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3. Efficacité et sécurité d’emploi du givosiran chez des patients atteints de porphyrie hépatique aiguë : résultats à 36 mois de l’essai clinique randomisé de phase 3 ENVISION

Author

Thapar, M., primary, Bonkovsky, H., additional, Monroy, S., additional, Ross, G., additional, Guillén-Navarro, E., additional, Cappellini, M.D., additional, Minder, A.E., additional, Liu, S., additional, Sweetser, M., additional, Lainé, A.F., additional, Poizat, L., additional, and Kuter, D., additional

Published
2022
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4. Deep Molecular Characterization of Milder Spinal Muscular Atrophy Patients Carrying the c.859G>C Variant in SMN2

Author

Blasco-Pérez, L., Costa-Roger, M., Leno-Colorado, J., Bernal, Sara, Alias, L., Codina Solà, Marta, Martínez-Cruz, D., Castiglioni, C., Bertini, E., Travaglini, L., Millán, J.M., Aller, E., Sotoca Fernández, Javier, Juntas, R., Hoei-Hansen, C.E., Moreno-Escribano, A., Guillén-Navarro, E., Costa-Comellas, L., Munell Casadesus, Francina, Boronat, S., Rojas-García, R., Povedano, M., Cusco, Ivon, Tizzano, E.F., Universitat Autònoma de Barcelona, Institut Català de la Salut, [Blasco-Pérez L, Costa-Roger M, Leno-Colorado J, Codina-Solà M, Martínez-Cruz D, Tizzano EF] Grup de Recerca de Medicina Genètica, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. Àrea de Genètica Clínica i Molecular, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. [Bernal S, Alias L] Genetics Department and Sant Pau Biomedical Research Institute, Hospital de la Santa Creu i Sant Pau, Barcelona, Spain. Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), Madrid, Spain. [Sotoca J, Juntas R] Unitat de Malalties Neuromusculars, Servei de Neurologia, Vall d’Hebron Hospital Universitari, Barcelona, Spain. [Costa-Comellas L, Munell F] Grup de Recerca en Neurologia Pediàtrica, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Vall d’Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. [Cuscó I] Grup de Recerca de Medicina Genètica, Vall d’Hebron Institut de Recerca (VHIR), Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. Àrea de Genètica Clínica i Molecular, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), Madrid, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects
técnicas de investigación::técnicas genéticas::estudios de asociación genética [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], SMN2 copies, Organic Chemistry, Muscular atrophy, enfermedades del sistema nervioso::enfermedades del sistema nervioso central::enfermedades de la médula espinal::atrofia muscular espinal [ENFERMEDADES], Phenotype-genotype correlations, General Medicine, positive modifiers, Catalysis, Genètica molecular, Computer Science Applications, spinal muscular atrophy, phenotype–genotype correlations, next-generation sequencing, Fenotip, Inorganic Chemistry, Phenotype, Atròfia muscular espinal - Aspectes genètics, Nervous System Diseases::Central Nervous System Diseases::Spinal Cord Diseases::Muscular Atrophy, Spinal [DISEASES], Physical and Theoretical Chemistry, Atròfia muscular, Molecular Biology, Spectroscopy, Investigative Techniques::Genetic Techniques::Genetic Association Studies [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT]
Abstract

Next-generation sequencing; Phenotype–genotype correlations; Spinal muscular atrophy Seqüenciació de nova generació; Correlacions fenotip-genotip; Atròfia muscular espinal Secuenciación de nueva generación; Correlaciones fenotipo-genotipo; Atrofia muscular espinal Spinal muscular atrophy (SMA) is a severe neuromuscular disorder caused by biallelic loss or pathogenic variants in the SMN1 gene. Copy number and modifier intragenic variants in SMN2, an almost identical paralog gene of SMN1, are known to influence the amount of complete SMN proteins. Therefore, SMN2 is considered the main phenotypic modifier of SMA, although genotype–phenotype correlation is not absolute. We present eleven unrelated SMA patients with milder phenotypes carrying the c.859G>C-positive modifier variant in SMN2. All were studied by a specific NGS method to allow a deep characterization of the entire SMN region. Analysis of two homozygous cases for the variant allowed us to identify a specific haplotype, Smn2-859C.1, in association with c.859G>C. Two other cases with the c.859G>C variant in their two SMN2 copies showed a second haplotype, Smn2-859C.2, in cis with Smn2-859C.1, assembling a more complex allele. We also identified a previously unreported variant in intron 2a exclusively linked to the Smn2-859C.1 haplotype (c.154-1141G>A), further suggesting that this region has been ancestrally conserved. The deep molecular characterization of SMN2 in our cohort highlights the importance of testing c.859G>C, as well as accurately assessing the SMN2 region in SMA patients to gain insight into the complex genotype–phenotype correlations and improve prognostic outcomes. This research was funded by grants from Biogen (ESP-SMG-17-11256), Roche, GaliciAME and Spanish Instituto de Salud Carlos III, Fondo de Investigaciones Sanitarias and co-funded with ERDF funds (grant no. FIS PI18/000687). A grant from Horizon 2020 IMI2 Screen4Care is acknowledged by E.B., and L.T., E.F.T., R.J., J.S., L.C.-C., F.M., E.B., and L.T. are members of the ERN NMD Network for Rare Diseases. E.F.T. is a member of the ERN ITHACA Network for Rare Diseases.

Published
2022

9. Heterozygous pathogenic variants in GLI1 are a common finding in isolated postaxial polydactyly A/B

Author

Palencia-Campos A, Martínez-Fernández ML, Altunoglu U, Soto-Bielicka P, Torres A, Marín P, Aller E, Sentürk L, Berköz Ö, Yildiran M, Kayserili H, Gil-Camarero E, Colli-Lista G, Sanchís-Calvo A, Carretero A, ECEMC Working Group on Polydactyly, Guillén-Navarro E, López-González V, Ballesta-Martínez M, Rosell J, Aglan MS, Temtamy S, Otaify GA, Cuevas-Catalina L, Torres-Saavedra MN, Nevado J, Tenorio J, Lapunzina P, Bermejo-Sánchez E, and Ruiz-Pérez VL

Subjects
integumentary system, incomplete penetrance, GLI1, limb development, postaxial polydactyly A, GLI1, Postaxial polydactyly A/B, hedgehog signaling, incomplete penetrance, limb development, hedgehog signaling
Abstract

Postaxial polydactyly (PAP) is a frequent limb malformation consisting in the duplication of the fifth digit of the hand or foot. Morphologically, this condition is divided into type A and B, with PAP-B corresponding to a more rudimentary extra-digit. Recently, bi-allelic truncating variants in the transcription factor GLI1 were reported to be associated with a recessive disorder, which in addition to PAP-A, may include syndromic features. Moreover, two heterozygous subjects carrying only one inactive copy of GLI1 were also identified with PAP. Herein, we aimed to determine the level of involvement of GLI1 in isolated PAP, a condition previously established to be autosomal dominantly inherited with incomplete penetrance. We analysed the coding region of GLI1 in 95 independent probands with non-syndromic PAP and found 11.57% of these subjects with single heterozygous pathogenic variants in this gene. The detected variants lead to premature termination codons or result in amino acid changes in the DNA-binding domain of GLI1 that diminish its transactivation activity. Family segregation analysis of these variants was consistent with dominant inheritance with incomplete penetrance. We conclude that heterozygous changes in GLI1 underlie a significant proportion of sporadic or familial cases of isolated PAP-A/B. This article is protected by copyright. All rights reserved.

