4.6 Article

Antiparasitic mebendazole (MBZ) effectively overcomes cisplatin resistance in human ovarian cancer cells by inhibiting multiple cancer-associated signaling pathways

AGING-US (2021)

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Journal

AGING-US
Volume 13, Issue 13, Pages 17407-17427

Publisher

IMPACT JOURNALS LLC

Keywords

ovarian cancer; cisplatin; chemoresistance; cisplatin resistance; mebendazole (MBZ); drug repurposing

Categories

Cell Biology Geriatrics & Gerontology

Funding

  1. National Institutes of Health [CA226303]
  2. Medical Scientist Training Program of the National Institutes of Health [T32 GM007281]
  3. University of Chicago Cancer Center Support Grant [P30CA014599]
  4. National Center for Advancing Translational Sciences of the National Institutes of Health [UL1 TR000430]
  5. Mabel Green Myers Research Endowment Fund
  6. University of Chicago Orthopaedics Alumni Fund
  7. University of Chicago SHOCK Fund

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Ovarian cancer is the second leading cause of gynecologic cancer death in women, and MBZ shows potential as a treatment drug by inhibiting ovarian cancer cell proliferation and migration, and inducing cell apoptosis.
Ovarian cancer is the third most common cancer and the second most common cause of gynecologic cancer death in women. Its routine clinical management includes surgical resection and systemic therapy with chemotherapeutics. While the first-line systemic therapy requires the combined use of platinum-based agents and paclitaxel, many ovarian cancer patients have recurrence and eventually succumb to chemoresistance. Thus, it is imperative to develop new strategies to overcome recurrence and chemoresistance of ovarian cancer. Repurposing previously-approved drugs is a cost-effective strategy for cancer drug discovery. The antiparasitic drug mebendazole (MBZ) is one of the most promising drugs with repurposing potential. Here, we investigate whether MBZ can overcome cisplatin resistance and sensitize chemoresistant ovarian cancer cells to cisplatin. We first established and characterized two stable and robust cisplatin-resistant (CR) human ovarian cancer lines and demonstrated that MBZ markedly inhibited cell proliferation, suppressed cell wounding healing/migration, and induced apoptosis in both parental and CR cells at low micromole range. Mechanistically, MBZ was revealed to inhibit multiple cancer-related signal pathways including ELK/SRF, NFKB, MYC/MAX, and E2F/DP1 in cisplatin-resistant ovarian cancer cells. We further showed that MBZ synergized with cisplatin to suppress cell proliferation, induce cell apoptosis, and blunt tumor growth in xenograft tumor model of human cisplatin-resistant ovarian cancer cells. Collectively, our findings suggest that MBZ may be repurposed as a synergistic sensitizer of cisplatin in treating chemoresistant human ovarian cancer, which warrants further clinical studies.

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