Your search keyword '"Díaz-López, Everardo Josué"' showing total 11 results

1. A murine model of BSCL2-associated Celia's encephalopathy

Author

Cobelo-Gómez, Silvia, Sánchez-Iglesias, Sofía, Rábano, Alberto, Senra, Ana, Aguiar, Pablo, Gómez-Lado, Noemí, García-Varela, Lara, Burgueño-García, Iván, Lampón-Fernández, Laura, Fernández-Pombo, Antía, Díaz-López, Everardo Josué, Prado-Moraña, Teresa, San Millán, Beatriz, and Araújo-Vilar, David

Published

2023

2. A cohort analysis of familial partial lipodystrophy from two Mediterranean countries.

Author

Fernández‐Pombo, Antía, Yildirim Simsir, Ilgin, Sánchez‐Iglesias, Sofía, Ozen, Samim, Castro, Ana I., Atik, Tahir, Loidi, Lourdes, Onay, Huseyin, Prado‐Moraña, Teresa, Adiyaman, Cem, Díaz‐López, Everardo Josué, Altay, Canan, Ginzo‐Villamayor, Maria José, Akinci, Baris, and Araújo‐Vilar, David

Subjects

TURKS, CORONARY artery disease, METABOLIC disorders, MYOCARDIAL infarction, SYMPTOMS

Abstract

Aim: To assess the disease burden of familial partial lipodystrophy (FPLD) caused by LMNA (FPLD2) and PPARG (FPLD3) variants to augment the knowledge of these rare disorders characterized by selective fat loss and metabolic complications. Materials and Methods: An observational longitudinal study, including 157 patients (FPLD2: 139 patients, mean age 46 ± 17 years, 70% women; FPLD3: 18 patients, mean age: 44 ± 17 years, 78% women) from 66 independent families in two countries (83 from Turkey and 74 from Spain), was conducted. Results: Patients were diagnosed at a mean age of 39 ± 19 years, 20 ± 16 years after the first clinical signs appeared. Men reported symptoms later than women. Symptom onset was earlier in FPLD2. Fat loss was less prominent in FPLD3. In total, 92 subjects (59%) had diabetes (age at diagnosis: 34 ± 1 years). Retinopathy was more commonly detected in FPLD3 (P <.05). Severe hypertriglyceridaemia was more frequent among patients with FPLD3 (44% vs. 17%, P =.01). Hepatic steatosis was detected in 100 subjects (66%) (age at diagnosis: 36 ± 2 years). Coronary artery disease developed in 26 patients (17%) and 17 (11%) suffered from a myocardial infarction. Turkish patients had a lower body mass index, a higher prevalence of hepatic steatosis, greater triglyceride levels and a tendency towards a higher prevalence of coronary artery disease. A total of 17 patients died, with a mean time to death of 75 ± 3 years, which was shorter in the Turkish cohort (68 ± 2 vs. 83 ± 4 years, P =.01). Cardiovascular events were a major cause of death. Conclusions: Our analysis highlights severe organ complications in patients with FPLD, showing differences between genotypes and Mediterranean countries. FPLD3 presents a milder phenotype than FPLD2, but with comparable or even greater severity of metabolic disturbances. [ABSTRACT FROM AUTHOR]

Published

2024

3. Lipodystrophic Laminopathies: From Dunnigan Disease to Progeroid Syndromes.

Author

Díaz-López, Everardo Josué, Sánchez-Iglesias, Sofía, Castro, Ana I., Cobelo-Gómez, Silvia, Prado-Moraña, Teresa, Araújo-Vilar, David, and Fernandez-Pombo, Antia

Subjects

*PROGERIA, *ADIPOSE tissues, *PREMATURE aging (Medicine), *LIPODYSTROPHY, *GENETIC variation, *DYSPLASIA

