Effect of in vivo administration of reprogramming factors in the mouse liver

Cancer is initiated by the transformation of stem cells or progenitor cells via a dedifferentiation process that leads to cancer stem cells; however, the process involves the activation of growth-promoting oncogenes and the inactivation of growth-constraining tumor suppressor genes. The introduction...

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Autores principales: TOMOKUNI, AKIRA, EGUCHI, HIDETOSHI, HOSHINO, HIROMITSU, DEWI, DYAH LAKSMI, NISHIKAWA, SHINPEI, KANO, YOSHIHIRO, MIYOSHI, NORIKATSU, TOJO, ARINOBU, KOBAYASHI, SEIICHIRO, GOTOH, NORIKO, HINOHARA, KUNIHIKO, FUSAKI, NOEMI, SAITO, TOSHIYUKI, SUEMIZU, HIROSHI, WADA, HIROSHI, KOBAYASHI, SHOGO, MARUBASHI, SHIGERU, TANEMURA, MASAHIRO, DOKI, YUICHIRO, MORI, MASAKI, ISHII, HIDESHI, NAGANO, HIROAKI
Formato: Online Artículo Texto
Lenguaje:English
Publicado: D.A. Spandidos 2013
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3789096/
https://www.ncbi.nlm.nih.gov/pubmed/24137324
http://dx.doi.org/10.3892/ol.2013.1418
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author TOMOKUNI, AKIRA
EGUCHI, HIDETOSHI
HOSHINO, HIROMITSU
DEWI, DYAH LAKSMI
NISHIKAWA, SHINPEI
KANO, YOSHIHIRO
MIYOSHI, NORIKATSU
TOJO, ARINOBU
KOBAYASHI, SEIICHIRO
GOTOH, NORIKO
HINOHARA, KUNIHIKO
FUSAKI, NOEMI
SAITO, TOSHIYUKI
SUEMIZU, HIROSHI
WADA, HIROSHI
KOBAYASHI, SHOGO
MARUBASHI, SHIGERU
TANEMURA, MASAHIRO
DOKI, YUICHIRO
MORI, MASAKI
ISHII, HIDESHI
NAGANO, HIROAKI
author_facet TOMOKUNI, AKIRA
EGUCHI, HIDETOSHI
HOSHINO, HIROMITSU
DEWI, DYAH LAKSMI
NISHIKAWA, SHINPEI
KANO, YOSHIHIRO
MIYOSHI, NORIKATSU
TOJO, ARINOBU
KOBAYASHI, SEIICHIRO
GOTOH, NORIKO
HINOHARA, KUNIHIKO
FUSAKI, NOEMI
SAITO, TOSHIYUKI
SUEMIZU, HIROSHI
WADA, HIROSHI
KOBAYASHI, SHOGO
MARUBASHI, SHIGERU
TANEMURA, MASAHIRO
DOKI, YUICHIRO
MORI, MASAKI
ISHII, HIDESHI
NAGANO, HIROAKI
author_sort TOMOKUNI, AKIRA
collection PubMed
description Cancer is initiated by the transformation of stem cells or progenitor cells via a dedifferentiation process that leads to cancer stem cells; however, the process involves the activation of growth-promoting oncogenes and the inactivation of growth-constraining tumor suppressor genes. The introduction of defined factors, such as those encoded by c-Myc, Sox2, Oct3/4 and Klf4, in normal somatic cells results in their dedifferentiation into induced pluripotent stem (iPS) cells. We previously reported that these defined factors induced the development of induced multipotent cancer (iPC) cells from gastrointestinal cancer cells by reducing tumor aggressiveness. Previous studies indicated that although reprogramming may be facilitated by p53 inhibition, gain-of-function oncogenic mutations in p53 and oncogenic mutations in Kras-stimulated tumorigenic activity, and their roles in vivo are imperfectly understood. Hence, in the present study, the effect of direct injection of a Sendai virus (SeV) vector encoding four defined factors in vivo was studied using various backgrounds of transgenic and knockout mice, and was compared with that of direct injection of microRNAs (miRNAs) diluted with cationic lipid. The in vivo imaging data revealed transformation hot spots for p53 deficiency or conditional activation of mutant Kras, and the sizes were concordant with those in immuno-deficient NOD/SCID and uPA-NOG mice, as well as larger compared with those in the control mice. Overall, the present data on in vivo reprogramming indicated that Kras activation may facilitate the effect of cellular reprogramming in normal liver cells, and the effect of Kras activation is more apparent than that of tumor suppressor p53 deficiency. The results also revealed that immunodeficiency may increase the effect of reprogramming, presumably by blocking the immunosurveillance of transformed cells. These findings provide a rationale for further studies to develop a therapeutic approach involving direct in vivo reprogramming.
