New C3H KitN824K/WT cancer mouse model develops late-onset malignant mammary tumors with high penetrance

Author:

Klein-Rodewald Tanja,Micklich Kateryna,Sanz-Moreno Adrián,Tost Monica,Calzada-Wack Julia,Adler Thure,Klaften Matthias,Sabrautzki Sibylle,Aigner Bernhard,Kraiger Markus,Gailus-Durner Valerie,Fuchs Helmut,Aguilar Pimentel Juan Antonio,Becker Lore,Garrett Lillian,Hölter Sabine M.,Prehn Cornelia,Rácz Ildikó,Rozman Jan,Puk Oliver,Schrewe Anja,Schulz Holger,Adamski Jerzy,Busch Dirk H.,Esposito Irene,Wurst Wolfgang,Stoeger Claudia,Gründer Albert,Pahl Heike,Wolf Eckhard,Hrabe de Angelis Martin,Rathkolb Birgit,

Abstract

AbstractGastro-intestinal stromal tumors and acute myeloid leukemia induced by activating stem cell factor receptor tyrosine kinase (KIT) mutations are highly malignant. Less clear is the role of KIT mutations in the context of breast cancer. Treatment success of KIT-induced cancers is still unsatisfactory because of primary or secondary resistance to therapy. Mouse models offer essential platforms for studies on molecular disease mechanisms in basic cancer research. In the course of the Munich N-ethyl-N-nitrosourea (ENU) mutagenesis program a mouse line with inherited polycythemia was established. It carries a base-pair exchange in the Kit gene leading to an amino acid exchange at position 824 in the activation loop of KIT. This KIT variant corresponds to the N822K mutation found in human cancers, which is associated with imatinib-resistance. C3H KitN824K/WT mice develop hyperplasia of interstitial cells of Cajal and retention of ingesta in the cecum. In contrast to previous Kit-mutant models, we observe a benign course of gastrointestinal pathology associated with prolonged survival. Female mutants develop mammary carcinomas at late onset and subsequent lung metastasis. The disease model complements existing oncology research platforms. It allows for addressing the role of KIT mutations in breast cancer and identifying genetic and environmental modifiers of disease progression.

Funder

Helmholtz Zentrum München - Deutsches Forschungszentrum für Gesundheit und Umwelt (GmbH)

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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1. Ponatinib: An update on its drug targets, therapeutic potential and safety;Biochimica et Biophysica Acta (BBA) - Reviews on Cancer;2023-09

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