Your search keyword '"Llano-Rivas, Isabel"' showing total 3 results

1. Prenatal and foetal autopsy findings in glutaric aciduria type II.

Author

Martinez-Aracil, Adriano, Ruiz-Onandi, Rebeca, Perez-Rodriguez, Alvaro, Sagasta, Amaia, Llano-Rivas, Isabel, and Perez de Nanclares, Guiomar

Abstract

Background: Glutaric aciduria type 2 is a rare, lethal disorder that affects metabolism of fatty acids caused by genetic defects in electron transfer (ETF) or in electron transfer flavoprotein dehydrogenase (ETFDH). We aimed to describe the pathological findings of 15 week old foetus, born from a consanguineous couple with 3 previous perinatal deaths. The last son died at 4 days of life and genetic analyses revealed a novel probably pathogenic variant at ETFDH (c.706dupG + c.706dupG) that codifies for a truncated protein (p.Glu236Glyfs*5 + p.Glu236Glyfs*5). Case: During the gestation, due to the medical familial history, prenatal echography and a chorial biopsy for ETFDH-associated glutaric aciduria analysis were carried out. Sanger sequencing confirmed the presence of the homozygous familial variant in the ETFDH gene. The gestation was terminated and the foetal autopsy performed. Autopsy revealed prominent forehead, flat nasal bridge, malformed ears, intrauterine growth retardation, polycystic kidneys and steatosis in the liver, consistent with the diagnosis of glutaric aciduria type II. The comparison of present cases with the previously reported in the literature confirmed the presence of classical criteria, but also revealed the association with urogenital deformities, not previously stated. Conclusions: Clinical and foetal findings allowed the characterisation of the novel variant (c.706dupG at ETDFH) as pathogenic. Genotype-phenotype relationship is important when studying rare genetic disorders such as glutaric aciduria type II, as variants are usually family-specific, leading to a difficulty in the characterisation of their pathogenicity. [ABSTRACT FROM AUTHOR]

Published

2020

2. Delineation of the clinically recognizable 17q22 contiguous gene deletion syndrome in a patient carrying the smallest microdeletion known to date.

Author

Martínez‐Fernández, María Luisa, Fernández‐Toral, Joaquin, Llano‐Rivas, Isabel, Bermejo‐Sánchez, Eva, MacDonald, Alexandra, and Martínez‐Frías, María Luisa

Abstract

We describe a patient with a 1.34 Mb microdeletion at chromosome band 17q22, which is also present in his affected mother. To better delineate this microdeletion syndrome, we compare the clinical and molecular characteristics of 10 previously reported cases and our patient. Of these, the present patient has the smallest deletion which includes five genes: MMD, TMEM100, PCTP, ANKFN1, and NOG. We compare the clinical manifestations described in relation to NOG, since this is the only gene whose loss is shared by our patient and the other eight patients. Previously, the clinical patterns associated with NOG mutations have been included under the general term ' NOG-related symphalangism spectrum disorder (NOG-SSD).' Based on our analyses, and considering that there is a clinical correlation observed in cases with a '17q22 microdeletion including NOG' of which the main characteristics can be contributed to loss of this gene, we propose that the clinical patterns observed in these patients should be named as NOG-spectrum disorder-contiguous gene syndrome (NOGSD-CGS). This designation is important for clinicians because when a patient has defects concordant with alterations of NOG but also presents other anomalies not related to this gene, they would be able to suspect the existence of a microdeletion affecting 17q22, therefore, allowing an early diagnosis. This will also enable the clinician to provide the family with adequate information about the prognosis and the risk of reoccurrence in future potential offspring. © 2015 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2015

3. A novel mutation in the IRF6 gene associated with facial asymmetry in a family affected with Van der Woude Syndrome.

Author

Miñones-Suárez, Lorena, Mas-Vidal, Alberto, Fernandez-Toral, Joaquin, Llano-Rivas, Isabel, and González-García, Manuel

Subjects

CASE studies, MISSENSE mutation, INTERFERON regulatory factors, CLEFT lip, CLEFT palate, HUMAN cytogenetics, KARYOTYPES

Abstract

This report describes a novel missense mutation in the interferon regulation factor 6 ( IRF6) gene associated to facial asymmetry. This new feature widens the phenotype spectrum of Van der Woude syndrome (VWS). [ABSTRACT FROM AUTHOR]

Published

2012