|
|||||
|
|
Identification of a homozygous splice site mutation in the dynein axonemal light chain 4 gene on 22q13.1 in a large consanguineous family from Pakistan with congenital mirror movement disorder |
|
| Authors: | Iltaf Ahmed Kirti Mittal Taimoor I Sheikh Nasim Vasli Muhammad Arshad Rafiq Anna Mikhailov Mehrnaz Ohadi Huda Mahmood Guy A Rouleau Attya Bhatti Muhammad Ayub Myriam Srour Peter John John B Vincent |
| Institution: | 1. Molecular Neuropsychiatry and Development (MiND) Lab, Centre For Addiction and Mental Health, Campbell Family Mental Health Research Institute, R32, 250 College Street, Toronto, ON, M5T 1R8, Canada 2. Atta-ur-Rehman School of Applied Biosciences (ASAB), National University of Sciences and Technology (NUST), Islamabad, Pakistan 8. Institute of Medical Science, University of Toronto, Toronto, ON, Canada 3. Montreal Neurological Institute and Hospital, McGill University, Montreal, QC, Canada 4. Division of Developmental Disabilities, Department of Psychiatry, Queen’s University, Kingston, ON, Canada 5. Division of Pediatric Neurology, Departments of Neurology/Neurosurgery, Montreal Children’s Hospital-McGill University Health Centre, Montreal, QC, Canada 6. Division of Pediatric Neurology, Department of Pediatrics, Montreal Children’s Hospital-McGill University Health Centre, Montreal, QC, Canada 7. Department of Psychiatry, University of Toronto, Toronto, ON, Canada |
| Abstract: | Mirror movements (MRMV) are involuntary movements on one side of the body that mirror voluntary movements on the opposite side. Congenital mirror movement disorder is a rare, typically autosomal-dominant disorder, although it has been suspected that some sporadic cases may be due to recessive inheritance. Using a linkage analysis and a candidate gene approach, two genes have been implicated in congenital MRMV disorder to date: DCC on 18q21.2 (MRMV1), which encodes a netrin receptor, and RAD51 on 15q15.1 (MRMV2), which is involved in the maintenance of genomic integrity. Here, we describe a large consanguineous Pakistani family with 11 cases of congenital MRMV disorder reported across five generations, with autosomal recessive inheritance likely. Sanger sequencing of DCC and RAD51 did not identify a mutation. We then employed microarray genotyping and autozygosity mapping to identify a shared region of homozygosity-by-descent among the affected individuals. We identified a large autozygous region of ~3.3 Mb on chromosome 22q13.1 (Chr22:36605976?39904648). We used Sanger sequencing to exclude several candidate genes within this region, including DMC1 and NPTXR. Whole exome sequencing was employed, and identified a splice site mutation in the dynein axonemal light chain 4 gene, DNAL4. This splice site change leads to skipping of exon 3, and omission of 28 amino acids from DNAL4 protein. Linkage analysis using Simwalk2 gives a maximum Lod score of 6.197 at this locus. Whether or how DNAL4 function may relate to the function of DCC or RAD51 is not known. Also, there is no suggestion of primary ciliary dyskinesis, situs inversus, or defective sperm in affected family members, which might be anticipated given a putative role for DNAL4 in axonemal-based dynein complexes. We suggest that DNAL4 plays a role in the cytoplasmic dynein complex for netrin-1-directed retrograde transport, and in commissural neurons of the corpus callosum in particular. This, in turn, could lead to faulty cross-brain wiring, resulting in MRMV. |
| Keywords: | |
| 本文献已被 SpringerLink 等数据库收录! | |