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3. Utilidad de las determinaciones analíticas al ingreso en una residencia

Author

B. J. Anía Lafuente, M. Fernández-Burriel Tercero, and J. L. Suárez Almenara

Subjects
Aging, Medicine (miscellaneous), Geriatrics and Gerontology
Abstract

Objetivo : Comprobar si existen variaciones de las magnitudes analiticas estudiadas en los ancianos con la edad, el sexo y la incapacidad funcional, para tenerlos en cuenta a la hora de realizar una valoracion de su estado de salud al ingreso en una residencia. Material Y Metodo : Se recogieron los datos de los analisis hematologicos, bioquimicos y de orina, incluidos en el protocolo de ingreso de 194 sujetos mayores de 65 anos, de los que 82 eran varones (44 asistidos) y 112 eran mujeres (91 asistidas). Resultados : Se encontro una prevalencia de un 27,6% de diabetes y un 15,6% de dislipemias. Cabe destacar una disminucion significativa en los asistidos de la hemoglobina, volumen corpuscular medio, hemoglobina corpuscular media, urato, proteinas totales, albumina, hierro, calcio y fosfato y un aumento de la amplitud de la distribucion eritrocitaria y del recuento de plaquetas. Aumentaban significativamente con la edad el recuento de leucocitos, y disminuian hemoglobina, colesterol, proteinas totales, albumina y sideremia. Ademas, se encontraron en varones valores significativamente mas elevados de volumen corpuscular medio y sideremia y mas bajos de fosfato. La presencia de hallazgos patologicos en la orina se asocio significativamente con el sexo femenino y la condicion de asistido. Conclusiones : Las mayores alteraciones analiticas se observaron en los ancianos asistidos, revelando un deficit nutricional mas o menos latente. Las determinaciones analiticas consideradas de mayor utilidad al ingreso son aquellas que sirven para detectar patologias graves y/o que se puedan tratar eficazmente: hemoglobina, albumina, colesterol, trigliceridos, glucosa, creatinina, ferritina, TSH y sedimento urinario.

Published
2001
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4. Clinical, molecular and biochemical characterization of nine Spanish families with Conradi-Hünermann-Happle syndrome: new insights into X-linked dominant chondrodysplasia punctata with a comprehensive review of the literature

Author

G. Pi-Castán, P. Unamuno, M. Artigas, M. Tejedor, E.M. Sánchez-Tapia, Antonio Torrelo, J. Garcia-Dorado, Jordi Rosell, T. Vendrell, Rogelio González-Sarmiento, Angela Hernández-Martín, M. Fernández-Burriel, Juan Luis García, Vicente García-Patos, M.T. Garcia-Silva, Francisco Martínez, A. Virós, S. Ciria, Javier Cañueto, E. Martín-Hernández, J. Valero, and M. Girós

Subjects
musculoskeletal diseases, Adult, Chondrodysplasia Punctata, Genotype, DISORDERS, EMOPAMIL-BINDING PROTEIN, DNA Mutational Analysis, Steroid Isomerases, MOSAICISM, Dermatology, Gene mutation, Biology, MOUSE, medicine.disease_cause, CHOLESTEROL-BIOSYNTHESIS, X-inactivation, X Chromosome Inactivation, medicine, Humans, Chondrodysplasia punctata, Gene, Genetics, Mutation, CHROMOSOME INACTIVATION, MUTATIONS, Cholestadienols, Infant, Genetic Diseases, X-Linked, medicine.disease, Phenotype, Cholesterol, Spain, biology.protein, lipids (amino acids, peptides, and proteins), Female, CDPX2
Abstract

[Background]: Conradi-Hünermann-Happle syndrome (CDPX2, OMIM 302960) is an inherited X-linked dominant variant of chondrodysplasia punctata which primarily affects the skin, bones and eyes. CDPX2 results from mutations in EBP (emopamil binding protein), and presents with increased levels of sterol precursors 8(9)-cholestenol and 8-dehydrocholesterol. [Objectives]: To expand the understanding of CDPX2, clinically, biochemically and genetically. [Methods]: We present one of the largest series reported to date, including 13 female patients belonging to nine Spanish families. Patients were studied biochemically using gas chromatography-mass spectrometry, genetically using polymerase chain reaction and in their methylation status using the HUMARA assay. [Results]: In our cases, there was a clear relationship between abnormal sterol profile and the EBP gene mutation. We describe three novel mutations in the EBP gene. EBP mutations were inherited in three out of nine families and were sporadic in the remaining cases. [Conclusions]: No clear genotype-phenotype correlation was found. Patients' biochemical profiles did not reveal a relationship between sterol profiles and severity of disease. A skewed X-chromosome inactivation may explain the clinical phenotype in CDPX2 in some familial cases. © 2011 The Authors. BJD © 2011 British Association of Dermatologists.

Published
2011

5. [Molecular diagnosis of adult dominant polycystic kidney disease in the Canary Islands]

Author

M J, Torres, J C, Rodríguez Pérez, C R, Hernández Socorro, A, Anabitarte, A, Caballero, C, Vázquez, M, Fernández-Burriel, P, Pérez Borges, and L, Palop

Subjects
Chromosomes, Human, Pair 14, Genetic Markers, Hypertension, Renal, TRPP Cation Channels, Genetic Carrier Screening, Polycystic Kidney, Autosomal Dominant, Sensitivity and Specificity, Early Diagnosis, Haplotypes, Renal Dialysis, Atlantic Islands, Humans, Lod Score, Chromosomes, Human, Pair 16, Microsatellite Repeats
Abstract

