2026-04-29 ゲーテ大学
Structure of the DNA-binding domain of a reactivated p53 cancer mutant in complex with a stabilizing DARPin. Image: Andreas Joerger, Goethe University Frankfurt
<関連情報>
- https://aktuelles.uni-frankfurt.de/english/cancer-research-mini-antibodies-reactivate-the-guardian-of-the-genome/
- https://www.pnas.org/doi/10.1073/pnas.2531747123
温度感受性p53癌変異体の汎再活性化因子としてのDARPins DARPins as pan-reactivators of temperature-sensitive p53 cancer mutants
Philipp Münick, Dimitrios-Ilias Balourdas, Julianne S. Funk, +12 , and Volker Dötsch
Proceedings of the National Academy of Sciences Published:April 28, 2026
DOI:https://doi.org/10.1073/pnas.2531747123
Significance
The tumor suppressor p53, a central guardian against malignant transformation, is inactivated by mutation in about half of all human cancers. Many p53 mutants are temperature-sensitive (TS), exhibiting reduced conformational stability yet retaining the potential for reactivation by stabilizing agents. However, the absence of suitable drug-binding pockets has limited the development of such molecules. Here, we introduce designed ankyrin repeat proteins (DARPins) as generic mutant p53 stabilizers that bind a nonfunctional site on the p53 DNA-binding domain. This interaction compensates for mutation-induced loss of thermal stability and restores p53 signaling in patient-derived cancer cells. Coupled with mRNA-based delivery, this approach could enable broad-spectrum reactivation of TS mutants for personalized cancer therapy.
Abstract
The tumor suppressor p53 is the most frequently mutated protein in tumors and a target for drug development. More than 2000 cancer-associated p53 missense mutations have been reported, most of them located in the DNA-binding domain (DBD). Due to the low intrinsic thermostability of the latter, they often lead to unfolding at physiological temperature. Stabilizing the DBD with small molecules has been shown to be effective in reactivating the cavity-creating cancer mutant Y220C. Unfortunately, the majority of p53 mutants seem to lack druggable binding pockets for small molecules. Here we show that a designed ankyrin repeat protein (DARPin) that binds to the p53 DBD stabilizes temperature-sensitive (TS) p53 cancer mutants, thereby compensating for mutation-induced loss of stability. We determined high-resolution crystal structures of multiple DARPin–mutant p53 complexes, providing mechanistic insights into this mode of stabilization. Reporter gene assays across a comprehensive panel of cancer-associated mutants revealed reactivation of the majority of TS mutants, whereas DNA-contact mutants and those with local misfolding of the DNA-binding surface remained inactive, as expected. We demonstrate that this reactivation induces the transcription of canonical p53 target genes and elicits antiproliferative effects in cancer cell lines. A combination of this DARPin with an mRNA/lipid nanoparticle-based transfection approach may have the potential to reactivate most TS p53 mutants and resensitize cancer cells to chemotherapy.
