Unveiling the biological effects of DNA G-quadruplex ligands through multi-omics data integration

Francesca Romano; Carolina Persico; Alessandra Barra; Gabriella Pinto; Anna Illiano; Angela Amoresano; Immacolata Aiello; Sara Abate; Ludovica D'Auria; Verdiana Martello; Nunzio D'Agostino; Mariateresa Giustiniano; Camilla Russo; Luana Izzo; Francesco Merlino; Diego Brancaccio; Bruno Pagano; Jussara Amato; Simona Marzano; Federica D'Aria; Stefano Amente; Rasmus Bro; Morten Arendt Rasmussen; Myrhiam Cassese; Rosario Ammendola; Fabio Cattaneo; Stefano De Tito; Nunzia Iaccarino; Anna Di Porzio; Antonio Randazzo

doi:10.1016/j.ijbiomac.2025.144325

Unveiling the biological effects of DNA G-quadruplex ligands through multi-omics data integration

Francesca Romano, Carolina Persico, Alessandra Barra, Gabriella Pinto, Anna Illiano, Angela Amoresano, Immacolata Aiello, Sara Abate, Ludovica D'Auria, Verdiana Martello, Nunzio D'Agostino, Mariateresa Giustiniano, Camilla Russo, Luana Izzo, Francesco Merlino, Diego Brancaccio, Bruno Pagano, Jussara Amato, Simona Marzano, Federica D'AriaStefano Amente, Rasmus Bro, Morten Arendt Rasmussen, Myrhiam Cassese, Rosario Ammendola, Fabio Cattaneo, Stefano De Tito, Nunzia Iaccarino^*, Anna Di Porzio^*, Antonio Randazzo^*

^*Corresponding author for this work

Research output: Contribution to journal › Journal article › Research › peer-review

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Abstract

G-quadruplexes (G4s) are non-canonical DNA structures that have proved to play a pivotal role in various biological processes, including telomere maintenance and gene expression regulation. Owing to their prevalence in tumor cells, G4s have emerged as promising targets for cancer therapy, with a substantial body of research demonstrating the potential of G4 ligands as anti-cancer tools. Nonetheless, a comprehensive multi-omics study to fully elucidate the mode of action of G-quadruplex ligands is still lacking. Such an investigation would be crucial for advancing the development of potent G4-based therapies against cancer. Herein, we employed a multi-omics approach, integrating transcriptomics, proteomics, and metabolomics, to identify key signaling pathways that mediate the anti-cancer effects of well-characterized G4-binding agents (berberine, pyridostatin and RHPS4) on human cervical adenocarcinoma (HeLa) cells. Particularly, we analyzed gene expression changes using RNA sequencing, quantified proteins by liquid-chromatography tandem mass spectrometry and examined metabolite levels via nuclear magnetic resonance. Our results revealed that, under the investigated experimental conditions, berberine treatment had only negligible cellular effects. In contrast, pyridostatin induced significant changes at the transcriptomic, proteomic, and metabolomic levels, decreasing the abundance of enzymes involved in cellular energy production, reducing the availability of precursors for lipid and nucleotide biosynthesis, and depleting essential cofactors and enzymes required for redox balance. Notably, RHPS4 could selectively disrupt mitochondrial activity, possibly through the specific stabilization of mitochondrial G-quadruplex structures. Overall, our findings provide a valuable multi-omics perspective on the cellular changes driven by G-quadruplex binders, that may accelerate the development of effective anti-cancer G4-targeted therapies.

Original language	English
Article number	144325
Journal	International Journal of Biological Macromolecules
Volume	313
Number of pages	13
ISSN	0141-8130
DOIs	https://doi.org/10.1016/j.ijbiomac.2025.144325
Publication status	Published - 2025

Bibliographical note

Publisher Copyright:
© 2025 The Authors

Keywords

Berberine
HeLa cells
Metabolomics
Proteomics
Pyridostatin
RHPS4
Transcriptomics profiling

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Romano, F., Persico, C., Barra, A., Pinto, G., Illiano, A., Amoresano, A., Aiello, I., Abate, S., D'Auria, L., Martello, V., D'Agostino, N., Giustiniano, M., Russo, C., Izzo, L., Merlino, F., Brancaccio, D., Pagano, B., Amato, J., Marzano, S., ... Randazzo, A. (2025). Unveiling the biological effects of DNA G-quadruplex ligands through multi-omics data integration. International Journal of Biological Macromolecules, 313, Article 144325. https://doi.org/10.1016/j.ijbiomac.2025.144325