Adult dominant polycystic kidney disease is an hereditary condition responsible for 6% of end-stage renal failure in Spain. Two genes were located in chromosomes 16 and 4 as related to this age-dependent disease in the 90s (PKD1 and PKD2). The diagnosis can be easily achieved by sonographic study, but molecular analysis by means of linkage analysis has the advantage of an early diagnosis in asymptomatic genetic carriers, with a view to the preventive follow-up of these subjects and genetic counselling. In this paper we present the results of molecular analysis of 30 families with Adult Dominant Polycystic Kidney Disease (from the province of Las Palmas Spain), carried out linkage analysis with two series of microsatellite markers located within or in the vicinity ofPKD1 (D16S521, KG8, AC2.5, CW2, SM7) and PKD2 (D4S1538, D4S1534, D4S423,D4S414) genes. The objectives of the study were: first, to verify the informativeness, and therefore, the usefulness of these markers for family studies in our population; and second,to assess the sensitivity and specificity of the genetic analysis in our population. Most of the markers showed a high heterozygosity, comparable to data in other studies. Considering the alleles of the different markers together in a chromosome as an haplotype increased the informativeness of the markers, and allowed the unequivocal identification of genetic data in 97.7% of patients and 88.7% of healthy subjects. The sensitivity and specificity of the genetic analysis were 90.7% (CI 95%: 85.7-95.7) and 86.8% (CI 95%: 80.6-93.0), respectively.

Published
2007

6. [Paroxysmal stereotypy-tic-dystonia syndrome]

Author

J C, Cabrera-López, M, Martí-Herrero, M, Fernández-Burriel, L, Toledo-Bravo de Laguna, S, Domínguez-Ramírez, and S, Fortea-Sevilla

Subjects
Adult, Diagnosis, Differential, Male, Dyskinesias, Dystonic Disorders, Child, Preschool, Tic Disorders, Humans, Infant, Stereotypic Movement Disorder, Child
Abstract

We report the cases of four males from four different families, who presented paroxysmal episodes from the 1st 2nd year. These episodes were characterised by asymmetrical bilateral dystonia of the upper limbs, predominantly in both hands, and were associated with orofacial dyskinesias, stereotipies (jumping, arm flapping, etc.), facial tics and, occasionally, phonic tics. Consciousness is not affected in any of the cases. These movements are triggered in situations where the patient is relaxed or excited. They occur daily and last from a few seconds to 30 minutes. Between the bouts, they remain asymptomatic. Family cases suggest it is inherited by autosomal dominant transmission, perhaps linked to the X chromosome; in addition, two cases are sporadic. In the only adult, the movements progress to a series of rhythmic bilateral dystonic myoclonias and facial tics dyskinesias. All the studies carried out, EEG, hemogram, biochemical analysis, neuroimaging, copper and ceruloplasmin levels, were normal.1. We report a non epileptic paroxysmal disorder originating in the extrapyramidal tracts with its own characteristics, with onset during early childhood, which is associated with stereotipies, tics and dystonia; 2. It occurs predominantly in males; 3. It is inherited by autosomal dominant transmission, or perhaps sex linked autosomal dominant inheritance, and there are also sporadic cases; 4. The range of clinical features is very wide and includes cases in which there are few symptoms to others where the extent and gravity of the disorder is very significant.

Published
2003

8. [Familial Pitt-Rogers-Danks: two new cases]

Author

J C, Cabrera López, M, Marti Herrero, M, Fernández Burriel, L, Toledo, R, de Andrés-Cofiño, and M A, Orera

Subjects
Male, Seizures, Child, Preschool, Intellectual Disability, Microcephaly, Humans, Female, Syndrome, Chromosome Deletion, Chromosomes, Human, Pair 4, Growth Disorders, Pedigree
Abstract

The Pitt Rogers Danks syndrome is characterized by prenatal and postnatal retardation of growth, mental retardation, microcephaly, convulsions and a peculiar facies. It is believed to represent a clinical variant of the Wolf Hirschhorn syndrome, since there is a deletion in the 4p16.3 region in both syndromes. We report two cases in the same family caused by maternal mal segregation of a 4:8 balanced translocation. We describe the clinical characteristics, investigations done and a review of the literature.

Published
2001

9. [Anemia and functional incapacity at admission to a geriatric home]

Author

B J, Anía Lafuente, M, Fernández-Burriel Tercero, J L, Suárez Almenara, C C, Betancort Mastrángelo, and L, Guerra Hernández

Subjects
Aged, 80 and over, Male, Prevalence, Homes for the Aged, Humans, Anemia, Disabled Persons, Female, Middle Aged, Aged
Abstract

To ascertain the prevalence of anemia on admission to a nursing home, and to assess the relationship between the observed cases of anemia and the functional status of those subjects.We studied 198 subjects: 82 men (41%) aged 75.8 +/- 8.8 years, and 116 women (59%) aged 78.2 +/- 8.3 years. Anemia was diagnosed according to the criteria of the World Health Organization. The classification as non-disabled, or physically or mentally disabled, was done according to the Scales of the Spanish Red Cross.Anemia was diagnosed in 36% of the males, being microcytic in 14%, normocytic in 83%, and macrocytic only in 3% of them. Among women there were 44% with anemia, which was microcytic in 16%, normocytic in 80%, and macrocytic in 4% of cases. The prevalence of anemia increased with age in both sexes. Among men, anemia was significantly associated (p = 0.013) with physical disability, whereas among women this association just fell off significance (p = 0.06). There was no association of anemia with mental disability. No association was found between serum concentrations of ferritin, vitamin B12, or folic acid, and the classification as non-disabled, or as physically or mentally disabled.Anemia is found in about 40% of the elderly on admission to our nursing home. Anemia is associated with older age and with physical disability, but not with mental disability. Whether anemia on admission entails a higher risk of disability onset during the stay in the nursing home remains to be elucidated.

