The histone modifier KAT2A presents a selective target in a subset of well-differentiated microsatellite-stable colorectal cancers.

Kufrin, Vida; Buchholz, Frank; Rahimian, Elahe; Baumgarten, Jonas; Wurm, Alexander Arthur; Rothfuß, Helen; Küchler, Sandra; Brilloff, Silke; Glimm, Hanno; Seiler, Annika; Ball, Claudia; Bill, Marius; Bornhäuser, Martin; Schäfer, Silvia; Ding, Li

doi:10.1038/s41418-025-01479-7

TY  - JOUR
AU  - Kufrin, Vida
AU  - Seiler, Annika
AU  - Brilloff, Silke
AU  - Rothfuß, Helen
AU  - Küchler, Sandra
AU  - Schäfer, Silvia
AU  - Rahimian, Elahe
AU  - Baumgarten, Jonas
AU  - Ding, Li
AU  - Buchholz, Frank
AU  - Ball, Claudia
AU  - Bornhäuser, Martin
AU  - Glimm, Hanno
AU  - Bill, Marius
AU  - Wurm, Alexander Arthur
TI  - The histone modifier KAT2A presents a selective target in a subset of well-differentiated microsatellite-stable colorectal cancers.
JO  - Cell death and differentiation
VL  - 32
SN  - 1350-9047
CY  - [London]
PB  - Springer Nature
M1  - DKFZ-2025-00648
SP  - 1259–1272
PY  - 2025
N1  - 32, pages 1259–1272
AB  - Lysine acetyltransferase 2 A (KAT2A) plays a pivotal role in epigenetic gene regulation across various types of cancer. In colorectal cancer (CRC), increased KAT2A expression is associated with a more aggressive phenotype. Our study aims to elucidate the molecular underpinnings of KAT2A dependency in CRC and assess the consequences of KAT2A depletion. We conducted a comprehensive analysis by integrating CRISPR-Cas9 screening data with genomics, transcriptomics, and global acetylation patterns in CRC cell lines to pinpoint molecular markers indicative of KAT2A dependency. Additionally, we characterized the phenotypic effect of a CRISPR-interference-mediated KAT2A knockdown in CRC cell lines and patient-derived 3D spheroid cultures. Moreover, we assessed the effect of KAT2A depletion within a patient-derived xenograft mouse model in vivo. Our findings reveal that KAT2A dependency is closely associated with microsatellite stability, lower mutational burden, and increased molecular differentiation signatures in CRC, independent of the KAT2A expression levels. KAT2A-dependent CRC cells display higher gene expression levels and enriched H3K27ac marks at gene loci linked to enterocytic differentiation. Furthermore, loss of KAT2A leads to decreased cell growth and viability in vitro and in vivo, downregulation of proliferation- and stem cell-associated genes, and induction of differentiation markers. Altogether, our data show that a specific subset of CRCs with a more differentiated phenotype relies on KAT2A. For these CRC cases, KAT2A might represent a promising novel therapeutic target.
LB  - PUB:(DE-HGF)16
C6  - pmid:40140561
DO  - DOI:10.1038/s41418-025-01479-7
UR  - https://inrepo02.dkfz.de/record/300162
ER  -

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