Published
2020

10. Novel CYP4F22 mutations associated with autosomal recessive congenital ichthyosis (ARCI). Study of the CYP4F22 c.1303C>T founder mutation

Author

Esperón-Moldes U, Ginarte-Val M, Rodríguez-Pazos L, Fachal L, Martín-Santiago A, Vicente-Villa MA, Jiménez-Gallo D, Guillén-Navarro E, Sampol LM, González-Enseñat MA, and Vega A

Abstract

Mutations in CYP4F22 cause autosomal recessive congenital ichthyosis (ARCI). However, less than 10% of all ARCI patients carry a mutation in CYP4F22. In order to identify the molecular basis of ARCI among our patients (a cohort of ninety-two Spanish individuals) we performed a mutational analysis using direct Sanger sequencing in combination with a multigene targeted NGS panel. From these, eight ARCI families (three of them with Moroccan origin) were found to carry five different CYP4F22 mutations, of which two were novel. Computational analysis showed that the mutations found were present in highly conserved residues of the protein and may affect its structure and function. Seven of the eight families were carriers of a highly recurrent CYP4F22 variant, c.1303C>T; p.(His435Tyr). A 12Mb haplotype was reconstructed in all c.1303C>T carriers by genotyping ten microsatellite markers flanking the CYP4F22 gene. A prevalent 2.52Mb haplotype was observed among Spanish carrier patients suggesting a recent common ancestor. A smaller core haplotype of 1.2Mb was shared by Spanish and Moroccan families. Different approaches were applied to estimate the time to the most recent common ancestor (TMRCA) of carrier patients with Spanish origin. The age of the mutation was calculated by using DMLE and BDMC2. The algorithms estimated that the c.1303C>T variant arose approximately 2925 to 4925 years ago, while Spanish carrier families derived from a common ancestor who lived in the XIII century. The present study reports five CYP4F22 mutations, two of them novel, increasing the number of CYP4F22 mutations currently listed. Additionally, our results suggest that the recurrent c.1303C>T change has a founder effect in Spanish population and c.1303C>T carrier families originated from a single ancestor with probable African ancestry.

Published
2020

11. Participant-funded clinical trials on rare diseases

Author

Dal-Ré R, Palau F, Guillén-Navarro E, and Ayuso C

Subjects
Clinical trials, Patient-funded, Orphan drugs, Self-funded, Crowdfunding, health care economics and organizations, Rare diseases
Abstract

The development of medicines for certain rare diseases can be frustrated by lack of funding. In certain cases the patients themselves, or their relatives, occasionally fund the clinical trial in which they will be treated with the investigational medicine. There are 3 models of self-funded research: 2 of them, "pay to try" and "pay to participate", have already been put into practice. The third, the "plutocratic" proposal, which has been recently put forward is still a theoretical model. In this work the scientific, social and ethical benefits and risks of the 2 clinical research models, "pay to participate" and the "plutocratic" proposal, are reviewed. Patient-funded clinical trials are frequently performed through crowdfunding. The most controversial aspects of this funding modality are also addressed in this article from several perspectives. Finally, a future scenario that would allow the launching of self-funded clinical trials in Spain by the "plutocratic" proposal is proposed. (C) 2020 Asociacion Espanola de Pediatria. Published by Elsevier Espana, S.L.U.

Published
2020

14. Comprehensive long-term efficacy and safety of recombinant human alpha-mannosidase (velmanase alfa) treatment in patients with alpha-mannosidosis

Author

Lund, A.M. (Allan), Borgwardt, L., Cattaneo, F., Ardigò, D., Geraci, S, Gil-Campos, M., Meirleir, L. (Linda) de, Laroche, C., Dolhem, P., Cole, D, Tylki-Szymanska, A., Lopez-Rodriguez, M., Guillén-Navarro, E., Dali, C.I., Héron, B., Fogh, J., Muschol, N., Phillips, D.E. (David E), Hout, J.M.P. (Johanna) van den, Jones, S.A. (Simon), Amraoui, Y., Harmatz, P., Guffon, N. (Nathalie), Lund, A.M. (Allan), Borgwardt, L., Cattaneo, F., Ardigò, D., Geraci, S, Gil-Campos, M., Meirleir, L. (Linda) de, Laroche, C., Dolhem, P., Cole, D, Tylki-Szymanska, A., Lopez-Rodriguez, M., Guillén-Navarro, E., Dali, C.I., Héron, B., Fogh, J., Muschol, N., Phillips, D.E. (David E), Hout, J.M.P. (Johanna) van den, Jones, S.A. (Simon), Amraoui, Y., Harmatz, P., and Guffon, N. (Nathalie)

Abstract

Introduction Long-term outcome data provide important insights into the clinical utility of enzyme replacement therapies. Such data are presented for velmanase alfa in the treatment of alpha-mannosidosis (AM). Methods Patient data (n = 33; 14 adults, 19 paediatric) from the clinical development programme for velmanase alfa were integrated in this prospectively-designed analysis of long-term efficacy and safety. Patients who participated in the phase I/II or phase III trials and were continuing to receive treatment after completion of the trials were invited to participate in a comprehensive evaluation visit to assess long-term outcomes. Primary endpoints were changes in serum oligosaccharide and the 3-minute stair climb test (3MSCT). Results Mean (SD) treatment exposure was 29.3 (15.2) months. Serum oligosaccharide levels were significantly reduced in the overall population at 12 months (mean change: –72.7%, P < 0.001) and remained statistically significant at last observation (−62.8%, P < 0.001). A mean improvement of +9.3% in 3MSCT was observed at 12 months (P = 0.013), which also remained statistically significant at last observation (+13.8%, P = 0.004), with a more pronounced improvement detected in the paediatric subgroup. No treatment-emergent adverse events were reported leading to permanent treatment discontinuation. Conclusions Patients treated with velmanase alfa experienced improvements in biochemical and functional measures that were maintained for up to 4 years. Long term follow-up is important and further supports the use of velmanase alfa as an effective and well-tolerated treatment for AM. Based on the currently available data set, no baseline characteristic can be predictive of treatment outcome. Early treatment during paediatric age showed better outcome in functional endpoints.

Published
2018
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15. Comprehensive long-term efficacy and safety of recombinant human alpha-mannosidase (velmanase alfa) treatment in patients with alpha-mannosidosis

Author

Lund, AM, Borgwardt, L, Cattaneo, F, Ardigò, D, Geraci, S, Gil-Campos, M, de Meirleir, L, Laroche, C, Dolhem, P, Cole, D, Tylki-Szymanska, A, Lopez-Rodriguez, M, Guillén-Navarro, E, Dali, CI, Héron, B, Fogh, J, Muschol, N, Phillips, D, van den Hout, Hannerieke, Jones, SA, Amraoui, Y, Harmatz, P, Guffon, N, Lund, AM, Borgwardt, L, Cattaneo, F, Ardigò, D, Geraci, S, Gil-Campos, M, de Meirleir, L, Laroche, C, Dolhem, P, Cole, D, Tylki-Szymanska, A, Lopez-Rodriguez, M, Guillén-Navarro, E, Dali, CI, Héron, B, Fogh, J, Muschol, N, Phillips, D, van den Hout, Hannerieke, Jones, SA, Amraoui, Y, Harmatz, P, and Guffon, N

