Zeitschriftenaufsatz | 2017 Open Access

Combined experience of six independent laboratories attempting to create an Ewing sarcoma mouse model

Autor:in

Minas, Tsion Zewdu; Surdez, Didier; Javaheri, Tahereh; Tanaka, Miwa; Howarth, Michelle; Kang, Hongjun; Han, Jenny; Han, Zhiyan; Sax, Barbara; Kream, B.; Hong, Sung-Hyeok; Celik, Haydar; Tirode, Franck; Tuckermann, Jan; Toretsky, Jeffrey; Kenner, Lukas; Kovar, Heinrich; Lee, Sean; Sweet-Cordero, E. Alejandro; Nakamura, Takuro; Moriggl, Richard; Delattre, Olivier; Uren, Aykut

Publikationen als Autor:in / Herausgeber:in der Vetmeduni

Kenner, Lukas

Journal

OncoTarget

Schlagwörter

Ewing sarcoma; EWS-FLI1; EWS-FLI1 driven transgenic mouse model

Dokumententyp

Originalarbeit

CC Lizenz

CC-BY

Open Access Type

Gold

DOI

10.18632/oncotarget.9388

WoS ID

WOS:000402051700017

PubMed ID

MEDLINE:27191748

Weitere Details

Band

8

Startseite

34141

Letzte Seite

34163

Nummer

21

Seitenanzahl

23

Ewing sarcoma (ES) involves a tumor-specific chromosomal translocation that produces the EWS-FLI1 protein, which is required for the growth of ES cells both in vitro and in vivo. However, an EWS-FLI1-driven transgenic mouse model is not currently available. Here, we present data from six independent laboratories seeking an alternative approach to express EWS-FLI1 in different murine tissues. We used the Runx2, Col1a2.3, Col1a3.6, Prx1, CAG, Nse, NEFL, Dermo1, P0, Sox9 and Osterix promoters to target EWS-FLI1 or Cre expression. Additional approaches included the induction of an endogenous chromosomal translocation, in utero knock-in, and the injection of Cre-expressing adenovirus to induce EWS-FLI1 expression locally in multiple lineages. Most models resulted in embryonic lethality or developmental defects. EWS-FLI1-induced apoptosis, promoter leakiness, the lack of potential cofactors, and the difficulty of expressing EWS-FLI1 in specific sites were considered the primary reasons for the failed attempts to create a transgenic mouse model of ES.

Georgetown University Medical Center

Univ Connecticut

Japanese Fdn Canc Res

Sorbonne Université

St. Anna Kinderspital GmbH

Stanford University

Medizinische Universität Wien - AKH

Ludwig Boltzmann Institut für Krebsforschung

Veterinärmedizinische Universität Wien

Japanese Foundation for Cancer Research

University of Connecticut

Universität Ulm

Tulane University

Georgetown University

Ludwig Boltzmann Institute

Download
RDF/XML-Format
JSON-LD-Format
Turtle-Format
N3-Format

Ewing sarcoma (ES) involves a tumor-specific chromosomal translocation that produces the EWS-FLI1 protein, which is required for the growth of ES cells both in vitro and in vivo. However, an EWS-FLI1-driven transgenic mouse model is not currently available. Here, we present data from six independent laboratories seeking an alternative approach to express EWS-FLI1 in different murine tissues. We used the Runx2, Col1a2.3, Col1a3.6, Prx1, CAG, Nse, NEFL, Dermo1, P0, Sox9 and Osterix promoters to target EWS-FLI1 or Cre expression. Additional approaches included the induction of an endogenous chromosomal translocation, in utero knock-in, and the injection of Cre-expressing adenovirus to induce EWS-FLI1 expression locally in multiple lineages. Most models resulted in embryonic lethality or developmental defects. EWS-FLI1-induced apoptosis, promoter leakiness, the lack of potential cofactors, and the difficulty of expressing EWS-FLI1 in specific sites were considered the primary reasons for the failed attempts to create a transgenic mouse model of ES.

Georgetown University Medical Center

Univ Connecticut

Japanese Fdn Canc Res

Sorbonne Université

St. Anna Kinderspital GmbH

Stanford University

Medizinische Universität Wien - AKH

Ludwig Boltzmann Institut für Krebsforschung

Veterinärmedizinische Universität Wien

Japanese Foundation for Cancer Research

University of Connecticut

Universität Ulm

Tulane University

Georgetown University

Ludwig Boltzmann Institute

Download
RDF/XML-Format
JSON-LD-Format
Turtle-Format
N3-Format