Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype

BACKGROUND: Carriers of apparently balanced translocations are usually phenotypically normal; however in about 6% of de novo cases, an abnormal phenotype is present. In the current study we investigated 12 patients, six de novo and six familial, with apparently balanced translocations and mental ret...

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Autores principales: Sismani, Carolina, Kitsiou-Tzeli, Sofia, Ioannides, Marios, Christodoulou, Christodoulos, Anastasiadou, Violetta, Stylianidou, Goula, Papadopoulou, Eleftheria, Kanavakis, Emanuel, Kosmaidou-Aravidou, Zoe, Patsalis, Philippos C
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2516517/
https://www.ncbi.nlm.nih.gov/pubmed/18644119
http://dx.doi.org/10.1186/1755-8166-1-15
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author Sismani, Carolina
Kitsiou-Tzeli, Sofia
Ioannides, Marios
Christodoulou, Christodoulos
Anastasiadou, Violetta
Stylianidou, Goula
Papadopoulou, Eleftheria
Kanavakis, Emanuel
Kosmaidou-Aravidou, Zoe
Patsalis, Philippos C
author_facet Sismani, Carolina
Kitsiou-Tzeli, Sofia
Ioannides, Marios
Christodoulou, Christodoulos
Anastasiadou, Violetta
Stylianidou, Goula
Papadopoulou, Eleftheria
Kanavakis, Emanuel
Kosmaidou-Aravidou, Zoe
Patsalis, Philippos C
author_sort Sismani, Carolina
collection PubMed
description BACKGROUND: Carriers of apparently balanced translocations are usually phenotypically normal; however in about 6% of de novo cases, an abnormal phenotype is present. In the current study we investigated 12 patients, six de novo and six familial, with apparently balanced translocations and mental retardation and/or congenital malformations by applying 1 Mb resolution array-CGH. In all de novo cases, only the patient was a carrier of the translocation and had abnormal phenotype. In five out of the six familial cases, the phenotype of the patient was abnormal, although the karyotype appeared identical to other phenotypically normal carriers of the family. In the sixth familial case, all carriers of the translocations had an abnormal phenotype. RESULTS: Chromosomal and FISH analyses suggested that the rearrangements were "truly balanced" in all patients. However, array-CGH, revealed cryptic imbalances in three cases (3/12, 25%), two de novo (2/12, 33.3%) and one familial (1/12, 16.6%). The nature and type of abnormalities differed among the cases. In the first case, what was identified as a de novo t(9;15)(q31;q26.1), a complex rearrangement was revealed involving a ~6.1 Mb duplication on the long arm of chromosome 9, an ~10 Mb deletion and an inversion both on the long arm of chromosome 15. These imbalances were located near the translocation breakpoints. In the second case of a de novo t(4;9)(q25;q21.2), an ~6.6 Mb deletion was identified on the short arm of chromosome 7 which is unrelated to the translocation. In the third case, of a familial, t(4;7)(q13.3;p15.3), two deletions of ~4.3 Mb and ~2.3 Mb were found, each at one of the two translocation breakpoints. In the remaining cases the translocations appeared balanced at 1 Mb resolution. CONCLUSION: This study investigated both de novo and familial apparently balanced translocations unlike other relatively large studies which are mainly focused on de novo cases. This study provides additional evidence that cryptic genomic imbalances are common in patients with abnormal phenotype and "apparently balanced" translocations not only in de novo but can also occur in familial cases. The use of microarrays with higher resolution such as oligo-arrays may reveal that the frequency of cryptic genomic imbalances among these patients is higher.
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spelling pubmed-25165172008-08-15 Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype Sismani, Carolina Kitsiou-Tzeli, Sofia Ioannides, Marios Christodoulou, Christodoulos Anastasiadou, Violetta Stylianidou, Goula Papadopoulou, Eleftheria Kanavakis, Emanuel Kosmaidou-Aravidou, Zoe Patsalis, Philippos C Mol Cytogenet Research BACKGROUND: Carriers of apparently balanced translocations are usually phenotypically normal; however in about 6% of de novo cases, an abnormal phenotype is present. In the current study we investigated 12 patients, six de novo and six familial, with apparently balanced translocations and mental retardation and/or congenital malformations by applying 1 Mb resolution array-CGH. In all de novo cases, only the patient was a carrier of the translocation and had abnormal phenotype. In five out of the six familial cases, the phenotype of the patient was abnormal, although the karyotype appeared identical to other phenotypically normal carriers of the family. In the sixth familial case, all carriers of the translocations had an abnormal phenotype. RESULTS: Chromosomal and FISH analyses suggested that the rearrangements were "truly balanced" in all patients. However, array-CGH, revealed cryptic imbalances in three cases (3/12, 25%), two de novo (2/12, 33.3%) and one familial (1/12, 16.6%). The nature and type of abnormalities differed among the cases. In the first case, what was identified as a de novo t(9;15)(q31;q26.1), a complex rearrangement was revealed involving a ~6.1 Mb duplication on the long arm of chromosome 9, an ~10 Mb deletion and an inversion both on the long arm of chromosome 15. These imbalances were located near the translocation breakpoints. In the second case of a de novo t(4;9)(q25;q21.2), an ~6.6 Mb deletion was identified on the short arm of chromosome 7 which is unrelated to the translocation. In the third case, of a familial, t(4;7)(q13.3;p15.3), two deletions of ~4.3 Mb and ~2.3 Mb were found, each at one of the two translocation breakpoints. In the remaining cases the translocations appeared balanced at 1 Mb resolution. CONCLUSION: This study investigated both de novo and familial apparently balanced translocations unlike other relatively large studies which are mainly focused on de novo cases. This study provides additional evidence that cryptic genomic imbalances are common in patients with abnormal phenotype and "apparently balanced" translocations not only in de novo but can also occur in familial cases. The use of microarrays with higher resolution such as oligo-arrays may reveal that the frequency of cryptic genomic imbalances among these patients is higher. BioMed Central 2008-07-21 /pmc/articles/PMC2516517/ /pubmed/18644119 http://dx.doi.org/10.1186/1755-8166-1-15 Text en Copyright © 2008 Sismani et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Sismani, Carolina
Kitsiou-Tzeli, Sofia
Ioannides, Marios
Christodoulou, Christodoulos
Anastasiadou, Violetta
Stylianidou, Goula
Papadopoulou, Eleftheria
Kanavakis, Emanuel
Kosmaidou-Aravidou, Zoe
Patsalis, Philippos C
Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
title Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
title_full Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
title_fullStr Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
title_full_unstemmed Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
title_short Cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
title_sort cryptic genomic imbalances in patients with de novo or familial apparently balanced translocations and abnormal phenotype
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2516517/
https://www.ncbi.nlm.nih.gov/pubmed/18644119
http://dx.doi.org/10.1186/1755-8166-1-15
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