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Genomic characterization of some Iranian children with idiopathic mental retardation using array comparative genomic hybridization
Authors:Farkhondeh Behjati  Saghar Ghasemi Firouzabadi  Roxana Kariminejad  Roshanak Vameghi  Firouzeh Sajedi  Yousef Shafaghati  Behruz Ebrahimizade Ghasemlou  Azadeh Shojaei  Peyman Jamali  Ideh Bahman  Hossein Najmabadi
Abstract:

BACKGROUND:

Mental retardation (MR) has a prevalence of 1-3% and genetic causes are present in more than 50% of patients. Chromosomal abnormalities are one of the most common genetic causes of MR and are responsible for 4-28% of mental retardation. However, the smallest loss or gain of material visible by standard cytogenetic is about 4 Mb and for smaller abnormalities, molecular cytogenetic techniques such as array comparative genomic hybridization (array CGH) should be used. It has been shown that 15-25% of idiopathic MR (IMR) has submicroscopic rearrangements detectable by array CGH. In this project, the genomic abnormalities were investigated in 32 MR patients using this technique.

MATERIALS AND METHODS:

Patients with IMR with dysmorphism were investigated in this study. Karyotype analysis, fragile X and metabolic tests were first carried out on the patients. The copy number variation was then assessed in a total of 32 patients with normal results for the mentioned tests using whole genome oligo array CGH. Multiple ligation probe amplification was carried out as a confirmation test.

RESULTS:

In total, 19% of the patients showed genomic abnormalities. This is reduced to 12.5% once the two patients with abnormal karyotypes (upon re-evaluation) are removed.

CONCLUSION:

The array CGH technique increased the detection rate of genomic imbalances in our patients by 12.5%. It is an accurate and reliable method for the determination of genomic imbalances in patients with IMR and dysmorphism.
Keywords:Array comparative genomic hybridization  chromosome abnormality  dysmorphism  genomic variation  idiopathic mental retardation
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