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3. Front Cover

Author

Ainhoa Pascual‐Alonso, Laura Blasco, Silvia Vidal, Esther Gean, Patricia Rubio, Mar O'Callaghan, Antonio F. Martínez‐Monseny, Alba Aina Castells, Clara Xiol, Vicenç Català, Nuria Brandi, Paola Pacheco, Carlota Ros, Miguel Campo, Encarna Guillén, Salva Ibañez, María J. Sánchez, Pablo Lapunzina, Julián Nevado, Fernando Santos, Elisabet Lloveras, Juan D. Ortigoza‐Escobar, María I. Tejada, Hiart Maortua, Francisco Martínez, Carmen Orellana, Mónica Roselló, María A. Mesas, María Obón, Alberto Plaja, Joaquín A. Fernández‐Ramos, Eduardo Tizzano, Rosario Marín, José L. Peña‐Segura, Soledad Alcántara, and Judith Armstrong

Subjects
Genetics, Genetics (clinical)
Published
2020
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4. Author response for 'Molecular characterisation of Spanish patients with MECP2 duplication syndrome'

Author

Eli Lloveras, Aina Alba Castells, José Luís Peña‐Segura, Maria Isabel Tejada, Soledad Alcántara, María Obón, Carmen Orellana, Hiart Maortua, María Aurora Mesas, Laura Blasco, Nuria Brandi, Silvia Vidal, Judith Armstrong, María José Puig Sánchez, Fernando Santos, Patricia Rubio, Julián Nevado, Esther Gean, Salva Ibañez, Vicenç Català, Joaquín A. Fernández-Ramos, Eduardo F. Tizzano, Mónica Roselló, Miguel Del Campo, Encarna Guillén, Francisco Martínez, Antonio Martinez-Monseny, Juan Darío Ortigoza-Escobar, Ainhoa Pascual-Alonso, Pablo Lapunzina, Mar O'Callaghan, Clara Xiol, Carlota Ros, Rosario Marín, Alberto Plaja, and Paola Pacheco

Subjects
Genetics, business.industry, MECP2 duplication syndrome, medicine, medicine.disease, business
Published
2020
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5. Molecular characterization of Spanish patients with MECP2 duplication syndrome

Author

Antonio Martinez-Monseny, Clara Xiol, María Aurora Mesas, Alberto Plaja, Carlota Ros, Judith Armstrong, Pablo Lapunzina, Soledad Alcántara, José Luís Peña‐Segura, Maria Sanchez, Vicenç Català, Mónica Roselló, Patricia Rubio, Alba-Aina Castells, Rosario Marín, Mar O'Callaghan, Eduardo F. Tizzano, Francisco Martínez, Carmen Orellana, Joaquín A. Fernández-Ramos, María Obón, Silvia Vidal, Salva Ibañez, Esther Gean, Encarna Guillén, Maria Isabel Tejada, Elisabet Lloveras, Paola Pacheco, Nuria Brandi, Laura Blasco, Fernando Santos, Ainhoa Pascual-Alonso, Miguel Del Campo, Juan Darío Ortigoza-Escobar, Hiart Maortua, and Julián Nevado

Subjects
Adult, Male, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, recurrent infections, IRAK1, Adolescent, Xq28-duplication, Methyl-CpG-Binding Protein 2, genotype-phenotype correlation, hypotonia, Developmental Disabilities, Genetic counseling, MECP2 duplication syndrome, 030105 genetics & heredity, Bioinformatics, Young Adult, 03 medical and health sciences, Neurodevelopmental disorder, Methyl-CpG-binding protein 2 (MECP2), Intellectual Disability, Gene duplication, Intellectual disability, Genetics, Humans, Medicine, Multiplex ligation-dependent probe amplification, Precision Medicine, Child, intellectual disability, Genetic Association Studies, Genetics (clinical), Chromosomes, Human, X, Comparative Genomic Hybridization, business.industry, Infant, medicine.disease, Hypotonia, Pedigree, Interleukin-1 Receptor-Associated Kinases, 030104 developmental biology, Child, Preschool, Mental Retardation, X-Linked, Muscle Hypotonia, Female, medicine.symptom, business, MECP2 duplication, Comparative genomic hybridization
Abstract

