Warning regarding hematological toxicity of tamoxifen activated CreERT2 in young Rosa26CreERT2 mice

The Cre-lox system is a versatile and powerful tool used in mouse genetics. It allows spatial and/or temporal control of the deletion of a target gene. The Rosa26-CreERT2 (R26CreERT2) mouse model allows ubiquitous expression of CreERT2. Once activated by tamoxifen, CreERT2 will enter into the nuclei...

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Bibliographic Details
Published in:Scientific reports 2023-04, Vol.13 (1), p.5976-5976, Article 5976
Main Authors: Rossi, Martina, Salomon, Aude, Chaumontel, Nicolas, Molet, Jenny, Bailly, Sabine, Tillet, Emmanuelle, Bouvard, Claire
Format: Article
Language:English
Subjects:
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631/208
631/443
Alleles
Animal models
Animals
Bone marrow
Cell proliferation
Disease Models, Animal
Gene deletion
Genetics
Hematology
Hematopoietic stem cells
Humanities and Social Sciences
Injection
Integrases - genetics
Integrases - metabolism
Life Sciences
Mice
Mice, Transgenic
Morbidity
multidisciplinary
Nucleotide sequence
Phenotypes
Science
Science (multidisciplinary)
Tamoxifen
Tamoxifen - toxicity
Toxicity
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Summary:The Cre-lox system is a versatile and powerful tool used in mouse genetics. It allows spatial and/or temporal control of the deletion of a target gene. The Rosa26-CreERT2 (R26CreERT2) mouse model allows ubiquitous expression of CreERT2. Once activated by tamoxifen, CreERT2 will enter into the nuclei and delete floxed DNA sequences. Here, we show that intraperitoneal injection of tamoxifen in young R26CreERT2 mice leads to morbidity and mortality within 10 days after the first injection, in the absence of a floxed allele. Activation of CreERT2 by tamoxifen led to severe hematological defects, with anemia and a strong disorganization of the bone marrow vascular bed. Cell proliferation was significantly reduced in the bone marrow and the spleen resulting in the depletion of several hematopoietic cells. However, not all cell types or organs were affected to the same extent. We realized that many research groups are not aware of the potential toxicity of Cre recombinases, resulting in misinterpretation of the observed phenotype and in a waste of time and resources. We discuss the necessity to include tamoxifen injected CreERT2 controls lacking a floxed allele in experimental designs and to improve communication about the limitations of Cre-lox mouse models among the scientific community.
ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-023-32633-1