Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice

Liposarcomas (LPSs) are the most common soft-tissue cancer. Because of the lack of animal models, the cellular origin and molecular regulation of LPS remain unclear. Here, we report that mice with adipocyte-specific activation of Notch signaling (Ad/N1ICD) develop LPS with complete penetrance. Linea...

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Autores principales: Bi, Pengpeng, Yue, Feng, Karki, Anju, Castro, Beatriz, Wirbisky, Sara E., Wang, Chao, Durkes, Abigail, Elzey, Bennett D., Andrisani, Ourania M., Bidwell, Christopher A., Freeman, Jennifer L., Konieczny, Stephen F., Kuang, Shihuan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2016
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5030803/
https://www.ncbi.nlm.nih.gov/pubmed/27573812
http://dx.doi.org/10.1084/jem.20160157
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author Bi, Pengpeng
Yue, Feng
Karki, Anju
Castro, Beatriz
Wirbisky, Sara E.
Wang, Chao
Durkes, Abigail
Elzey, Bennett D.
Andrisani, Ourania M.
Bidwell, Christopher A.
Freeman, Jennifer L.
Konieczny, Stephen F.
Kuang, Shihuan
author_facet Bi, Pengpeng
Yue, Feng
Karki, Anju
Castro, Beatriz
Wirbisky, Sara E.
Wang, Chao
Durkes, Abigail
Elzey, Bennett D.
Andrisani, Ourania M.
Bidwell, Christopher A.
Freeman, Jennifer L.
Konieczny, Stephen F.
Kuang, Shihuan
author_sort Bi, Pengpeng
collection PubMed
description Liposarcomas (LPSs) are the most common soft-tissue cancer. Because of the lack of animal models, the cellular origin and molecular regulation of LPS remain unclear. Here, we report that mice with adipocyte-specific activation of Notch signaling (Ad/N1ICD) develop LPS with complete penetrance. Lineage tracing confirms the adipocyte origin of Ad/N1ICD LPS. The Ad/N1ICD LPS resembles human dedifferentiated LPS in histological appearance, anatomical localization, and gene expression signature. Before transformation, Ad/N1ICD adipocytes undergo dedifferentiation that leads to lipodystrophy and metabolic dysfunction. Although concomitant Pten deletion normalizes the glucose metabolism of Ad/N1ICD mice, it dramatically accelerates the LPS prognosis and malignancy. Transcriptomes and lipidomics analyses indicate that Notch activation suppresses lipid metabolism pathways that supply ligands to Pparγ, the master regulator of adipocyte homeostasis. Accordingly, synthetic Pparγ ligand supplementation induces redifferentiation of Ad/N1ICD adipocytes and tumor cells, and prevents LPS development in Ad/N1ICD mice. Importantly, the Notch target HES1 is abundantly expressed in human LPS, and Notch inhibition suppresses the growth of human dedifferentiated LPS xenografts. Collectively, ectopic Notch activation is sufficient to induce dedifferentiation and tumorigenic transformation of mature adipocytes in mouse.
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spelling pubmed-50308032017-03-19 Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice Bi, Pengpeng Yue, Feng Karki, Anju Castro, Beatriz Wirbisky, Sara E. Wang, Chao Durkes, Abigail Elzey, Bennett D. Andrisani, Ourania M. Bidwell, Christopher A. Freeman, Jennifer L. Konieczny, Stephen F. Kuang, Shihuan J Exp Med Research Articles Liposarcomas (LPSs) are the most common soft-tissue cancer. Because of the lack of animal models, the cellular origin and molecular regulation of LPS remain unclear. Here, we report that mice with adipocyte-specific activation of Notch signaling (Ad/N1ICD) develop LPS with complete penetrance. Lineage tracing confirms the adipocyte origin of Ad/N1ICD LPS. The Ad/N1ICD LPS resembles human dedifferentiated LPS in histological appearance, anatomical localization, and gene expression signature. Before transformation, Ad/N1ICD adipocytes undergo dedifferentiation that leads to lipodystrophy and metabolic dysfunction. Although concomitant Pten deletion normalizes the glucose metabolism of Ad/N1ICD mice, it dramatically accelerates the LPS prognosis and malignancy. Transcriptomes and lipidomics analyses indicate that Notch activation suppresses lipid metabolism pathways that supply ligands to Pparγ, the master regulator of adipocyte homeostasis. Accordingly, synthetic Pparγ ligand supplementation induces redifferentiation of Ad/N1ICD adipocytes and tumor cells, and prevents LPS development in Ad/N1ICD mice. Importantly, the Notch target HES1 is abundantly expressed in human LPS, and Notch inhibition suppresses the growth of human dedifferentiated LPS xenografts. Collectively, ectopic Notch activation is sufficient to induce dedifferentiation and tumorigenic transformation of mature adipocytes in mouse. The Rockefeller University Press 2016-09-19 /pmc/articles/PMC5030803/ /pubmed/27573812 http://dx.doi.org/10.1084/jem.20160157 Text en © 2016 Bi et al. This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 3.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/3.0/).
spellingShingle Research Articles
Bi, Pengpeng
Yue, Feng
Karki, Anju
Castro, Beatriz
Wirbisky, Sara E.
Wang, Chao
Durkes, Abigail
Elzey, Bennett D.
Andrisani, Ourania M.
Bidwell, Christopher A.
Freeman, Jennifer L.
Konieczny, Stephen F.
Kuang, Shihuan
Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
title Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
title_full Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
title_fullStr Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
title_full_unstemmed Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
title_short Notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
title_sort notch activation drives adipocyte dedifferentiation and tumorigenic transformation in mice
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5030803/
https://www.ncbi.nlm.nih.gov/pubmed/27573812
http://dx.doi.org/10.1084/jem.20160157
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