MECP2 duplication syndrome (MDS) is an X-linked neurodevelopmental disorder characterized by a severe to profound intellectual disability, early onset hypotonia and diverse psycho-motor and behavioural features. To date, fewer than 200 cases have been published. We report the clinical and molecular characterization of a Spanish MDS cohort that included 19 boys and 2 girls. Clinical suspicions were confirmed by array comparative genomic hybridization and multiplex ligation-dependent probe amplification (MLPA). Using, a custom in-house MLPA assay, we performed a thorough study of the minimal duplicated region, from which we concluded a complete duplication of both MECP2 and IRAK1 was necessary for a correct MDS diagnosis, as patients with partial MECP2 duplications lacked some typical clinical traits present in other MDS patients. In addition, the duplication location may be related to phenotypic severity. This observation may provide a new approach for genotype-phenotype correlations, and thus more personalized genetic counselling.

Published
2020

6. Two cases of misinterpretation of molecular results in incontinentia pigmenti, and a PCR-based method to discriminate NEMO/IKK? dene deletion

Author

E. Tarantino, Angela Sparago, Michele D'Urso, Vincenzo Mercadante, Tiziana Bardaro, Esther Gean Molins, Matilde Valeria Ursini, Geppino Falco, Bardaro, Tiziana, Falco, Geppino, Sparago, Angela, Mercadante, Vincenzo, Molins, Esther Gean, Tarantino, Enrico, Ursini, Matilde Valeria, and D'Urso, Michele

Subjects
Genetic counseling, Pseudogene, IKBKG, DNA Mutational Analysis, Molecular Sequence Data, IKKγ, Protein Serine-Threonine Kinases, Biology, Polymerase Chain Reaction, X-inactivation, Exon, NEMO, Genetics, medicine, Humans, Incontinentia Pigmenti, Diagnostic Errors, Gene, Genetics (clinical), I-Kappa-B Kinase, NF-κB essential modulator, Incontinentia pigmenti, medicine.disease, I-kappa B Kinase, Pedigree, Molecular diagnosi, Molecular Diagnostic Techniques, IP, Female, Gene Deletion, Pseudogenes
Abstract

Familial incontinentia pigmenti (IP) is a rare X-linked dominant disorder that affects ectodermal tissues. Over 90% of IP carrier females have a recurrent genomic deletion of exons 4-10 of the NEMO (IKBKG-IKKgamma) gene, which encodes a regulatory component of the IkB kinase complex, required to activate the NF-kB pathway. In IP, mutations in NEMO lead to the complete loss of NF-kB activation creating a susceptibility to cellular apoptosis in response to TNF-alpha. This condition is lethal for males during embryogenesis while females, who are mosaic as a result of X-inactivation, can survive. Recently, a second nonfunctional copy of the gene, DeltaNEMO, was identified, opposite in direction to NEMO in a 35.5-kb duplicated sequence tract. PCR-based detection of the NEMO deletion is diagnostic for IP disease. However, we present instances in which ex 4-10 DeltaNEMO pseudogene deletion occurs in unaffected parents of two females with clinically characteristic IP These were missed by the currently standard PCR- based method, but can be easily discriminated by a new PCR-based test reported here that permits unambiguous molecular diagnosis and proper familial genetic counseling for IP.

