Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.

Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.

Human induced pluripotent stem cells (iPSCs) are reprogrammed by transient expression of transcription factors in somatic cells. Approximately 1% of somatic cells can be reprogrammed into iPSCs, while the remaining somatic cells are differentially reprogrammed. Here, we established induced pluripote...

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Main Authors: Shogo Nagata, Kunio Hirano, Michele Kanemori, Liang-Tso Sun, Takashi Tada
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3493587?pdf=render
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spelling doaj-c9e49c29a3884879b4f18fdac9e719a22020-11-25T00:11:17ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01711e4869910.1371/journal.pone.0048699Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.Shogo NagataKunio HiranoMichele KanemoriLiang-Tso SunTakashi TadaHuman induced pluripotent stem cells (iPSCs) are reprogrammed by transient expression of transcription factors in somatic cells. Approximately 1% of somatic cells can be reprogrammed into iPSCs, while the remaining somatic cells are differentially reprogrammed. Here, we established induced pluripotent cancer stem-like cells (iCSCs) as self-renewing pluripotent cell clones. Stable iCSC lines were established from unstable induced epithelial stem cell (iESC) lines through re-plating followed by embryoid body formation and serial transplantation. iCSCs shared the expression of pluripotent marker genes with iPSCs, except for REX1 and LIN28, while exhibited the expression of somatic marker genes EMP1 and PPARγ. iESCs and iCSCs could generate teratomas with high efficiency by implantation into immunodeficient mice. The second iCSCs isolated from dissociated cells of teratoma from the first iCSCs were stably maintained, showing a gene expression profile similar to the first iCSCs. In the first and second iCSCs, transgene-derived Oct4, Sox2, Klf4, and c-Myc were expressed. Comparative global gene expression analyses demonstrated that the first iCSCs were similar to iESCs, and clearly different from human iPSCs and somatic cells. In iCSCs, gene expression kinetics of the core pluripotency factor and the Myc-related factor were pluripotent type, whereas the polycomb complex factor was somatic type. These findings indicate that pluripotent tumorigenicity can be conferred on somatic cells through up-regulation of the core pluripotency and Myc-related factors, prior to establishment of the iPSC molecular network by full reprogramming through down-regulation of the polycomb complex factor.http://europepmc.org/articles/PMC3493587?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Shogo Nagata
Kunio Hirano
Michele Kanemori
Liang-Tso Sun
Takashi Tada
spellingShingle Shogo Nagata
Kunio Hirano
Michele Kanemori
Liang-Tso Sun
Takashi Tada
Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
PLoS ONE
author_facet Shogo Nagata
Kunio Hirano
Michele Kanemori
Liang-Tso Sun
Takashi Tada
author_sort Shogo Nagata
title Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
title_short Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
title_full Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
title_fullStr Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
title_full_unstemmed Self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
title_sort self-renewal and pluripotency acquired through somatic reprogramming to human cancer stem cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Human induced pluripotent stem cells (iPSCs) are reprogrammed by transient expression of transcription factors in somatic cells. Approximately 1% of somatic cells can be reprogrammed into iPSCs, while the remaining somatic cells are differentially reprogrammed. Here, we established induced pluripotent cancer stem-like cells (iCSCs) as self-renewing pluripotent cell clones. Stable iCSC lines were established from unstable induced epithelial stem cell (iESC) lines through re-plating followed by embryoid body formation and serial transplantation. iCSCs shared the expression of pluripotent marker genes with iPSCs, except for REX1 and LIN28, while exhibited the expression of somatic marker genes EMP1 and PPARγ. iESCs and iCSCs could generate teratomas with high efficiency by implantation into immunodeficient mice. The second iCSCs isolated from dissociated cells of teratoma from the first iCSCs were stably maintained, showing a gene expression profile similar to the first iCSCs. In the first and second iCSCs, transgene-derived Oct4, Sox2, Klf4, and c-Myc were expressed. Comparative global gene expression analyses demonstrated that the first iCSCs were similar to iESCs, and clearly different from human iPSCs and somatic cells. In iCSCs, gene expression kinetics of the core pluripotency factor and the Myc-related factor were pluripotent type, whereas the polycomb complex factor was somatic type. These findings indicate that pluripotent tumorigenicity can be conferred on somatic cells through up-regulation of the core pluripotency and Myc-related factors, prior to establishment of the iPSC molecular network by full reprogramming through down-regulation of the polycomb complex factor.
url http://europepmc.org/articles/PMC3493587?pdf=render
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AT kuniohirano selfrenewalandpluripotencyacquiredthroughsomaticreprogrammingtohumancancerstemcells
AT michelekanemori selfrenewalandpluripotencyacquiredthroughsomaticreprogrammingtohumancancerstemcells
AT liangtsosun selfrenewalandpluripotencyacquiredthroughsomaticreprogrammingtohumancancerstemcells
AT takashitada selfrenewalandpluripotencyacquiredthroughsomaticreprogrammingtohumancancerstemcells
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