Open Access

Cell Death and Disease

, volume 16 , issue 1 , publication number 342

Targeting metabolic vulnerability by combining NAMPT inhibitors and disulfiram for treatment of recurrent ovarian cancer

Kei KUDO ^{1, 2}

Yoshimi Endo Greer ¹

Daniel R Crooks ^{3, 4}

Ye Yang ^{3, 4}

Jeffrey R Brender ^{3, 4}

Teruhiko YOSHIDA ⁵

Brittney S Harrington ¹

Rahul Kamdar ¹

Soumya Korrapati ¹

Yusuke Shibuya ²

Leah Henegar ⁶

Jeffrey Kopp ⁵

Takeo Fujii ¹

Stanley Lipkowitz ¹

Christina M. Annunziata ¹

Hide authors affiliations Show authors affiliations: 6 affiliations

Women’s Malignancies Branch, National Cancer Institute, National Institutes of Health, Bethesda, USA |

Department of Obstetrics and Gynecology, Division of Gynecologic Oncology, Tohoku University School of Medicine, Miyagi, Japan |

Urologic Oncology Branch, National Cancer Institute, National Institutes of Health, Bethesda, USA |

⁴

Clinical Cancer Metabolism Facility, Center for Cancer Research, National Cancer Institute, Bethesda, USA |

⁵

Kidney Disease Section, Kidney Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, USA |

⁶

Karyopharm Therapeutics, Newton, USA |

Publication type: Journal Article

Publication date: 2025-04-25

Springer Nature

Cell Death and Disease

scimago Q1

wos Q1

SJR: 2.773

CiteScore: 15.4

Impact factor: 9.6

ISSN: 20414889

DOI: 10.1038/s41419-025-07672-3

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Abstract

Ovarian cancer (OV) has the highest mortality rate among gynecological cancers. As OV progresses, tumor cells spread outside the ovaries to the peritoneal and abdominal cavities, forming cell clusters that float in the ascitic fluid caused by peritonitis carcinomatosa, leading to further dissemination and metastasis. These cell clusters are enriched with cancer stem cells (CSCs) which are responsible for treatment resistance, recurrence, and metastasis. Therefore, targeting CSCs is a potentially effective approach for treating OV. However, understanding how CSCs acquire treatment resistance and identifying targets against CSCs remains challenging. In this study, we demonstrate that 3D-spheroids of OV cell lines exhibit higher stemness than conventional adherent cells. Metabolomics profiling studies have revealed that 3D-spheroids maintain a high-energy state through increased glucose utilization in the citric acid cycle (TCA), efficient nucleotide phosphorylation, and elevated phosphocreatine as an energy buffer. We also found that nicotinamide phosphoribosyltransferase (NAMPT), the rate-limiting enzyme for NAD⁺ production, is highly expressed in OV. Furthermore, the approach based on NAMPT dependence rather than histology found NAMPT to be a potential therapeutic target against CSCs, while also serving as a prognostic indicator in OV. Moreover, we identified a previously unrecognized anti-tumor mechanism whereby disulfiram, an aldehyde dehydrogenase (ALDH) inhibitor, synergistically inhibited mitochondrial function when combined with NAMPT inhibitors - leading to cell cycle arrest in G2/M. Finally, the combination of a NAMPT inhibitor and disulfiram showed significant anti-tumor effects and extended survival in an animal model. Our findings demonstrate the potential of spheroids as a preclinical model for targeting OV CSCs and also indicate that the combination of NAMPT inhibitors and disulfiram is a promising therapeutic strategy to overcome recurrent OV.

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KUDO K. et al. Targeting metabolic vulnerability by combining NAMPT inhibitors and disulfiram for treatment of recurrent ovarian cancer // Cell Death and Disease. 2025. Vol. 16. No. 1. 342

GOST all authors (up to 50) Copy

KUDO K., Greer Y. E., Crooks D. R., Yang Y., Brender J. R., YOSHIDA T., Harrington B. S., Kamdar R., Korrapati S., Shibuya Y., Henegar L., Kopp J., Fujii T., Lipkowitz S., Annunziata C. M. Targeting metabolic vulnerability by combining NAMPT inhibitors and disulfiram for treatment of recurrent ovarian cancer // Cell Death and Disease. 2025. Vol. 16. No. 1. 342

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RIS Copy

TY - JOUR

DO - 10.1038/s41419-025-07672-3

UR - https://www.nature.com/articles/s41419-025-07672-3

TI - Targeting metabolic vulnerability by combining NAMPT inhibitors and disulfiram for treatment of recurrent ovarian cancer

T2 - Cell Death and Disease

AU - KUDO, Kei

AU - Greer, Yoshimi Endo

AU - Crooks, Daniel R

AU - Yang, Ye

AU - Brender, Jeffrey R

AU - YOSHIDA, Teruhiko

AU - Harrington, Brittney S

AU - Kamdar, Rahul

AU - Korrapati, Soumya

AU - Shibuya, Yusuke

AU - Henegar, Leah

AU - Kopp, Jeffrey

AU - Fujii, Takeo

AU - Lipkowitz, Stanley

AU - Annunziata, Christina M.

PY - 2025

DA - 2025/04/25

PB - Springer Nature

IS - 1

VL - 16

SN - 2041-4889

ER -

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BibTex (up to 50 authors) Copy

@article{2025_KUDO,

author = {Kei KUDO and Yoshimi Endo Greer and Daniel R Crooks and Ye Yang and Jeffrey R Brender and Teruhiko YOSHIDA and Brittney S Harrington and Rahul Kamdar and Soumya Korrapati and Yusuke Shibuya and Leah Henegar and Jeffrey Kopp and Takeo Fujii and Stanley Lipkowitz and Christina M. Annunziata},

title = {Targeting metabolic vulnerability by combining NAMPT inhibitors and disulfiram for treatment of recurrent ovarian cancer},

journal = {Cell Death and Disease},

year = {2025},

volume = {16},

publisher = {Springer Nature},

month = {apr},

url = {https://www.nature.com/articles/s41419-025-07672-3},

number = {1},

pages = {342},

doi = {10.1038/s41419-025-07672-3}

}

Publisher

Springer Nature

Journal

Cell Death and Disease

scimago Q1

wos Q1

SJR

2.773

CiteScore

15.4

Impact factor

9.6

ISSN

20414889 (Electronic)

Profiles

Stanley Lipkowitz