Published
2002
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7. Adults with Sotos syndrome: Review of 21 adults with molecularly confirmed NSD1 alterations, including a detailed case report of the oldest person

Author

Angela E. Lin, Nina Tolkoff-Rubin, Enrique Galán, Valeria Romanelli, Joaquín Fernández Toral, Matthew R. Fickie, Esther Gean, Pablo Lapunzina, Jennifer K. Gentile, Daniela Kroshinsky, and Loreto Martorell

Subjects
Adult, Male, Pediatrics, medicine.medical_specialty, Genotype, Scoliosis, Fibromuscular dysplasia, Craniofacial Abnormalities, Genetics, medicine, Humans, Craniofacial, Genetics (clinical), Sotos Syndrome, Learning Disabilities, Sotos syndrome, business.industry, Incidence (epidemiology), Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Histone-Lysine N-Methyltransferase, Middle Aged, medicine.disease, Phenotype, Carcinoma, Basal Cell, Overgrowth syndrome, Carcinoma, Squamous Cell, Histone Methyltransferases, Female, Haploinsufficiency, business, Kidney disease
Abstract

Sotos syndrome is a well-described multiple anomaly syndrome characterized by overgrowth, distinctive craniofacial appearance, and variable learning disabilities. The diagnosis of Sotos syndrome relied solely on these clinical criteria until haploinsufficiency of the NSD1 gene was identified as causative. We describe a 63-year-old woman with classic features and a pathogenic NSD1 mutation, who we believe to be the oldest reported person with Sotos syndrome. She is notable for the diagnosis of Sotos syndrome late in life, mild cognitive limitation, and chronic kidney disease attributed to fibromuscular dysplasia for which she recently received a transplant. She has basal cell and squamous cell carcinoma for which her lifetime of sun exposure and fair cutaneous phototype are viewed as risk factors. We also reviewed previous literature reports (n = 11) for adults with Sotos syndrome, and studied patients ascertained in the Spanish Overgrowth Syndrome Registry (n = 15). Analysis was limited to 21/27 (78%) total patients who had molecular confirmation of Sotos syndrome (15 with a mutation, 6 with a microdeletion). With a mean age of 26 years, the most common features were learning disabilities (90%), scoliosis (52%), eye problems (43%), psychiatric issues (30%), and brain imaging anomalies (28%). Learning disabilities were more severe in patients with a microdeletion than in those with a point mutation. From this small study with heterogeneous ascertainment we suggest modest adjustments to the general healthcare monitoring of individuals with Sotos syndrome. Although this series includes neoplasia in four cases, this should not be interpreted as incidence. Age-appropriate cancer surveillance should be maintained. © 2011 Wiley-Liss, Inc.

Published
2011
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8. Beckwith–Wiedemann syndrome and uniparental disomy 11p: fine mapping of the recombination breakpoints and evaluation of several techniques

Author

Esther Gean, Victor Martinez-Glez, Ricardo Gracia-Bouthelier, Encarna Guillén, Loreto Martorell, Julián Nevado, Sixto García-Miñaur, Mario F. Fraga, Victoria Esteban Marfil, Pablo Lapunzina, Luis Morís Fernández, Heloisa Meneses, and Valeria Romanelli

Subjects
Epigenomics, Beckwith-Wiedemann Syndrome, Beckwith–Wiedemann syndrome, Chromosome Breakpoints, Biology, Article, Genomic Imprinting, Insulin-Like Growth Factor II, Genetics, Macroglossia, medicine, Humans, Genetics (clinical), Oligonucleotide Array Sequence Analysis, Polydactyly, Mosaicism, Chromosomes, Human, Pair 11, Chromosome Mapping, Sequence Analysis, DNA, DNA Methylation, Uniparental Disomy, medicine.disease, Uniparental disomy, Phenotype, Overgrowth syndrome, medicine.symptom, Genomic imprinting, Visceromegaly, Microsatellite Repeats
Abstract

