Somatic gene delivery for flexiblein vivomodeling of high-risk sarcoma

Author:

Imle RolandORCID,Blösel Daniel,Kommoss Felix K.F.,Zhao Eric Stutheit,Autry Robert,Blume Christina,Lupar Dmitry,Schmitt Lukas,Winter Claudia,Wagner Lena,Placke Sara,von Eicke Malte,Hertwig Michael,Peterziel Heike,Oehme Ina,Scheuerman Sophia,Seitz Christian,Geyer Florian H.,Cidre-Aranaz Florencia,Grünewald Thomas G. P.,Vokuhl Christian,Chudasama Priya,Scholl Claudia,Schmidt Claudia,Günther Patrick,Sill Martin,Jones Kevin B.ORCID,Pfister Stefan M.,Banito AnaORCID

Abstract

ABSTRACTA particular challenge hampering therapeutic advancements for high-risk sarcoma patients is the broad spectrum of molecularly distinct sarcoma entities and the corresponding lack of suitable model systems to recapitulate and study these diseases. To overcome this predicament, we developed a novel genetically-controlled, yet versatile mouse modeling platform allowing delivery of different genetic lesions by electroporation (EPO) of the thigh muscle wildtype mice. This optimized sarcoma EPO-GEMM (EPO-based genetically engineered mouse model) platform allowed the generation of ten biologically distinct sarcoma entities, including Synovial Sarcoma (SS), fusion-positive and fusion-negative Rhabdomyosarcoma (RMS), Alveolar Soft Part Sarcoma (ASPS), Undifferentiated Pleomorphic Sarcoma (UPS) and Infantile Fibrosarcoma (IFS). Comprehensive molecular profiling and cross-species analyses confirmed faithful recapitulation of the human disease, including the expression of relevant immunotherapy targets. Syngeneic allografting enabled reliable preservation and scalability of Sarcoma-EPO-GEMMs for treatment trials, such as B7-H3-directed CAR-T cell therapy in an immunocompetent background.

Publisher

Cold Spring Harbor Laboratory

Reference79 articles.

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