A 9-YEAR-OLD-GIRL WITH PHELAN McDERMID
SYNDROME, WHO HAD BEEN DIAGNOSED WITH AN
AUTISM SPECTRUM DISORDER
Görker I, Gürkan H, Demir Ulusal S, Atlı E, Ikbal Atlı E
*Corresponding Author: Işık Görker, Child and Adolescent Psychiatry Department, Trakya University, Faculty of Medicine,
Balkan Yerleskesi, 22030, Edirne, Turkey. Tel: +90-532-355-9277. Fax: +90-284-435-7652. E-mail: isikgorker@gmail.com
page: 85
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Abstract
Phelan McDermid Syndrome (PHMDS) (OMIM
#606232), is a contiguous gene disorder resulting from
deletion of the distal long arm of chromosome 22. The
22q13.3 deletions and mutations that lead to a loss of
a functional copy of SHANK3 (OMIM *606230) cause
the syndrome, characterized by moderate to profound intellectual
disability, severely delayed or absent speech,
hypotonia, and autism spectrum disorder (ASD) or ASD
traits. In this study, we present the case of a 9-year-old girl
who had earlier been diagnosed with an ASD. Our findings
were a clinically mild intellectual disability, rounded
face, pointed chin but no autistic findings. We learned that
her neuromotor development was delayed and she had
neonatal hypotonia in her history. A heterozygous deletion
of MLC1, SBF1, MAPK8IP2, ARSA, SHANK3 and ACR
genes, located on 22q13.33, was defined by multiplex
ligation-dependent probe amplification (MLPA). Deletion
of 22q13.3 (ARSA) region was confirmed by a fluorescent
in situ hybridization (FISH) technique. The 22q13.3
deletion was found to be de novo in our patient, and she
was diagnosed with PHMDS. We confirmed the 22q13.3
deletion and also determined a gain of 8p23.3-23.2 by
array comparative genomic hybridization (aCGH). Fluorescent
in situ hybridization was performed to determine
whether the deletion was of parental origin and to identify
regions of chromosomes where the extra 8p may have been
located. The parents were found to be normal. The extra
copy of 8p was observed on 22q in the patient. She is the
first case reported in association with the 22q deletion of
8p duplications in the literature.
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