Beckwith–Wiedemann syndrome (BWS) is a phenotypically and genotypically heterogeneous overgrowth syndrome characterized by somatic overgrowth, macroglossia and abdominal wall defects. Other usual findings are hemihyperplasia, embryonal tumours, adrenocortical cytomegaly, ear anomalies, visceromegaly, renal abnormalities, neonatal hypoglycaemia, cleft palate, polydactyly and a positive family history. BWS is a complex, multigenic disorder associated, in up to 90% of patients, with alteration in the expression or function of one or more genes in the 11p15.5 imprinted gene cluster. There are several molecular anomalies associated with BWS and the large proportion of cases, about 85%, is sporadic and karyotypically normal. One of the major categories of BWS molecular alteration (10–20% of cases) is represented by mosaic paternal uniparental disomy (pUPD), namely patients with two paternally derived copies of chromosome 11p15 and no maternal contribution for that. In these patients, in addition to the effects of IGF2 overexpression, a decreased level of the maternally expressed gene CDKN1C may contribute to the BWS phenotype. In this paper, we reviewed a series of nine patients with BWS because of pUPD using several methods with the aim to evaluate the percentage of mosaicism, the methylation status at both loci, the extension of the pUPD at the short arm and the breakpoints of recombination. Fine mapping of mitotic recombination breakpoints by single-nucleotide polymorphism-array in individuals with UPD and fine estimation of epigenetic defects will provide a basis for understanding the aetiology of BWS, allowing more accurate prognostic predictions and facilitating management and surveillance of individuals with this disorder.

Published
2011
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9. Van der Woude Syndrome and Lower Lip Pits Treatment

Author

Angeles M. Sancho, Francisco Jose Parri, Elena Muñoz, Lucas Krauel, Morales L, and Esther Gean

Subjects
Male, business.industry, Cleft Lip, Oral Surgical Procedures, Lower lip, Dentistry, Syndrome, Anatomy, medicine.disease, Lip, Otorhinolaryngology, medicine, Humans, Female, Surgery, Van der Woude syndrome, Oral Surgery, business, High penetrance
Abstract

sed w lip p d s in t trus 89%). F 4 had b cleft l wing o tidisc rgic tients. reof an der Woude Syndrome (VWS) (OMIM 119300 n autosomal dominant developmental disorder ch cterized by lower lip pits or sinuses and cleft alate. Although first described by Demarqu 1845), it was Van der Woude (1954) 2 who exten ively reviewed these features and established a ionship between lower lip pits and cleft lip or p ntroducing a new clinical entity and describing ode of heredity. VWS has a variable expressivity high penetrance ranging from 89% to 99%. Its lence varies from 1:35,000 to 1:100,000 live birth 3-5

Published
2008
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10. [Diploid/triploid mosaicism: a variable but characteristic phenotype]

Author

Daniel, Natera-De Benito, Pilar, Poo, Esther, Gean, Asunción, Vicente-Villa, Angels, García-Cazorla, and M Carmen, Fons-Estupiña

Subjects
Heart Defects, Congenital, Hypopigmentation, Abortion, Habitual, Fetal Growth Retardation, Mosaicism, Infant, Newborn, Abnormal Karyotype, Fibroblasts, Triploidy, Phenotype, Epilepsy, Absence, Face, Intellectual Disability, Obesity, Abdominal, Infant, Small for Gestational Age, Humans, Abnormalities, Multiple, Female, Lymphocytes, Syndactyly, Retrospective Studies
Abstract