Published
2018

16. A New Overgrowth Syndrome is due to Mutations inRNF125

Author

Tenorio J, Mansilla A, Valencia M, Martínez-Glez V, Romanelli V, Arias P, Castrejon N, Poletta F, Guillén-Navarro E, Gordo G, Mansilla E, García-Santiago F, González-Casado I, Vallespín E, Palomares M, Mori MA, Santos-Simarro F, García-Miñaur S, Fernández L, Mena R, Benito-Sanz S, del Pozo Á, Silla JC, Ibañez K, López-Granados E, Martín-Trujillo A, Montaner D, SOGRI Consortium, Heath KE, Campos-Barros Á, Dopazo J, Nevado J, Monk D, Ruiz-Pérez VL, and Lapunzina P

Subjects
Male, CIENCIAS MÉDICAS Y DE LA SALUD, RNF125, Ubiquitin-Protein Ligases, Inmunología, Hypoglycemia, Biology, macrocephaly, medicine.disease_cause, Downregulation and upregulation, Intellectual disability, Genetics, medicine, Humans, Missense mutation, Registries, overgrowth, Growth Disorders, Genetics (clinical), Mutation, Macrocephaly, Syndrome, medicine.disease, Pedigree, Ubiquitin ligase, Medicina Básica, intellectual disability, Spain, Overgrowth syndrome, biology.protein, Cancer research, Female, medicine.symptom, autoimmune disorder
Abstract

Overgrowth syndromes (OGS) are a group of disorders in which all parameters of growth and physical development are above the mean for age and sex. We evaluated a series of 270 families from the Spanish Overgrowth Syndrome Registry with no known OGS. We identified one de novo deletion and three missense mutations in RNF125 in six patients from four families with overgrowth, macrocephaly, intellectual disability, mild hydrocephaly, hypoglycemia, and inflammatory diseases resembling Sjögren syndrome. RNF125 encodes an E3 ubiquitin ligase and is a novel gene of OGS. Our studies of the RNF125 pathway point to upregulation of RIG-I-IPS1-MDA5 and/or disruption of the PI3K-AKT and interferon signaling pathways as the putative final effectors. Fil: Tenorio, Jair. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Mansilla, Alicia. Instituto Cajal. Madrid; España Fil: Valencia, María. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Martínez Glez, Víctor. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Romanelli, Valeria. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España Fil: Arias, Pedro. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Castrejón, Nerea. Hospital San Juan de Dios. Barcelona; España Fil: Poletta, Fernando Adrián. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Parque Centenario. CEMIC-CONICET. Centro de Educaciones Médicas e Investigaciones Clínicas ; Argentina Fil: Guillén Navarro, Encarna. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Hospital Virgen de la Arrixaca. Murcia; España Fil: Gordo, Gema. Universidad Autónoma de Madrid; España Fil: Mansilla, Elena. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: García Santiago, Fé. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: González Casado, Isabel. Hospital Universitario La Paz. Madrid; España Fil: Vallespín, Elena. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Palomares, María. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Mori, María A.. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Santos Simarro, Fernando. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: García Miñaur, Sixto. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Fernández, Luis. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Mena, Rocío. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Benito Sanz, Sara. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: del Pozo, Ángela. Hospital Universitario La Paz. Madrid; España Fil: Silla, Juan Carlos. Hospital Universitario La Paz. Madrid; España Fil: Ibañez, Kristina. Hospital Universitario La Paz. Madrid; España Fil: López Granados, Eduardo. Hospital Universitario La Paz. Madrid; España Fil: Martín Trujillo, Alex. Cancer Epigenetics and Biology Program. Barcelona; España Fil: Montaner, David. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Centro de Investigación Príncipe Felipe. Valencia; España Fil: The SOGRI Consortium. Hospital Universitario La Paz. Madrid; España Fil: Heath, Karen E. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Hospital Universitario La Paz. Madrid; España Fil: Campos Barros, Ángel. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Hospital Universitario La Paz. Madrid; España Fil: Dopazo, Joaquín. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Centro de Investigación Príncipe Felipe. Valencia; España Fil: Nevado, Julián. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Hospital Universitario La Paz. Madrid; España Fil: Monk, David. Cancer Epigenetics and Biology Program. Barcelona; España Fil: Ruiz Pérez, Víctor. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España Fil: Lapunzina, Pablo. Centro de Investigación Biomédica en Red de Enfermedades Raras. Madrid; España. Universidad Autónoma de Madrid; España

Published
2014

20. Cardiofaciocutaneous syndrome, a Noonan syndrome related disorder: Clinical and molecular findings in 11 patients

Author

Carcavilla A, García-Miñaúr S, Pérez-Aytés A, Vendrell T, Pinto I, Guillén-Navarro E, González-Meneses A, Aoki Y, Grinberg D, and Ezquieta B

Subjects
MAP2K1, Genotype-phenotype correlation, Pulmonary valve stenosis, RAS-MAPK pathway, Noonan syndrome, PTPN11, LEOPARD syndrome, Cardiofaciocutaneous syndrome, Hypertrophic cardiomyopathy, Rasopathy, BRAF
Abstract

Objectives: To describe 11 patients with cardiofaciocutaneous syndrome (CFC) and compare them with 130 patients with other RAS-MAPK syndromes (111 Noonan syndrome patients [NS] and 19 patients with LEOPARD syndrome). Patients and methods: Clinical data from patients submitted for genetic analysis were collected. Bidirectional sequencing analysis of PTPN11, SOS1, RAF1, BRAF, and MAP2K1 focused on exons carrying recurrent mutations, and of all KRAS exons were performed. Results: Six different mutations in BRAF were identified in 9 patients, as well as 2 MAP2K1 mutations. Short stature, developmental delay, language difficulties and ectodermal anomalies were more frequent in CFC patients when compared with other neuro-cardio-faciocutaneous syndromes (P

Published
2015

21. Síndrome cardiofaciocutáneo, un trastorno relacionado con el síndrome de Noonan: hallazgos clínicos y moleculares en 11 pacientes

Author

Carcavilla A, García-Miñaúr S, Pérez-Aytés A, Vendrell T, Pinto I, Guillén-Navarro E, González-Meneses A, Aoki Y, Grinberg-Vaisman DR, and Ezquieta B

Subjects
BRAF, Cardiofaciocutaneous syndrome, Correlación genotipo-fenotipo, Estenosis pulmonar valvular, Genotype-phenotype correlation, Hypertrophic cardiomyopathy, LEOPARD syndrome, MAP2K1, Miocardiopatía hipertrófica, Noonan syndrome, PTPN11, Pulmonary valve stenosis, RAS-MAPK pathway, Rasopathy, Rasopatía, Síndrome LEOPARD, Síndrome cardiofaciocutáneo, Síndrome de Noonan, Vía RAS-MAPK
Abstract

To describe 11 patients with cardiofaciocutaneous syndrome (CFC) and compare them with 130 patients with other RAS-MAPK syndromes (111 Noonan syndrome patients [NS] and 19 patients with LEOPARD syndrome).

Published
2015

27. Larger aggregates of mutant seipin in Celia's Encephalopathy, a new protein misfolding neurodegenerative disease

Author

Ruiz-Riquelme, A., Sánchez-Iglesias, S., Rábano, A., Guillén-Navarro, E., Domingo-Jiménez, R., Ramos, A., Rosa, I., Senra, A., Nilsson, Peter, García, Á., Araújo-Vilar, D., Requena, J. R., Ruiz-Riquelme, A., Sánchez-Iglesias, S., Rábano, A., Guillén-Navarro, E., Domingo-Jiménez, R., Ramos, A., Rosa, I., Senra, A., Nilsson, Peter, García, Á., Araújo-Vilar, D., and Requena, J. R.

