What does this research mean for the field?

ULK2 overcomes cisplatin resistance in ovarian cancer by downregulating glycolysis through phosphorylation-induced degradation of c-Jun. Novelty: ClaimNovelty.NOVEL_FINDING. Consensus alignment: ConsensusAlignment.CHALLENGES_CONSENSUS.

What question did this study set out to answer?

Investigate ULK2's role in chemoresistance and its mechanisms in ovarian cancer organoids.

February 22, 2026Open Access

ULK2 suppresses glycolysis to attenuate cisplatin resistance in ovarian cancer organoid via c-Jun phosphorylation

Key Points

Investigate ULK2's role in chemoresistance and its mechanisms in ovarian cancer organoids.
Survival analysis using Kaplan-Meier plotter database
Immunohistochemical profiling of ULK2 in tissue samples and organoids
Lentiviral vector transduction for ULK2 overexpression
Phosphoproteomics to examine phosphorylated proteins
CCK-8 and in vivo experiments to assess chemosensitivity
ULK2 overexpression increased chemosensitivity and conferred survival advantage in ovarian cancer organoids.
Phosphoproteomics indicated ULK2's role in metabolic processes, particularly glycolysis suppression.
Phosphorylation of c-Jun at Ser243 was identified as a mechanism by which ULK2 attenuates glycolysis.
c-Jun overexpression counteracted the chemosensitivity effects of ULK2 overexpression.

Abstract

Objective Resistance to platinum-based chemotherapy remains a key obstacle in ovarian cancer treatment. This study aims to investigate the role of Uncoordinated 51-like kinase 2 (ULK2) in chemoresistance of ovarian cancer and elucidate its underlying mechanisms using 3D patient-derived organoids. Methods Survival analysis was first performed using the Kaplan‒Meier plotter database. Immunohistochemical profiling delineated differential ULK2 expression patterns between chemoresistant and chemosensitive ovarian cancer tissue samples and organoids. ULK2 overexpression was achieved in cisplatin-resistant ovarian cancer organoids via lentiviral vector transduction. Then, we conducted an in-depth examination of the alterations in phosphorylated proteins induced by ULK2 overexpression using phosphoproteomics technology. To investigate the influence of ULK2 on chemosensitivity in ovarian cancer, Cell Counting Kit-8 (CCK-8) and in vivo experiments were conducted. Glycolysis was quantitatively assessed, and the underlying molecular mechanism was systematically investigated. Results ULK2 high-expression ovarian cancer exhibited enhanced chemosensitivity and conferred survival advantage. CCK-8 and mouse experiments demonstrated that ULK2 overexpression decreased cisplatin resistance in patient-derived organoids. Gene Ontology (GO) analysis of phosphoproteomics profiling highlighted the predominant role of ULK2 in metabolic processes with experimental validation demonstrating its suppression of glycolysis. Mechanistically, ULK2 attenuated c-Jun expression by phosphorylation of c-Jun at Ser243. Moreover, c-Jun overexpression counteracted the chemosensitivity and glycolytic suppression induced by the ectopic ULK2 expression in ovarian cancer. Conclusions ULK2 overcomes cisplatin resistance in ovarian cancer by downregulating glycolysis, a process mediated by phosphorylation-induced c-Jun degradation. These findings emphasized the role of ULK2 as a tumor suppressor, offering novel insights for chemotherapy in ovarian cancer.

ULK2 suppresses glycolysis to attenuate cisplatin resistance in ovarian cancer organoid via c-Jun phosphorylation

Key Points

Abstract

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