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NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope

Changes in the peripheral distribution and amount of condensed chromatin are observed in a number of diseases linked to mutations in the lamin A protein of the nuclear envelope. We postulated that lamin A interactions with nuclear envelope transmembrane proteins (NETs) that affect chromatin structur...

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Autores principales: Malik, Poonam, Zuleger, Nikolaj, de las Heras, Jose I., Saiz-Ros, Natalia, Makarov, Alexandr A., Lazou, Vassiliki, Meinke, Peter, Waterfall, Martin, Kelly, David A., Schirmer, Eric C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4227661/
https://www.ncbi.nlm.nih.gov/pubmed/25386906
http://dx.doi.org/10.1371/journal.pone.0111851
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author Malik, Poonam
Zuleger, Nikolaj
de las Heras, Jose I.
Saiz-Ros, Natalia
Makarov, Alexandr A.
Lazou, Vassiliki
Meinke, Peter
Waterfall, Martin
Kelly, David A.
Schirmer, Eric C.
author_facet Malik, Poonam
Zuleger, Nikolaj
de las Heras, Jose I.
Saiz-Ros, Natalia
Makarov, Alexandr A.
Lazou, Vassiliki
Meinke, Peter
Waterfall, Martin
Kelly, David A.
Schirmer, Eric C.
author_sort Malik, Poonam
collection PubMed
description Changes in the peripheral distribution and amount of condensed chromatin are observed in a number of diseases linked to mutations in the lamin A protein of the nuclear envelope. We postulated that lamin A interactions with nuclear envelope transmembrane proteins (NETs) that affect chromatin structure might be altered in these diseases and so screened thirty-one NETs for those that promote chromatin compaction as determined by an increase in the number of chromatin clusters of high pixel intensity. One of these, NET23 (also called STING, MITA, MPYS, ERIS, Tmem173), strongly promoted chromatin compaction. A correlation between chromatin compaction and endogenous levels of NET23/STING was observed for a number of human cell lines, suggesting that NET23/STING may contribute generally to chromatin condensation. NET23/STING has separately been found to be involved in innate immune response signaling. Upon infection cells make a choice to either apoptose or to alter chromatin architecture to support focused expression of interferon genes and other response factors. We postulate that the chromatin compaction induced by NET23/STING may contribute to this choice because the cells expressing NET23/STING eventually apoptose, but the chromatin compaction effect is separate from this as the condensation was still observed when cells were treated with Z-VAD to block apoptosis. NET23/STING-induced compacted chromatin revealed changes in epigenetic marks including changes in histone methylation and acetylation. This indicates a previously uncharacterized nuclear role for NET23/STING potentially in both innate immune signaling and general chromatin architecture.
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spelling pubmed-42276612014-11-18 NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope Malik, Poonam Zuleger, Nikolaj de las Heras, Jose I. Saiz-Ros, Natalia Makarov, Alexandr A. Lazou, Vassiliki Meinke, Peter Waterfall, Martin Kelly, David A. Schirmer, Eric C. PLoS One Research Article Changes in the peripheral distribution and amount of condensed chromatin are observed in a number of diseases linked to mutations in the lamin A protein of the nuclear envelope. We postulated that lamin A interactions with nuclear envelope transmembrane proteins (NETs) that affect chromatin structure might be altered in these diseases and so screened thirty-one NETs for those that promote chromatin compaction as determined by an increase in the number of chromatin clusters of high pixel intensity. One of these, NET23 (also called STING, MITA, MPYS, ERIS, Tmem173), strongly promoted chromatin compaction. A correlation between chromatin compaction and endogenous levels of NET23/STING was observed for a number of human cell lines, suggesting that NET23/STING may contribute generally to chromatin condensation. NET23/STING has separately been found to be involved in innate immune response signaling. Upon infection cells make a choice to either apoptose or to alter chromatin architecture to support focused expression of interferon genes and other response factors. We postulate that the chromatin compaction induced by NET23/STING may contribute to this choice because the cells expressing NET23/STING eventually apoptose, but the chromatin compaction effect is separate from this as the condensation was still observed when cells were treated with Z-VAD to block apoptosis. NET23/STING-induced compacted chromatin revealed changes in epigenetic marks including changes in histone methylation and acetylation. This indicates a previously uncharacterized nuclear role for NET23/STING potentially in both innate immune signaling and general chromatin architecture. Public Library of Science 2014-11-11 /pmc/articles/PMC4227661/ /pubmed/25386906 http://dx.doi.org/10.1371/journal.pone.0111851 Text en © 2014 Malik 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
Malik, Poonam
Zuleger, Nikolaj
de las Heras, Jose I.
Saiz-Ros, Natalia
Makarov, Alexandr A.
Lazou, Vassiliki
Meinke, Peter
Waterfall, Martin
Kelly, David A.
Schirmer, Eric C.
NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope
title NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope
title_full NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope
title_fullStr NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope
title_full_unstemmed NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope
title_short NET23/STING Promotes Chromatin Compaction from the Nuclear Envelope
title_sort net23/sting promotes chromatin compaction from the nuclear envelope
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4227661/
https://www.ncbi.nlm.nih.gov/pubmed/25386906
http://dx.doi.org/10.1371/journal.pone.0111851
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