Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms

The key pathogenic steps leading to spinal muscular atrophy (SMA), a genetic disease characterized by selective motor neuron degeneration, are not fully clarified. The full-length SMN protein (FL-SMN), the main protein product of the disease gene SMN1, plays an established role in the cytoplasm in s...

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Autores principales: Locatelli, Denise, Terao, Mineko, Kurosaki, Mami, Zanellati, Maria Clara, Pletto, Daniela Rita, Finardi, Adele, Colciaghi, Francesca, Garattini, Enrico, Battaglia, Giorgio Stefano
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4516248/
https://www.ncbi.nlm.nih.gov/pubmed/26214005
http://dx.doi.org/10.1371/journal.pone.0134163
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author Locatelli, Denise
Terao, Mineko
Kurosaki, Mami
Zanellati, Maria Clara
Pletto, Daniela Rita
Finardi, Adele
Colciaghi, Francesca
Garattini, Enrico
Battaglia, Giorgio Stefano
author_facet Locatelli, Denise
Terao, Mineko
Kurosaki, Mami
Zanellati, Maria Clara
Pletto, Daniela Rita
Finardi, Adele
Colciaghi, Francesca
Garattini, Enrico
Battaglia, Giorgio Stefano
author_sort Locatelli, Denise
collection PubMed
description The key pathogenic steps leading to spinal muscular atrophy (SMA), a genetic disease characterized by selective motor neuron degeneration, are not fully clarified. The full-length SMN protein (FL-SMN), the main protein product of the disease gene SMN1, plays an established role in the cytoplasm in snRNP biogenesis ultimately leading to mRNA splicing within the nucleus. It is also involved in the mRNA axonal transport. However, to what extent the impairment of these two SMN functions contributes to SMA pathogenesis remains unknown. A shorter SMN isoform, axonal-SMN or a-SMN, with more specific axonal localization, has been discovered, but whether it might act in concert with FL-SMN in SMA pathogenesis is not known. As a first step in defining common or divergent intracellular roles of FL-SMN vs a-SMN proteins, we here characterized the turn-over of both proteins and investigated which pathway contributed to a-SMN degradation. We performed real time western blot and confocal immunofluorescence analysis in easily controllable in vitro settings. We analyzed co-transfected NSC34 and HeLa cells and cell clones stably expressing both a-SMN and FL-SMN proteins after specific blocking of transcript or protein synthesis and inhibition of known intracellular degradation pathways. Our data indicated that whereas the stability of both FL-SMN and a-SMN transcripts was comparable, the a-SMN protein was characterized by a much shorter half-life than FL-SMN. In addition, as already demonstrated for FL-SMN, the Ub/proteasome pathway played a major role in the a-SMN protein degradation. We hypothesize that the faster degradation rate of a-SMN vs FL-SMN is related to the protection provided by the protein complex in which FL-SMN is assembled. The diverse a-SMN vs FL-SMN C-terminus may dictate different protein interactions and complex formation explaining the different localization and role in the neuronal compartment, and the lower expression and stability of a-SMN.
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spelling pubmed-45162482015-07-29 Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms Locatelli, Denise Terao, Mineko Kurosaki, Mami Zanellati, Maria Clara Pletto, Daniela Rita Finardi, Adele Colciaghi, Francesca Garattini, Enrico Battaglia, Giorgio Stefano PLoS One Research Article The key pathogenic steps leading to spinal muscular atrophy (SMA), a genetic disease characterized by selective motor neuron degeneration, are not fully clarified. The full-length SMN protein (FL-SMN), the main protein product of the disease gene SMN1, plays an established role in the cytoplasm in snRNP biogenesis ultimately leading to mRNA splicing within the nucleus. It is also involved in the mRNA axonal transport. However, to what extent the impairment of these two SMN functions contributes to SMA pathogenesis remains unknown. A shorter SMN isoform, axonal-SMN or a-SMN, with more specific axonal localization, has been discovered, but whether it might act in concert with FL-SMN in SMA pathogenesis is not known. As a first step in defining common or divergent intracellular roles of FL-SMN vs a-SMN proteins, we here characterized the turn-over of both proteins and investigated which pathway contributed to a-SMN degradation. We performed real time western blot and confocal immunofluorescence analysis in easily controllable in vitro settings. We analyzed co-transfected NSC34 and HeLa cells and cell clones stably expressing both a-SMN and FL-SMN proteins after specific blocking of transcript or protein synthesis and inhibition of known intracellular degradation pathways. Our data indicated that whereas the stability of both FL-SMN and a-SMN transcripts was comparable, the a-SMN protein was characterized by a much shorter half-life than FL-SMN. In addition, as already demonstrated for FL-SMN, the Ub/proteasome pathway played a major role in the a-SMN protein degradation. We hypothesize that the faster degradation rate of a-SMN vs FL-SMN is related to the protection provided by the protein complex in which FL-SMN is assembled. The diverse a-SMN vs FL-SMN C-terminus may dictate different protein interactions and complex formation explaining the different localization and role in the neuronal compartment, and the lower expression and stability of a-SMN. Public Library of Science 2015-07-27 /pmc/articles/PMC4516248/ /pubmed/26214005 http://dx.doi.org/10.1371/journal.pone.0134163 Text en © 2015 Locatelli et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Locatelli, Denise
Terao, Mineko
Kurosaki, Mami
Zanellati, Maria Clara
Pletto, Daniela Rita
Finardi, Adele
Colciaghi, Francesca
Garattini, Enrico
Battaglia, Giorgio Stefano
Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms
title Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms
title_full Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms
title_fullStr Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms
title_full_unstemmed Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms
title_short Different Stability and Proteasome-Mediated Degradation Rate of SMN Protein Isoforms
title_sort different stability and proteasome-mediated degradation rate of smn protein isoforms
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4516248/
https://www.ncbi.nlm.nih.gov/pubmed/26214005
http://dx.doi.org/10.1371/journal.pone.0134163
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