Your search keyword '"Llano-Rivas, Isabel"' showing total 4 results

1. Novel APOB mutation in familial hypobetalipoproteinemia.

Author

Domenech, M., Llano-Rivas, Isabel, Arroyo, Vicente, and Ortega, Emilio

Subjects

GENETIC mutation, GENETIC disorders, APOLIPOPROTEINS, LIPID metabolism disorders, RARE diseases

Abstract

• Familial hypobetalipoproteinemia (type1 and 2) is a rare codominant genetic disorder • More than 50% of FHBL1 heterozygous individuals have APOB gene variants • Loss-of-function mutations in ANGPTL3 cause FHBL2 • We report a family with a novel APOB variant coexisting with a known ANGPTL3 variant [ABSTRACT FROM AUTHOR]

Published

2022

2. P87-F Severe congenital myopathy related to a novel mutation in the titin gene. A case report

Author

Sánchez-Horvath, Miriam, Marcelino-Salas, Keyla, Llano-Rivas, Isabel, Martínez González, María Jesús, García-Ribes, Ainhoa, Fernández-Bedoya, Ana Isabel, Martínez-Zuluaga, Ana, San Martín, Imanol Lambarri, and Yurrebaso-Santamaría, Izaskun

Published

2019

3. Interaction between a Domain of the Negative Regulator of the Ras-ERK Pathway, SPRED1 Protein, and the GTPase-activating Protein-related Domain of Neurofibromin Is Implicated in Legius Syndrome and Neurofibromatosis Type 1.

Author

Yasuko Hirata, Brems, Hilde, Mayu Suzuki, Mitsuhiro Kanamori, Masahiro Okada, Rimpei Morita, Llano-Rivas, Isabel, Toyoyuki Ose, Messiaen, Ludwine, Legius, Eric, and Akihiko Yoshimura

Subjects

*RAS proteins, *EXTRACELLULAR signal-regulated kinases, *GTPASE-activating protein, *NEUROFIBROMIN, *NEUROFIBROMATOSIS 1, *GENETIC mutation

Abstract

Constitutional heterozygous loss-of-function mutations in the SPRED1 gene cause a phenotype known as Legius syndrome, which consists of symptoms of multiple café-au-lait macules, axillary freckling, learning disabilities, and macrocephaly. Legius syndrome resembles a mild neurofibromatosis type 1 (NF1) phenotype. It has been demonstrated that SPRED1 functions as a negative regulator of the Ras-ERK pathway and interacts with neurofibromin, the NF1 gene product However, the molecular details of this interaction and the effects of the mutations identified in Legius syndrome and NF1 on this interaction have not yet been investigated. In this study, using a yeast two-hybrid system and an immunoprecipitation assay in HEK293 cells, we found that the SPRED1 EVH1 domain interacts with the N-terminal 16 amino acids and the C-terminal 20 amino acids of the GTPase-activating protein (GAP)-related domain (GRD) of neurofibromin, which form two crossing α-helix coils outside the GAP domain. These regions have been shown to be dispensable for GAP activity and are not present in p120GAP. Several mutations in these N- and C-terminal regions of the GRD in NF1 patients and pathogenic missense mutations in the EVH1 domain of SPRED1 in Legius syndrome reduced the binding affinity between the EVH1 domain and the GRD. EVH1 domain mutations with reduced binding to the GRD also disrupted the ERK suppression activity of SPRED1. These data clearly demonstrate that SPRED1 inhibits the Ras-ERK pathway by recruiting neurofibromin to Ras through the EVH1-GRD interaction, and this study also provides molecular basis for the pathogenic mutations of NF1 and Legius syndrome. [ABSTRACT FROM AUTHOR]

Published

2016

4. Exome sequencing identifies CTSK mutations in patients originally diagnosed as intermediate osteopetrosis.

Author

Pangrazio, Alessandra, Puddu, Alessandro, Oppo, Manuela, Valentini, Maria, Zammataro, Luca, Vellodi, Ashok, Gener, Blanca, Llano-Rivas, Isabel, Raza, Jamal, Atta, Irum, Vezzoni, Paolo, Superti-Furga, Andrea, Villa, Anna, and Sobacchi, Cristina

Subjects

*NUCLEOTIDE sequence, *GENETIC mutation, *GENETIC disorders, *OSTEOPETROSIS, *BONE density, *RADIOGRAPHY, *ORTHOPEDICS, *GENETICS, *DIAGNOSIS

Abstract

Abstract: Autosomal Recessive Osteopetrosis is a genetic disorder characterized by increased bone density due to lack of resorption by the osteoclasts. Genetic studies have widely unraveled the molecular basis of the most severe forms, while cases of intermediate severity are more difficult to characterize, probably because of a large heterogeneity. Here, we describe the use of exome sequencing in the molecular diagnosis of 2 siblings initially thought to be affected by “intermediate osteopetrosis”, which identified a homozygous mutation in the CTSK gene. Prompted by this finding, we tested by Sanger sequencing 25 additional patients addressed to us for recessive osteopetrosis and found CTSK mutations in 4 of them. In retrospect, their clinical and radiographic features were found to be compatible with, but not typical for, Pycnodysostosis. We sought to identify modifier genes that might have played a role in the clinical manifestation of the disease in these patients, but our results were not informative. In conclusion, we underline the difficulties of differential diagnosis in some patients whose clinical appearance does not fit the classical malignant or benign picture and recommend that CTSK gene be included in the molecular diagnosis of high bone density conditions. [Copyright &y& Elsevier]

Published

2014