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Citations to this article

PPARγ agonists enhance ET-743–induced adipogenic differentiation in a transgenic mouse model of myxoid round cell liposarcoma
Elizabeth Charytonowicz, … , Robert N. Taub, Igor Matushansky
Elizabeth Charytonowicz, … , Robert N. Taub, Igor Matushansky
Published February 1, 2012
Citation Information: J Clin Invest. 2012;122(3):886-898. https://doi.org/10.1172/JCI60015.
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Research Article Oncology Article has an altmetric score of 15

PPARγ agonists enhance ET-743–induced adipogenic differentiation in a transgenic mouse model of myxoid round cell liposarcoma

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Abstract

Myxoid round cell liposarcoma (MRCLS) is a common liposarcoma subtype characterized by a translocation that results in the fusion protein TLS:CHOP as well as by mixed adipocytic histopathology. Both the etiology of MRCLS and the mechanism of action of TLS:CHOP remain poorly understood. It was previously shown that ET-743, an antitumor compound with an unclear mechanism of action, is highly effective in patients with MRCLS. To identify the cellular origin of MRCLS, we engineered a mouse model in which TLS:CHOP was expressed under the control of a mesodermally restricted promoter (Prx1) in a p53-depleted background. This model resembled MRCLS histologically as well as functionally in terms of its specific adipocytic differentiation–based response to ET-743. Specifically, endogenous mesenchymal stem cells (MSCs) expressing TLS:CHOP developed into MRCLS in vivo. Gene expression and microRNA analysis of these MSCs showed that they were committed to adipocytic differentiation, but unable to terminally differentiate. We also explored the method of action of ET-743. ET-743 downregulated TLS:CHOP expression, which correlated with CEBPα expression and adipocytic differentiation. Furthermore, PPARγ agonists enhanced the differentiation process initiated by ET-743. Our work highlights how clinical observations can lead to the generation of a mouse model that recapitulates human disease and may be used to develop rational treatment combinations, such as ET-743 plus PPARγ agonists, for the treatment of MRCLS.

Authors

Elizabeth Charytonowicz, Melissa Terry, Katherine Coakley, Leonid Telis, Fabrizio Remotti, Carlos Cordon-Cardo, Robert N. Taub, Igor Matushansky

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Total citations by year

Year: 2024 2022 2021 2020 2019 2018 2017 2016 2015 2014 2013 2012 2009 Total
Citations: 2 2 1 3 2 1 4 3 5 4 4 4 1 36
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Citations to this article (36)

Title and authors Publication Year
Deciphering the role of FUS::DDIT3 expression and tumor microenvironment in myxoid liposarcoma development
Ranji P, Jonasson E, Andersson L, Filges S, Luna Santamaría M, Vannas C, Dolatabadi S, Gustafsson A, Myklebost O, Håkansson J, Fagman H, Landberg G, Åman P, Ståhlberg A
Journal of Translational Medicine 2024
FUS::DDIT3 Fusion Protein in the Development of Myxoid Liposarcoma and Possible Implications for Therapy.
Hou X, Shi W, Luo W, Luo Y, Huang X, Li J, Ji N, Chen Q
Biomolecules 2024
FUS-DDIT3 Fusion Oncoprotein Expression Affects JAK-STAT Signaling in Myxoid Liposarcoma.
Dolatabadi S, Jonasson E, Andersson L, Luna Santamaría M, Lindén M, Österlund T, Åman P, Ståhlberg A
Frontiers in Oncology 2022
Lipidomics and Transcriptomics Differ Liposarcoma Differentiation Characteristics That Can Be Altered by Pentose Phosphate Pathway Intervention
Song Z, Wang S, Lu L, Xu J, Zhou Q, Lu W, Tong H, Zhang Y, Liu W, Wang Z, Li W, You Y, Zhang C, Guo X, Luo R, Hou Y, Wang C, Wang Y, Sun L, Huang H, Zhou Y
Metabolites 2022
Recent Advancement in Atypical Lipomatous Tumor Research
E Mashima, Y Sawada, M Nakamura
International journal of molecular sciences 2021
Emerging role of tumor cell plasticity in modifying therapeutic response
S Qin, J Jiang, Y Lu, EC Nice, C Huang, J Zhang, W He
Signal Transduction and Targeted Therapy 2020
The Intimate Relationship among EMT, MET and TME: A T(ransdifferentiation) E(nhancing) M(ix) to Be Exploited for Therapeutic Purposes
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Oncology Letters 2020
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