Romano, F, Persico, C, Barra, A, Pinto, G, Illiano, A, Amoresano, A, Aiello, I, Abate, S, D'Auria, L, Martello, V, D'Agostino, N, Giustiniano, M, Russo, C, Izzo, L, Merlino, F, Brancaccio, D, Pagano, B, Amato, J, Marzano, S, D'Aria, F, Amente, S, Bro, R , Rasmussen, MA, Cassese, M, Ammendola, R, Cattaneo, F, De Tito, S, Iaccarino, N, Di Porzio, A & Randazzo, A 2025, 'Unveiling the biological effects of DNA G-quadruplex ligands through multi-omics data integration', International Journal of Biological Macromolecules, vol. 313, 144325. https://doi.org/10.1016/j.ijbiomac.2025.144325

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title = "Unveiling the biological effects of DNA G-quadruplex ligands through multi-omics data integration",

abstract = "G-quadruplexes (G4s) are non-canonical DNA structures that have proved to play a pivotal role in various biological processes, including telomere maintenance and gene expression regulation. Owing to their prevalence in tumor cells, G4s have emerged as promising targets for cancer therapy, with a substantial body of research demonstrating the potential of G4 ligands as anti-cancer tools. Nonetheless, a comprehensive multi-omics study to fully elucidate the mode of action of G-quadruplex ligands is still lacking. Such an investigation would be crucial for advancing the development of potent G4-based therapies against cancer. Herein, we employed a multi-omics approach, integrating transcriptomics, proteomics, and metabolomics, to identify key signaling pathways that mediate the anti-cancer effects of well-characterized G4-binding agents (berberine, pyridostatin and RHPS4) on human cervical adenocarcinoma (HeLa) cells. Particularly, we analyzed gene expression changes using RNA sequencing, quantified proteins by liquid-chromatography tandem mass spectrometry and examined metabolite levels via nuclear magnetic resonance. Our results revealed that, under the investigated experimental conditions, berberine treatment had only negligible cellular effects. In contrast, pyridostatin induced significant changes at the transcriptomic, proteomic, and metabolomic levels, decreasing the abundance of enzymes involved in cellular energy production, reducing the availability of precursors for lipid and nucleotide biosynthesis, and depleting essential cofactors and enzymes required for redox balance. Notably, RHPS4 could selectively disrupt mitochondrial activity, possibly through the specific stabilization of mitochondrial G-quadruplex structures. Overall, our findings provide a valuable multi-omics perspective on the cellular changes driven by G-quadruplex binders, that may accelerate the development of effective anti-cancer G4-targeted therapies.",

keywords = "Berberine, HeLa cells, Metabolomics, Proteomics, Pyridostatin, RHPS4, Transcriptomics profiling",

author = "Francesca Romano and Carolina Persico and Alessandra Barra and Gabriella Pinto and Anna Illiano and Angela Amoresano and Immacolata Aiello and Sara Abate and Ludovica D'Auria and Verdiana Martello and Nunzio D'Agostino and Mariateresa Giustiniano and Camilla Russo and Luana Izzo and Francesco Merlino and Diego Brancaccio and Bruno Pagano and Jussara Amato and Simona Marzano and Federica D'Aria and Stefano Amente and Rasmus Bro and Rasmussen, {Morten Arendt} and Myrhiam Cassese and Rosario Ammendola and Fabio Cattaneo and {De Tito}, Stefano and Nunzia Iaccarino and {Di Porzio}, Anna and Antonio Randazzo",

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year = "2025",

doi = "10.1016/j.ijbiomac.2025.144325",

language = "English",

volume = "313",

journal = "International Journal of Biological Macromolecules",

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T1 - Unveiling the biological effects of DNA G-quadruplex ligands through multi-omics data integration