Published
2001

10. Anemia e incapacidad funcional al ingreso en una residencia geriátrica

Author

M. Fernández-Burriel Tercero, C. C. Betancort Mastrángelo, J. L. Suárez Almenara, B. J. Anía Lafuente, and L. Guerra Hernández

Subjects
Pediatrics, medicine.medical_specialty, Physical disability, biology, Anemia, business.industry, Anciano válido, Anciano asistido, medicine.disease, Incapacidad, World health, Ferritin, Folic acid, hemic and lymphatic diseases, Internal Medicine, medicine, biology.protein, Functional status, Vitamin B12, Nursing homes, business, Residencia geriátrica
Abstract

Objetivo: Establecer la prevalencia de anemia en ancianos al ingreso en una residencia, así como la relación de las anemias detectadas con el estado funcional de dichos sujetos. Método: Se estudiaron 198 sujetos: 82 varones (41 %) con 75,8±8,8 años y 116 mujeres (59%) con 78,2±8,3 años. Se diagnosticó anemia según los criterios de la Organización Mundial de la Salud, y la clasificación en válidos o asistidos físicos o mentales se llevó a cabo mediante las Escalas de Incapacidad Física y Mental de Cruz Roja. Resultados: El 36% de los varones tenía anemia, que era microcítica en el 14%, normocítica en el 83% y macrocítica sólo en el 3%. Entre las mujeres había un 44% con anemia, que era microcítica en el 16%, normocítica en el 80% y macrocítica en el 4% de los casos. La prevalencia de anemia aumentó con la edad en ambos sexos. Entre los varones la anemia se asoció significativamente (P=0,013) a la incapacidad física, mientras que en las mujeres dicha asociación estuvo en el límite de la significación (P=0,06). La anemia no se asoció a la incapacidad mental en ninguno de los sexos. No hubo asociación entre las concentraciones séricas de ferritina, vitamina B12 o ácido fólico y la clasificación en válidos y asistidos físicos o mentales. Conclusiones: Alrededor del 40% de los ancianos que ingresan en nuestra residencia presentan anemia. La anemia se asocia a la mayor edad y a la incapacidad física, pero no a la incapacidad mental. Queda por determinar si la anemia al ingreso condiciona un mayor riesgo de incapacitación durante la estancia en la residencia

Published
2001
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11. [Thyroid function in the aged admitted to a nursing home]

Author

B J, Anía Lafuente, J L, Suárez Almenara, M, Fernández-Burriel Tercero, L, Guerra Hernández, and C, Betancort Mastrángelo

Subjects
Aged, 80 and over, Male, Thyroid Hormones, Persons with Mental Disabilities, Age Factors, Thyrotropin, Euthyroid Sick Syndromes, Nursing Homes, Diagnosis, Differential, Thyroxine, Sex Factors, Hypothyroidism, Spain, Humans, Disabled Persons, Female, Geriatric Assessment, Aged
Abstract

Intrinsic thyroid diseases and so-called sick euthyroid syndrome are frequent among the elderly. Therefore, we set out to assess the usefulness of the measurement of thyroid hormones and TSH on admission to a public nursing home.A medical history, physical examination, geriatric assessment and a venous sample were taken from 201 elderly subjects on admission to a nursing home. Thyroid hormones and TSH were measured in all cases. All subjects were classified as valid, mentally impaired, or physically impaired, according to the Spanish Red Cross Scales.Sixty non-disabled and 141 disabled elders were studied. Sixteen (7.9%) cases of primary hypothyroidism were found, of whom 7 (3.5%) were deemed deserving treatment with L-thyroxine, their mean daily dose being 114.3 mcg. Sick euthyroid syndrome was considered to be present in 28 (13.9%) cases, of whom 25 had a normal T4, three had a low T4, and none had a high T4. No cases of hyperthyroidism were detected. Thyroid hormone abnormalities were not statistically associated with age, gender, or physical or mental disability.On admission to the nursing home, nearly 8% of the elders have hypothyroidism, and an additional 14% have the sick euthyroid syndrome. Routine measurement of T4 and TSH in elders on admission to a nursing home has a favorable cost-utility ratio.

Published
2000

12. Síndrome de estereotipias-tics-distonía paroxística

Author

L Toledo-Bravo de Laguna, S Domínguez-Ramírez, M Martí-Herrero, S Fortea-Sevilla, M Fernández-Burriel, and J.C. Cabrera-López

Subjects
business.industry, Medicine, Neurology (clinical), General Medicine, business, Humanities
Abstract

Casos clinicos. Presentamos cuatro varones, pertenecientes a cuatro familias diferentes, que presentan, a partir del 1.er­2.o ano, unos episodios de presentacion paroxistica, que se caracterizan por distonia bilateral asimetrica de los miembros superiores, que predominan en ambas manos y que se asocian a discinesias orofaciales, estereotipias (saltos, aleteo, etc.), tics faciales y, a veces, tics fonicos. En ningun caso hay compromiso de la conciencia. Estos movimientos se desencadenan en situaciones de relajacion o excitacion. Son de frecuencia diaria y duran de segundos a 30 minutos. Entre los episodios permanecen asintomaticos. Los casos familiares sugieren herencia autosomica dominante o, quizas, ligada al cromosoma X; ademas, dos casos son esporadicos. En el unico adulto, los movimientos evolucionaron a una serie de mioclonias distonicas bilaterales ritmicas y tics (discinesias faciales). Todos los estudios realizados ?EEG, hemograma, bioquimica, neuroimagen, cupremia y ceruloplasmina? fueron normales. Conclusiones. 1. Presentamos un trastorno paroxistico no epileptico de origen extrapiramidal con caracteristicas propias, de inicio en la infancia, que asocia estereotipias, tics y distonia; 2. Predominio en varones; 3. Su herencia es autosomica dominante o, quizas, herencia ligada al sexo, y tambien hay casos esporadicos; 4. El espectro clinico del cuadro es muy amplio, y abarca desde casos poco sintomaticos hasta otros con una importante afectacion.

Published
2003
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13. Identification of an elusive spliceogenic MYBPC3 variant in an otherwise genotype-negative hypertrophic cardiomyopathy pedigree.

