Your search keyword '"Emmanouil Manolakos"' showing total 5 results

1. A de novo 2.9 Mb interstitial deletion at 13q12.11 in a child with developmental delay accompanied by mild dysmorphic characteristics

Author

Michael B. Petersen, Loretta Thomaidis, Emmanouil Manolakos, George Daskalakis, Magdalini Lagou, George Kitsos, Eleftherios Anastasakis, Ioannis Papoulidis, Maria Kontodiou, Vasileios Papadopoulos, and Sandro Orru

Subjects

medicine.medical_specialty, Microcephaly, congenital, hereditary, and neonatal diseases and abnormalities, Clinodactyly, Array-CGH, Chromosomal translocation, Case Report, Biology, Biochemistry, Deletion, 03 medical and health sciences, medicine, Genetics, Genetics(clinical), Molecular Biology, Genetics (clinical), 030304 developmental biology, Chromosome 13, Biochemistry, medical, 0303 health sciences, 13q12.11, 030305 genetics & heredity, Biochemistry (medical), Cytogenetics, Karyotype, medicine.disease, Phenotype, Human genetics, Mild dysmorphic features, Molecular Medicine, medicine.symptom

Abstract

BACKGROUND: Proximal deletions in the 13q12.11 region are very rare. Much larger deletions including this region have been described and are associated with complex phenotypes of mental retardation, developmental delay and various others anomalies.RESULTS: We report on a 3-year-old girl with a rare 2.9 Mb interstitial deletion at 13q12.11 due to a de novo unbalanced t(13;14) translocation. She had mild mental retardation and relatively mild dysmorphic features such as microcephaly, flat nasal bridge, moderate micrognathia and clinodactyly of 5(th) finger. Molecular karyotyping revealed a deletion on the long arm of chromosome 13 as involving sub-bands 13q12.11, a deletion of about 2.9 Mb.DISCUSSION: The clinical application of array-CGH has made it possible to detect submicroscopical genomic rearrangements that are associated with varying phenotypes.The description of more patients with deletions of the 13q12.11 region will allow a more precise genotype-phenotype correlation.

Published

2014

2. Prenatal diagnosis of two de novo 4q35-qter deletions characterized by array-CGH

Author

Natasa Psara, Nikolaos Vrachnis, George Daskalakis, Annalisa Vetro, Elisa Siomou, Ioannis Papoulidis, Eirini Sevastopoulou, Konstantinos Kefalas, Loretta Thomaidis, Anastasia E. Konstantinidou, Orsetta Zuffardi, Emmanouil Manolakos, Eirini Oikonomidou, and Elena Papageorgiou

Subjects

medicine.medical_specialty, Array-CGH, Prenatal diagnosis, Chromosomal translocation, Biology, Biochemistry, medicine, Genetics, Genetics(clinical), Molecular Biology, Genetics (clinical), Biochemistry, medical, Research, Biochemistry (medical), Cytogenetics, Karyotype, medicine.disease, Human genetics, Chromosome 4, Molecular Medicine, 4q- syndrome, Deletion 4q35.1, Ventriculomegaly, Comparative genomic hybridization

Abstract

Background The 4q- syndrome is a well known genetic condition caused by a partial terminal or interstitial deletion in the long arm of chromosome 4. The great variability in the extent of these deletions and the possible contribution of additional genetic rearrangements, such as unbalanced translocations, lead to a wide spectrum of clinical manifestations. The majority of reports of 4q- cases are associated with large deletions identified by conventional chromosome analysis; however, the widespread clinical use of novel molecular techniques such as array comparative genomic hybridization (a-CGH) has increased the detection rate of submicroscopic chromosomal aberrations associated with 4q- phenotype. Results Herein we report two prenatal cases of 4qter deletions which presented the first with no sonographic findings and the second with brain ventriculomegaly combined with oligohydramnios. Standard karyotyping demonstrated a deletion at band q35.1 of chromosome 4 in both cases. The application of a-CGH confirmed the diagnosis and offered a precise characterization of the genetic defect. Conclusions We provide a review of the currently available literature on the prenatal diagnostic approach of 4q- syndrome and we compare our results with other published cases. Our data suggest that the identification and the precise molecular characterization of new cases with 4q- syndrome will contribute in elucidating the genetic spectrum of this disorder.

