A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity.
Spatial regulation of the tumor suppressor PTEN is exerted through alternative plasma membrane, cytoplasmic, and nuclear subcellular locations. The N-terminal region of PTEN is important for the control of PTEN subcellular localization and function. It contains both an active nuclear localization si...
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doaj-7c5f9fb4d69d4bfb8a1203d8c51bc64a2020-11-24T21:10:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01104e011928710.1371/journal.pone.0119287A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity.Anabel GilIsabel Rodríguez-EscuderoMiriam StumpfMaría MolinaVíctor J CidRafael PulidoSpatial regulation of the tumor suppressor PTEN is exerted through alternative plasma membrane, cytoplasmic, and nuclear subcellular locations. The N-terminal region of PTEN is important for the control of PTEN subcellular localization and function. It contains both an active nuclear localization signal (NLS) and an overlapping PIP2-binding motif (PBM) involved in plasma membrane targeting. We report a comprehensive mutational and functional analysis of the PTEN N-terminus, including a panel of tumor-related mutations at this region. Nuclear/cytoplasmic partitioning in mammalian cells and PIP3 phosphatase assays in reconstituted S. cerevisiae defined categories of PTEN N-terminal mutations with distinct PIP3 phosphatase and nuclear accumulation properties. Noticeably, most tumor-related mutations that lost PIP3 phosphatase activity also displayed impaired nuclear localization. Cell proliferation and soft-agar colony formation analysis in mammalian cells of mutations with distinctive nuclear accumulation and catalytic activity patterns suggested a contribution of both properties to PTEN tumor suppressor activity. Our functional dissection of the PTEN N-terminus provides the basis for a systematic analysis of tumor-related and experimentally engineered PTEN mutations.http://europepmc.org/articles/PMC4398541?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Anabel Gil Isabel Rodríguez-Escudero Miriam Stumpf María Molina Víctor J Cid Rafael Pulido |
spellingShingle |
Anabel Gil Isabel Rodríguez-Escudero Miriam Stumpf María Molina Víctor J Cid Rafael Pulido A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity. PLoS ONE |
author_facet |
Anabel Gil Isabel Rodríguez-Escudero Miriam Stumpf María Molina Víctor J Cid Rafael Pulido |
author_sort |
Anabel Gil |
title |
A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity. |
title_short |
A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity. |
title_full |
A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity. |
title_fullStr |
A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity. |
title_full_unstemmed |
A functional dissection of PTEN N-terminus: implications in PTEN subcellular targeting and tumor suppressor activity. |
title_sort |
functional dissection of pten n-terminus: implications in pten subcellular targeting and tumor suppressor activity. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2015-01-01 |
description |
Spatial regulation of the tumor suppressor PTEN is exerted through alternative plasma membrane, cytoplasmic, and nuclear subcellular locations. The N-terminal region of PTEN is important for the control of PTEN subcellular localization and function. It contains both an active nuclear localization signal (NLS) and an overlapping PIP2-binding motif (PBM) involved in plasma membrane targeting. We report a comprehensive mutational and functional analysis of the PTEN N-terminus, including a panel of tumor-related mutations at this region. Nuclear/cytoplasmic partitioning in mammalian cells and PIP3 phosphatase assays in reconstituted S. cerevisiae defined categories of PTEN N-terminal mutations with distinct PIP3 phosphatase and nuclear accumulation properties. Noticeably, most tumor-related mutations that lost PIP3 phosphatase activity also displayed impaired nuclear localization. Cell proliferation and soft-agar colony formation analysis in mammalian cells of mutations with distinctive nuclear accumulation and catalytic activity patterns suggested a contribution of both properties to PTEN tumor suppressor activity. Our functional dissection of the PTEN N-terminus provides the basis for a systematic analysis of tumor-related and experimentally engineered PTEN mutations. |
url |
http://europepmc.org/articles/PMC4398541?pdf=render |
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