Drugs Targeting Tumor-Initiating Cells Prolong Survival in a Post-Surgery, Post-Chemotherapy Ovarian Cancer Relapse Model

dc.contributor.author

Harrington, Brittney S

dc.contributor.author

Ozaki, Michelle K

dc.contributor.author

Caminear, Michael W

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Hernandez, Lidia F

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Jordan, Elizabeth

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Kalinowski, Nicholas J

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Goldlust, Ian S

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Guha, Rajarshi

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Ferrer, Marc

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Thomas, Craig

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Shetty, Jyoti

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Tran, Bao

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Wong, Nathan

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House, Carrie D

dc.contributor.author

Annunziata, Christina M

dc.date.accessioned

2022-11-29T19:52:39Z

dc.date.available

2022-11-29T19:52:39Z

dc.date.updated

2022-11-29T19:52:36Z

dc.description.abstract

<jats:p>Disease recurrence is the major cause of morbidity and mortality of ovarian cancer (OC). In terms of maintenance therapies after platinum-based chemotherapy, PARP inhibitors significantly improve the overall survival of patients with BRCA mutations but is of little benefit to patients without homologous recombination deficiency (HRD). The stem-like tumor-initiating cell (TIC) population within OC tumors are thought to contribute to disease recurrence and chemoresistance. Therefore, there is a need to identify drugs that target TICs to prevent relapse in OC without HRD. RNA sequencing analysis of OC cells grown in TIC conditions revealed a strong enrichment of genes involved in drug metabolism, oxidative phosphorylation and reactive oxygen species (ROS) pathways. Concurrently, a high-throughput drug screen identified drugs that showed efficacy against OC cells grown as TICs compared to adherent cells. Four drugs were chosen that affected drug metabolism and ROS response: disulfiram, bardoxolone methyl, elesclomol and salinomycin. The drugs were tested in vitro for effects on viability, sphere formation and markers of stemness CD133 and ALDH in TICs compared to adherent cells. The compounds promoted ROS accumulation and oxidative stress and disulfiram, elesclomol and salinomycin increased cell death following carboplatin treatment compared to carboplatin alone. Disulfiram and salinomycin were effective in a post-surgery, post-chemotherapy OC relapse model in vivo, demonstrating that enhancing oxidative stress in TICs can prevent OC recurrence.</jats:p>

dc.identifier.issn

2072-6694

dc.identifier.uri

https://hdl.handle.net/10161/26241

dc.language

en

dc.publisher

MDPI AG

dc.relation.ispartof

Cancers

dc.relation.isversionof

10.3390/cancers12061645

dc.title

Drugs Targeting Tumor-Initiating Cells Prolong Survival in a Post-Surgery, Post-Chemotherapy Ovarian Cancer Relapse Model

dc.type

Journal article

pubs.begin-page

1645

pubs.end-page

1645

pubs.issue

6

pubs.organisational-group

Duke

pubs.organisational-group

School of Medicine

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Student

pubs.organisational-group

Basic Science Departments

pubs.organisational-group

Pharmacology & Cancer Biology

pubs.publication-status

Published online

pubs.volume

12

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