Published

2013

3. Prenatal diagnosis of Wolf-Hirschhorn syndrome confirmed by comparative genomic hybridization array: report of two cases and review of the literature

Author

Maria Kontodiou, Emmanouil Manolakos, Sandro Orru, Dimitra Kappou, Orsetta Zuffardi, Anastasia Konstandinidou, Ioannis Papoulidis, Stavros Sifakis, Panagiotis Peitsidis, Nikolaos Vrachnis, Annalisa Vetro, and Antonios Garas

Subjects

medicine.medical_specialty, Comparative genomic hybridization array, lcsh:QH426-470, Fluorescent situ hybridization, Prenatal diagnosis, Oligohydramnios, Case Report, Bioinformatics, Biochemistry, medicine, Genetics, Genetics(clinical), 4p- syndrome, Wolf–Hirschhorn syndrome, Molecular Biology, Genetics (clinical), Biochemistry, medical, Wolf-Hirschhorn syndrome, business.industry, Biochemistry (medical), Cytogenetics, "Greek warrior" helmet profile, Karyotype, medicine.disease, Human genetics, lcsh:Genetics, Chromosome 4, Molecular Medicine, business, Comparative genomic hybridization

Abstract

Wolf-Hirschhorn syndrome (WHS) is a well known genetic condition caused by a partial deletion of the short arm of chromosome 4. The great variability in the extent of the 4p deletion and the possible contribution of additional genetic rearrangements lead to a wide spectrum of clinical manifestations. The majority of the reports of prenatally diagnosed WHS cases are associated with large 4p deletions identified by conventional chromosome analysis; however, the widespread clinical use of novel molecular techniques such as array comparative genomic hybridization (a-CGH) has increased the detection rate of submicroscopic chromosomal aberrations associated with WHS phenotype. We provide a report of two fetuses with WHS presenting with intrauterine growth restriction as an isolated finding or combined with oligohydramnios and abnormal Doppler waveform in umbilical artery and uterine arteries. Standard karyotyping demonstrated a deletion on chromosome 4 in both cases [del(4)(p15.33) and del(4)(p15.31), respectively] and further application of a-CGH confirmed the diagnosis and offered a precise characterization of the genetic defect. A detailed review of the currently available literature on the prenatal diagnostic approach of WHS in terms of fetal sonographic assessment and molecular cytogenetic investigation is also provided.

Published

2012

4. Correction: Characterization of a prenatally assessed de novo supernumerary minute ring chromosome 20 in a phenotypically normal male

Author

Sofia Kitsiou-Tzeli, Emmanouil Manolakos, Magdalini Lagou, Katerina Anagnostopoulou, Maria Kontodiou, Nadezda Kosyakova, Elisabeth Ewers, Anja Weise, Antonios Garas, Sandro Orru, Thomas Liehr, and Aikaterini Metaxotou

Subjects

Biochemistry, medical, lcsh:Genetics, lcsh:QH426-470, Biochemistry (medical), Genetics, Molecular Medicine, Correction, Genetics(clinical), Biochemistry, Molecular Biology, Genetics (clinical)

