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Smaug variants in neural and non-neuronal cells

Mammalian Smaug1/Samd4a is an mRNA regulator involved in synapse plasticity and additional non-neuronal functions. Here we analyzed the expression of Smaug1/Samd4a variants and Smaug2/Samd4b in primary hippocampal neurons and non-neuronal cell lines. We found that multiple Smaug proteins are present...

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Autores principales: Fernández-Alvarez, Ana Julia, Pascual, Malena Lucía, Boccaccio, Graciela Lidia, Thomas, María Gabriela
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4857778/
https://www.ncbi.nlm.nih.gov/pubmed/27195061
http://dx.doi.org/10.1080/19420889.2016.1139252
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author Fernández-Alvarez, Ana Julia
Pascual, Malena Lucía
Boccaccio, Graciela Lidia
Thomas, María Gabriela
author_facet Fernández-Alvarez, Ana Julia
Pascual, Malena Lucía
Boccaccio, Graciela Lidia
Thomas, María Gabriela
author_sort Fernández-Alvarez, Ana Julia
collection PubMed
description Mammalian Smaug1/Samd4a is an mRNA regulator involved in synapse plasticity and additional non-neuronal functions. Here we analyzed the expression of Smaug1/Samd4a variants and Smaug2/Samd4b in primary hippocampal neurons and non-neuronal cell lines. We found that multiple Smaug proteins are present in several mammalian cell lines, including a canonical full length Smaug1, a Smaug1 variant that lacks the third exon, termed ΔEIII, and Smaug2, the product of a highly homologous gene. These three major isoforms are expressed differentially along neuron development and form cytosolic bodies when transfected in cell lines. By using luciferase reporters, we found that the ΔEIII isoform, which lacks 10 amino acids in the sterile α motif involved in RNA binding, shows a RNA-binding capacity and repressor activity comparable to that of the full length Smaug1. These observations are an important groundwork for molecular studies of the Smaug post-transcriptional pathway, which is relevant to neuron development, mitochondrial function and muscle physiology in health and disease.
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spelling pubmed-48577782016-05-18 Smaug variants in neural and non-neuronal cells Fernández-Alvarez, Ana Julia Pascual, Malena Lucía Boccaccio, Graciela Lidia Thomas, María Gabriela Commun Integr Biol Short Communication Mammalian Smaug1/Samd4a is an mRNA regulator involved in synapse plasticity and additional non-neuronal functions. Here we analyzed the expression of Smaug1/Samd4a variants and Smaug2/Samd4b in primary hippocampal neurons and non-neuronal cell lines. We found that multiple Smaug proteins are present in several mammalian cell lines, including a canonical full length Smaug1, a Smaug1 variant that lacks the third exon, termed ΔEIII, and Smaug2, the product of a highly homologous gene. These three major isoforms are expressed differentially along neuron development and form cytosolic bodies when transfected in cell lines. By using luciferase reporters, we found that the ΔEIII isoform, which lacks 10 amino acids in the sterile α motif involved in RNA binding, shows a RNA-binding capacity and repressor activity comparable to that of the full length Smaug1. These observations are an important groundwork for molecular studies of the Smaug post-transcriptional pathway, which is relevant to neuron development, mitochondrial function and muscle physiology in health and disease. Taylor & Francis 2016-02-18 /pmc/articles/PMC4857778/ /pubmed/27195061 http://dx.doi.org/10.1080/19420889.2016.1139252 Text en © 2016 Taylor & Francis open-access
spellingShingle Short Communication
Fernández-Alvarez, Ana Julia
Pascual, Malena Lucía
Boccaccio, Graciela Lidia
Thomas, María Gabriela
Smaug variants in neural and non-neuronal cells
title Smaug variants in neural and non-neuronal cells
title_full Smaug variants in neural and non-neuronal cells
title_fullStr Smaug variants in neural and non-neuronal cells
title_full_unstemmed Smaug variants in neural and non-neuronal cells
title_short Smaug variants in neural and non-neuronal cells
title_sort smaug variants in neural and non-neuronal cells
topic Short Communication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4857778/
https://www.ncbi.nlm.nih.gov/pubmed/27195061
http://dx.doi.org/10.1080/19420889.2016.1139252
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