Diploid/triploid mosaicism is a rare chromosomal abnormality. It is caused by a failure in the postzygotic division during embryonic development. It results in the coexistence of two genetically heterogeneous cell lines (46,XX and 69,XXX) in one individual. His clinical phenotype is characteristic. Pigmentary changes with a distribution pattern following Blaschko's lines abnormalities in other ectoderm-derived tissues are the main diagnostic signs.Three cases of diploid/triploid mosaicism are described, and compared to the previously reported cases. The most frequently observed symptoms were mental retardation, truncal obesity, short stature, hemihypertrophy, small and narrow hands with clino and camptodactyly. Phenotypic characteristics of our three patients were similar to those of previously reported cases. Although there is no single and specific phenotype associated with mosaicism diploid/triploid, there are some dysmorphic features that shape a recognizable malformative syndrome. Peripheral blood lymphocytes karyotype was normal in our patients. Diagnosis was reached performing a fibroblast karyotype from hypopigmented skin.Intellectual disability associated with truncal obesity, short stature, hemihypertrophy or clino/camptodactyly should suggest to clinicians the possible existence of a diploid/triploid mosaicism. In most cases, karyotype from fibroblasts is needed to reach the diagnosis.Mosaicismo diploide/triploide: un fenotipo variable, pero caracteristico.Introduccion. El mosaicismo diploide/triploide es una alteracion cromosomica poco frecuente. La produce un fallo en la division poscigotica durante el desarrollo embrionario. Da lugar a la coexistencia de dos lineas celulares con diferente constitucion cromosomica (46,XX y 69,XXX) en un mismo individuo. Su fenotipo clinico es caracteristico. Las alteraciones pigmentarias con un patron de distribucion que sigue las lineas de Blaschko son el principal signo guia, asi como las alteraciones de otros tejidos derivados del ectodermo. Casos clinicos. Describimos las caracteristicas clinicas de tres pacientes afectos de mosaicismo diploide/triploide y realizamos una comparacion de su fenotipo clinico con el de los casos publicados previamente en la bibliografia. Las alteraciones observadas con mayor frecuencia fueron alteraciones cutaneas, discapacidad intelectual, obesidad troncular, talla baja, hemihipertrofia, y manos pequeñas y estrechas con clino y camptodactilia. Las caracteristicas fenotipicas de nuestros pacientes fueron similares a las de los casos comunicados previamente. Aunque no existe un fenotipo unico y especifico asociado al mosaicismo diploide/triploide, existen malformaciones caracteristicas que conforman un sindrome malformativo bien definido. El cariotipo realizado en linfocitos de sangre periferica en las tres pacientes fue normal, y se logro el diagnostico mediante cariotipo en fibroblastos cultivados tras biopsia de piel hipopigmentada. Conclusiones. La presencia de discapacidad intelectual asociada a obesidad troncular, talla baja, hemihipertrofia o clino y camptodactilia, ademas de las alteraciones cutaneas, debe hacer pensar en la posible existencia de un mosaicismo diploide/triploide. En la mayoria de los casos, es necesario el estudio del cariotipo en los fibroblastos para llegar al diagnostico.

Published
2014

11. Axenfeld-Rieger ocular anomaly and retinoblastoma caused by constitutional chromosome 13q deletion

Author

Ana Roche, Jaume Mora, Belen Perez, Andreu Parareda, Joan Prat, Maria del Mar Perez, Esther Gean, Jaume Català, Ofelia Cruz, Mar O'Callaghan, and Carmen de Torres

Subjects
Chemotherapy, Pathology, medicine.medical_specialty, business.industry, Retinoblastoma, Systemic chemotherapy, medicine.medical_treatment, Intra arterial chemotherapy, Chromosome, Cryotherapy, Hematology, medicine.disease, eye diseases, Oncology, Pediatrics, Perinatology and Child Health, medicine, In patient, sense organs, business, Development delay
Abstract

Axenfeld-Rieger (AR) ocular anomaly might be due to deletions of different chromosomes. No association between AR, mental retardation, and retinoblastoma has been described. We report a 2-month-old female with general development delay and dysmorphic features. AR anomaly was detected, and a retinoblastoma (RB) was diagnosed in a very early stage. De novo 13q deletion was identified. Systemic chemotherapy, focal cryotherapy, transpupillary thermotherapy, brachytherapy, and intra-arterial chemotherapy were needed to control the RB. This is the first report of an association of AR, 13q deletion, and retinoblastoma, to be disclosed in patients born with such ocular and dysmorphic features.

Published
2009
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12. The ciliary EVC/EVC2 complex interacts with Smo and controls Hedgehog pathway activity in chondrocytes by regulating Sufu/Gli3 dissociation and Gli3 trafficking in primary cilia

Author

María Valencia, Edel Reytor, María Pacheco, Esther Gean, Victor L. Ruiz-Perez, Margarita Fernández, José A. Caparrós-Martín, Antonio Perez-Aytes, Pablo Lapunzina, Judith A. Goodship, Heiko Peters, Ministerio de Ciencia e Innovación (España), European Commission, and Fundación Ramón Areces

