Deep CRISPR mutagenesis characterizes the functional diversity of TP53 mutations - Research portal of Justus Liebig University Giessen:

Journal article

Deep CRISPR mutagenesis characterizes the functional diversity of TP53 mutations

Authors list: Funk, Julianne S.; Klimovich, Maria; Drangenstein, Daniel; Pielhoop, Ole; Hunold, Pascal; Borowek, Anna; Noeparast, Maxim; Pavlakis, Evangelos; Neumann, Michelle; Balourdas, Dimitrios-Ilias; Kochhan, Katharina; Merle, Nastasja; Bullwinkel, Imke; Wanzel, Michael; Elmshäuser, Sabrina; Teply-Szymanski, Julia; Nist, Andrea; Procida, Tara; Bartkuhn, Marek; Humpert, Katharina; Mernberger, Marco; Savai, Rajkumar; Soussi, Thierry; Joerger, Andreas C.; Stiewe, Thorsten

Publication year: 2025

Pages: 140-153

Journal: Nature Genetics

Volume number: 57

Issue number: 1

ISSN: 1061-4036

eISSN: 1546-1718

DOI Link: https://doi.org/10.1038/s41588-024-02039-4

Publisher: Nature Research

Abstract:
The mutational landscape of TP53, a tumor suppressor mutated in about half of all cancers, includes over 2,000 known missense mutations. To fully leverage TP53 mutation status for personalized medicine, a thorough understanding of the functional diversity of these mutations is essential. We conducted a deep mutational scan using saturation genome editing with CRISPR-mediated homology-directed repair to engineer 9,225 TP53 variants in cancer cells. This high-resolution approach, covering 94.5% of all cancer-associated TP53 missense mutations, precisely mapped the impact of individual mutations on tumor cell fitness, surpassing previous deep mutational scan studies in distinguishing benign from pathogenic variants. Our results revealed even subtle loss-of-function phenotypes and identified promising mutants for pharmacological reactivation. Moreover, we uncovered the roles of splicing alterations and nonsense-mediated messenger RNA decay in mutation-driven TP53 dysfunction. These findings underscore the power of saturation genome editing in advancing clinical TP53 variant interpretation for genetic counseling and personalized cancer therapy.

Authors/Editors

- Uni.-Prof. Dr. Marek Bartkuhn

Citation Styles

Harvard Citation style: Funk, J., Klimovich, M., Drangenstein, D., Pielhoop, O., Hunold, P., Borowek, A., et al. (2025) Deep CRISPR mutagenesis characterizes the functional diversity of TP53 mutations, Nature Genetics, 57(1), pp. 140-153. https://doi.org/10.1038/s41588-024-02039-4

APA Citation style: Funk, J., Klimovich, M., Drangenstein, D., Pielhoop, O., Hunold, P., Borowek, A., Noeparast, M., Pavlakis, E., Neumann, M., Balourdas, D., Kochhan, K., Merle, N., Bullwinkel, I., Wanzel, M., Elmshäuser, S., Teply-Szymanski, J., Nist, A., Procida, T., Bartkuhn, M., ...Stiewe, T. (2025). Deep CRISPR mutagenesis characterizes the functional diversity of TP53 mutations. Nature Genetics. 57(1), 140-153. https://doi.org/10.1038/s41588-024-02039-4