Literature DB >> 26492136

Using the GEMM-ESC strategy to study gene function in mouse models.

Ivo J Huijbers1, Jessica Del Bravo1, Rahmen Bin Ali1, Colin Pritchard1, Tanya M Braumuller1, Martine H van Miltenburg2, Linda Henneman2, Ewa M Michalak2, Anton Berns2,3,4, Jos Jonkers2.   

Abstract

Preclinical in vivo validation of target genes for therapeutic intervention requires careful selection and characterization of the most suitable animal model in order to assess the role of these genes in a particular process or disease. To this end, genetically engineered mouse models (GEMMs) are typically used. However, the appropriate engineering of these models is often cumbersome and time consuming. Recently, we and others described a modular approach for fast-track modification of existing GEMMs by re-derivation of embryonic stem cells (ESCs) that can be modified by recombinase-mediated transgene insertion and subsequently used for the production of chimeric mice. This 'GEMM-ESC strategy' allows for rapid in vivo analysis of gene function in the chimeras and their offspring. Moreover, this strategy is compatible with CRISPR/Cas9-mediated genome editing. This protocol describes when and how to use the GEMM-ESC strategy effectively, and it provides a detailed procedure for re-deriving and manipulating GEMM-ESCs under feeder- and serum-free conditions. This strategy produces transgenic mice with the desired complex genotype faster than traditional methods: generation of validated GEMM-ESC clones for controlled transgene integration takes 9-12 months, and recombinase-mediated transgene integration and chimeric cohort production takes 2-3 months. The protocol requires skills in embryology, stem cell biology and molecular biology, and it is ideally performed within, or in close collaboration with, a transgenic facility.

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Year:  2015        PMID: 26492136     DOI: 10.1038/nprot.2015.114

Source DB:  PubMed          Journal:  Nat Protoc        ISSN: 1750-2799            Impact factor:   13.491


  59 in total

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10.  CAS9 transcriptional activators for target specificity screening and paired nickases for cooperative genome engineering.

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  20 in total

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Journal:  J Mammary Gland Biol Neoplasia       Date:  2019-11-15       Impact factor: 2.673

2.  Engineering Inducible Knock-In Mice to Model Oncogenic Brain Tumor Mutations from Endogenous Loci.

Authors:  Jon D Larson; Suzanne J Baker
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Journal:  J Mammary Gland Biol Neoplasia       Date:  2019-06-19       Impact factor: 2.673

Review 4.  CRISPR in cancer biology and therapy.

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Review 6.  Preclinical mouse solid tumour models: status quo, challenges and perspectives.

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7.  Strategies to Study the Functions of Pseudogenes in Mouse Models of Cancer.

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8.  Insertional mutagenesis identifies drivers of a novel oncogenic pathway in invasive lobular breast carcinoma.

Authors:  Sjors M Kas; Julian R de Ruiter; Koen Schipper; Stefano Annunziato; Eva Schut; Sjoerd Klarenbeek; Anne Paulien Drenth; Eline van der Burg; Christiaan Klijn; Jelle J Ten Hoeve; David J Adams; Marco J Koudijs; Jelle Wesseling; Micha Nethe; Lodewyk F A Wessels; Jos Jonkers
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Review 9.  Recent advances in preclinical models for lung squamous cell carcinoma.

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Journal:  Oncogene       Date:  2021-03-11       Impact factor: 9.867

10.  An In Vivo Kras Allelic Series Reveals Distinct Phenotypes of Common Oncogenic Variants.

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Journal:  Cancer Discov       Date:  2020-08-12       Impact factor: 38.272

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