Subtelomeric study of 132 patients with mental retardation reveals 9 chromosomal anomalies and contributes to the delineation of submicroscopic deletions of 1pter, 2qter, 4pter, 5qter and 9qter

Sogaard, Marie; Tümer, Zeynep; Hjalgrim, Helle; Hahnemann, Johanne M D; Friis, B; Ledaal, P; Pedersen, Vibeke Faurholt; Baekgaard, Peter; Tommerup, Niels; Cingoz, Sultan; Dunø, Morten; Brøndum‐Nielsen, Karen

doi:10.1186/1471-2350-6-21

Cited by 29 publications

(22 citation statements)

References 31 publications

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“…Nearly 100 individuals carrying isolated, primarily terminal deletions with breakpoint at or within chromosome 2 region q37 have been reported previously [Gorski et al, 1989;Lamb et al, 1990;Coldwell et al, 1992;Lin et al, 1992;Oley et al, 1992;Haag et al, 1993;Waters et al, 1993;Fisher et al, 1994;Stratton et al, 1994;Wang et al, 1994;Conrad et al, 1995;Phelan et al, 1995;Wilson et al, 1995;Rauch et al, 1996;Friedman et al, 1997;Power et al, 1997;Wenger et al, 1997;Viot-Szoboszlai et al, 1998;Ghaziuddin and Burmeister, 1999;Reddy et al, 1999;Lehman et al, 2001;Smith et al, 2001;Anderlid et al, 2002;Wolff et al, 2002;van Karnebeek et al, 2002;Giardino et al, 2003;Aldred et al, 2004;Casas et al, 2004;Chassaing et al, 2004;Lukusa et al, 2004;Polityko et al, 2004;Shrimpton et al, 2004;Adeyinka et al, 2005;Sogaard et al, 2005;Chaabouni et al, 2006;Lacbawan et al, 2006;Masumoto et al, 2006;Ravnan et al, 2006], though some of the reports have not included detailed clinical characterization. In addition Nearly 100 individuals carrying isolat...…”

Section: Introductionmentioning

confidence: 88%

“…Clinically significant microdeletions usually occur as de novo events, but exceptions have been noted. Sogaard et al [2005] reported a phenotypically normal mother with the 2q37.3 deletion polymorphism whose child had mental retardation and physical anomalies associated with a larger 6.8 Mb 2q37 microdeletion. van Karnebeek et al [2002] …”

Section: Molecular Aspects Of Deletion 2q37mentioning

confidence: 98%

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Chromosome 2q37 deletion: Clinical and molecular aspects

Falk

Casas

2007

American J of Med Genetics Pt C

111

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Terminal deletions of chromosome 2 with breakpoints at or within band 2q37, ranging from visible abnormalities to cryptic, subtelomeric deletions, have been recognized with increasing frequency among children with mild-moderate mental retardation, characteristic facial appearance, and behavioral manifestations which often place them on the autism spectrum. The stereotypic facial characteristics include prominent forehead, thin, highly arched eyebrows, depressed nasal bridge, full cheeks, deficient nasal alae and prominent columella, thin upper lip, and various minor anomalies of the pinnae. Abnormal nipples, including inverted nipples, have been reported in a number of cases. CNS, ocular, cardiac, gastrointestinal, renal, and other GU anomalies have been noted in nearly one-third of patients. Of note, coarctation or hypoplasia of the aorta has been described in several affected children. Wilms tumor, renal dysplasia, and tracheomalacia have been reported only with the most proximal breakpoint at band 2q37.1 while a range of GI anomalies, pyloric stenosis, and diaphragmatic defects have been reported with breakpoints throughout the region. A subset of patients with the most distal deletion present phenotypic features which mimic Albright hereditary osteodystrophy (AHO). In addition to the AHO-like phenotype, later onset findings include seizures and cystic kidneys. Timely diagnosis of this recognizable syndrome provides a basis for genetic counseling, appropriate surveillance, and intervention, and avoids unnecessary and expensive diagnostic testing.

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Section: Introductionmentioning

confidence: 88%

Section: Molecular Aspects Of Deletion 2q37mentioning

confidence: 98%

Chromosome 2q37 deletion: Clinical and molecular aspects

Falk

Casas

2007

American J of Med Genetics Pt C

111

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“…A polymorphism at the 2q telomere was first identified by Macina et al [1994] and using multiple subtelomeric probes in a study of 150 patients, indicated that 6% of these patients had a 2qtel deletion and they concluded that the deletion of the locus D2S2986 in the 2qtel region was a common variant. Sogaard et al [2005] reported a phenotypically normal mother with a 2q37.3 deletion polymorphism whose child had clinical manifestations associated with a larger microdeletion (6.8 Mb). Similarly, Van Karnebeek et al [2002] described a microdeletion distal to 2q37.3 in a phenotypically normal father whose daughter showed clinical manifestations of a 2q37.3 terminal deletion.…”

Section: Genotype-phenotype Correlationmentioning

confidence: 98%

Molecular characterization of a new patient with a non‐recurrent inv dup del 2q and review of the mechanisms for this rearrangement

Vera-Carbonell

López-Expósito

Bafalliu

et al. 2010

American J of Med Genetics Pt A

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We report on newborn baby with microcephaly, facial anomalies, congenital heart defects, hypotonia, wrist contractures, long fingers, adducted thumbs, and club feet. Cytogenetic studies revealed an inverted duplication with terminal deletion (inv dup del) of 2q in the patient and a paternal 2qter deletion polymorphism. Microsatellite markers demonstrated that the inv dup del was maternal in origin and intrachromosomal. Intra or interchromosomal rearrangements may cause this aberration either by a U-type exchange (end-to-end fusion), an unequal crossover between inverted repeats (non-allelic homologous recombination: NAHR), or through breakage-fusion-bridge (BFB) cycles leading to a sister chromatid fusion by non-homologous end joining (NHEJ). A high-resolution oligo array-CGH (244 K) defined the breakpoints and did not detect a single copy region with a size exceeding 12.93 Kb in the fusion site. The size of the duplicated segment was 38.75 Mb, extending from 2q33.1 to 2q37.3 and the size of the terminal deletion was 2.85 Mb in 2q37.3. Our results indicate that the inv dup del (2q) is likely a non-recurrent chromosomal rearrangement generated by a NHEJ mechanism. The major clinical characteristics associated with this 2q rearrangement overlap with those commonly found in patients with 2q duplication reported in the literature.

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“…A precise mapping of the deletions, however, was carried out in only a few studies (27/115 patients). [1][2][3][4][5][6][7][8][9][10]13,14,24,25,30,32 The patients with purely distal deletions (seven females, three males) included in the DECIPHER database (http://decipher.sanger.ac.uk/) had various deletion sizes ranging from 3 to 9.9 Mb. Unfortunately, clinical features were only mentioned for 2 of the 10 patients.…”

Section: Mappingmentioning

confidence: 99%