Abstract

Celia's Encephalopathy (MIM #. 615924) is a recently discovered fatal neurodegenerative syndrome associated with a new BSCL2 mutation (c.985C>T) that results in an aberrant isoform of seipin (Celia seipin). This mutation is lethal in both homozygosity and compounded heterozygosity with a lipodystrophic BSCL2 mutation, resulting in a progressive encephalopathy with fatal outcomes at ages 6-8. Strikingly, heterozygous carriers are asymptomatic, conflicting with the gain of toxic function attributed to this mutation. Here we report new key insights about the molecular pathogenic mechanism of this new syndrome. Intranuclear inclusions containing mutant seipin were found in brain tissue from a homozygous patient suggesting a pathogenic mechanism similar to other neurodegenerative diseases featuring brain accumulation of aggregated, misfolded proteins. Sucrose gradient distribution showed that mutant seipin forms much larger aggregates as compared with wild type (wt) seipin, indicating an impaired oligomerization. On the other hand, the interaction between wt and Celia seipin confirmed by coimmunoprecipitation (CoIP) assays, together with the identification of mixed oligomers in sucrose gradient fractionation experiments can explain the lack of symptoms in heterozygous carriers. We propose that the increased aggregation and subsequent impaired oligomerization of Celia seipin leads to cell death. In heterozygous carriers, wt seipin might prevent the damage caused by mutant seipin through its sequestration into harmless mixed oligomers., QC 20151125

Published
2015
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28. Mutations in PLOD2 cause autosomal-recessive connective tissue disorders within the Bruck syndrome-Osteogenesis imperfecta phenotypic spectrum

Author

Puig-Hervás, M., Temtamy, S., Aglan, M., Valencia, M., Martínez-Glez, V., Ballesta-Martínez, M., López-González, V., Ashour, A., Amr, K., Pulido, V., Guillén-Navarro, E., Lapunzina, P., Caparrós-Martín, Jose, Ruiz-Perez, V., Puig-Hervás, M., Temtamy, S., Aglan, M., Valencia, M., Martínez-Glez, V., Ballesta-Martínez, M., López-González, V., Ashour, A., Amr, K., Pulido, V., Guillén-Navarro, E., Lapunzina, P., Caparrós-Martín, Jose, and Ruiz-Perez, V.

Abstract

PLOD2 and FKBP10 are genes mutated in Bruck syndrome (BS), a condition resembling osteogenesis imperfecta (OI), but that is also typically associated with congenital joint contractures. Herein, we sought mutations in six consanguineous BS families and detected changes in either PLOD2 or FKBP10 in all cases. Two probands were found with a homozygous frameshift mutation in the alternative exon 13a of PLOD2, indicating that specific inactivation of the longer protein isoform encoded by this gene is sufficient to cause BS. In addition, by homozygosity mapping, followed by a candidate gene approach, we identified a homozygous donor splice site mutation in PLOD2 in a patient with autosomal-recessive OI (AR-OI). Screening of additional samples also revealed compound heterozygous mutations in PLOD2 in two brothers, one affected with mild AR-OI and the other with mild BS. Thus, PLOD2 in addition to causing BS is also associated with AR-OI phenotypes of variable severity. © 2012 Wiley Periodicals, Inc.

Published
2012

35. CARTAS AL EDITOR.

Author

Martínez Sánchez, L., Velasco Rodríguez, J., Panzino Occhiuzzo, F., Simó Nebot, M., García Algar, O., Luaces Cubells, C., Ibáñez Micó, S., Domingo Jiménez, R., Guillén Navarro, E., Casas Fernández, C., Araújo-Vilar, D., Cardona-Hernández, R., Suárez-Ortega, L., Torres, M., Barrio Torres, J., López Carreira, M., Gandolfo Cano, M., Rivero Martín, M. J., Martinón-Torres, N., and Pías Peleteiro, L.

Published
2011

36. Variability in Phelan-McDermid Syndrome in a Cohort of 210 Individuals

Author

Julián, Nevado, Sixto, García-Miñaúr, María, Palomares-Bralo, Elena, Vallespín, Encarna, Guillén-Navarro, Jordi, Rosell, Cristina, Bel-Fenellós, María Ángeles, Mori, Montserrat, Milá, Miguel, Del Campo, Pilar, Barrúz, Fernando, Santos-Simarro, Gabriela, Obregón, Carmen, Orellana, Harry, Pachajoa, Jair Antonio, Tenorio, Enrique, Galán, Juan C, Cigudosa, Angélica, Moresco, César, Saleme, Silvia, Castillo, Elisabeth, Gabau, Luis, Pérez-Jurado, Ana, Barcia, Maria Soledad, Martín, Elena, Mansilla, Isabel, Vallcorba, Pedro, García-Murillo, Franco, Cammarata-Scalisi, Natálya, Gonçalves Pereira, Raquel, Blanco-Lago, Mercedes, Serrano, Juan Dario, Ortigoza-Escobar, Blanca, Gener, Verónica Adriana, Seidel, Pilar, Tirado, Pablo, Lapunzina, Rodríguez-Revenga, Laia, Institut Català de la Salut, [Nevado J, García-Miñaúr S, Palomares-Bralo M, Vallespín E] Instituto de Genética Médica y Molecular (INGEMM)-IdiPAZ, Hospital Universitario La Paz, Madrid, Spain. CIBERER, Centro de Investigación Biomédica en Red de Enfermedades Raras, ISCIII, Madrid, Spain. ITHACA-European Reference Network, Hospital La Paz, Madrid, Spain. [Guillén-Navarro E] Hospital Virgen de la Arrixaca, Murcia, Spain. [Rosell J] Hospital Son Espases, Palma de Mallorca, Spain. [del Campo M] Vall d’Hebron Hospital Universitari, Barcelona, Spain, Vall d'Hebron Barcelona Hospital Campus, and FIBHULP Auchan Reserch Project

Subjects
Identification, Rearrangements, intellectual disabilities (ID), 22q13.3 deletion syndrome, Subtelomeric deletion syndrome, Microarray, Genetic Phenomena::Genetic Variation::Polymorphism, Genetic::Genomic Structural Variation::DNA Copy Number Variations [PHENOMENA AND PROCESSES], subtelomeric deletion syndrome, Autistic behavior, Association, Clinical characterization, Shank3 gene, Spectrum, Genetics, Other subheadings::Other subheadings::/genetics [Other subheadings], SHANK3, Genetics (clinical), enfermedades y anomalías neonatales congénitas y hereditarias::anomalías congénitas::trastornos cromosómicos [ENFERMEDADES], fenómenos genéticos::variación genética::polimorfismo genético::variación estructural genómica::variaciones del número de copias de ADN [FENÓMENOS Y PROCESOS], autistic behavior, Otros calificadores::Otros calificadores::/genética [Otros calificadores], Polimorfisme genètic, Congenital, Hereditary, and Neonatal Diseases and Abnormalities::Congenital Abnormalities::Chromosome Disorders [DISEASES], trastornos mentales::trastornos del desarrollo neurológico [PSIQUIATRÍA Y PSICOLOGÍA], Cromosomes humans - Anomalies, Phelan-McDermid syndrome (PMS), Molecular characterization, 22q13 deletion syndrome, Intellectual disabilities (ID), Molecular Medicine, Malalties congènites, Abnormalities, Mental Disorders::Neurodevelopmental Disorders [PSYCHIATRY AND PSYCHOLOGY]
Abstract

