Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform

Immortalizing primary cells with human telomerase reverse transcriptase (hTERT) has been common practice to enable primary cells to be of extended use in the laboratory because they avoid replicative senescence. Studying exogenously expressed hTERT in cells also affords scientists models of early ca...

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Autores principales: Bikkul, Mehmet U., Faragher, Richard G. A., Worthington, Gemma, Meinke, Peter, Kerr, Alastair R. W., Sammy, Aakila, Riyahi, Kumars, Horton, Daniel, Schirmer, Eric C., Hubank, Michael, Kill, Ian R., Anderson, Rhona M., Slijepcevic, Predrag, Makarov, Evgeny, Bridger, Joanna M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Inc. 2019
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6590296/
https://www.ncbi.nlm.nih.gov/pubmed/30474255
http://dx.doi.org/10.1002/gcc.22711
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author Bikkul, Mehmet U.
Faragher, Richard G. A.
Worthington, Gemma
Meinke, Peter
Kerr, Alastair R. W.
Sammy, Aakila
Riyahi, Kumars
Horton, Daniel
Schirmer, Eric C.
Hubank, Michael
Kill, Ian R.
Anderson, Rhona M.
Slijepcevic, Predrag
Makarov, Evgeny
Bridger, Joanna M.
author_facet Bikkul, Mehmet U.
Faragher, Richard G. A.
Worthington, Gemma
Meinke, Peter
Kerr, Alastair R. W.
Sammy, Aakila
Riyahi, Kumars
Horton, Daniel
Schirmer, Eric C.
Hubank, Michael
Kill, Ian R.
Anderson, Rhona M.
Slijepcevic, Predrag
Makarov, Evgeny
Bridger, Joanna M.
author_sort Bikkul, Mehmet U.
collection PubMed
description Immortalizing primary cells with human telomerase reverse transcriptase (hTERT) has been common practice to enable primary cells to be of extended use in the laboratory because they avoid replicative senescence. Studying exogenously expressed hTERT in cells also affords scientists models of early carcinogenesis and telomere behavior. Control and the premature ageing disease—Hutchinson‐Gilford progeria syndrome (HGPS) primary dermal fibroblasts, with and without the classical G608G mutation have been immortalized with exogenous hTERT. However, hTERT immortalization surprisingly elicits genome reorganization not only in disease cells but also in the normal control cells, such that whole chromosome territories normally located at the nuclear periphery in proliferating fibroblasts become mislocalized in the nuclear interior. This includes chromosome 18 in the control fibroblasts and both chromosomes 18 and X in HGPS cells, which physically express an isoform of the LINC complex protein SUN1 that has previously only been theoretical. Additionally, this HGPS cell line has also become genomically unstable and has a tetraploid karyotype, which could be due to the novel SUN1 isoform. Long‐term treatment with the hTERT inhibitor BIBR1532 enabled the reduction of telomere length in the immortalized cells and resulted that these mislocalized internal chromosomes to be located at the nuclear periphery, as assessed in actively proliferating cells. Taken together, these findings reveal that elongated telomeres lead to dramatic chromosome mislocalization, which can be restored with a drug treatment that results in telomere reshortening and that a novel SUN1 isoform combined with elongated telomeres leads to genomic instability. Thus, care should be taken when interpreting data from genomic studies in hTERT‐immortalized cell lines.
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spelling pubmed-65902962019-07-08 Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform Bikkul, Mehmet U. Faragher, Richard G. A. Worthington, Gemma Meinke, Peter Kerr, Alastair R. W. Sammy, Aakila Riyahi, Kumars Horton, Daniel Schirmer, Eric C. Hubank, Michael Kill, Ian R. Anderson, Rhona M. Slijepcevic, Predrag Makarov, Evgeny Bridger, Joanna M. Genes Chromosomes Cancer Research Articles Immortalizing primary cells with human telomerase reverse transcriptase (hTERT) has been common practice to enable primary cells to be of extended use in the laboratory because they avoid replicative senescence. Studying exogenously expressed hTERT in cells also affords scientists models of early carcinogenesis and telomere behavior. Control and the premature ageing disease—Hutchinson‐Gilford progeria syndrome (HGPS) primary dermal fibroblasts, with and without the classical G608G mutation have been immortalized with exogenous hTERT. However, hTERT immortalization surprisingly elicits genome reorganization not only in disease cells but also in the normal control cells, such that whole chromosome territories normally located at the nuclear periphery in proliferating fibroblasts become mislocalized in the nuclear interior. This includes chromosome 18 in the control fibroblasts and both chromosomes 18 and X in HGPS cells, which physically express an isoform of the LINC complex protein SUN1 that has previously only been theoretical. Additionally, this HGPS cell line has also become genomically unstable and has a tetraploid karyotype, which could be due to the novel SUN1 isoform. Long‐term treatment with the hTERT inhibitor BIBR1532 enabled the reduction of telomere length in the immortalized cells and resulted that these mislocalized internal chromosomes to be located at the nuclear periphery, as assessed in actively proliferating cells. Taken together, these findings reveal that elongated telomeres lead to dramatic chromosome mislocalization, which can be restored with a drug treatment that results in telomere reshortening and that a novel SUN1 isoform combined with elongated telomeres leads to genomic instability. Thus, care should be taken when interpreting data from genomic studies in hTERT‐immortalized cell lines. John Wiley & Sons, Inc. 2019-01-07 2019-06 /pmc/articles/PMC6590296/ /pubmed/30474255 http://dx.doi.org/10.1002/gcc.22711 Text en © 2018 The Authors. Genes, Chromosomes & Cancer published by Wiley Periodicals, Inc. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Research Articles
Bikkul, Mehmet U.
Faragher, Richard G. A.
Worthington, Gemma
Meinke, Peter
Kerr, Alastair R. W.
Sammy, Aakila
Riyahi, Kumars
Horton, Daniel
Schirmer, Eric C.
Hubank, Michael
Kill, Ian R.
Anderson, Rhona M.
Slijepcevic, Predrag
Makarov, Evgeny
Bridger, Joanna M.
Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform
title Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform
title_full Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform
title_fullStr Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform
title_full_unstemmed Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform
title_short Telomere elongation through hTERT immortalization leads to chromosome repositioning in control cells and genomic instability in Hutchinson‐Gilford progeria syndrome fibroblasts, expressing a novel SUN1 isoform
title_sort telomere elongation through htert immortalization leads to chromosome repositioning in control cells and genomic instability in hutchinson‐gilford progeria syndrome fibroblasts, expressing a novel sun1 isoform
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6590296/
https://www.ncbi.nlm.nih.gov/pubmed/30474255
http://dx.doi.org/10.1002/gcc.22711
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