candidate gene was screened for mutations by conventional sequencing. Results: Linkage mapping located the disease gene to a 15.5cM interval at Xq24-q26.3, between markers DXS1212 and DXS1062 with a maximum two-point LOD score of 4.24 with both markers DXS8044 and DXS994 (φ=0). Multipoint analysis indicated a LOD score of 4.54 and a critical gene interval of 8.0 cM. No mutations were found in the MBNL3 gene in this pedigree. Conclusions: We describe a family with an unusual inheritance pattern most consistent with X-linked recessive inheritance with X inactivation causing manifesting females. We refine the linkage interval for X-linked recessive congenital idiopathic nystagmus and exclude MBNL3 as the causative gene in this family. ©2006 Molecular Vision.

History

Publication title

Molecular Vision

Volume

12

Issue

136-38

Pagination

1211-1216

ISSN

1090-0535

Department/School

Medicine

Publisher

Molecular Vision

Publication status

  • Published

Place of publication

USA

Socio-economic Objectives

200199 Clinical health not elsewhere classified

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