Phelan-McDermid syndrome; Intellectual disabilities; Subtelomeric deletion syndrome Síndrome de Phelan-McDermid; Discapacidades intelectuales; Síndrome de deleción subtelomérica Síndrome de Phelan-McDermid; Discapacitats intel·lectuals; Síndrome de deleció subtelomèrica Phelan-McDermid syndrome (PMS, OMIM# 606232) results from either different rearrangements at the distal region of the long arm of chromosome 22 (22q13.3) or pathogenic sequence variants in the SHANK3 gene. SHANK3 codes for a structural protein that plays a central role in the formation of the postsynaptic terminals and the maintenance of synaptic structures. Clinically, patients with PMS often present with global developmental delay, absent or severely delayed speech, neonatal hypotonia, minor dysmorphic features, and autism spectrum disorders (ASD), among other findings. Here, we describe a cohort of 210 patients with genetically confirmed PMS. We observed multiple variant types, including a significant number of small deletions (

Published
2022

37. Clinical features and health-related quality of life in adult patients with mucopolysaccharidosis IVA: the Spanish experience

Author

Elena Arranz Canales, Elisenda Cortès-Saladelafont, Elena Martín-Hernández, Ricardo Gil Sánchez, Guillem Pintos-Morell, Javier Blasco-Alonso, Mónica A. López Rodríguez, David Moreno-Martinez, Encarna Guillén-Navarro, María Juliana Ballesta-Martínez, María Teresa García-Silva, María L. Couce, Pilar Quijada-Fraile, Montserrat Morales Conejo, Salvador García Morillo, Marc Moltó-Abad, Institut Català de la Salut, [Quijada-Fraile P, Martín-Hernández E] Unidad de Enfermedades Mitocondriales y Enfermedades Metabólicas Hereditarias, Servicio de Pediatría, Hospital Universitario 12 de Octubre, CSUR Enfermedades Metabólicas, MetabERN, Instituto de Investigación Sanitaria Hospital 12 de octubre (imas12), CIBERER, Madrid, Spain. [Arranz Canales E] Servicio de Medicina Interna, CSUR Enfermedades Metabólicas, MetabERN, Instituto de Investigación Sanitaria Hospital 12 de octubre (imas12), Hospital Universitario 12 de Octubre, Madrid, Spain. [Ballesta-Martínez MJ, Guillén-Navarro E] Sección de Genética Médica, Hospital Clínico Universitario Virgen de la Arrixaca, IMIB Arrixaca, Universidad de Murcia, Murcia, Spain. CIBERER-ISCIII, Madrid, Spain. [Pintos-Morell G, Moltó-Abad M] Divisió de Malalties Minoritàries, Centre de Referència de Trastorns Metabòlics Hereditaris, Vall d’Hebron Hospital Universitari, Barcelona, Spain. [Moreno-Martínez D] Divisió de Malalties Minoritàries, Centre de Referència de Trastorns Metabòlics Hereditaris, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Lysosomal Storage Disorders Unit, The Royal Free Hospital NHS Foundation Trust and University College London, London, UK, and Vall d'Hebron Barcelona Hospital Campus

Subjects
Adult, Ligamentous laxity, medicine.medical_specialty, Health-related quality of life, Mucopolysaccharidosis, Otros calificadores::Otros calificadores::/farmacoterapia [Otros calificadores], Other subheadings::Other subheadings::/drug therapy [Other subheadings], Hip dysplasia (canine), Young Adult, chemistry.chemical_compound, Elosulfase alfa, Quality of life, Interquartile range, Internal medicine, medicine, Hip Dislocation, Humans, Enzyme Replacement Therapy, Pharmacology (medical), Malalties rares - Tractament, Mucopolysaccharidosis IVA, Elosulfase alfa, Health-related quality of life, Mobility, Morquio A syndrome, Mucopolysaccharidosis IVA, terapéutica::farmacoterapia::terapia enzimática::tratamiento de sustitución enzimática [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Genetics (clinical), ambiente y salud pública::salud pública::medidas epidemiológicas::demografía::estado de salud::calidad de vida [ATENCIÓN DE SALUD], Mobility, business.industry, Research, Enzims - Ús terapèutic, Mucopolysaccharidosis IV, General Medicine, Enzyme replacement therapy, medicine.disease, Self Care, Environment and Public Health::Public Health::Epidemiologic Measurements::Demography::Health Status::Quality of Life [HEALTH CARE], Metabolisme, Errors congènits del - Tractament, enfermedades nutricionales y metabólicas::enfermedades metabólicas::alteraciones congénitas del metabolismo::trastornos congénitos del metabolismo de los carbohidratos::mucopolisacaridosis::enfermedades nutricionales y metabólicas::enfermedades metabólicas::alteraciones congénitas del metabolismo::mucopolisacaridosis IV [ENFERMEDADES], chemistry, Dysplasia, Quality of Life, Medicine, Nutritional and Metabolic Diseases::Metabolic Diseases::Metabolism, Inborn Errors::Carbohydrate Metabolism, Inborn Errors::Mucopolysaccharidoses::Nutritional and Metabolic Diseases::Metabolic Diseases::Metabolism, Inborn Errors::Mucopolysaccharidosis IV [DISEASES], sense organs, business, Morquio A syndrome, Therapeutics::Drug Therapy::Enzyme Therapy::Enzyme Replacement Therapy [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT]
Abstract

Background Mucopolysaccharidosis (MPS) IVA or Morquio A syndrome is a progressive and disabling disease characterized by a deficiency of the enzyme N-acetylgalactosamine-6-sulphate sulphatase. Its clinical presentation is very heterogeneous and poorly understood in adults. The aim of this study was to describe the clinical manifestations of MPS IVA in adult patients in Spain and to assess their health-related quality of life (HRQoL). Results Thirty-three patients from nine reference centres participated in the study. The median age was 32 (interquartile range [IQR]: 20.5–40.5) years. The phenotype was classical in 54.5% of patients, intermediate in 33.3% of patients, and non-classical in 12.1% of patients. The most common clinical manifestation was bone dysplasia, with a median height of 118 (IQR: 106–136) cm. Other frequent clinical manifestations were hearing loss (75.7%), ligamentous laxity (72.7%), odontoid dysplasia (69.7%), limb deformities that required orthopaedic aids (mainly hip dysplasia and genu valgus) (63.6%), and corneal clouding (60.6%). In addition, 36.0% of patients had obstructive sleep apnoea/hypopnoea syndrome and 33.3% needed non-invasive ventilation. Cervical surgery and varisation osteotomy were the most common surgical interventions (36.4% each). Almost 80% of patients had mobility problems and 36.4% used a wheelchair at all times. Furthermore, 87.9% needed help with self-care, 33.3% were fully dependent, and 78.8% had some degree of pain. HRQoL according to the health assessment questionnaire was 1.43 (IQR: 1.03–2.00) in patients with the non-classical phenotype, but 2.5 (IQR: 1.68–3.00) in those with the classical phenotype. Seven patients were initiated on enzyme replacement therapy (ERT), but two of them were lost to follow-up. Lung function improved in four patients and slightly worsened in one patient. The distance achieved in the six-minute walk test increased in the four patients who could perform it. HRQoL was better in patients treated with elosulfase alfa, with a median (IQR) of 1.75 (1.25–2.34) versus 2.25 (1.62–3.00) in patients not treated with ERT. Conclusions The study provides real-world data on patients with MPS IVA. Limited mobility, difficulties with self-care, dependence, and pain were common, together with poor HRQoL. The severity and heterogeneity of clinical manifestations require the combined efforts of multidisciplinary teams.