Author

Torrado M, Maneiro E, Lamounier Junior A, Fernández-Burriel M, Sánchez Giralt S, Martínez-Carapeto A, Cazón L, Santiago E, Ochoa JP, McKenna WJ, Santomé L, and Monserrat L

Subjects
Cytoskeletal Proteins genetics, Haploinsufficiency, Humans, Mutation, Pedigree, RNA, Messenger, Cardiomyopathy, Hypertrophic diagnosis, Cardiomyopathy, Hypertrophic genetics, Carrier Proteins genetics
Abstract

The finding of a genotype-negative hypertrophic cardiomyopathy (HCM) pedigree with several affected members indicating a familial origin of the disease has driven this study to discover causative gene variants. Genetic testing of the proband and subsequent family screening revealed the presence of a rare variant in the MYBPC3 gene, c.3331-26T>G in intron 30, with evidence supporting cosegregation with the disease in the family. An analysis of potential splice-altering activity using several splicing algorithms consistently yielded low scores. Minigene expression analysis at the mRNA and protein levels revealed that c.3331-26T>G is a spliceogenic variant with major splice-altering activity leading to undetectable levels of properly spliced transcripts or the corresponding protein. Minigene and patient mRNA analyses indicated that this variant induces complete and partial retention of intron 30, which was expected to lead to haploinsufficiency in carrier patients. As most spliceogenic MYBPC3 variants, c.3331-26T>G appears to be non-recurrent, since it was identified in only two additional unrelated probands in our large HCM cohort. In fact, the frequency analysis of 46 known splice-altering MYBPC3 intronic nucleotide substitutions in our HCM cohort revealed 9 recurrent and 16 non-recurrent variants present in a few probands (≤ 4), while 21 were not detected. The identification of non-recurrent elusive MYBPC3 spliceogenic variants that escape detection by in silico algorithms represents a challenge for genetic diagnosis of HCM and contributes to solving a fraction of genotype-negative HCM cases., (© 2022. The Author(s).)

Published
2022
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14. TBL1XR1 associated intellectual disability, a new missense variant with dysmorphic features plus autism: Expanding the phenotypic spectrum.

Author

Arroyo Carrera I, Fernández-Burriel M, Lapunzina P, Tenorio JA, García Navas VD, and Márquez Isidro E

Subjects
Child, Preschool, Humans, Male, Phenotype, Autistic Disorder genetics, Intellectual Disability genetics, Mutation, Missense genetics, Receptors, Cytoplasmic and Nuclear genetics, Repressor Proteins genetics
Abstract

Missense and frameshift pathogenic variants and microdeletions involving TBL1XR1 gene have been described in patients with intellectual disability, autism, Rett-like features and schizophrenia, some of them with the clinical diagnosis of Pierpont syndrome, a rare pattern of multiple congenital anomalies, but others without dysmorphic findings or with non-specific ones, and also patients with only some of the features associated with Pierpont syndrome. We here present a case with a de novo novel missense variant in TBL1XR1 gene with overlapping features with Pierpont syndrome and autism, a neurobehavioral manifestation not previously reported in Pierpont syndrome. This patient expands the phenotypic spectrum of TBL1XR1 gene pathogenic variants., (© 2021 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2021
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15. Cystinuria: urine sediment as a diagnostic test.

Author

Pierna M, Abdelgabar M, Fernández-Rivas R, and Fernández-Burriel M

Abstract

Objectives: To demonstrate the importance of carrying out the urinary sediment study with the correct interpretation and crystals typification as a clinical laboratory diagnostic tool, as well as the elaboration of protocols that determine the need to realize this type of microscopic urinary sediment examination routinely., Case Presentation: Elderly male patient with no personal or family history of interest that presented with left iliac fossa fixed and non-irradiated pain lasting three days. This is the first time that he suffered pain episodes of this type. The urine analysis reveals proteinuria, hematuria and the sediment shows abundant flat and hexagonal crystals, typical of cystine. Amino acid analysis confirms the finding, showing high dibasic amino acids and cystine concentrations., Conclusions: The study of the urinary sediment by the clinical laboratory reveals the presence of a case of cystinuria due to the appearance of their pathognomonic crystals at an advanced age and without a previous history. The case reported in this paper is of interest for clinical laboratory practice, as it demonstrates the utility of urine sediment examination in the diagnosis of a genetic disease that manifests as a simple renal colic., (© 2020 María Pierna et al., published by De Gruyter, Berlin/Boston.)

Published
2020
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16. High-throughput sequencing for the molecular diagnosis of Usher syndrome reveals 42 novel mutations and consolidates CEP250 as Usher-like disease causative.

Author

Fuster-García C, García-García G, Jaijo T, Fornés N, Ayuso C, Fernández-Burriel M, Sánchez-De la Morena A, Aller E, and Millán JM

Subjects
Female, Humans, Male, Pedigree, Phenotype, Autoantigens genetics, Cell Cycle Proteins genetics, DNA Mutational Analysis methods, Genetic Markers, High-Throughput Nucleotide Sequencing methods, Mutation, Usher Syndromes diagnosis, Usher Syndromes genetics
Abstract

Usher syndrome is a rare disorder causing retinitis pigmentosa, together with sensorineural hearing loss. Due to the phenotypic and genetic heterogeneity of this disease, the best method to screen the causative mutations is by high-throughput sequencing. In this study, we tested a semiconductor chip based sequencing approach with 77 unrelated patients, as a molecular diagnosis routine. In addition, Multiplex Ligation-dependent Probe Amplification and microarray-based Comparative Genomic Hybridization techniques were applied to detect large rearrangements, and minigene assays were performed to confirm the mRNA processing aberrations caused by splice-site mutations. The designed panel included all the USH causative genes (MYO7A, USH1C, CDH23, PCDH15, USH1G, CIB2, USH2A, ADGRV1, WHRN and CLRN1) as well as four uncertainly associated genes (HARS, PDZD7, CEP250 and C2orf71). The outcome showed an overall mutation detection ratio of 82.8% and allowed the identification of 42 novel putatively pathogenic mutations. Furthermore, we detected two novel nonsense mutations in CEP250 in a patient with a disease mimicking Usher syndrome that associates visual impairment due to cone-rod dystrophy and progressive hearing loss. Therefore, this approach proved reliable results for the molecular diagnosis of the disease and also allowed the consolidation of the CEP250 gene as disease causative for an Usher-like phenotype.

