Functional and structural deficiencies of Gemin5 variants associated with neurological disorders

Dysfunction of RNA-binding proteins is often linked to a wide range of human disease, particularly with neurological conditions. Gemin5 is a member of the survival of the motor neurons (SMN) complex, a ribosome-binding protein and a translation reprogramming factor. Recently, pathogenic mutations in...

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Autores principales: Francisco-Velilla, Rosario, Embarc-Buh, Azman, del Caño-Ochoa, Francisco, Abellan, Salvador, Vilar, Marçal, Alvarez, Sara, Fernandez-Jaen, Alberto, Kour, Sukhleen, Rajan, Deepa S, Pandey, Udai Bhan, Ramón-Maiques, Santiago, Martinez-Salas, Encarnacion
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Life Science Alliance LLC 2022
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8989681/
https://www.ncbi.nlm.nih.gov/pubmed/35393353
http://dx.doi.org/10.26508/lsa.202201403
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author Francisco-Velilla, Rosario
Embarc-Buh, Azman
del Caño-Ochoa, Francisco
Abellan, Salvador
Vilar, Marçal
Alvarez, Sara
Fernandez-Jaen, Alberto
Kour, Sukhleen
Rajan, Deepa S
Pandey, Udai Bhan
Ramón-Maiques, Santiago
Martinez-Salas, Encarnacion
author_facet Francisco-Velilla, Rosario
Embarc-Buh, Azman
del Caño-Ochoa, Francisco
Abellan, Salvador
Vilar, Marçal
Alvarez, Sara
Fernandez-Jaen, Alberto
Kour, Sukhleen
Rajan, Deepa S
Pandey, Udai Bhan
Ramón-Maiques, Santiago
Martinez-Salas, Encarnacion
author_sort Francisco-Velilla, Rosario
collection PubMed
description Dysfunction of RNA-binding proteins is often linked to a wide range of human disease, particularly with neurological conditions. Gemin5 is a member of the survival of the motor neurons (SMN) complex, a ribosome-binding protein and a translation reprogramming factor. Recently, pathogenic mutations in Gemin5 have been reported, but the functional consequences of these variants remain elusive. Here, we report functional and structural deficiencies associated with compound heterozygosity variants within the Gemin5 gene found in patients with neurodevelopmental disorders. These clinical variants are located in key domains of Gemin5, the tetratricopeptide repeat (TPR)–like dimerization module and the noncanonical RNA-binding site 1 (RBS1). We show that the TPR-like variants disrupt protein dimerization, whereas the RBS1 variant confers protein instability. All mutants are defective in the interaction with protein networks involved in translation and RNA-driven pathways. Importantly, the TPR-like variants fail to associate with native ribosomes, hampering its involvement in translation control and establishing a functional difference with the wild-type protein. Our study provides insights into the molecular basis of disease associated with malfunction of the Gemin5 protein.
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spelling pubmed-89896812022-04-27 Functional and structural deficiencies of Gemin5 variants associated with neurological disorders Francisco-Velilla, Rosario Embarc-Buh, Azman del Caño-Ochoa, Francisco Abellan, Salvador Vilar, Marçal Alvarez, Sara Fernandez-Jaen, Alberto Kour, Sukhleen Rajan, Deepa S Pandey, Udai Bhan Ramón-Maiques, Santiago Martinez-Salas, Encarnacion Life Sci Alliance Research Articles Dysfunction of RNA-binding proteins is often linked to a wide range of human disease, particularly with neurological conditions. Gemin5 is a member of the survival of the motor neurons (SMN) complex, a ribosome-binding protein and a translation reprogramming factor. Recently, pathogenic mutations in Gemin5 have been reported, but the functional consequences of these variants remain elusive. Here, we report functional and structural deficiencies associated with compound heterozygosity variants within the Gemin5 gene found in patients with neurodevelopmental disorders. These clinical variants are located in key domains of Gemin5, the tetratricopeptide repeat (TPR)–like dimerization module and the noncanonical RNA-binding site 1 (RBS1). We show that the TPR-like variants disrupt protein dimerization, whereas the RBS1 variant confers protein instability. All mutants are defective in the interaction with protein networks involved in translation and RNA-driven pathways. Importantly, the TPR-like variants fail to associate with native ribosomes, hampering its involvement in translation control and establishing a functional difference with the wild-type protein. Our study provides insights into the molecular basis of disease associated with malfunction of the Gemin5 protein. Life Science Alliance LLC 2022-04-07 /pmc/articles/PMC8989681/ /pubmed/35393353 http://dx.doi.org/10.26508/lsa.202201403 Text en © 2022 Francisco-Velilla et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Francisco-Velilla, Rosario
Embarc-Buh, Azman
del Caño-Ochoa, Francisco
Abellan, Salvador
Vilar, Marçal
Alvarez, Sara
Fernandez-Jaen, Alberto
Kour, Sukhleen
Rajan, Deepa S
Pandey, Udai Bhan
Ramón-Maiques, Santiago
Martinez-Salas, Encarnacion
Functional and structural deficiencies of Gemin5 variants associated with neurological disorders
title Functional and structural deficiencies of Gemin5 variants associated with neurological disorders
title_full Functional and structural deficiencies of Gemin5 variants associated with neurological disorders
title_fullStr Functional and structural deficiencies of Gemin5 variants associated with neurological disorders
title_full_unstemmed Functional and structural deficiencies of Gemin5 variants associated with neurological disorders
title_short Functional and structural deficiencies of Gemin5 variants associated with neurological disorders
title_sort functional and structural deficiencies of gemin5 variants associated with neurological disorders
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8989681/
https://www.ncbi.nlm.nih.gov/pubmed/35393353
http://dx.doi.org/10.26508/lsa.202201403
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