Published
2021

38. Identification of copy-number variants in patients with overgrowth disorders.

Author

Parra A, Tenorio-Castano J, Nevado J, Cazalla M, Miranda-Alcaraz L, Gallego-Zazo N, Silván C, Arias P, Pozo-Román J, Ballesta-Martínez MJ, Guillén-Navarro E, Arroyo I, Lotersztein V, Cosentino V, González-Meneses A, Galán E, Rosell J, Ramos F, and Lapunzina P

Subjects
Humans, Female, Male, Whole Genome Sequencing, Child, Adolescent, Child, Preschool, Genetic Predisposition to Disease, Chromosomes, Human, Pair 15 genetics, DNA Copy Number Variations genetics, Growth Disorders genetics, Growth Disorders pathology, Polymorphism, Single Nucleotide genetics
Abstract

Overgrowth syndromes (OGS) comprise a heterogeneous group of disorders whose main characteristic is that the weight, height or the head circumference are above the 97th centile or 2-3 standard deviations above the mean for age, gender, and ethnic group. Several copy-number variants (CNVs) have been associated with the development of OGS, such as the 5q35 microdeletion or the duplication of the 15q26.1-qter, among many others. In this study, we have applied 850K SNP-arrays to 112 patients and relatives with OGS from the Spanish OverGrowth Registry Initiative. We have identified CNVs associated with the disorder in nine individuals (8%). Subsequently, whole genome sequencing (WGS) analysis was performed in these nine samples in order to better understand these genomic imbalances. All the CNVs were detected by both techniques, settling that WGS is a useful tool for CNV detection. We have found six patients with genomic abnormalities associated with previously well-established disorders and three patients with CNVs of unknown significance, which may be related to OGS, based on scientific literature. In this report, we describe these findings and comment on genes associated with OGS that are located within the CNV regions., (© 2024 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2024
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39. European Achondroplasia Forum Practical Considerations for Following Adults with Achondroplasia.

Author

Fredwall S, AlSayed M, Ben-Omran T, Boero S, Cormier-Daire V, Fauroux B, Guillén-Navarro E, Innig F, Kunkel P, Lampe C, Maghnie M, Mohnike K, Mortier G, Pejin Z, Sessa M, Sousa SB, and Irving M

Subjects
Humans, Adult, Checklist, Spinal Stenosis therapy, Spinal Stenosis complications, Europe, Transition to Adult Care, Sleep Apnea, Obstructive therapy, Achondroplasia complications, Achondroplasia therapy
Abstract

Achondroplasia is a lifelong condition requiring lifelong management. There is consensus that infants and children with achondroplasia should be managed by a multidisciplinary team experienced in the condition. However, many people are lost to follow-up after the transition from paediatric to adult care, and there is no standardised approach for management in adults, despite the recent availability of international consensus guidelines. To address this, the European Achondroplasia Forum has developed a patient-held checklist to support adults with achondroplasia in managing their health. The checklist highlights key symptoms of spinal stenosis and obstructive sleep apnoea, both among the most frequent and potentially severe medical complications in adults with achondroplasia. The checklist acts as a framework to support individuals and their primary care provider in completing a routine review. General advice on issues such as blood pressure, pain, hearing, weight, adaptive aids, and psychosocial aspects are also included. The checklist provides key symptoms to be aware of, in addition to action points so that people can approach their primary care provider and be directed to the appropriate specialist, if needed. Additionally, the European Achondroplasia Forum offers some ideas on implementing the checklist during the transition from paediatric to adult care, thus ensuring the existing multidisciplinary team model in place during childhood can support in engaging individuals and empowering them to take responsibility for their own care as they move into adulthood., (© 2024. The Author(s).)

Published
2024
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40. HELIX Syndrome, a Claudinopathy with Relevant Dermatological Manifestations: Report of Two New Cases.

Author

Martínez-Romero MC, Hernández-Contreras ME, Bafalliu-Vidal JA, Barreda-Sánchez M, Martínez-Menchón T, Cabello-Chaves V, and Guillén-Navarro E

Subjects
Humans, Male, Adult, Ichthyosis genetics, Ichthyosis pathology, Hypohidrosis genetics, Ectodermal Dysplasia genetics, Ectodermal Dysplasia pathology, Pedigree, Phenotype, Claudins genetics
Abstract

HELIX syndrome (Hypohidrosis-Electrolyte disturbances-hypoLacrimia-Ichthyosis-Xerostomia) (MIM#617671) (ORPHA:528105), described in 2017, is due to an abnormal claudin 10 b protein, secondary to pathogenic CLDN10 variants. So far, only ten families have been described. We aim to describe the phenotype in the first Spanish family identified, highlight the skin anomalies as an important clue, and expand the genotypic spectrum. Two adult brothers from consanguineous parents with suspected ectodermal dysplasia (ED) since early childhood were re-evaluated. A comprehensive phenotypic exam and an aCGH + SNP4 × 180 K microarray followed by Sanger sequencing of the CLDN10 gene were performed. They presented hypohidrosis, xerosis, mild ichthyosis, plantar keratosis, palm hyperlinearity, alacrima, and xerostomia. In adulthood, they also developed a salt-losing nephropathy with hypokalemia and hypermagnesemia. The molecular study in both patients revealed a novel pathogenic homozygous deletion of 8 nucleotides in exon 2 of the CLDN10 gene [ CLDN10 (NM&#95;0006984.4): c.322&#95;329delGGCTCCGA, p.Gly108fs*] leading to a premature truncation of the protein. Both parents were heterozygous carriers. Hypohidrosis, ichthyosis, and plantar keratosis associated with alacrima and xerostomia should raise suspicion for HELIX syndrome, which also includes nephropathy and electrolyte disturbances in adults. Given the potential for ED misdiagnosis in infancy, it is important to include the CLDN10 gene in a specific genodermatosis next-generation sequencing (NGS) panel to provide early diagnosis, accurate management, and genetic counseling.

Published
2024
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41. The burden of disease and quality of life in patients with acute hepatic porphyria: COPHASE study.

Author

Castelbón Fernández FJ, Barreda Sánchez M, Arranz Canales E, Hernández Contreras ME, Solares I, Morales Conejo M, Muñoz Cuadrado Á, Casado Gómez A, Yébenes Cortés M, and Guillén Navarro E

Subjects
Humans, Female, Adult, Middle Aged, Male, Depression etiology, Cost of Illness, Pain etiology, Quality of Life, Porphyrias, Hepatic
Abstract

Background: Acute hepatic porphyria (AHP) comprises a group of rare genetic diseases characterized by neurovisceral crises that are manifested by abdominal pain and neurological and/or psychological symptoms that interfere with the ability to lead a normal life. Our objective was to determine the burden of the disease in one year and the health-related quality of life (HRQoL) in patients with AHP., Results: 28 patients were analyzed. The mean age was 36.6±10.2 years, 89.3% were women, and the average number of crises was 1.9±1.5. The average annual cost per patient was €38,255.40. 80.2% of the costs was direct medical costs, 17.5% was associated with loss of productivity and 2.3% was direct non-medical costs. 85.9% of the total cost corresponded to the crises. The intercrisis period accounted for the remaining 14.1%. The global index of the EQ-5D-5L (HRQoL) was 0.75±0.24. The dimensions of pain/discomfort, anxiety/depression and daily activities were the most affected. Leisure, travel/vacations and household activities were the most affected daily activities. 53.6% of patients required a caregiver due to AHP. 92.9% did not present overload and 7.1% presented extreme overload., Conclusions: Patients with AHP are associated with a high economic impact and an affected HRQoL in the pain/discomfort dimension, with a negative impact on the performance of daily activities and a risk of psychiatric diseases., (Copyright © 2023 Elsevier España, S.L.U. All rights reserved.)

