Lomitapide enhances cytotoxic effects of temozolomide in chemotherapy-resistant glioblastoma
Alyona Ivanova, Taylor M. Wilson, Kimia Ghannad-Zadeh, Esmond Tse, Robert Flick, Megan Wu, Sunit Das
Alyona Ivanova, Taylor M. Wilson, Kimia Ghannad-Zadeh, Esmond Tse, Robert Flick, Megan Wu, Sunit Das
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Research Article Cell biology Oncology

Lomitapide enhances cytotoxic effects of temozolomide in chemotherapy-resistant glioblastoma

Abstract

More than a third of patients with glioblastoma experience tumor progression during adjuvant therapy. In this study, we performed a high-throughput drug repurposing screen of FDA-approved agents capable of crossing the blood-brain barrier in order to find agents to counteract acquired or inherent glioma cell resistance to temozolomide-associated cytotoxicity. We identified the cholesterol processing inhibitor, lomitapide, as a potential chemosensitizer in glioblastoma. In vitro treatment of temozolomide-resistant glioblastoma cells with lomitapide resulted in decreased intracellular ubiquinone levels and sensitized cells to temozolomide-induced ferroptosis. Concomitant treatment with lomitapide and temozolomide (TMZ) prolonged survival and delayed tumor recurrence in a mouse glioblastoma model, compared with treatment xwith TMZ alone. Our data identified lomitapide as a potential adjunct for treatment of temozolomide-resistant glioblastoma.

Authors

Alyona Ivanova, Taylor M. Wilson, Kimia Ghannad-Zadeh, Esmond Tse, Robert Flick, Megan Wu, Sunit Das

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Figure 2

Lomitapide targets GBM cells and sensitizes them to the effects of TMZ, while minimizing damage to normal cells.

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Lomitapide targets GBM cells and sensitizes them to the effects of TMZ, ...
Cytotoxicity estimated at 72 hours after treatment by Cell Viability Assay. Compared with TMZ alone, CTL-(A) and TR-U251 (B) cell lines treated concomitantly with lomitapide and TMZ had significantly decreased cell viability. Concentration of lomitapide near its IC80 value added in combination with TMZ significantly reduces cell viability, compared with TMZ treatment alone in GSC lines GliNS1 (C), 811 (D), 818 (E). CTL-U251 (F), TR-U251 (G), GliNS1 (H), 811 (I), 818 (J) cells treated with doses of TMZ 0–100 μM with or without lomitapide. Cell viability normalized to 2 μM lomitapide treatment without TMZ for CTL-U251 and TR-U251 cells. Data in AG is presented as individual measurements with mean ± SD. Data is normalized to untreated control, mean ± SD (HJ). (K and L) Dose-response curves. Data is represented as mean ± SD (K), individual measurements (L) are normalized to untreated control with mean ± SD. 2-tailed Student’s t tests were used for statistical comparisons between 2 groups. **P < 0.01; ***P < 0.001; ****P < 0.0001.