NudC deacetylation regulates mitotic progression.

NudC deacetylation regulates mitotic progression.

Mitosis is largely driven by posttranslational modifications of proteins. Recent studies suggest that protein acetylation is prevalent in mitosis, but how protein acetylation/deacetylation regulates mitotic progression remains unclear. Nuclear distribution protein C (NudC), a conserved protein that...

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Main Authors: Carol Chuang, Jing Pan, David H Hawke, Sue-Hwa Lin, Li-yuan Yu-Lee
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3777959?pdf=render
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spelling doaj-cb548612c3fa4308818b7e775b6bb26d2020-11-24T21:47:47ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0189e7384110.1371/journal.pone.0073841NudC deacetylation regulates mitotic progression.Carol ChuangJing PanDavid H HawkeSue-Hwa LinLi-yuan Yu-LeeMitosis is largely driven by posttranslational modifications of proteins. Recent studies suggest that protein acetylation is prevalent in mitosis, but how protein acetylation/deacetylation regulates mitotic progression remains unclear. Nuclear distribution protein C (NudC), a conserved protein that regulates cell division, was previously shown to be acetylated. We found that NudC acetylation was decreased during mitosis. Using mass spectrometry analysis, we identified K39 to be an acetylation site on NudC. Reconstitution of NudC-deficient cells with wild-type or K39R acetylation-defective NudC rescued mitotic phenotypes, including chromosome misalignment, chromosome missegregation, and reduced spindle width, observed after NudC protein knockdown. In contrast, the K39Q acetylation-mimetic NudC was unable to rescue these mitotic phenotypes, suggesting that NudC deacetylation is important for mitotic progression. To examine proteins that may play a role in NudC deacetylation during mitosis, we found that NudC co-localizes on the mitotic spindle with the histone deacetylase HDAC3, an HDAC shown to regulate mitotic spindle stability. Further, NudC co-immunoprecipitates with HDAC3 and loss of function of HDAC3 either by protein knockdown or inhibition with a small molecule inhibitor increased NudC acetylation. These observations suggest that HDAC3 may be involved in NudC deacetylation during mitosis. Cells with NudC or HDAC3 knockdown exhibited overlapping mitotic abnormalities, including chromosomes arranged in a "dome-like" configuration surrounding a collapsed mitotic spindle. Our studies suggest that NudC acetylation/deacetylation regulates mitotic progression and NudC deacetylation, likely through HDAC3, is critical for spindle function and chromosome congression.http://europepmc.org/articles/PMC3777959?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Carol Chuang
Jing Pan
David H Hawke
Sue-Hwa Lin
Li-yuan Yu-Lee
spellingShingle Carol Chuang
Jing Pan
David H Hawke
Sue-Hwa Lin
Li-yuan Yu-Lee
NudC deacetylation regulates mitotic progression.
PLoS ONE
author_facet Carol Chuang
Jing Pan
David H Hawke
Sue-Hwa Lin
Li-yuan Yu-Lee
author_sort Carol Chuang
title NudC deacetylation regulates mitotic progression.
title_short NudC deacetylation regulates mitotic progression.
title_full NudC deacetylation regulates mitotic progression.
title_fullStr NudC deacetylation regulates mitotic progression.
title_full_unstemmed NudC deacetylation regulates mitotic progression.
title_sort nudc deacetylation regulates mitotic progression.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Mitosis is largely driven by posttranslational modifications of proteins. Recent studies suggest that protein acetylation is prevalent in mitosis, but how protein acetylation/deacetylation regulates mitotic progression remains unclear. Nuclear distribution protein C (NudC), a conserved protein that regulates cell division, was previously shown to be acetylated. We found that NudC acetylation was decreased during mitosis. Using mass spectrometry analysis, we identified K39 to be an acetylation site on NudC. Reconstitution of NudC-deficient cells with wild-type or K39R acetylation-defective NudC rescued mitotic phenotypes, including chromosome misalignment, chromosome missegregation, and reduced spindle width, observed after NudC protein knockdown. In contrast, the K39Q acetylation-mimetic NudC was unable to rescue these mitotic phenotypes, suggesting that NudC deacetylation is important for mitotic progression. To examine proteins that may play a role in NudC deacetylation during mitosis, we found that NudC co-localizes on the mitotic spindle with the histone deacetylase HDAC3, an HDAC shown to regulate mitotic spindle stability. Further, NudC co-immunoprecipitates with HDAC3 and loss of function of HDAC3 either by protein knockdown or inhibition with a small molecule inhibitor increased NudC acetylation. These observations suggest that HDAC3 may be involved in NudC deacetylation during mitosis. Cells with NudC or HDAC3 knockdown exhibited overlapping mitotic abnormalities, including chromosomes arranged in a "dome-like" configuration surrounding a collapsed mitotic spindle. Our studies suggest that NudC acetylation/deacetylation regulates mitotic progression and NudC deacetylation, likely through HDAC3, is critical for spindle function and chromosome congression.
url http://europepmc.org/articles/PMC3777959?pdf=render
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AT jingpan nudcdeacetylationregulatesmitoticprogression
AT davidhhawke nudcdeacetylationregulatesmitoticprogression
AT suehwalin nudcdeacetylationregulatesmitoticprogression
AT liyuanyulee nudcdeacetylationregulatesmitoticprogression
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