Published
2024
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42. Multidisciplinary management improves the genetic diagnosis of hereditary kidney diseases in the next generation sequencing (NGS) era.

Author

Galán Carrillo I, Galbis Martínez L, Martínez V, Roca Meroño S, Ramos F, González Rodríguez JD, Piñero Fernández J, and Guillén Navarro E

Subjects
Humans, Female, High-Throughput Nucleotide Sequencing, Mutation, Kidney pathology, Hematuria, Nephritis, Hereditary diagnosis, Nephritis, Hereditary genetics, Nephritis, Hereditary pathology
Abstract

Background and Objective: Hereditary kidney diseases (HKD) are a frequent cause of chronic kidney disease, and their diagnosis has increased since the introduction of next generation sequencing (NGS). In 2018, the Multidisciplinary Unit for Hereditary Kidney Diseases of the Region of Murcia (UMERH-RM) was founded based on the genetic study of HKD. The objective of this study is to analyze the results obtained in the first 3 years of operation, and to analyze the clinical factors associated to a final genetic diagnosis., Materials and Methods: All the patients studied with the HKD gene panel were included. The characteristics between those who obtained a final genetic diagnosis and those who did not were compared., Results: A total of 360 patients were studied, detecting genetic variants in 164 not related patients (45.6%). 45 of these were variants of uncertain significance requiring a family co-segregation study, which was facilitated by the multidisciplinary unit. Overall, considering the results obtained with the NGS panel and the extended genomic studies, a final diagnostic yield of HRD of 33.3% (120/360) was achieved, and including incidental findings 35.6% (128/360). Two hundred and twenty-three patients with suspected Alport syndrome were studied. Diagnosis was confirmed in 28.5% (COL4A4 most frequent gene), more frequently women with an obvious compatible family history. They also had frequently microhematuria, although 5 patients without microhematuria confirmed the diagnosis. There were no differences in age, proteinuria, renal function, hearing loss, or ophthalmologic abnormalities. The most frequent finding in the renal biopsy was mesangial proliferation. We estimate that 39 patients avoided renal biopsy. A total of 101 patients with suspected PKD were also studied, 49.5% had a conclusive genetic result (most frequent gene PKD1), more frequently women, with larger kidney sizes (although 9 patients with normal kidney size confirmed diagnosis). Again, the most predictive characteristic of genetic outcome was family history., Conclusions: The implementation of an NGS panel for HKD, together with the multidisciplinary approach to cases, has improved the diagnostic performance of HKD. In our sample, autosomal dominant Alport syndrome is of highest incidence. Ophthalmological and auditory examinations did not contribute to the diagnosis. We have seen a significant decrease in the indication of renal biopsies thanks to molecular diagnosis. The multidisciplinary approach, with the active participation of nephrologists, paediatricians, clinical and molecular geneticists, with insistence on adequate patient phenotyping and review of their family history, offers a better interpretation of genetic variants, allowing reclassification of the diagnosis of some nephropathies, thus improving their management and genetic advice., (Copyright © 2024. Published by Elsevier España, S.L.U.)

Published
2024
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43. Efficacy and safety of givosiran for acute hepatic porphyria: Final results of the randomized phase III ENVISION trial.

Author

Kuter DJ, Bonkovsky HL, Monroy S, Ross G, Guillén-Navarro E, Cappellini MD, Minder AE, Hother-Nielsen O, Ventura P, Jia G, Sweetser MT, and Thapar M

Abstract

Background & Aims: Acute hepatic porphyria (AHP) is caused by defects in hepatic heme biosynthesis, leading to disabling acute neurovisceral attacks and chronic symptoms. In ENVISION (NCT03338816), givosiran treatment for 6 months reduced attacks and other disease manifestations compared with placebo. Herein, we report data from the 36-month final analysis of ENVISION., Methods: Ninety-four patients with AHP (age ≥12 years) and recurrent attacks were randomized 1:1 to monthly double-blind subcutaneous givosiran 2.5 mg/kg (n = 48) or placebo (n = 46) for 6 months. In the open-label extension (OLE) period, 93 patients received givosiran 2.5 or 1.25 mg/kg for 6 months or more before transitioning to 2.5 mg/kg. Endpoints were exploratory unless otherwise noted., Results: During givosiran treatment, the median annualized attack rate (AAR) was 0.4. Through Month 36, annualized days of hemin use remained low in the continuous givosiran group (median, 0.0 to 0.4) and decreased in the placebo crossover group (16.2 to 0.4). At end of OLE, in the continuous givosiran and placebo crossover groups, 86% and 92%, respectively, had 0 attacks. AAR was lower than historical AAR in 98% and 100%, respectively (post hoc analysis), and there were 0 days of hemin use in 88% and 90%, respectively. The 12-item short-form health survey physical and mental component summary scores increased by 8.6 and 8.1, respectively (continuous givosiran) and 9.4 and 3.2, respectively (placebo crossover). EQ-5D health-related questionnaire scores increased by 18.9 (continuous givosiran) and 9.9 (placebo crossover). Lower urinary delta-aminolevulinic acid and porphobilinogen levels were sustained. Safety findings demonstrated a continued positive risk/benefit profile for givosiran., Conclusions: Long-term monthly givosiran treatment provides sustained and continued improvement in clinical manifestations of AHP., Gov Identifier: NCT03338816., Eudract Number: 2017-002432-17., Impact and Implications: Acute hepatic porphyria (AHP) is a group of rare, chronic, multisystem disorders associated with overproduction and accumulation of neurotoxic heme intermediates (delta-aminolevulinic acid and porphobilinogen), sometimes resulting in recurrent acute attacks and long-term complications. Givosiran, a small-interfering RNA that prevents accumulation of delta-aminolevulinic acid and porphobilinogen, is approved for the treatment of AHP. These final 36-month results of ENVISION, a phase III study of givosiran in patients with AHP and recurrent attacks, show that long-term monthly treatment with givosiran leads to continuous and sustained reductions in annualized attack rate and use of hemin over time, as well as improved quality of life, with an acceptable safety profile. These results are important for physicians, patients, families, and caregivers who are grappling with this debilitating and potentially life-threatening disease with few effective and tolerable treatment options., (Copyright © 2023 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published
2023
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46. Genotypic Findings in Noonan and Non-Noonan RASopathies and Patient Eligibility for Growth Hormone Treatment.