Abstract

The heterogeneous group of small supernumerary marker chromosomes (sSMCs) presents serious counseling problems, especially if they are present de novo and diagnosed prenatally. The incidence has been estimated at 1 in 1000 prenatal samples. We present a case of mosaic sSMC diagnosed prenatally after amniocentesis. The sSMC was characterized by various molecular cytogenetic techniques and determined to be a r(20) chromosome. After genetic counseling, the parents decided to continue the pregnancy, and a boy with minor phenotypic variants was born after 39 weeks of pregnancy. The case is compared with four other cases of prenatally detected r(20) mosaicism.Here we describe a 3 months old male child with normal pre- and postnatal development and with a de novo ring supernumerary marker chromosome in amniocytes cultures. Using new fluorescence in situ hybridization (FISH) techniques, three distinguishable sSMCs (cryptic mosaicism), all derived from chromosome 20, were observed, including ring and minute chromosomes. This heterogeneity was impossible to detect by the conventional G-banding technique or conventional FISH technique that were used before the application of new FISH techniques (subcentromere-specific multicolor-FISH [subcenM-FISH]) and a probe, specific for the 20p12.2 band. The sSMC present in 25% of the cells was present as r(20)(::p12.2~12.3-q11.1::)5/r(20;20)(::p12.1-q11.1::q11.1p12.1::)2/min(20;20)(:p12.1-q11.1::q11.1-p12.1:)1. The final karyotype was 47,XY,+r(20)[25%]/46,XY[75%].We emphasize the importance of application of molecular cytogenetics in a prenatally diagnostic laboratory and description of more cases to enable a better genetic counseling and risk evaluation.

Published

2009

5. Characterization of a prenatally assessed de novo supernumerary minute ring chromosome 20 in a phenotypically normal male

Author

Elisabeth Ewers, Thomas Liehr, Sandro Orru, Aikaterini Metaxotou, Anja Weise, Maria Kontodiou, Emmanouil Manolakos, Antonios Garas, Sofia Kitsiou-Tzeli, Magdalini Lagou, and Nadezda Kosyakova

Subjects

medicine.medical_specialty, lcsh:QH426-470, Marker chromosome, Ring chromosome 20, Case Report, Biology, Biochemistry, Molecular cytogenetics, medicine, Genetics, Supernumerary, Genetics(clinical), Molecular Biology, Genetics (clinical), Gynecology, Biochemistry, medical, medicine.diagnostic_test, Biochemistry (medical), Cytogenetics, Karyotype, medicine.disease, lcsh:Genetics, Molecular Medicine, Chromosome 20, Fluorescence in situ hybridization

Abstract

Background The heterogeneous group of small supernumerary marker chromosomes (sSMCs) presents serious counseling problems, especially if they are present de novo and diagnosed prenatally. The incidence has been estimated at 1 in 1000 prenatal samples. We present a case of mosaic sSMC diagnosed prenatally after amniocentesis. The sSMC was characterized by various molecular cytogenetic techniques and determined to be a r(20) chromosome. After genetic counseling, the parents decided to continue the pregnancy, and a boy with minor phenotypic variants was born after 39 weeks of pregnancy. The case is compared with four other cases of prenatally detected r(20) mosaicism. Results Here we describe a 3 months old male child with normal pre- and postnatal development and with a de novo ring supernumerary marker chromosome in amniocytes cultures. Using new fluorescence in situ hybridization (FISH) techniques, three distinguishable sSMCs (cryptic mosaicism), all derived from chromosome 20, were observed, including ring and minute chromosomes. This heterogeneity was impossible to detect by the conventional G-banding technique or conventional FISH technique that were used before the application of new FISH techniques (subcentromere-specific multicolor-FISH [subcenM-FISH]) and a probe, specific for the 20p12.2 band. The sSMC present in 25% of the cells was present as r(20)(::p12.2~12.3->q11.1::)[5]/r(20;20)(::p12.1->q11.1::q11.1 >p12.1::)[2]/min(20;20)(:p12.1->q11.1::q11.1->p12.1:)[1]. The final karyotype was 47,XY,+r(20)[25%]/46,XY[75%]. Conclusion We emphasize the importance of application of molecular cytogenetics in a prenatally diagnostic laboratory and description of more cases to enable a better genetic counseling and risk evaluation.

Published

2009