Simultaneous MLPA-based multiplex point mutation and deletion analysis of the <Emphasis Type="Italic">Dystrophin</Emphasis> gene |
| |
| Authors: | David J Bunyan Alison C Skinner Emma J Ashton Julie Sillibourne Tom Brown Amanda L Collins Nicholas C P Cross John F Harvey David O Robinson |
| |
| Institution: | (1) National Genetics Reference Laboratory (Wessex), Salisbury Hospital NHS Trust, SP2 8BJ Salisbury, Wiltshire;(2) Wessex Regional Genetics Labortory, Salisbury Hospital NHS Trust, SP2 8BJ Salisbury, Wiltshire;(3) DNA Laboratory, 8th Floor, Guy's Tower, Guy's Hospital, St. Thomas Street, SE1 9RT London;(4) School of Chemistry, Universty of Southampton, SO17 1BJ Soathampton, Hampshire;(5) Wessex Clinical Genetics Service, Princess Anne Hospital, Coxford Road, SO16 5YA Southampton, Hamphire, UK |
| |
| Abstract: | The Multiplex Ligation-dependent Probe Amplification assay (MLPA) is the method of choice for the initial mutation screen
in the analysis of a large number of genes where partial or total gene deletion is part of the mutation spectrum. Although
MLPA dosage probes are usually designed to bind to normal DNA sequence to identify dosage imbalance, point mutation-specific
MLPA probes can also be made. Using the dystrophin gene as a model, we have designed two MLPA probe multiplexes that are specific
to a number of commonly listed point mutations in the Leiden dystrophin point mutation database (http://www.dmd.nl). The point
mutation probes are designed to work simultaneously with two widely used dystrophin MLPA multiplexes, allowing both full dosage
analysis and partial point mutation analysis in a single test. This approach may be adapted for other syndromes with well
defined common point mutations or polymorphisms. |
| |
| Keywords: | MLPA point mutations dystrophin dosage |
| 本文献已被 PubMed SpringerLink 等数据库收录! |
|