Author

Carcavilla A, Cambra A, Santomé JL, Seidel V, Cruz J, Alonso M, Pozo J, Valenzuela I, Guillén-Navarro E, Santos-Simarro F, González-Casado I, Rodríguez A, Medrano C, López-Siguero JP, and Ezquieta B

Abstract

Molecular study has become an invaluable tool in the field of RASopathies. Treatment with recombinant human growth hormone is approved in Noonan syndrome but not in the other RASopathies. The aim of this study was to learn about the molecular base of a large cohort of patients with RASopathies, with particular emphasis on patients with pathogenic variants in genes other than PTPN11 , and its potential impact on rGH treatment indication. We reviewed the clinical diagnosis and molecular findings in 451 patients with a genetically confirmed RASopathy. HRAS alterations were detected in only 2 out of 19 patients referred with a Costello syndrome suspicion, whereas pathogenic variants in RAF1 and SHOC2 were detected in 3 and 2, respectively. In 22 patients referred with a generic suspicion of RASopathy, including cardiofaciocutaneous syndrome, pathogenic alterations in classic Noonan syndrome genes ( PTPN11 , SOS1 , RAF1 , LZTR1, and RIT1 ) were found in 7 patients and pathogenic variants in genes associated with other RASopathies ( HRAS , SHOC2, and PPPCB1) in 4. The correct nosological classification of patients with RASopathies is critical to decide whether they are candidates for treatment with rhGH. Our data illustrate the complexity of differential diagnosis in RASopathies, as well as the importance of genetic testing to guide the diagnostic orientation in these patients.

Published
2023
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47. Validation of clinical exome sequencing in the diagnostic procedure of patients with intellectual disability in clinical practice.

Author

Ballesta-Martínez MJ, Pérez-Fernández V, López-González V, Sánchez-Soler MJ, Serrano-Antón AT, Rodríguez-Peña LI, Barreda-Sánchez M, Armengol-Dulcet L, and Guillén-Navarro E

Subjects
Humans, Exome Sequencing, Exome genetics, High-Throughput Nucleotide Sequencing, Intellectual Disability diagnosis, Intellectual Disability genetics
Abstract

Intellectual disability (ID) has a prevalence of 1-3% and aproximately 30-50% of ID cases have a genetic cause. Development of next-generation sequencing has shown a high diagnostic potential. The aim of this work was to evaluate the diagnostic yield of clinical exome sequencing in 188 ID patients and the economic impact of its introduction in clinical practice. An analysis of diagnostic yield according to the different clinical variables was performed in order to establish an efficient diagnostic protocol for ID patients. Diagnostic yield of clinical exome sequencing was significant (34%) supporting its utility in diagnosis of ID patients. Wide genetic heterogeneity and predominance of autosomal dominant de novo variants in ID patients were observed. Time to diagnosis was shortened and diagnostic study costs decreased by 62% after implementation of clinical exome sequencing. No association was found between any of the variables analyzed and a higher diagnostic yield; added to the fact that many of the diagnoses weren't clinically detectable, the reduction of time to diagnosis and the economic savings with respect to classical diagnostic studies, strengthen the clinical and economical convenience of early implementation of clinical exome sequencing in the diagnostic workup of ID patients in clinical practice., (© 2023. The Author(s).)

Published
2023
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48. Real-world evidence in achondroplasia: considerations for a standardized data set.

Author

Alanay Y, Mohnike K, Nilsson O, Alves I, AlSayed M, Appelman-Dijkstra NM, Baujat G, Ben-Omran T, Breyer S, Cormier-Daire V, Gregersen PA, Guillén-Navarro E, Högler W, Maghnie M, Mukherjee S, Cohen S, Pimenta J, Selicorni A, Semler JO, Sigaudy S, Popkov D, Sabir I, Noval S, Sessa M, and Irving M

Subjects
Humans, Europe, Registries, Quality of Life, Achondroplasia epidemiology
Abstract

Background: Collection of real-world evidence (RWE) is important in achondroplasia. Development of a prospective, shared, international resource that follows the principles of findability, accessibility, interoperability, and reuse of digital assets, and that captures long-term, high-quality data, would improve understanding of the natural history of achondroplasia, quality of life, and related outcomes., Methods: The Europe, Middle East, and Africa (EMEA) Achondroplasia Steering Committee comprises a multidisciplinary team of 17 clinical experts and 3 advocacy organization representatives. The committee undertook an exercise to identify essential data elements for a standardized prospective registry to study the natural history of achondroplasia and related outcomes., Results: A range of RWE on achondroplasia is being collected at EMEA centres. Whereas commonalities exist, the data elements, methods used to collect and store them, and frequency of collection vary. The topics considered most important for collection were auxological measures, sleep studies, quality of life, and neurological manifestations. Data considered essential for a prospective registry were grouped into six categories: demographics; diagnosis and patient measurements; medical issues; investigations and surgical events; medications; and outcomes possibly associated with achondroplasia treatments., Conclusions: Long-term, high-quality data are needed for this rare, multifaceted condition. Establishing registries that collect predefined data elements across age spans will provide contemporaneous prospective and longitudinal information and will be useful to improve clinical decision-making and management. It should be feasible to collect a minimum dataset with the flexibility to include country-specific criteria and pool data across countries to examine clinical outcomes associated with achondroplasia and different therapeutic approaches., (© 2023. The Author(s).)

Published
2023
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49. Clinical Heterogeneity and Different Phenotypes in Patients with SETD2 Variants: 18 New Patients and Review of the Literature.

Author

Parra A, Rabin R, Pappas J, Pascual P, Cazalla M, Arias P, Gallego-Zazo N, Santana A, Arroyo I, Artigas M, Pachajoa H, Alanay Y, Akgun-Dogan O, Ruaud L, Couque N, Levy J, Porras-Hurtado GL, Santos-Simarro F, Ballesta-Martinez MJ, Guillén-Navarro E, Muñoz-Hernández H, Nevado J, Spanish OverGrowth Registry Initiative, Tenorio-Castano J, and Lapunzina P

Subjects
Humans, Muscle Hypotonia genetics, Phenotype, Syndrome, Autism Spectrum Disorder genetics, Intellectual Disability genetics
Abstract

SETD2 belongs to the family of histone methyltransferase proteins and has been associated with three nosologically distinct entities with different clinical and molecular features: Luscan-Lumish syndrome (LLS), intellectual developmental disorder, autosomal dominant 70 (MRD70), and Rabin-Pappas syndrome (RAPAS). LLS [MIM #616831] is an overgrowth disorder with multisystem involvement including intellectual disability, speech delay, autism spectrum disorder (ASD), macrocephaly, tall stature, and motor delay. RAPAS [MIM #6201551] is a recently reported multisystemic disorder characterized by severely impaired global and intellectual development, hypotonia, feeding difficulties with failure to thrive, microcephaly, and dysmorphic facial features. Other neurologic findings may include seizures, hearing loss, ophthalmologic defects, and brain imaging abnormalities. There is variable involvement of other organ systems, including skeletal, genitourinary, cardiac, and potentially endocrine. Three patients who carried the missense variant p.Arg1740Gln in SETD2 were reported with a moderately impaired intellectual disability, speech difficulties, and behavioral abnormalities. More variable findings included hypotonia and dysmorphic features. Due to the differences with the two previous phenotypes, this association was then named intellectual developmental disorder, autosomal dominant 70 [MIM 620157]. These three disorders seem to be allelic and are caused either by loss-of-function, gain-of-function, or missense variants in the SETD2 gene. Here we describe 18 new patients with variants in SETD2 , most of them with the LLS phenotype, and reviewed 33 additional patients with variants in SETD2 that have been previously reported in the scientific literature. This article offers an expansion of the number of reported individuals with LLS and highlights the clinical features and the similarities and differences among the three phenotypes associated with SETD2 .

Published
2023
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