Published
2018
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17. Clinical, molecular and biochemical characterization of nine Spanish families with Conradi-Hünermann-Happle syndrome: new insights into X-linked dominant chondrodysplasia punctata with a comprehensive review of the literature.

Author

Cañueto J, Girós M, Ciria S, Pi-Castán G, Artigas M, García-Dorado J, García-Patos V, Virós A, Vendrell T, Torrelo A, Hernández-Martín A, Martín-Hernández E, Garcia-Silva MT, Fernández-Burriel M, Rosell J, Tejedor M, Martínez F, Valero J, García JL, Sánchez-Tapia EM, Unamuno P, and González-Sarmiento R

Subjects
Adult, Cholestadienols metabolism, Cholesterol metabolism, Chondrodysplasia Punctata metabolism, DNA Mutational Analysis methods, Female, Genetic Diseases, X-Linked metabolism, Genotype, Humans, Infant, Phenotype, Spain, Chondrodysplasia Punctata genetics, Genetic Diseases, X-Linked genetics, Mutation genetics, Steroid Isomerases genetics, X Chromosome Inactivation genetics
Abstract

Background: Conradi-Hünermann-Happle syndrome (CDPX2, OMIM 302960) is an inherited X-linked dominant variant of chondrodysplasia punctata which primarily affects the skin, bones and eyes. CDPX2 results from mutations in EBP (emopamil binding protein), and presents with increased levels of sterol precursors 8(9)-cholesterol and 8-dehydrocholesterol., Objectives: To expand the understanding of CDPX2, clinically, biochemically and genetically., Methods: We present one of the largest series reported to date, including 13 female patients belonging to nine Spanish families. Patients were studied biochemically using gas chromatography-mass spectrometry, genetically using polymerase chain reaction and in their methylation status using the HUMARA assay., Results: In our cases, there was a clear relationship between abnormal sterol profile and the EBP gene mutation. We describe three novel mutations in the EBP gene. EBP mutations were inherited in three out of nine families and were sporadic in the remaining cases., Conclusions: No clear genotype-phenotype correlation was found. Patients' biochemical profiles did not reveal a relationship between sterol profiles and severity of disease. A skewed X-chromosome inactivation may explain the clinical phenotype in CDPX2 in some familial cases., (© 2011 The Authors. BJD © 2011 British Association of Dermatologists.)

Published
2012
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18. Xq26.2-q26.3 microduplication in two brothers with intellectual disabilities: clinical and molecular characterization.

Author

Madrigal I, Fernández-Burriel M, Rodriguez-Revenga L, Cabrera JC, Martí M, Mur A, and Milà M

Subjects
Adolescent, Carrier Proteins genetics, Gene Duplication, Guanine Nucleotide Exchange Factors genetics, Humans, Hypoxanthine Phosphoribosyltransferase genetics, Male, Repressor Proteins, Rho Guanine Nucleotide Exchange Factors, Sex Chromosome Aberrations, Sex Chromosome Disorders genetics, Sodium-Hydrogen Exchangers genetics, Trisomy genetics, Young Adult, Chromosomes, Human, X genetics, Genes, X-Linked, X-Linked Intellectual Disability genetics
Abstract

Partial duplications involving the long arm of the X chromosome are associated with mental retardation, short stature, microcephaly, hypopituitarism and a wide range of physical findings. We identified an inherited Xq26.2-Xq26.3 duplication in two brothers with severe mental retardation, hypotonia, growth delay, craniofacial disproportion and dental malocclusion. Chromosome analysis was normal and multiplex ligation-dependent probe amplification analysis detected duplication on Xq26. Further characterization by array comparative genomic hybridization and quantitative PCR helped to determine proximal and distal duplication breakpoints giving a size of approximately 2.8 Mb. The duplication encompasses 24 known genes, including the X-linked mental retardation genes ARHGEF6, PHF6, HPRT1 and SLC9A6. Clinical and molecular characterization of Xq duplications will shed more light into the phenotypic implication of functional disomy of X-chromosome genes.

Published
2010
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19. Mutation update of spinal muscular atrophy in Spain: molecular characterization of 745 unrelated patients and identification of four novel mutations in the SMN1 gene.

Author

Alías L, Bernal S, Fuentes-Prior P, Barceló MJ, Also E, Martínez-Hernández R, Rodríguez-Alvarez FJ, Martín Y, Aller E, Grau E, Peciña A, Antiñolo G, Galán E, Rosa AL, Fernández-Burriel M, Borrego S, Millán JM, Hernández-Chico C, Baiget M, and Tizzano EF

Subjects
DNA Mutational Analysis, Female, Humans, Male, Molecular Sequence Data, Mutation, Spain, Muscular Atrophy, Spinal genetics, Survival of Motor Neuron 1 Protein genetics
Abstract

Spinal muscular atrophy (SMA) is caused by mutations in the SMN1 gene. We have studied the molecular pathology of SMA in 745 unrelated Spanish patients using PCR-RFLP, SMN gene dosage analysis, linkage studies, long-range PCR and direct sequencing. Our systematic approach allowed us to complete genetic testing and risk assessment in 736 SMA patients (98.8%). Females were more frequently affected by the acute form of the disease (type I), whereas chronic forms (type II-III) predominated in males (p<0.008). Absence of the SMN1 gene was detected in 671 patients (90%), and hybrid SMN1-SMN2 genes were observed in 37 cases (5%). Furthermore, we detected 13 small mutations in 28 patients (3.8%), four of which were previously identified in other populations (c.91dupT; c.770&#95;780dup11; p.Tyr272Cys and p.Thr274Ile), while five mutations were found to date only in Spanish patients (c.399&#95;402delAGAG, p.Ile116Phe, p.Gln136Glu, c.740dupC and c.834+2T>G). The c.399&#95;402delAGAG mutation accounted for 1.9% of all Spanish SMA patients. Finally, we discovered four novel mutations: c.312dupA, c.411delT, p.Trp190X and p.Met263Thr. Our results confirm that most SMA cases are due to large genetic rearrangements in the repetitive region of the SMA locus, resulting in absence-dysfunction of the SMN1 gene. By contrast, ancestrally inherited small mutations are responsible for only a small number of cases. Four prevalent changes in exons 3 and 6 (c.399&#95;402delAGAG; c.770&#95;780dup11; p.Tyr272Cys; p.Thr274Ile) accounted for almost 70% of our patients with these subtle mutations. An SMN-SMN dimer model featuring tight hydrophobic-aromatic interactions is proposed to explain the impact of mutations at the C-terminal end of the protein.

