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Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells

The age of tissues and cells can be accurately estimated by DNA methylation analysis. The multitissue DNA methylation (DNAm) age predictor combines the DNAm levels of 353 CpG dinucleotides to arrive at an age estimate referred to as DNAm age. Recent studies based on short‐term observations showed th...

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Autores principales: Søraas, Arne, Matsuyama, Mieko, de Lima, Marcos, Wald, David, Buechner, Jochen, Gedde‐Dahl, Tobias, Søraas, Camilla Lund, Chen, Brian, Ferrucci, Luigi, Dahl, John Arne, Horvath, Steve, Matsuyama, Shigemi
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/PMC6413751/
https://www.ncbi.nlm.nih.gov/pubmed/30712319
http://dx.doi.org/10.1111/acel.12897
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author Søraas, Arne
Matsuyama, Mieko
de Lima, Marcos
Wald, David
Buechner, Jochen
Gedde‐Dahl, Tobias
Søraas, Camilla Lund
Chen, Brian
Ferrucci, Luigi
Dahl, John Arne
Horvath, Steve
Matsuyama, Shigemi
author_facet Søraas, Arne
Matsuyama, Mieko
de Lima, Marcos
Wald, David
Buechner, Jochen
Gedde‐Dahl, Tobias
Søraas, Camilla Lund
Chen, Brian
Ferrucci, Luigi
Dahl, John Arne
Horvath, Steve
Matsuyama, Shigemi
author_sort Søraas, Arne
collection PubMed
description The age of tissues and cells can be accurately estimated by DNA methylation analysis. The multitissue DNA methylation (DNAm) age predictor combines the DNAm levels of 353 CpG dinucleotides to arrive at an age estimate referred to as DNAm age. Recent studies based on short‐term observations showed that the DNAm age of reconstituted blood following allogeneic hematopoietic stem cell transplantation (HSCT) reflects the age of the donor. However, it is not known whether the DNAm age of donor blood remains independent of the recipient's age over the long term. Importantly, long‐term studies including child recipients have the potential to clearly reveal whether DNAm age is cell‐intrinsic or whether it is modulated by extracellular cues in vivo. Here, we address this question by analyzing blood methylation data from HSCT donor and recipient pairs who greatly differed in chronological age (age differences between 1 and 49 years). We found that the DNAm age of the reconstituted blood was not influenced by the recipient's age, even 17 years after HSCT, in individuals without relapse of their hematologic disorder. However, the DNAm age of recipients with relapse of leukemia was unstable. These data are consistent with our previous findings concerning the abnormal DNAm age of cancer cells, and it can potentially be exploited to monitor the health of HSCT recipients. Our data demonstrate that transplanted human hematopoietic stem cells have an intrinsic DNAm age that is unaffected by the environment in a recipient of a different age.
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spelling pubmed-64137512019-04-01 Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells Søraas, Arne Matsuyama, Mieko de Lima, Marcos Wald, David Buechner, Jochen Gedde‐Dahl, Tobias Søraas, Camilla Lund Chen, Brian Ferrucci, Luigi Dahl, John Arne Horvath, Steve Matsuyama, Shigemi Aging Cell Original Papers The age of tissues and cells can be accurately estimated by DNA methylation analysis. The multitissue DNA methylation (DNAm) age predictor combines the DNAm levels of 353 CpG dinucleotides to arrive at an age estimate referred to as DNAm age. Recent studies based on short‐term observations showed that the DNAm age of reconstituted blood following allogeneic hematopoietic stem cell transplantation (HSCT) reflects the age of the donor. However, it is not known whether the DNAm age of donor blood remains independent of the recipient's age over the long term. Importantly, long‐term studies including child recipients have the potential to clearly reveal whether DNAm age is cell‐intrinsic or whether it is modulated by extracellular cues in vivo. Here, we address this question by analyzing blood methylation data from HSCT donor and recipient pairs who greatly differed in chronological age (age differences between 1 and 49 years). We found that the DNAm age of the reconstituted blood was not influenced by the recipient's age, even 17 years after HSCT, in individuals without relapse of their hematologic disorder. However, the DNAm age of recipients with relapse of leukemia was unstable. These data are consistent with our previous findings concerning the abnormal DNAm age of cancer cells, and it can potentially be exploited to monitor the health of HSCT recipients. Our data demonstrate that transplanted human hematopoietic stem cells have an intrinsic DNAm age that is unaffected by the environment in a recipient of a different age. John Wiley and Sons Inc. 2019-02-02 2019-04 /pmc/articles/PMC6413751/ /pubmed/30712319 http://dx.doi.org/10.1111/acel.12897 Text en © 2019 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Papers
Søraas, Arne
Matsuyama, Mieko
de Lima, Marcos
Wald, David
Buechner, Jochen
Gedde‐Dahl, Tobias
Søraas, Camilla Lund
Chen, Brian
Ferrucci, Luigi
Dahl, John Arne
Horvath, Steve
Matsuyama, Shigemi
Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
title Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
title_full Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
title_fullStr Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
title_full_unstemmed Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
title_short Epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
title_sort epigenetic age is a cell‐intrinsic property in transplanted human hematopoietic cells
topic Original Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6413751/
https://www.ncbi.nlm.nih.gov/pubmed/30712319
http://dx.doi.org/10.1111/acel.12897
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