Abstract

Lipodystrophic laminopathies are a group of ultra-rare disorders characterised by the presence of pathogenic variants in the same gene (LMNA) and other related genes, along with an impaired adipose tissue pattern and other features that are specific of each of these disorders. The most fascinating traits include their complex genotype-phenotype associations and clinical heterogeneity, ranging from Dunnigan disease, in which the most relevant feature is precisely adipose tissue dysfunction and lipodystrophy, to the other laminopathies affecting adipose tissue, which are also characterised by the presence of signs of premature ageing (Hutchinson Gilford-progeria syndrome, LMNA-atypical progeroid syndrome, mandibuloacral dysplasia types A and B, Nestor-Guillermo progeria syndrome, LMNA-associated cardiocutaneous progeria). This raises several questions when it comes to understanding how variants in the same gene can lead to similar adipose tissue disturbances and, at the same time, to such heterogeneous phenotypes and variable degrees of metabolic abnormalities. The present review aims to gather the molecular basis of adipose tissue impairment in lipodystrophic laminopathies, their main clinical aspects and recent therapeutic strategies. In addition, it also summarises the key aspects for their differential diagnosis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Natural history and comorbidities of generalised and partial lipodystrophy syndromes in Spain

Author

Fernández-Pombo, Antía, primary, Sánchez-Iglesias, Sofía, additional, Castro-Pais, Ana I., additional, Ginzo-Villamayor, Maria José, additional, Cobelo-Gómez, Silvia, additional, Prado-Moraña, Teresa, additional, Díaz-López, Everardo Josué, additional, Casanueva, Felipe F., additional, Loidi, Lourdes, additional, and Araújo-Vilar, David, additional

Published

2023

5. Should we suspect primary aldosteronism in patients with hypokalaemic rhabdomyolysis? A systematic review

Author

Díaz-López, Everardo Josué, primary, Villar-Taibo, Rocio, additional, Rodriguez-Carnero, Gemma, additional, Fernandez-Pombo, Antia, additional, Garcia-Peino, Roberto, additional, Blanco-Freire, Manuel Narciso, additional, Pena-Dubra, Alberto, additional, Prado-Moraña, Teresa, additional, Fernández-Xove, Irea-, additional, Pérez-Béliz, Edurne, additional, Cameselle-Teijeiro, Jose Manuel, additional, Hermida-Ameijeiras, Alvaro, additional, and Martinez-Olmos, Miguel Angel, additional

Published

2023

6. A murine model of BSCL2-associated Celia's encephalopathy

Author

Universidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicas, Rabano, Alberto, Burgueño-García, Iván, Lampón-Fernández, Laura, Díaz-López, Everardo Josué, Prado-Moraña, Teresa, San Millán, Beatriz, Cobelo Gómez, Silvia, Sánchez Iglesias, Sofía, Senra, Ana, Aguiar, Pablo, Gómez Lado, Noemí, García Varela, Lara, Fernández-Pombo, Antía, Araújo-Vilar, David, Universidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicas, Rabano, Alberto, Burgueño-García, Iván, Lampón-Fernández, Laura, Díaz-López, Everardo Josué, Prado-Moraña, Teresa, San Millán, Beatriz, Cobelo Gómez, Silvia, Sánchez Iglesias, Sofía, Senra, Ana, Aguiar, Pablo, Gómez Lado, Noemí, García Varela, Lara, Fernández-Pombo, Antía, and Araújo-Vilar, David