Published
2009
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20. A novel delins mutation in the alpha-TTP gene in a family segregating ataxia with isolated vitamin E deficiency.

Author

Fernández-Burriel M, Martínez-Rubio D, Lupo V, Pérez-Colosía V, Piñán-López E, Palau F, and Espinós C

Subjects
Adolescent, Apolipoprotein A-I blood, Apolipoproteins B blood, Ataxia blood, Dietary Supplements, Humans, Male, Pedigree, Vitamin E administration & dosage, Vitamin E blood, Vitamin E therapeutic use, Vitamin E Deficiency diet therapy, Ataxia genetics, Carrier Proteins genetics, Mutation genetics, Vitamin E Deficiency genetics
Abstract

Ataxia with isolated vitamin E deficiency is a rare autosomal recessive neurodegenerative disease due to mutations in the alpha-tocopherol transfer protein gene. In ataxia with isolated vitamin E deficiency, the biochemical hallmark is the low plasmatic levels of vitamin E and, in most of the patients, vitamin E supplementation allows a stabilization of the neurologic conditions. We have investigated the genetic cause of ataxia and reduced levels of vitamin E, and apolipoproteins A1 and B in a 16-y-old patient. Results revealed that our propositus is a compound heterozygote for the c.227&#95;229delinsATT/c.744delA mutations in the alpha-tocopherol transfer protein gene, each inherited from one of the two parents. His sister is also a compound heterozygote for both mutations, and she presents a biochemical pattern similar to that of his brother. After receiving the vitamin E supplementation, plasmatic levels of vitamin E and apolipoprotein A1 have been normalized in the propositus. The detected mutations would justify the undetectable levels of vitamin E, but would not explain the also decreased levels of the apolipoproteins, as neither that after treatment with vitamin E, the levels of apolipoprotein B do not become normal. These findings suggest that other genes may play a role in producing this atypical biochemical profile.

Published
2008
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21. MLPA as first screening method for the detection of microduplications and microdeletions in patients with X-linked mental retardation.

Author

Madrigal I, Rodríguez-Revenga L, Badenas C, Sánchez A, Martinez F, Fernandez I, Fernández-Burriel M, and Milà M

Subjects
DNA Primers, DNA Probes genetics, Humans, In Situ Hybridization, Fluorescence, Male, Nucleic Acid Amplification Techniques methods, Pedigree, Chromosome Aberrations, Chromosomes, Human, X genetics, Gene Duplication, Genetic Testing methods, X-Linked Intellectual Disability genetics, Sequence Deletion genetics
Abstract

Purpose: Routine protocols for the study of mental retardation include karyotype, analysis for fragile X syndrome, and subtelomeric rearrangements. Nevertheless, detection of cryptic rearrangements requires more sensitive techniques. Mutation screening in all known genes responsible for X-linked mental retardation is not feasible, and linkage analysis is sometimes limited. Multiplex ligation probe amplification is a recently developed technique based on the amplification of specific probes that allows relative quantification of 40 to 46 different target DNA sequences in a single reaction., Methods: In the present study, we assessed multiplex ligation probe amplification for the detection of microduplications/microdeletions in 80 male patients with suspicion of X-linked mental retardation., Results: We detected four copy number aberrations (5%): three duplications (GDI1, RPS6KA3, and ARHGEF6) and one deletion (OPHN1). All these changes were confirmed by other molecular techniques, and patients were clinically re-evaluated., Conclusions: We strongly recommend the use of multiplex ligation probe amplification as a first screening method for the detection of copy number aberrations in patients with mental retardation because of its cost-effectiveness.

Published
2007
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22. [Molecular diagnosis of adult dominant polycystic kidney disease in the Canary Islands].

Author

Torres MJ, Rodríguez Pérez JC, Hernández Socorro CR, Anabitarte A, Caballero A, Vázquez C, Fernández-Burriel M, Pérez Borges P, and Palop L

Subjects
Atlantic Islands epidemiology, Early Diagnosis, Genetic Carrier Screening, Genetic Markers, Haplotypes genetics, Humans, Hypertension, Renal epidemiology, Hypertension, Renal etiology, Lod Score, Microsatellite Repeats, Polycystic Kidney, Autosomal Dominant epidemiology, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant therapy, Renal Dialysis, Sensitivity and Specificity, Chromosomes, Human, Pair 14 genetics, Chromosomes, Human, Pair 16 genetics, Polycystic Kidney, Autosomal Dominant diagnosis, TRPP Cation Channels analysis
Abstract

Adult dominant polycystic kidney disease is an hereditary condition responsible for 6% of end-stage renal failure in Spain. Two genes were located in chromosomes 16 and 4 as related to this age-dependent disease in the 90s (PKD1 and PKD2). The diagnosis can be easily achieved by sonographic study, but molecular analysis by means of linkage analysis has the advantage of an early diagnosis in asymptomatic genetic carriers, with a view to the preventive follow-up of these subjects and genetic counselling. In this paper we present the results of molecular analysis of 30 families with Adult Dominant Polycystic Kidney Disease (from the province of Las Palmas Spain), carried out linkage analysis with two series of microsatellite markers located within or in the vicinity ofPKD1 (D16S521, KG8, AC2.5, CW2, SM7) and PKD2 (D4S1538, D4S1534, D4S423,D4S414) genes. The objectives of the study were: first, to verify the informativeness, and therefore, the usefulness of these markers for family studies in our population; and second,to assess the sensitivity and specificity of the genetic analysis in our population. Most of the markers showed a high heterozygosity, comparable to data in other studies. Considering the alleles of the different markers together in a chromosome as an haplotype increased the informativeness of the markers, and allowed the unequivocal identification of genetic data in 97.7% of patients and 88.7% of healthy subjects. The sensitivity and specificity of the genetic analysis were 90.7% (CI 95%: 85.7-95.7) and 86.8% (CI 95%: 80.6-93.0), respectively.