AU - Romano, Francesca

AU - Persico, Carolina

AU - Barra, Alessandra

AU - Pinto, Gabriella

AU - Illiano, Anna

AU - Amoresano, Angela

AU - Aiello, Immacolata

AU - Abate, Sara

AU - D'Auria, Ludovica

AU - Martello, Verdiana

AU - D'Agostino, Nunzio

AU - Giustiniano, Mariateresa

AU - Russo, Camilla

AU - Izzo, Luana

AU - Merlino, Francesco

AU - Brancaccio, Diego

AU - Pagano, Bruno

AU - Amato, Jussara

AU - Marzano, Simona

AU - D'Aria, Federica

AU - Amente, Stefano

AU - Bro, Rasmus

AU - Rasmussen, Morten Arendt

AU - Cassese, Myrhiam

AU - Ammendola, Rosario

AU - Cattaneo, Fabio

AU - De Tito, Stefano

AU - Iaccarino, Nunzia

AU - Di Porzio, Anna

AU - Randazzo, Antonio

PY - 2025

Y1 - 2025

N2 - G-quadruplexes (G4s) are non-canonical DNA structures that have proved to play a pivotal role in various biological processes, including telomere maintenance and gene expression regulation. Owing to their prevalence in tumor cells, G4s have emerged as promising targets for cancer therapy, with a substantial body of research demonstrating the potential of G4 ligands as anti-cancer tools. Nonetheless, a comprehensive multi-omics study to fully elucidate the mode of action of G-quadruplex ligands is still lacking. Such an investigation would be crucial for advancing the development of potent G4-based therapies against cancer. Herein, we employed a multi-omics approach, integrating transcriptomics, proteomics, and metabolomics, to identify key signaling pathways that mediate the anti-cancer effects of well-characterized G4-binding agents (berberine, pyridostatin and RHPS4) on human cervical adenocarcinoma (HeLa) cells. Particularly, we analyzed gene expression changes using RNA sequencing, quantified proteins by liquid-chromatography tandem mass spectrometry and examined metabolite levels via nuclear magnetic resonance. Our results revealed that, under the investigated experimental conditions, berberine treatment had only negligible cellular effects. In contrast, pyridostatin induced significant changes at the transcriptomic, proteomic, and metabolomic levels, decreasing the abundance of enzymes involved in cellular energy production, reducing the availability of precursors for lipid and nucleotide biosynthesis, and depleting essential cofactors and enzymes required for redox balance. Notably, RHPS4 could selectively disrupt mitochondrial activity, possibly through the specific stabilization of mitochondrial G-quadruplex structures. Overall, our findings provide a valuable multi-omics perspective on the cellular changes driven by G-quadruplex binders, that may accelerate the development of effective anti-cancer G4-targeted therapies.

AB - G-quadruplexes (G4s) are non-canonical DNA structures that have proved to play a pivotal role in various biological processes, including telomere maintenance and gene expression regulation. Owing to their prevalence in tumor cells, G4s have emerged as promising targets for cancer therapy, with a substantial body of research demonstrating the potential of G4 ligands as anti-cancer tools. Nonetheless, a comprehensive multi-omics study to fully elucidate the mode of action of G-quadruplex ligands is still lacking. Such an investigation would be crucial for advancing the development of potent G4-based therapies against cancer. Herein, we employed a multi-omics approach, integrating transcriptomics, proteomics, and metabolomics, to identify key signaling pathways that mediate the anti-cancer effects of well-characterized G4-binding agents (berberine, pyridostatin and RHPS4) on human cervical adenocarcinoma (HeLa) cells. Particularly, we analyzed gene expression changes using RNA sequencing, quantified proteins by liquid-chromatography tandem mass spectrometry and examined metabolite levels via nuclear magnetic resonance. Our results revealed that, under the investigated experimental conditions, berberine treatment had only negligible cellular effects. In contrast, pyridostatin induced significant changes at the transcriptomic, proteomic, and metabolomic levels, decreasing the abundance of enzymes involved in cellular energy production, reducing the availability of precursors for lipid and nucleotide biosynthesis, and depleting essential cofactors and enzymes required for redox balance. Notably, RHPS4 could selectively disrupt mitochondrial activity, possibly through the specific stabilization of mitochondrial G-quadruplex structures. Overall, our findings provide a valuable multi-omics perspective on the cellular changes driven by G-quadruplex binders, that may accelerate the development of effective anti-cancer G4-targeted therapies.

KW - Berberine

KW - HeLa cells

KW - Metabolomics

KW - Proteomics

KW - Pyridostatin

KW - RHPS4

KW - Transcriptomics profiling

U2 - 10.1016/j.ijbiomac.2025.144325

DO - 10.1016/j.ijbiomac.2025.144325

M3 - Journal article

C2 - 40383348

AN - SCOPUS:105005115957

SN - 0141-8130

VL - 313

JO - International Journal of Biological Macromolecules

JF - International Journal of Biological Macromolecules

M1 - 144325

ER -