Chromosome 13q neocentromeres: Molecular cytogenetic characterization of three additional cases and clinical spectrum

Li, Shulan; Malafiej, Paul; Levy, Brynn; Mahmood, Radma; Field, Michael; Hughes, Thomas E.; Lockhart, Lillian H.; Wu, Zhanhe; Huang, Melissa; Hirschhorn, Kurt; Velagaleti, Golpalrao V.N.; Daniel, Art; Warburton, Peter E.

doi:10.1002/ajmg.10454

Cited by 26 publications

(31 citation statements)

References 30 publications

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“…In addition, the DNA of the neocentromere supports the formation of a functional kinetochore with almost the correct complement of proteins. Kinetochore proteins CENP-A, CENP-C, CENP-E and CENP-I are found at neocentromeres, however CENP-B is not (Choo, 2001;Assumpcao et al, 2002;Li et al, 2002;Alonso et al, 2003;Craig et al, 2003;Amor et al, 2004). The formation of neocentromeres has been induced in the laboratory in Drosophila (Williams et al, 1998;Maggert and Karpen, 2001) and in a human and mouse hybrid somatic cell (Shen et al, 2001).…”

Section: Construction Of Mammalian Artificial Chromosomesmentioning

confidence: 99%

Mammalian artificial chromosomes: modern day feats of engineering – Isambard Kingdom Brunel style

Bridger

2004

Cytogenet Genome Res

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Section: Construction Of Mammalian Artificial Chromosomesmentioning

confidence: 99%

Mammalian artificial chromosomes: modern day feats of engineering – Isambard Kingdom Brunel style

Bridger

2004

Cytogenet Genome Res

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“…The majority of neocentromeres represent inverted duplications of distal autosome regions, most commonly 15q25, 3q and 13q, and present as supernumerary marker chromosomes resulting in partial tri- or tetrasomy [4]. The clinical spectrum of phenotypes is variable and likely stems from the degree of duplication, mosaicism and tissue distribution of the supernumerary neocentromere chromosome [2]. There is only one report of prenatal detection of a supernumerary neocentromere chromosome 13 or neo(13) [5].…”

Section: Novel Insightsmentioning

confidence: 99%

“…The second was an unbalanced, nonmosaic karyotype with 47 chromosomes consisting of a r(13)(pter→q14.1) and an inv dup(13)(q14→qter), resulting in trisomy for 13q14→qter [9]. The third case involves a mosaic supernumerary inv dup(13)(q14→qter), resulting in tetrasomy for 13q14→qter (case 2) [2]. The fourth case had a supernumerary neocentric 13q21→13q22 chromosome with a balancing reciprocal deletion [10].…”

Section: Novel Insightsmentioning

confidence: 99%

“…The complexity and variability of the clinical phenotypes seen in patients with polysomy for 13q21→qter preclude any genotype-phenotype correlation due to the wide range of mosaicism [2]. The most frequent features observed in patients with partial trisomy/tetrasomy of 13q include facial dysmorphisms, hypotelorism, ear abnormalities and severe learning difficulties [12].…”

Section: Novel Insightsmentioning

confidence: 99%

“…Centromeres, and the proteinaceous kinetochores that form there, are required for proper chromosome segregation during mitosis and meiosis. Neocentromeres are defined as a group of mitotically stable human derivative centromeres without alpha-satellite DNA that are able to form a primary constriction and participate in kinetochore formation [1,2,3]. Neocentromeres suggest that centromere formation is not solely dependent on alpha-satellite DNA, but on a distinct chromatin structure [4].…”

Section: Novel Insightsmentioning

confidence: 99%

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Origin of a Prenatal Mosaic Supernumerary Neocentromeric Derivative Chromosome 13 Determined by QF-PCR

et al. 2012

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Neocentromeres are mitotically stable human derivative centromeres without alpha-satellite DNA which are able to provide stability to rearranged chromosome fragments that would otherwise be acentric and rapidly lost. A female fetus was found to be mosaic for a supernumerary marker chromosome: 47,XX,+mar[3]/46,XX[36]. The marker was identified by fluorescence in situ hybridization and G-band as an inversion duplication of 13q21→13qter, with a neocentromere present at 13q21, in approximately 9% of colonies examined. Parental blood karyotypes were normal. QF-PCR performed on blood samples from both parents and the second amniotic fluid sample showed evidence of a second maternal allele at markers D13S258 (13q21) and D13S628 (13q31–q32), indicating formation at maternal meiosis I/II. This is the first reported case where the detection and origin of a low-level mosaic prenatal neo(13) were confirmed by QF-PCR.

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A new neocentromere locus on chromosome 13 resulting in mosaic tetrasomy for distal 13q and an asymmetric phenotype

Mazzaschi

Bint

Ogilvie

et al. 2004

American J of Med Genetics Pt A

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An 8-year-old girl was referred to the Genetics Centre with mild developmental delay, mild dysmorphic features, and a head circumference on the 98th centile. She was noted to have large irregular ear lobes, torticollis, and mild hemihypertrophy. Karyotype analysis of cultured peripheral lymphocytes and skin fibroblasts revealed the presence of a symmetrical supernumerary marker chromosome in 13% of cells from both tissue types. Further analysis showed that this marker chromosome originated from the distal region of chromosome 13 and contained no centromeric alpha-satellite DNA. The marker chromosome was not found in blood from the parents. This case represents a novel symmetrical structure with a previously unreported neocentromere locus, leading to an unusual phenotype. Similar cases of individuals with a chromosome 13 with a neocentromere have been reported. They are reviewed and compared with the current case. The importance of scanning metaphases for abnormalities in individuals presenting with asymmetry is emphasized.

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Chromosome 13q neocentromeres: Molecular cytogenetic characterization of three additional cases and clinical spectrum

Cited by 26 publications

References 30 publications

Mammalian artificial chromosomes: modern day feats of engineering – Isambard Kingdom Brunel style

Mammalian artificial chromosomes: modern day feats of engineering – Isambard Kingdom Brunel style

Origin of a Prenatal Mosaic Supernumerary Neocentromeric Derivative Chromosome 13 Determined by QF-PCR

A new neocentromere locus on chromosome 13 resulting in mosaic tetrasomy for distal 13q and an asymmetric phenotype

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