Subjects
Morphogenesis, Kruppel-Like Transcription Factors, Nerve Tissue Proteins, Biology, Receptors, G-Protein-Coupled, Mice, Chondrocytes, Zinc Finger Protein Gli3, GLI3, Genetics, Gene silencing, Animals, Hedgehog Proteins, Cilia, Molecular Biology, Hedgehog, Genetics (clinical), Cilium, Membrane Proteins, General Medicine, Smoothened Receptor, Hedgehog signaling pathway, Mice, Mutant Strains, Cell biology, Repressor Proteins, Protein Transport, Intercellular Signaling Peptides and Proteins, Signal transduction
Abstract

et al., Hedgehog (Hh) signaling is involved in patterning and morphogenesis of most organs in the developing mammalian embryo. Despite many advances in understanding core components of the pathway, little is known about how the activity of the Hh pathway is adjusted in organ- and tissue-specific developmental processes. Mutations in EVC or EVC2 disrupt Hh signaling in tooth and bone development. Using mouse models, we show here that Evc and Evc2 are mutually required for localizing to primary cilia and also for maintaining their normal protein levels. Consistent with Evc and Evc2 functioning as a complex, the skeletal phenotypes in either single or double homozygous mutant mice are virtually indistinguishable. Smo translocation to the cilium was normal in Evc2-deficient chondrocytes following Hh activation with the Smo-agonist SAG. However, Gli3 recruitment to cilia tips was reduced and Sufu/Gli3 dissociation was impaired. Interestingly, we found Smo to co-precipitate with Evc/Evc2, indicating that in some cells Hh signaling requires direct interaction of Smo with the Evc/Evc2 complex. Expression of a dominantly acting Evc2 mutation previously identified in Weyer's acrodental dysostosis (Evc2ο43) caused mislocalization of Evc/Evc2ο43 within the cilium and also reproduced the Gli3-related molecular defects observed in Evc2-/- chondrocytes. Moreover, Evc silencing in Sufu-/- cells attenuated the output of the Hh pathway, suggesting that Evc/Evc2 also promote Hh signaling in the absence of Sufu. Together our data reveal that the Hh pathway involves Evc/Evc2-dependent modulations that are necessary for normal endochondral bone formation. © The Author 2012. Published by Oxford University Press. All rights reserved., This work was funded by the Spanish Ministry of Science and Innovation (SAF-17901), the European Union (LSHM-CT-2007-03741) and the Ramón Areces Foundation.

Published
2013

13. Macrocephaly-capillary malformation: Analysis of 13 patients and review of the diagnostic criteria

Author

Esther Gean, Loreto Martorell, Pablo Lapunzina, María A. Mori, Valeria Romanelli, Mabel Segovia, Ricardo Gracia, Antonio González-Meneses, Victor Martinez-Glez, and Juan Carlos López-Gutiérrez

Subjects
Genetic Markers, Male, medicine.medical_specialty, Capillary malformation, Adolescent, DNA Copy Number Variations, Genotype, Port-Wine Stain, Skin Diseases, Vascular, Neuroimaging, Gene Frequency, Genetics, Medicine, Humans, Abnormalities, Multiple, Copy-number variation, Telangiectasis, Child, Genetics (clinical), Livedo Reticularis, business.industry, Macrocephaly, Syndrome, medicine.disease, Megalencephaly, Capillaries, Macrocephaly-capillary malformation, Overgrowth syndrome, Child, Preschool, Reticular connective tissue, Etiology, Radiology, medicine.symptom, business
Abstract

Macrocephaly-capillary malformation (M-CM) is a genetic syndrome of unknown etiology characterized by an enlarged head circumference and patchy, reticular capillary malformation. We describe the clinical features of 13 cases, report on the genome-wide Copy Number Variation characterization of these patients, analyze the main clinical features of this syndrome and propose a modification of the current diagnostic criteria: the inclusion of both overgrowth/asymmetry and neuroimaging alterations as major criteria.