Published
2006

23. DFNA49, a novel locus for autosomal dominant non-syndromic hearing loss, maps proximal to DFNA7/DFNM1 region on chromosome 1q21-q23.

Author

Moreno-Pelayo MA, Modamio-Høybjør S, Mencía A, del Castillo I, Chardenoux S, Fernández-Burriel M, Lathrop M, Petit C, and Moreno F

Subjects
Adolescent, Child, Female, Genes, Recessive genetics, Genetic Linkage, Haplotypes genetics, Hearing Loss, Bilateral diagnosis, Hearing Loss, Bilateral genetics, Hearing Loss, Sensorineural diagnosis, Humans, Male, Pedigree, Spain, Syndrome, Chromosomes, Human, Pair 1 genetics, Genes, Dominant genetics, Genetic Markers genetics, Hearing Loss, Sensorineural genetics, Physical Chromosome Mapping methods
Published
2003
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24. A simple method of screening for the common connexin-26 gene 35delG mutation in nonsyndromic neurosensory autosomal recessive deafness.

Author

Fernández-Burriel M and Rodríguez-Quiñones F

Subjects
Base Sequence, Connexin 26, DNA Mutational Analysis methods, DNA Primers genetics, Genes, Recessive, Humans, Polymerase Chain Reaction methods, Spain, Connexins genetics, Deafness genetics, Genetic Testing methods, Sequence Deletion
Abstract

Mutations in the Connexin-26 gene are responsible for up to 60% of nonsyndromic, neurosensory autosomal recessive deafness (NSRD). Amongst all the mutations described to date, 35delG (a deletion of a G in a tract of five Gs at positions 30-35) is the most common and has been found in virtually all of the populations studied. Because its frequency varies in different populations, a rapid and simple method of detection of this mutation would be very helpful in population studies. A wide variety of methods for this detection have been described, but we herein present a very simple method using a PCR with primers designed to provide an amplicon of 94 or 93 nucleotides for the normal or mutant alleles, respectively, that can be easily distinguished in an 8% polyacrylamide gel. The entire protocol can be completed in a morning, thus supporting multiple runs. This assay will be useful in screening the large sample sizes required for population studies.

Published
2003
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25. [Adult cystic fibrosis: new clinical presentations].

Author

Cabrera Roca G, Fernández-Burriel Tercero M, and Cabrera Navarro P

Subjects
Adult, Cystic Fibrosis Transmembrane Conductance Regulator genetics, DNA Mutational Analysis, Humans, Phenotype, Point Mutation genetics, Cystic Fibrosis diagnosis, Cystic Fibrosis genetics
Published
2003

26. [Paroxysmal stereotypy-tic-dystonia syndrome].

Author

Cabrera-López JC, Martí-Herrero M, Fernández-Burriel M, Toledo-Bravo de Laguna L, Domínguez-Ramírez S, and Fortea-Sevilla S

Subjects
Adult, Child, Child, Preschool, Diagnosis, Differential, Dyskinesias genetics, Dystonic Disorders genetics, Humans, Infant, Male, Stereotypic Movement Disorder genetics, Tic Disorders genetics, Dyskinesias physiopathology, Dystonic Disorders physiopathology, Stereotypic Movement Disorder physiopathology, Tic Disorders physiopathology
Abstract

Case Reports: We report the cases of four males from four different families, who presented paroxysmal episodes from the 1st 2nd year. These episodes were characterised by asymmetrical bilateral dystonia of the upper limbs, predominantly in both hands, and were associated with orofacial dyskinesias, stereotipies (jumping, arm flapping, etc.), facial tics and, occasionally, phonic tics. Consciousness is not affected in any of the cases. These movements are triggered in situations where the patient is relaxed or excited. They occur daily and last from a few seconds to 30 minutes. Between the bouts, they remain asymptomatic. Family cases suggest it is inherited by autosomal dominant transmission, perhaps linked to the X chromosome; in addition, two cases are sporadic. In the only adult, the movements progress to a series of rhythmic bilateral dystonic myoclonias and facial tics dyskinesias. All the studies carried out, EEG, hemogram, biochemical analysis, neuroimaging, copper and ceruloplasmin levels, were normal., Conclusions: 1. We report a non epileptic paroxysmal disorder originating in the extrapyramidal tracts with its own characteristics, with onset during early childhood, which is associated with stereotipies, tics and dystonia; 2. It occurs predominantly in males; 3. It is inherited by autosomal dominant transmission, or perhaps sex linked autosomal dominant inheritance, and there are also sporadic cases; 4. The range of clinical features is very wide and includes cases in which there are few symptoms to others where the extent and gravity of the disorder is very significant.

Published
2003

28. [Familial Pitt-Rogers-Danks: two new cases].

Author

Cabrera López JC, Marti Herrero M, Fernández Burriel M, Toledo L, de Andrés-Cofiño R, and Orera MA

Subjects
Child, Preschool, Chromosome Deletion, Chromosomes, Human, Pair 4 genetics, Female, Growth Disorders complications, Humans, Intellectual Disability complications, Male, Microcephaly complications, Pedigree, Seizures complications, Syndrome, Growth Disorders genetics, Intellectual Disability genetics, Microcephaly genetics, Seizures genetics
Abstract

Introduction and Clinical Cases: The Pitt Rogers Danks syndrome is characterized by prenatal and postnatal retardation of growth, mental retardation, microcephaly, convulsions and a peculiar facies. It is believed to represent a clinical variant of the Wolf Hirschhorn syndrome, since there is a deletion in the 4p16.3 region in both syndromes. We report two cases in the same family caused by maternal mal segregation of a 4:8 balanced translocation. We describe the clinical characteristics, investigations done and a review of the literature.

