A small recurrent deletion within 15q13.3 is associated with a range of neurodevelopmental phenotypes.

Marwan Shinawi,Christian P. Schaaf,Samarth Bhatt,Zhilian Xia,Ankita Patel,Sau Wai Cheung,Brendan Lanpher,Sandra Nagl,Heinrich Stephan Herding,Claudia Nevinny-Stickel,LaDonna Immken,Gayle Patel,Jennifer Ruth German,Arthur L. Beaudet,Pawel Stankiewicz

A small recurrent deletion within 15q13.3 is associated with a range of neurodevelopmental phenotypes.

2009

Marwan Shinawi
Christian P. Schaaf
Samarth Bhatt
Zhilian Xia
Ankita Patel
Sau Wai Cheung
Brendan Lanpher
Sandra Nagl
Heinrich Stephan Herding
Claudia Nevinny-Stickel
LaDonna Immken
Gayle Patel
Jennifer Ruth German
Arthur L. Beaudet
Pawel Stankiewicz

We report a recurrent 680-kb deletion within chromosome 15q13.3 in ten individuals, from four unrelated families, with neurodevelopmental phenotypes including developmental delay, mental retardation and seizures. This deletion likely resulted from nonallelic homologous recombination between low-copy repeats on the normal and inverted region of chromosome 15q13.3. Although this deletion also affects OTUD7A, accumulated data suggest that haploinsufficiency of CHRNA7 is causative for the majority of neurodevelopmental phenotypes in the 15q13.3 microdeletion syndrome.

Keywords:

Microdeletion syndrome
CHRNA7
Phenotype
Genetics
Chromosome
Intellectual disability
Non-allelic homologous recombination
Molecular biology
Haploinsufficiency
Biology

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