Published
2010

14. Phylloid Hypomelanosis and Mosaic Partial Trisomy 13

Author

Esther Gean, Vicenç Català, Rudolf Happle, M. Antonia González-Enseñat, Asunción Vicente, P Póo, Carme Fuster, and M. Mar Pérez-Iribarne

Subjects
Pathology, medicine.medical_specialty, Clinodactyly, Adolescent, Skin Pigmentation, Trisomy, Dermatology, Diagnosis, Differential, medicine, Humans, Trichomegaly, Syndactyly, Child, In Situ Hybridization, Fluorescence, Hypopigmentation, Chromosomes, Human, Pair 13, Mosaicism, business.industry, General Medicine, medicine.disease, Phenotype, Tetrasomy, Phylloid hypomelanosis, Female, medicine.symptom, business, Patau's syndrome
Abstract

Background Phylloid hypomelanosis is a rare neurocutaneous syndrome characterized by a pattern of hypopigmentation consisting of leaflike or oblong macules reminiscent of floral ornaments. Associated extracutaneous anomalies include cerebral, ocular, and skeletal defects. Recently it has been suggested that this phenotype originates from mosaic partial or complete trisomy 13. We report clinical and cytogenetic data for 2 cases. Observations A bizarre pattern of multiple leaflike macules was noted in 2 girls with mental deficiency. In patient 1, additional anomalies included syndactyly, clinodactyly, trichomegaly of the eyelashes, low frontal hairline, and several pale pink telangiectatic macules. In patient 2, epileptic seizures, dental malposition, oligodontia, preauricular fistulas, scoliosis, tethered cord, and syringomyelia were noted. A diagnosis of phylloid hypomelanosis was made in both patients. In both patients, blood lymphocytes showed a normal karyotype 46,XX; however, fibroblasts derived from lesional skin demonstrated tetrasomy of chromosome 13q21-qter in patient 1 and trisomy of 13q22-qter in patient 2. Conclusions These 2 cases lend further support to the concept that phylloid hypomelanosis is a distinct clinicogenetic entity that should no longer be confused with pigmentary mosaicism of the Ito type. From a comparison of our cytogenetic findings with those documented in previous articles, we infer that phylloid hypomelanosis is most likely related to the 13q region.

Published
2009
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15. White matter alterations associated with chromosomal disorders

Author

P Póo, Angels García-Cazorla, Jaume Campistol, María Dolores García-Bargo, Miguel Baquero, Esther Gean, A Sans, and Montse Arellano

Subjects
Male, Pediatrics, medicine.medical_specialty, Adolescent, Developmental Disabilities, Leukomalacia, Periventricular, Physiology, Periventricular white matter, White matter, Developmental Neuroscience, medicine, Image Processing, Computer-Assisted, Dementia, Humans, In patient, Abnormalities, Multiple, Child, Chromosome Aberrations, White matter alterations, medicine.diagnostic_test, Dementia, Vascular, Infant, Newborn, Brain, Infant, Karyotype, Magnetic resonance imaging, Syndrome, medicine.disease, Image Enhancement, Magnetic Resonance Imaging, medicine.anatomical_structure, Child, Preschool, Karyotyping, Pediatrics, Perinatology and Child Health, Female, Neurology (clinical), Trisomy, Psychology
Abstract

White matter alterations in chromosomal disorders have been reported mainly in 18q-syndrome. Our aim was to evaluate white matter alterations in patients with chromosomal abnormalities detected through conventional cytogenetic techniques. Forty-four patients with chromosomal abnormalities, excluding trisomy 21, were diagnosed in our hospital between May 1999 and December 2002 (24 males, 20 females; mean age 6 years 4 months [SD 3 years 2 months], range 0 to 18 years). Of the 44 patients, 14 had brain magnetic resonance imaging (12 males, 2 females; mean age 4 years 2 months [SD 4 years 4 months]; five with sex chromosomal disorders [SCD] and nine with autosomal chromosomal disorders [ACD]). Of these 14 patients, eight (four with SCD and four with ACD) had abnormal white matter findings of similar patterns. These patients had pseudonodular, subcortical, and periventricular white matter high signal intensity images in T2, and fluid-attenuated inversion recovery sequences that were isolated or confluent. The images did not correlate with the neurological clinical state. Given that eight of the 14 patients showed these lesions, their prevalence in different chromosomal abnormalities appears to be high, even though they have not been well reported in the literature. To our knowledge, these alterations have never been described in SCD. We concluded that unknown factors related to the myelination processes may be localized in different chromosomes.

