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KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation

Euchromatic histone methyltransferases (EHMTs), members of the KMT1 family, methylate histone and non‐histone proteins. Here, we uncover a novel role for EHMTs in regulating heterochromatin anchorage to the nuclear periphery (NP) via non‐histone methylation. We show that EHMTs methylate and stabiliz...

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Autores principales: Rao, Radhika Arasala, Ketkar, Alhad Ashok, Kedia, Neelam, Krishnamoorthy, Vignesh K, Lakshmanan, Vairavan, Kumar, Pankaj, Mohanty, Abhishek, Kumar, Shilpa Dilip, Raja, Sufi O, Gulyani, Akash, Chaturvedi, Chandra Prakash, Brand, Marjorie, Palakodeti, Dasaradhi, Rampalli, Shravanti
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6501005/
https://www.ncbi.nlm.nih.gov/pubmed/30858340
http://dx.doi.org/10.15252/embr.201643260
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author Rao, Radhika Arasala
Ketkar, Alhad Ashok
Kedia, Neelam
Krishnamoorthy, Vignesh K
Lakshmanan, Vairavan
Kumar, Pankaj
Mohanty, Abhishek
Kumar, Shilpa Dilip
Raja, Sufi O
Gulyani, Akash
Chaturvedi, Chandra Prakash
Brand, Marjorie
Palakodeti, Dasaradhi
Rampalli, Shravanti
author_facet Rao, Radhika Arasala
Ketkar, Alhad Ashok
Kedia, Neelam
Krishnamoorthy, Vignesh K
Lakshmanan, Vairavan
Kumar, Pankaj
Mohanty, Abhishek
Kumar, Shilpa Dilip
Raja, Sufi O
Gulyani, Akash
Chaturvedi, Chandra Prakash
Brand, Marjorie
Palakodeti, Dasaradhi
Rampalli, Shravanti
author_sort Rao, Radhika Arasala
collection PubMed
description Euchromatic histone methyltransferases (EHMTs), members of the KMT1 family, methylate histone and non‐histone proteins. Here, we uncover a novel role for EHMTs in regulating heterochromatin anchorage to the nuclear periphery (NP) via non‐histone methylation. We show that EHMTs methylate and stabilize LaminB1 (LMNB1), which associates with the H3K9me2‐marked peripheral heterochromatin. Loss of LMNB1 methylation or EHMTs abrogates heterochromatin anchorage at the NP. We further demonstrate that the loss of EHMTs induces many hallmarks of aging including global reduction of H3K27methyl marks and altered nuclear morphology. Consistent with this, we observe a gradual depletion of EHMTs, which correlates with loss of methylated LMNB1 and peripheral heterochromatin in aging human fibroblasts. Restoration of EHMT expression reverts peripheral heterochromatin defects in aged cells. Collectively, our work elucidates a new mechanism by which EHMTs regulate heterochromatin domain organization and reveals their impact on fundamental changes associated with the intrinsic aging process.
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spelling pubmed-65010052019-05-09 KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation Rao, Radhika Arasala Ketkar, Alhad Ashok Kedia, Neelam Krishnamoorthy, Vignesh K Lakshmanan, Vairavan Kumar, Pankaj Mohanty, Abhishek Kumar, Shilpa Dilip Raja, Sufi O Gulyani, Akash Chaturvedi, Chandra Prakash Brand, Marjorie Palakodeti, Dasaradhi Rampalli, Shravanti EMBO Rep Articles Euchromatic histone methyltransferases (EHMTs), members of the KMT1 family, methylate histone and non‐histone proteins. Here, we uncover a novel role for EHMTs in regulating heterochromatin anchorage to the nuclear periphery (NP) via non‐histone methylation. We show that EHMTs methylate and stabilize LaminB1 (LMNB1), which associates with the H3K9me2‐marked peripheral heterochromatin. Loss of LMNB1 methylation or EHMTs abrogates heterochromatin anchorage at the NP. We further demonstrate that the loss of EHMTs induces many hallmarks of aging including global reduction of H3K27methyl marks and altered nuclear morphology. Consistent with this, we observe a gradual depletion of EHMTs, which correlates with loss of methylated LMNB1 and peripheral heterochromatin in aging human fibroblasts. Restoration of EHMT expression reverts peripheral heterochromatin defects in aged cells. Collectively, our work elucidates a new mechanism by which EHMTs regulate heterochromatin domain organization and reveals their impact on fundamental changes associated with the intrinsic aging process. John Wiley and Sons Inc. 2019-03-12 2019-05 /pmc/articles/PMC6501005/ /pubmed/30858340 http://dx.doi.org/10.15252/embr.201643260 Text en © 2019 The Authors. Published under the terms of the CC BY 4.0 license https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Articles
Rao, Radhika Arasala
Ketkar, Alhad Ashok
Kedia, Neelam
Krishnamoorthy, Vignesh K
Lakshmanan, Vairavan
Kumar, Pankaj
Mohanty, Abhishek
Kumar, Shilpa Dilip
Raja, Sufi O
Gulyani, Akash
Chaturvedi, Chandra Prakash
Brand, Marjorie
Palakodeti, Dasaradhi
Rampalli, Shravanti
KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
title KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
title_full KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
title_fullStr KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
title_full_unstemmed KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
title_short KMT1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
title_sort kmt1 family methyltransferases regulate heterochromatin–nuclear periphery tethering via histone and non‐histone protein methylation
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6501005/
https://www.ncbi.nlm.nih.gov/pubmed/30858340
http://dx.doi.org/10.15252/embr.201643260
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