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Combined Molecular and Cytogenetic Analysis for the Rapid Diagnosis of Fragile X Syndrome

Published online by Cambridge University Press:  01 August 2014

C. Bussani Mastellone*
Affiliation:
Human Genetics Service, University of Florence, Florence, Italy
M.L. Giovannucci Uzielli
Affiliation:
Human Genetics Service, University of Florence, Florence, Italy
M. Grasso
Affiliation:
Genetics Centre, Galliera Hospital, Genoa, Italy
P. Chiurazzi
Affiliation:
Institute of Medical Genetics, Catholic University, Rome, Italy
G. Neri
Affiliation:
Institute of Medical Genetics, Catholic University, Rome, Italy
Q. Wang
Affiliation:
Division of Medical and Molecular Genetics, Paediatric Research Unit, Guy's Hospital, London, England
*
Human Genetics Service, University of Florence, Via Masaccio 209, Florence 50132, Italy

Abstract

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The fragile X mutation is the result of an abnormal expansion of a CGG repeat sequence in the FMR-1 gene.

Molecular techniques enable the detection of the mutation and also of the exact length of this DNA sequence, allowing the classification of the tested subjects as normal, carrier or affected.

We propose a protocol of analysis that combines a method of non-radioactive PCR, Southern blotting and cytogenetic testing.

This protocol can be used for screening programme of selected groups of mentally retarded individuals and for prevention studies in families at risk.

Type
Research Article
Copyright
Copyright © The International Society for Twin Studies 1996

References

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