Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons

The role of posttranslational modifications in axonal injury and regeneration has been widely studied but there has been little consensus over the mechanism by which each modification affects adult axonal growth. Acetylation is known to play an important role in a variety of neuronal functions and i...

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Autores principales: Lin, Shen, Sterling, Noelle A., Junker, Ian P., Helm, Courtney T., Smith, George M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5432171/
https://www.ncbi.nlm.nih.gov/pubmed/28505206
http://dx.doi.org/10.1371/journal.pone.0177496
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author Lin, Shen
Sterling, Noelle A.
Junker, Ian P.
Helm, Courtney T.
Smith, George M.
author_facet Lin, Shen
Sterling, Noelle A.
Junker, Ian P.
Helm, Courtney T.
Smith, George M.
author_sort Lin, Shen
collection PubMed
description The role of posttranslational modifications in axonal injury and regeneration has been widely studied but there has been little consensus over the mechanism by which each modification affects adult axonal growth. Acetylation is known to play an important role in a variety of neuronal functions and its homeostasis is controlled by two enzyme families: the Histone Deacetylases (HDACs) and Histone Acetyl Transferases (HATs). Recent studies show that HDAC5 deacetylates microtubules in the axonal cytoplasm as part of an injury-induced regeneration response, but little is known about how acetylation of microtubules plays a role. Alpha-tubulin acetyl transferase (αTAT1) is a microtubule specific acetyl transferase that binds to microtubules and directly affects microtubule stability in cells. We hypothesize that increasing tubulin acetylation may play an important role in increasing the rate of axonal growth. In this study, we infected cultured adult DRG neurons with αTAT1 and αTAT1-D157N, a catalytically inactive mutant, and HDAC5, using lentiviruses. We found that αTAT1 significantly increases tubulin acetylation in 293T cells and DRG neurons but αTAT1-D157N does not. Furthermore, in neurons infected with αTAT1, a significant increase in acetylated tubulin was detected towards the distal portion of the axon but this increase was not detected in neurons infected with αTAT1-D157N. However, we found a significant increase in axon lengths of DRG neurons after αTAT1 and αTAT1-D157N infection, but no effect on axon lengths after infection with HDAC5. Our results suggest that while αTAT1 may play a role in axon growth in vitro, the increase is not directly due to acetylation of axonal microtubules. Our results also show that HDAC5 overexpression in the axonal cytoplasm does not play a crucial role in axonal regeneration of cultured DRG neurons. We expressed these genes in DRG neurons in adult rats and performed a sciatic nerve crush. We found that axons did not regenerate any better when infected with any of the constructs compared with control animals. Thus, while αTAT1 may be important for axonal growth in vitro, neither αTAT1 nor HDAC5 had an effect in vivo on the regeneration of sciatic nerves.
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spelling pubmed-54321712017-05-26 Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons Lin, Shen Sterling, Noelle A. Junker, Ian P. Helm, Courtney T. Smith, George M. PLoS One Research Article The role of posttranslational modifications in axonal injury and regeneration has been widely studied but there has been little consensus over the mechanism by which each modification affects adult axonal growth. Acetylation is known to play an important role in a variety of neuronal functions and its homeostasis is controlled by two enzyme families: the Histone Deacetylases (HDACs) and Histone Acetyl Transferases (HATs). Recent studies show that HDAC5 deacetylates microtubules in the axonal cytoplasm as part of an injury-induced regeneration response, but little is known about how acetylation of microtubules plays a role. Alpha-tubulin acetyl transferase (αTAT1) is a microtubule specific acetyl transferase that binds to microtubules and directly affects microtubule stability in cells. We hypothesize that increasing tubulin acetylation may play an important role in increasing the rate of axonal growth. In this study, we infected cultured adult DRG neurons with αTAT1 and αTAT1-D157N, a catalytically inactive mutant, and HDAC5, using lentiviruses. We found that αTAT1 significantly increases tubulin acetylation in 293T cells and DRG neurons but αTAT1-D157N does not. Furthermore, in neurons infected with αTAT1, a significant increase in acetylated tubulin was detected towards the distal portion of the axon but this increase was not detected in neurons infected with αTAT1-D157N. However, we found a significant increase in axon lengths of DRG neurons after αTAT1 and αTAT1-D157N infection, but no effect on axon lengths after infection with HDAC5. Our results suggest that while αTAT1 may play a role in axon growth in vitro, the increase is not directly due to acetylation of axonal microtubules. Our results also show that HDAC5 overexpression in the axonal cytoplasm does not play a crucial role in axonal regeneration of cultured DRG neurons. We expressed these genes in DRG neurons in adult rats and performed a sciatic nerve crush. We found that axons did not regenerate any better when infected with any of the constructs compared with control animals. Thus, while αTAT1 may be important for axonal growth in vitro, neither αTAT1 nor HDAC5 had an effect in vivo on the regeneration of sciatic nerves. Public Library of Science 2017-05-15 /pmc/articles/PMC5432171/ /pubmed/28505206 http://dx.doi.org/10.1371/journal.pone.0177496 Text en © 2017 Lin 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Lin, Shen
Sterling, Noelle A.
Junker, Ian P.
Helm, Courtney T.
Smith, George M.
Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons
title Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons
title_full Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons
title_fullStr Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons
title_full_unstemmed Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons
title_short Effects of αTAT1 and HDAC5 on axonal regeneration in adult neurons
title_sort effects of αtat1 and hdac5 on axonal regeneration in adult neurons
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5432171/
https://www.ncbi.nlm.nih.gov/pubmed/28505206
http://dx.doi.org/10.1371/journal.pone.0177496
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AT helmcourtneyt effectsofatat1andhdac5onaxonalregenerationinadultneurons
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