Published
2001

29. [Anemia and functional incapacity at admission to a geriatric home].

Author

Anía Lafuente BJ, Fernández-Burriel Tercero M, Suárez Almenara JL, Betancort Mastrángelo CC, and Guerra Hernández L

Subjects
Aged, Aged, 80 and over, Female, Homes for the Aged, Humans, Male, Middle Aged, Prevalence, Anemia epidemiology, Persons with Disabilities
Abstract

Aim: To ascertain the prevalence of anemia on admission to a nursing home, and to assess the relationship between the observed cases of anemia and the functional status of those subjects., Methods: We studied 198 subjects: 82 men (41%) aged 75.8 +/- 8.8 years, and 116 women (59%) aged 78.2 +/- 8.3 years. Anemia was diagnosed according to the criteria of the World Health Organization. The classification as non-disabled, or physically or mentally disabled, was done according to the Scales of the Spanish Red Cross., Results: Anemia was diagnosed in 36% of the males, being microcytic in 14%, normocytic in 83%, and macrocytic only in 3% of them. Among women there were 44% with anemia, which was microcytic in 16%, normocytic in 80%, and macrocytic in 4% of cases. The prevalence of anemia increased with age in both sexes. Among men, anemia was significantly associated (p = 0.013) with physical disability, whereas among women this association just fell off significance (p = 0.06). There was no association of anemia with mental disability. No association was found between serum concentrations of ferritin, vitamin B12, or folic acid, and the classification as non-disabled, or as physically or mentally disabled., Conclusions: Anemia is found in about 40% of the elderly on admission to our nursing home. Anemia is associated with older age and with physical disability, but not with mental disability. Whether anemia on admission entails a higher risk of disability onset during the stay in the nursing home remains to be elucidated.

Published
2001

30. Detection of the fragile X syndrome protein for the evaluation of FMR1 intermediate alleles.

Author

Castellví-Bel S, Fernández-Burriel M, Rifé M, Jiménez D, Mallolas J, Sánchez A, Ramos F, and Milà M

Subjects
Alleles, Child, Child, Preschool, Fragile X Mental Retardation Protein, Genetic Testing, Humans, Nerve Tissue Proteins metabolism, Fragile X Syndrome metabolism, Intellectual Disability genetics, Nerve Tissue Proteins genetics, RNA-Binding Proteins, Trinucleotide Repeat Expansion genetics
Abstract

Molecular screening programs in mentally retarded individuals have been performed in several populations worldwide. One finding has been an excess of FMR1 intermediate alleles in a population with learning difficulties. However, other published reports with similar characteristics did not corroborate those previous results. In order to contribute additional data from our population, we studied 563 patients affected with nonspecific mental retardation (MRX) that did not present a CGG expansion in the FMR1 gene and 208 individuals as a control population. Forty MRX patients presented alleles within the intermediate range. Among them, one case showed a pattern of expression of the FMR1 protein (FMRP) concordant with a fragile X syndrome case with an intermediate allele/full mutation mosaicism, although it was not detected by Southern blot analysis. Statistical analysis was performed again showing no statistically significant difference regarding the intermediate allele frequency in the MRX and control populations. This finding is in agreement with the hypothesis that the incidence of intermediate FMR1 alleles in MRX populations does not seem to be higher than in control populations, and it emphasizes the importance of FMRP detection as a diagnostic tool for fragile X syndrome.

Published
2000
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31. [Thyroid function in the aged admitted to a nursing home].

Author

Anía Lafuente BJ, Suárez Almenara JL, Fernández-Burriel Tercero M, Guerra Hernández L, and Betancort Mastrángelo C

Subjects
Age Factors, Aged, Aged, 80 and over, Diagnosis, Differential, Persons with Disabilities, Euthyroid Sick Syndromes blood, Euthyroid Sick Syndromes diagnosis, Female, Geriatric Assessment, Humans, Hypothyroidism diagnosis, Hypothyroidism drug therapy, Male, Nursing Homes, Persons with Intellectual Disabilities, Sex Factors, Spain epidemiology, Thyroid Hormones blood, Thyrotropin blood, Thyroxine therapeutic use, Euthyroid Sick Syndromes epidemiology, Hypothyroidism epidemiology
Abstract

Background: Intrinsic thyroid diseases and so-called sick euthyroid syndrome are frequent among the elderly. Therefore, we set out to assess the usefulness of the measurement of thyroid hormones and TSH on admission to a public nursing home., Methods: A medical history, physical examination, geriatric assessment and a venous sample were taken from 201 elderly subjects on admission to a nursing home. Thyroid hormones and TSH were measured in all cases. All subjects were classified as valid, mentally impaired, or physically impaired, according to the Spanish Red Cross Scales., Results: Sixty non-disabled and 141 disabled elders were studied. Sixteen (7.9%) cases of primary hypothyroidism were found, of whom 7 (3.5%) were deemed deserving treatment with L-thyroxine, their mean daily dose being 114.3 mcg. Sick euthyroid syndrome was considered to be present in 28 (13.9%) cases, of whom 25 had a normal T4, three had a low T4, and none had a high T4. No cases of hyperthyroidism were detected. Thyroid hormone abnormalities were not statistically associated with age, gender, or physical or mental disability., Conclusions: On admission to the nursing home, nearly 8% of the elders have hypothyroidism, and an additional 14% have the sick euthyroid syndrome. Routine measurement of T4 and TSH in elders on admission to a nursing home has a favorable cost-utility ratio.

Published
2000

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