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spelling pubmed-37890962013-10-17 Effect of in vivo administration of reprogramming factors in the mouse liver TOMOKUNI, AKIRA EGUCHI, HIDETOSHI HOSHINO, HIROMITSU DEWI, DYAH LAKSMI NISHIKAWA, SHINPEI KANO, YOSHIHIRO MIYOSHI, NORIKATSU TOJO, ARINOBU KOBAYASHI, SEIICHIRO GOTOH, NORIKO HINOHARA, KUNIHIKO FUSAKI, NOEMI SAITO, TOSHIYUKI SUEMIZU, HIROSHI WADA, HIROSHI KOBAYASHI, SHOGO MARUBASHI, SHIGERU TANEMURA, MASAHIRO DOKI, YUICHIRO MORI, MASAKI ISHII, HIDESHI NAGANO, HIROAKI Oncol Lett Articles Cancer is initiated by the transformation of stem cells or progenitor cells via a dedifferentiation process that leads to cancer stem cells; however, the process involves the activation of growth-promoting oncogenes and the inactivation of growth-constraining tumor suppressor genes. The introduction of defined factors, such as those encoded by c-Myc, Sox2, Oct3/4 and Klf4, in normal somatic cells results in their dedifferentiation into induced pluripotent stem (iPS) cells. We previously reported that these defined factors induced the development of induced multipotent cancer (iPC) cells from gastrointestinal cancer cells by reducing tumor aggressiveness. Previous studies indicated that although reprogramming may be facilitated by p53 inhibition, gain-of-function oncogenic mutations in p53 and oncogenic mutations in Kras-stimulated tumorigenic activity, and their roles in vivo are imperfectly understood. Hence, in the present study, the effect of direct injection of a Sendai virus (SeV) vector encoding four defined factors in vivo was studied using various backgrounds of transgenic and knockout mice, and was compared with that of direct injection of microRNAs (miRNAs) diluted with cationic lipid. The in vivo imaging data revealed transformation hot spots for p53 deficiency or conditional activation of mutant Kras, and the sizes were concordant with those in immuno-deficient NOD/SCID and uPA-NOG mice, as well as larger compared with those in the control mice. Overall, the present data on in vivo reprogramming indicated that Kras activation may facilitate the effect of cellular reprogramming in normal liver cells, and the effect of Kras activation is more apparent than that of tumor suppressor p53 deficiency. The results also revealed that immunodeficiency may increase the effect of reprogramming, presumably by blocking the immunosurveillance of transformed cells. These findings provide a rationale for further studies to develop a therapeutic approach involving direct in vivo reprogramming. D.A. Spandidos 2013-08 2013-06-20 /pmc/articles/PMC3789096/ /pubmed/24137324 http://dx.doi.org/10.3892/ol.2013.1418 Text en Copyright © 2013, Spandidos Publications http://creativecommons.org/licenses/by/3.0 This is an open-access article licensed under a Creative Commons Attribution-NonCommercial 3.0 Unported License. The article may be redistributed, reproduced, and reused for non-commercial purposes, provided the original source is properly cited.
spellingShingle Articles
TOMOKUNI, AKIRA
EGUCHI, HIDETOSHI
HOSHINO, HIROMITSU
DEWI, DYAH LAKSMI
NISHIKAWA, SHINPEI
KANO, YOSHIHIRO
MIYOSHI, NORIKATSU
TOJO, ARINOBU
KOBAYASHI, SEIICHIRO
GOTOH, NORIKO
HINOHARA, KUNIHIKO
FUSAKI, NOEMI
SAITO, TOSHIYUKI
SUEMIZU, HIROSHI
WADA, HIROSHI
KOBAYASHI, SHOGO
MARUBASHI, SHIGERU
TANEMURA, MASAHIRO
DOKI, YUICHIRO
MORI, MASAKI
ISHII, HIDESHI
NAGANO, HIROAKI
Effect of in vivo administration of reprogramming factors in the mouse liver
title Effect of in vivo administration of reprogramming factors in the mouse liver
title_full Effect of in vivo administration of reprogramming factors in the mouse liver
title_fullStr Effect of in vivo administration of reprogramming factors in the mouse liver
title_full_unstemmed Effect of in vivo administration of reprogramming factors in the mouse liver
title_short Effect of in vivo administration of reprogramming factors in the mouse liver
title_sort effect of in vivo administration of reprogramming factors in the mouse liver
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3789096/
https://www.ncbi.nlm.nih.gov/pubmed/24137324
http://dx.doi.org/10.3892/ol.2013.1418
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