Published
2004

16. Identification of a novel rhodopsin mutation (Met-44-Thr) in a simplex case of retinitis pigmentosa

Author

Carmen Ayuso, Jaume Antich, Miguel Carballo, Carlos Reig, Esther Gean, Blanca Garcia-Sandoval, and Carmen Ramos

Subjects
Male, Threonine, Rhodopsin, genetic structures, Adolescent, DNA Mutational Analysis, medicine.disease_cause, Polymerase Chain Reaction, Exon, Methionine, Retinitis pigmentosa, Genetics, medicine, Humans, Point Mutation, Genetics (clinical), Aged, Gel electrophoresis, Electrophoresis, Agar Gel, Mutation, biology, Genetic heterogeneity, Point mutation, Exons, Middle Aged, medicine.disease, Phenotype, Molecular biology, eye diseases, Pedigree, biology.protein, Female, sense organs, Retinitis Pigmentosa
Abstract

Retinitis pigmentosa (RP) is a group of genetically heterogeneous retinal degenerations that can be autosomal dominant (ADRP), autosomal recessive (ARRP), or X-linked. Approximately 30% of ADRP patients show point mutations or small deletions in the rhodopsin gene. However, over 50% of the RP patients are simplex cases (sporadic). Screening for mutations in the rhodopsin gene of 33 patients with simplex RP by denaturing gradient gel electrophoresis (DGGE) was carried out. One patient, with D-type (diffuse) RP and consanguineous parents, showed an altered electrophoretic pattern for the 5′ half of exon 1. Direct sequencing revealed a new mutation ATG to ACG in codon 44; this predicts a change of Met-44-Thr in rhodopsin. The position and amino acid substitution suggest that this mutation causes the RP phenotype. Implications for genetic counselling are discussed.

Published
1994

17. Displasia septóptica

Author

Lidia Martínez Sánchez, Amalia Arce, Josep Caritg Bosch, Jaume Campistol Plana, Carlos Pavía Sesma, and Esther Gean Molins

Subjects
Neurology (clinical), General Medicine
Published
2002
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19. White matter alterations associated with chromosomal disorders.

Author

Angels García-Cazorla, Anna Sans, Miguel Baquero, María Dolores García-Bargo, Montse Arellano, Pilar Poo, Esther Gean, and Jaume Campistol

Subjects
CHROMOSOME abnormalities, SEX chromosome abnormalities, CYTOGENETICS, TRISOMY, MAGNETIC resonance imaging
Abstract

White matter alterations in chromosomal disorders have been reported mainly in 18q–syndrome. Our aim was to evaluate white matter alterations in patients with chromosomal abnormalities detected through conventional cytogenetic techniques. Forty-four patients with chromosomal abnormalities, excluding trisomy 21, were diagnosed in our hospital between May 1999 and December 2002 (24 males, 20 females; mean age 6 years 4 months [SD 3 years 2 months], range 0 to 18 years). Of the 44 patients, 14 had brain magnetic resonance imaging (12 males, 2 females; mean age 4 years 2 months [SD 4 years 4 months]; five with sex chromosomal disorders [SCD] and nine with autosomal chromosomal disorders [ACD]). Of these 14 patients, eight (four with SCD and four with ACD) had abnormal white matter findings of similar patterns. These patients had pseudonodular, subcortical, and periventricular white matter high signal intensity images in T2, and fluid-attenuated inversion recovery sequences that were isolated or confluent. The images did not correlate with the neurological clinical state. Given that eight of the 14 patients showed these lesions, their prevalence in different chromosomal abnormalities appears to be high, even though they have not been well reported in the literature. To our knowledge, these alterations have never been described in SCD. We concluded that unknown factors related to the myelination processes may be localized in different chromosomes. [ABSTRACT FROM AUTHOR]

Published
2004

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