4.5 Article

A novel biguanide (IM1761065) inhibits bioenergetics of glioblastoma tumorspheres

JOURNAL OF NEURO-ONCOLOGY (2022)

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Journal

JOURNAL OF NEURO-ONCOLOGY
Volume 156, Issue 1, Pages 139-151

Publisher

SPRINGER
DOI: 10.1007/s11060-021-03903-7

Keywords

Biguanide; Glioblastoma; Tumorsphere; IM1761065; Bioenergetics

Categories

Oncology Clinical Neurology

Funding

  1. National Research Foundation of Korea (NRF) - Korean government (MSIT) [NRF-2019R1A2C3004155]
  2. NRF - Ministry of Science ICT [NRF-2020M3E5E2037960, NRF-2020M2D9A2092372, NRF-2020M3A9E8024890]
  3. Team Science Award of Yonsei University College of Medicine [6-2021-0006]

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IM1761065 is a potent inhibitor of oxidative phosphorylation in GBM-TS, showing significant effects on reducing viability, stemness, and invasive properties of tumorspheres. The compound also exhibited promising results in in vivo mouse models, suggesting its potential as a new drug for GBM treatment.
Purpose Glioblastoma (GBM) is a rapidly growing tumor in the central nervous system with altered metabolism. Depleting the bioenergetics of tumors with biguanides have been suggested as an effective therapeutic approach for treating GBMs. The purpose of this study was to determine the effects of IM1761065, a novel biguanide with improved pharmacokinetics, on GBM-tumorspheres (TSs). Methods The biological activities of IM1761065 on GBM-TSs, including their effects on viability, ATP levels, cell cycle, stemness, invasive properties, and transcriptomes were examined. The in vivo efficacy of IM1761065 was tested in a mouse orthotopic xenograft model. Results IM1761065 decreased the viability and ATP levels of GBM-TSs in a dose-dependent manner, and reduced basal and spare respiratory capacity in patient-derived GBM-TS, as measured by the oxygen consumption rate. Sphere formation, expression of stemness-related proteins, and invasive capacity of GBM-TSs were also significantly suppressed by IM1761065. A gene-ontology comparison of IM1761065-treated groups showed that the expression levels of stemness-related, epithelial mesenchymal transition-related, and mitochondrial complex I genes were also significantly downregulated by IM1761065. An orthotopic xenograft mouse model showed decreased bioluminescence in IM1761065-treated cell-injected mice at 5 weeks. IM1761065-treated group showed longer survival than the control group (P = 0.0289, log-rank test). Conclusion IM1761065 is a potent inhibitor of oxidative phosphorylation. The inhibitory effect of IM1761065 on the bioenergetics of GBM-TS suggests that this novel compound could be used as a new drug for the treatment of GBM.

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