What question did this study set out to answer?

The study aims to identify essential chromatin regulators for spheroid formation in high-grade serous ovarian cancer by utilizing a CRISPR screen.

April 5, 2026

Abstract 1927: Epigenetic CRISPR screen identifies chromatin regulators essential for ovarian cancer spheroid formation.

Key Points

The study aims to identify essential chromatin regulators for spheroid formation in high-grade serous ovarian cancer by utilizing a CRISPR screen.
Conducted a CRISPR knockout screen targeting 800 epigenetic and chromatin regulators in OVCAR-3 spheroids.
Assessed gene essentiality by analyzing sgRNA enrichment after 3D selection for spheroid growth.
Validated top candidates in various BRCA1 genetic backgrounds by evaluating spheroid morphology and viability.
Identified key chromatin regulators, including BRCA1 and Polycomb complex members, necessary for spheroid formation.
BRCA1-WT and LOH cell lines produced compact spheroids, while BRCA1-mutant lines formed disorganized aggregates.
Results suggest a significant role of BRCA1 in maintaining 3D organization and stem-like behavior.

Abstract

Abstract Background: Cancer stem-like cells (CSCs) contribute to recurrence and chemoresistance in high-grade serous ovarian cancer (HGSOC). Spheroid formation in ultra-low attachment (ULA) cultures models CSC self-renewal, yet the epigenetic regulators and molecular dependencies sustaining this 3D phenotype remain largely undefined. Methods: A focused CRISPR knockout screen targeting 800 epigenetic and chromatin regulators was performed in OVCAR-3 spheroids. sgRNA enrichment after 3D selection identified genes essential for spheroid growth. Top candidates were functionally validated in BRCA1-wildtype, BRCA1-LOH, and BRCA1-mutant cell lines by assessing spheroid morphology, compaction, viability, and proliferative behavior. Results: The screen identified a high-confidence set of regulators required for spheroid formation, including DNA damage response genes (BRCA1, PARG), Polycomb complex members (SUZ12, BMI1), RNA-binding proteins (NCL, SYNCRIP), and cell cycle regulators (CDK2, PBRM1). These hits converge on chromatin remodeling, histone methylation, and transcriptional control pathways, linking epigenetic regulation with DDR signaling.Functional assays revealed a striking BRCA1 dependency: while BRCA1-WT and LOH cell lines formed compact, viable spheroids, BRCA1-mutant cells produced disorganized, loosely aggregated, hyperproliferative structures with poor architectural integrity. This indicates that BRCA1 is essential not for proliferation per se, but for establishing and maintaining 3D stem-like organization. Integration of the CRISPR hits with phenotypic outcomes suggests a cooperative network between DDR factors, RNA-binding regulators, and chromatin modifiers in sustaining CSC-like behavior. Conclusions: Our findings demonstrate that BRCA1 function underpins the epigenetic and chromatin-based control of spheroid architecture, revealing a mechanistic link between DNA repair fidelity, chromatin integrity, and cancer stemness. The identified vulnerabilities highlight potential therapeutic targets for BRCA1-deficient ovarian and breast cancers. Citation Format: Deren Demirel Yavuz, Irem Durmaz Sahin. Epigenetic CRISPR screen identifies chromatin regulators essential for ovarian cancer spheroid formation abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 1 (Regular Abstracts); 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86(7 Suppl):Abstract nr 1927.

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