Molecular cytogenetic characterization of the first reported case of inv dup del 20p compatible with a U‐type exchange model

Leclercq, Sandrine; Maincent, Kim; Baverel, Françoise; Tessier, Dominique Le; Letourneur, Franck; Lebbar, Aziza; Dupont, Jean‐Michel

doi:10.1002/ajmg.a.32640

Cited by 20 publications

(28 citation statements)

References 59 publications

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“…They did not detect a single copy region but were able to narrow down the region ''fusion site'' to $11 Kb. Wang et al [2008], using array-CGH and FISH did not identify a single copy region exceeding 100 Kb in an inv dup del 5p and neither could Leclercq et al [2009] detect a single copy segment exceeding 6 Kb using an oligo array-CGH (244 K) in an inv dup del 20p. Duplicated and deleted regions, interrupted by a very small single copy segment, have only been reported on two occasions [Ballif et al, 2003;Bonaglia et al, 2009].…”

Section: Discussion Rearrangementmentioning

confidence: 75%

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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Section: Discussion Rearrangementmentioning

confidence: 75%

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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“…Our patient is another with a subtelomeric loss of 20p13 [Baker et al, 2002; Adeyinka et al, 2005; Leclercq et al, 2009; Stevens et al, 2009; McGill et al, 2010]. Apart from patients described in more detailed by McGill et al The others harbor deletions as a result of complex [Leclercq et al, 2009; Stevens et al, 2009] or familial rearrangements [Baker et al, 2002, Adeyinka et al, 2005]. In addition, there are previously described patients with terminal deletions of the short arm of chromosome 20 which encompass the JAG1 gene, known to cause Alagille syndrome [Krantz et al, 1997] as well as or cytogenetically visible aberrations [Schinzel, 2001].…”

Section: Discussionmentioning

confidence: 95%

1.15 Mb microdeletion in chromosome band 20p13 associated with moderate developmental delay—Additional case and data's review

Jezela‐Stanek

Kucharczyk

Pelc

et al. 2012

American J of Med Genetics Pt A

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We report on a 9-year-old girl with subtelomeric 20p microdeletion. She was referred for genetic counseling because of learning difficulties/school problems. During the evaluation short stature, hypoplastic fingernails, submucous cleft palate with cleft uvula, flat feet, and frequent upper respiratory infections, as well as the large fontanelle after birth were observed. No facial dysmorphic features specific for chromosomal aberrations were present. The diagnosis of deletion of 20p13 was established by MLPA, and delineated by arrayCGH. Our report describes the third individual with this approximate deletion, and presents detailed molecular and phenotypic characteristics providing new data supporting future genotype-phenotype study.

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“…Although 20p13 deletions may be associated with developmental delays in motor and speech, mental retardation and epilepsy at various levels of severity, and facial dysmorphism (Moutton et al, ), the typical characteristics of such cases remain enigmatic, leading to diagnostic delays. Interestingly, previous studies showed that patients who simultaneously harbored a duplication and subtelomeric deletion of 20p exhibited facial dysmorphism, psychomotor retardation, delayed development, and speech difficulties (Leclercq et al, ; Trachoo, Assanatham, Jinawath, & Nongnuch, ). However, the precise mechanisms underlying duplications and/or deletions of the 20p13 chromosome band remain unclear and require further study.…”

Section: Discussionmentioning

confidence: 99%

Phenotypic features of a microdeletion in chromosome band 20p13: A case report and review of the literature

Fang

Liu

Wang

et al. 2019

Molec Gen & Gen Med

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Background 20p13 microdeletion syndrome has been reported to be associated with developmental delays, intellectual disability, epilepsy, and unspecific dysmorphic characteristics. However, only a few cases of 20p13 microdeletion have been described, and therefore its typical features and precise pathogenesis remain elusive. Methods and Results In this article, we report the case of a 9‐month‐old infant who presented with a large fontanelle, facial dysmorphism, and failure to thrive. Array‐comparative genomic hybridization (aCGH) analysis confirmed a 2.01‐Mb microdeletion in chromosome band 20p13 that involved SOX12 and NRSN2 , both of which are considered paramount causative genes in patients with 20p13 microdeletion. To elucidate the typical features of 20p13 microdeletion, we further reviewed these previously reported cases and found that motor delay (90%) was the most common manifestation, followed by language delay (60%), abnormal digits (60%), mental retardation (50%), large fontanelle (50%), electroencephalography abnormalities (50%), and seizure (40%). Conclusion This report highlights the potential of aCGH as a practical and powerful tool with which to detect submicroscopic chromosomal abnormalities in individuals presenting with a wide spectrum of phenotypes, ranging from facial dysmorphism to failure to thrive. Additionally, the literature review casts new light on the clinical features of 20p13 microdeletion.

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Molecular cytogenetic characterization of the first reported case of inv dup del 20p compatible with a U‐type exchange model

Cited by 20 publications

References 59 publications

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

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

1.15 Mb microdeletion in chromosome band 20p13 associated with moderate developmental delay—Additional case and data's review

Phenotypic features of a microdeletion in chromosome band 20p13: A case report and review of the literature

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