Abstract

Celia's encephalopathy or progressive encephalopathy with/without lipodystrophy is a neurodegenerative disease with a fatal prognosis in childhood. It is generally caused by the c.985C > T variant in the BSCL2 gene, leading to the skipping of exon 7 and resulting in an aberrant seipin protein (Celia-seipin). To precisely define the temporal evolution and the mechanisms involved in neurodegeneration, lipodystrophy and fatty liver in Celia's encephalopathy, our group has generated the first global knock-in murine model for the aberrant human transcript of BSCL2 (Bscl2Celia/Celia) using a strategy based on the Cre/loxP recombination system. In order to carry out a characterization at the neurological, adipose tissue and hepatic level, behavioral studies, brain PET, metabolic, histological and molecular studies were performed. Around 12% of homozygous and 5.4% of heterozygous knock-in mice showed severe neurological symptoms early in life, and their life expectancy was dramatically reduced. Severe generalized lipodystrophy and mild hepatic steatosis were present in these affected animals, while serum triglycerides and glucose metabolism were normal, with no insulin resistance. Furthermore, the study revealed a reduction in brain glucose uptake, along with patchy loss of Purkinje cells and the presence of intranuclear inclusions in cerebellar cortex cells. Homozygous, non-severely-affected knock-in mice showed a decrease in locomotor activity and greater anxiety compared with their wild type littermates. Bscl2Celia/Celia is the first murine model of Celia's encephalopathy which partially recapitulates the phenotype and severe neurodegenerative picture suffered by these patients. This model will provide a helpful tool to investigate both the progressive encephalopathy with/without lipodystrophy and congenital generalized lipodystrophy.

Published

2023

7. Natural history and comorbidities of generalised and partial lipodystrophy syndromes in Spain

Author

Universidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicas, Fernández-Pombo, Antía, Sánchez-Iglesias, Sofía, Castro Pais, Ana I., Ginzo Villamayor, María José, Cobelo Gómez, Silvia, Prado-Moraña, Teresa, Díaz-López, Everardo Josué, Casanueva, Felipe F., Loidi, Lourdes, Universidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicas, Fernández-Pombo, Antía, Sánchez-Iglesias, Sofía, Castro Pais, Ana I., Ginzo Villamayor, María José, Cobelo Gómez, Silvia, Prado-Moraña, Teresa, Díaz-López, Everardo Josué, Casanueva, Felipe F., and Loidi, Lourdes

Abstract

The rarity of lipodystrophies implies that they are not well-known, leading to delays in diagnosis/misdiagnosis. The aim of this study was to assess the natural course and comorbidities of generalised and partial lipodystrophy in Spain to contribute to their understanding. Thus, a total of 140 patients were evaluated (77.1% with partial lipodystrophy and 22.9% with generalised lipodystrophy). Clinical data were collected in a longitudinal setting with a median follow-up of 4.7 (0.5-17.6) years. Anthropometry and body composition studies were carried out and analytical parameters were also recorded. The estimated prevalence of all lipodystrophies in Spain, excluding Köbberling syndrome, was 2.78 cases/million. The onset of phenotype occurred during childhood in generalised lipodystrophy and during adolescence-adulthood in partial lipodystrophy, with the delay in diagnosis being considerable for both cohorts. There are specific clinical findings that should be highlighted as useful features to take into account when making the differential diagnosis of these disorders. Patients with generalised lipodystrophy were found to develop their first metabolic abnormalities sooner and a different lipid profile has also been observed. Mean time to death was 83.8 ± 2.5 years, being shorter among patients with generalised lipodystrophy. These results provide an initial point of comparison for ongoing prospective studies such as the ECLip Registry study.

Published

2023

8. Clinical characterisation and comorbidities of acquired generalised lipodystrophy: a 14-year follow-up study

Author

Universidade de Santiago de Compostela. Departamento de Psiquiatría, Radioloxía, Saúde Pública, Enfermaría e Medicina, Fernández-Pombo, Antía, Prado-Moraña, Teresa, Díaz-López, Everardo Josué, Sánchez Iglesias, Sofía, Castro, Ana I., Cobelo Gómez, Silvia, Araújo-Vilar, David, Universidade de Santiago de Compostela. Departamento de Psiquiatría, Radioloxía, Saúde Pública, Enfermaría e Medicina, Fernández-Pombo, Antía, Prado-Moraña, Teresa, Díaz-López, Everardo Josué, Sánchez Iglesias, Sofía, Castro, Ana I., Cobelo Gómez, Silvia, and Araújo-Vilar, David

