Prenatal diagnosis of a fetus with pure partial trisomy 1q32‐44 due to a familial balanced rearrangement

Kímya, Yalçın; Yakut, Tahsin; Egelí, Ünal; Özerkan, Kemal

doi:10.1002/pd.403

Cited by 18 publications

(26 citation statements)

References 20 publications

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“…The patients with pure trisomy for 1q32 ! qter show a fairly consistent pattern of congenital anomalies: severe pre-and postnatal growth retardation, macrocephaly, wide sutures and fontanelles, prominent forehead, triangular faces, broad and flat nasal bridge, midface hypoplasia, and visceral malformations, including urogenital and cardiac anomalies [Bartsch et al, 2001;Kimya et al, 2002;Nowaczyk et al, 2003]. There is, however, substantial phenotypic variability observed in patients with trisomy 1q and accompanying monosomy for another chromosomal region [Rasmussen et al, 1990;Johnson, 1991].…”

Section: Discussionmentioning

confidence: 97%

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Attenuated phenotype in a child with trisomy for 1q due to unbalanced X;1 translocation [46,X,der(X),t(X;1)(q28;q32.1)]

Yatsenko

Sahoo

Rosenkranz

et al. 2004

American J of Med Genetics Pt A

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We report a case of an X;1 translocation in a 9-month-old female infant with mild dysmorphic features and developmental delay. High-resolution chromosome analysis revealed a de novo, unbalanced translocation between chromosomes X and 1 [46,X,der(X),t(X;1)(q28;q32.1)]. Breakpoints on the derivative X and the size of the translocated segment have been defined by fluorescence in situ hybridization (FISH) with Xq and 1q specific probes. The rearrangement in this patient results in monosomy for Xq28-qter and trisomy for 1q32.1-qter. Replication studies demonstrated late replication of the derivative X in 80% of the observed cells, with the exception of 20% of the cells where X inactivation failed to spread into the translocated 1q segment. Patients with pure trisomy for the distal segment of 1q present a considerably more severe phenotype compared to that seen in our patient, including facial dysmorphisms, urogenital and cardiac anomalies. We suggest that the absence of many of the characteristic features for trisomy 1q in our patient, may reflect a mosaic pattern of inactivation of the translocated autosomal segment on the derivative X chromosome.

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Section: Discussionmentioning

confidence: 97%

“…qter [Flatz and Fonatsch, 1979;Fryns et al, 1980;Clark et al, 1994;Duba et al, 1997;Kimya et al, 2002;Nowaczyk et al, 2003]. Numerator refers to the number of patients reported to have a given anomaly; denominator is the number of patients in whom this anomaly was investigated.…”

Section: Discussionmentioning

confidence: 97%

Attenuated phenotype in a child with trisomy for 1q due to unbalanced X;1 translocation [46,X,der(X),t(X;1)(q28;q32.1)]

Yatsenko

Sahoo

Rosenkranz

et al. 2004

American J of Med Genetics Pt A

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“…Distal 1q duplication syndrome is characterized by the signs present in almost all previously reported cases, namely intellectual disability/delayed neuropsychomotor development, a triangular face, slanted and narrow palpebral fissures, broad nasal bridge, pointed small nose, micrognathia, and low-set and posteriorly rotated ears with poorly formed helices ( table 1 ). Heart defects have been found in all patients (including patient 2) except for those reported by Lungarotti et al [1980] and Kimya et al [1979]. Though not described in all patients, cardiac defects are a common finding and, therefore, should be evaluated in patients with distal duplications of 1q.…”

Section: Discussionmentioning

confidence: 99%

“…In most cases, the duplication is the result of an unbalanced translocation with a possible imbalance of the other participating chromosome [Kimya et al, 1979;Concolino et al, 1998;Emberger et al, 2001;Percesepe et al, 2007;Utine et al, 2007]. It is difficult to evaluate the contribution of the 1q trisomy to the phenotype in cases involving another chromosome.…”

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confidence: 99%

Partial 1q Duplications and Associated Phenotype

Morris¹,

Baroneza²,

Teixeira³

et al. 2015

Mol Syndromol

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Duplications of the long arm of chromosome 1 are rare. Distal duplications are the most common and have been reported as either pure trisomy or unbalanced translocations. The paucity of cases with pure distal 1q duplications has made it difficult to delineate a partial distal trisomy 1q syndrome. Here, we report 2 patients with overlapping 1q duplications detected by G-banding. Array CGH and FISH were performed to characterize the duplicated segments, exclude the involvement of other chromosomes and determine the orientation of the duplication. Patient 1 presents with a mild phenotype and carries a 22.5-Mb 1q41q43 duplication. Patient 2 presents with a pure 1q42.13qter inverted duplication of 21.5 Mb, one of the smallest distal 1q duplications ever described and one of the few cases characterized by array CGH, thus contributing to a better characterization of distal 1q duplication syndrome.

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“…The homology of ECA30 extends in an inverted order from HSA1q31 ] q42. Human patients with partial trisomy 1 syndrome exhibit numerous congenital abnormalities which can include polydactyly (Kimya et al, 2002).…”

Section: Autosomal Trisomymentioning

confidence: 99%

Equine clinical cytogenetics: the past and future

Lear

Bailey

2008

Cytogenet Genome Res

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Cytogenetic analyses of horses have benefited the horse industry by identifying chromosomal aberrations causing congenital abnormalities, embryonic loss and infertility. Technical advances in cytogenetics enabled the identification of chromosome specific aberrations. More recently, advances in genomic tools have been used to more precisely define chromosome abnormalities. In this report we review the history of equine clinical cytogenetics, identify historical landmarks for equine clinical cytogenetics, discuss how the current use of genomic tools has benefited this area, and how future genomics tools may enhance clinical cytogenetic studies in the horse.

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Prenatal diagnosis of a fetus with pure partial trisomy 1q32‐44 due to a familial balanced rearrangement

Cited by 18 publications

References 20 publications

Attenuated phenotype in a child with trisomy for 1q due to unbalanced X;1 translocation [46,X,der(X),t(X;1)(q28;q32.1)]

Attenuated phenotype in a child with trisomy for 1q due to unbalanced X;1 translocation [46,X,der(X),t(X;1)(q28;q32.1)]

Partial 1q Duplications and Associated Phenotype

Equine clinical cytogenetics: the past and future

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