Abstract

Acquired generalised lipodystrophy (AGL) is a rare disorder characterised by the gradual loss of fat that tends to generalise over time, the origin of which is still not fully clarified. The aim of this study was to offer a detailed description of seven patients with AGL (five women, 33.8 ± 18.6 years of age), evaluated over the last 14 years, in order to augment the knowledge of this disorder. The onset of the phenotype occurred during childhood and adolescence in five cases, and in adulthood in two cases. Three patients reported infections or vaccine administration prior to the development of lipodystrophy, and two subjects reported nodular swelling. The most frequent physical features were phlebomegaly, umbilical protrusion/hernia, and acanthosis nigricans. Skinfolds and body composition analysis showed the generalised absence of fat, with the exception of one patient in whom fat loss was spared in the trunk. The loss of fat in the palms/soles was observed in five subjects. Regarding metabolic comorbidities, throughout follow-up, two patients developed type 1 diabetes and one type 2 diabetes; three also presented hypertriglyceridaemia, one of whom developed acute pancreatitis, and no macrovascular complications were observed. Only one patient showed decreased complement C4. Autoimmunity was present in all cases, and six patients manifested Hashimoto’s thyroiditis, type 1 diabetes, autoimmune hepatitis, and/or celiac disease. Thus, there are certain clinical characteristics of AGL that may be considered important diagnostic criteria to differentiate this disorder from other lipodystrophy subtypes

Published

2023

9. Clinical spectrum of LMNA-associated type 2 familial partial lipodystrophy: a systematic review

Author

Universidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicas, Universidade de Santiago de Compostela. Departamento de Bioquímica e Bioloxía Molecular, Universidade de Santiago de Compostela. Departamento de Psiquiatría, Radioloxía, Saúde Pública, Enfermaría e Medicina, Fernández-Pombo, Antía, Díaz-López, Everardo Josué, Castro, Ana I., Sánchez-Iglesias, Sofía, Cobelo Gómez, Silvia, Prado-Moraña, Teresa, Araújo-Vilar, David, Universidade de Santiago de Compostela. Centro de Investigación en Medicina Molecular e Enfermidades Crónicas, Universidade de Santiago de Compostela. Departamento de Bioquímica e Bioloxía Molecular, Universidade de Santiago de Compostela. Departamento de Psiquiatría, Radioloxía, Saúde Pública, Enfermaría e Medicina, Fernández-Pombo, Antía, Díaz-López, Everardo Josué, Castro, Ana I., Sánchez-Iglesias, Sofía, Cobelo Gómez, Silvia, Prado-Moraña, Teresa, and Araújo-Vilar, David

Abstract

Type 2 familial partial lipodystrophy (FPLD2) is a laminopathic lipodystrophy due to pathogenic variants in the LMNA gene. Its rarity implies that it is not well-known. The aim of this review was to explore the published data regarding the clinical characterisation of this syndrome in order to better describe FPLD2. For this purpose, a systematic review through a search on PubMed until December 2022 was conducted and the references of the retrieved articles were also screened. A total of 113 articles were included. FPLD2 is characterised by the loss of fat starting around puberty in women, affecting limbs and trunk, and its accumulation in the face, neck and abdominal viscera. This adipose tissue dysfunction conditions the development of metabolic complications associated with insulin resistance, such as diabetes, dyslipidaemia, fatty liver disease, cardiovascular disease, and reproductive disorders. However, a great degree of phenotypical variability has been described. Therapeutic approaches are directed towards the associated comorbidities, and recent treatment modalities have been explored. A comprehensive comparison between FPLD2 and other FPLD subtypes can also be found in the present review. This review aimed to contribute towards augmenting knowledge of the natural history of FPLD2 by bringing together the main clinical research in this field

Published

2023

10. Clinical spectrum of Type 2 Familial Partial Lipodystrophy

Author

Cobelo-Gómez, Silvia, Prado-Moraña, Teresa, Díaz-López, Everardo Josué, Castro, Ana I., Araujo-Vilar, David, Sánchez-Iglesias, Sofía, and Antía Fernández-Pombo

Subjects

Endocrinology, Diabetes, and Metabolism, Lipodystrophy, Dyslipidemia, Laminopathies, Diabetes, Medicine and Health Sciences, Medical Specialties, LMNA, Adipose tissue, Insulin resistance

Abstract

Hypothesis To explore the published data regarding the clinical characterisation of type 2 Familial Partial Lipodystrophy. Design Plan Study type A systematic review of published studies. Blinding No blinding is involved in this study. Is there any additional blinding in this study? None Study design To show the current knowledge about the clinical characteristics, organ abnormalities and associated comorbidities of FPLD2, a systematic review based on the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) protocol was conducted. For this purpose, a search on PubMed was performed using the terms “Dunnigan” OR “familial partial lipodystrophy” OR “FPLD”. The database was searched up to December 2022, without a time limitation and without language restrictions. To identify additional studies and expand our search, the references of the retrieved articles were also screened. A total of 788 articles were identified through this database search. Studies that report clinical and/or biochemical data on patients with FPLD2 were eligible for inclusion in the current review. The main exclusion criteria were a) articles not fulfilling the topic of interest of this review; b) review articles, meta-analyses, individual case reports, editorials or comments; and c) studies not conducted on humans. Two authors independently reviewed the abstracts of the retrieved articles, applying the previously-mentioned inclusion and exclusion criteria and, subsequently reviewed the full text of the studies to determine their final inclusion. 2.3. Identification and inclusion of studies From the 788 articles initially found, 454 were excluded taking into account that they did not fulfil the topic of interest of this review, two were excluded because they were published errata and 66 were excluded because they were focused on other FPLD subtypes or laminopathies other than Dunnigan disease. During the screening and eligibility processes, 79 review articles or meta-analyses, 71 individual case reports, eight letters to the editor and one comment were also excluded. In addition, a total of 6 studies were finally included after the screening of the references of the initial pool of retrieved articles. Thus, finally, 113 articles were included in the current review.

Published

2023

11. Clinical Spectrum of LMNA-Associated Type 2 Familial Partial Lipodystrophy: A Systematic Review

Author

Sánchez-Iglesias, Sofía, Cobelo-Gómez, Silvia, Díaz-López, Everardo Josué, Castro, Ana I., Prado-Moraña, Teresa, Araujo-Vilar, David, and Antía Fernández-Pombo

Subjects

Hypertriglyceridemia, Endocrinology, Diabetes, and Metabolism, Lipodystrophy, Diabetes, Laminopathies, Medicine and Health Sciences, Medical Specialties, LMNA, Insulin resistance, General Medicine

Abstract

Type 2 familial partial lipodystrophy (FPLD2) is a laminopathic lipodystrophy due to pathogenic variants in the LMNA gene. Its rarity implies that it is not well-known. The aim of this review was to explore the published data regarding the clinical characterisation of this syndrome in order to better describe FPLD2. For this purpose, a systematic review through a search on PubMed until December 2022 was conducted and the references of the retrieved articles were also screened. A total of 113 articles were included. FPLD2 is characterised by the loss of fat starting around puberty in women, affecting limbs and trunk, and its accumulation in the face, neck and abdominal viscera. This adipose tissue dysfunction conditions the development of metabolic complications associated with insulin resistance, such as diabetes, dyslipidaemia, fatty liver disease, cardiovascular disease, and reproductive disorders. However, a great degree of phenotypical variability has been described. Therapeutic approaches are directed towards the associated comorbidities, and recent treatment modalities have been explored. A comprehensive comparison between FPLD2 and other FPLD subtypes can also be found in the present review. This review aimed to contribute towards augmenting knowledge of the natural history of FPLD2 by bringing together the main clinical research in this field.

Published

2023