期刊
NEURO-ONCOLOGY
卷 24, 期 9, 页码 1438-1451出版社
OXFORD UNIV PRESS INC
DOI: 10.1093/neuonc/noac041
关键词
diffuse midline glioma (DMG); ClpP; integrated stress response (ISR); ONC201; ONC206
资金
- Isabella Kerr Molina Foundation (London UK)
- ChadTough Defeat DIPG Foundation (Saline, MI)
- We Love You Connie Foundation (Ontario, CA)
- Yuvaan Tiwari Foundation (Atlanta, GA)
- Kortney Rose Foundation (Oceanport, NJ)
- Minderoo Foundation (Perth, Australia)
- Storm the Heaven Foundation (Philadelphia, PA)
- in Memory of Austin Klaus (Hamburg Germany)
- Smashing Walnuts Fund (Middleburg, VA)
- Rising Tide Foundation (Schaffhausen, Switzerland)
- V Foundation (Atlanta, GA)
- Musella Foundation (Hewlett, NY)
- PNOC Foundation (San Rafael, CA)
- Prayers from Maria (Rocky River, OH)
- Matthew Larson Foundation (Franklin Lake, NJ)
- Run DIPG Foundation (St Leonards, NSW)
- Lilabean Foundation for Pediatric Brain Cancer Research (Silver Spring, MD)
- The Swifty Foundation (Woodridge, IL)
- Child Initiative, The Swiss National Science Foundation (SNSF) [CRSII5-198739]
- Kisses 4 Kayla Foundation (Willow Grove, PA)
- Brad Kaminsky Foundation (Ashburn VA)
- NIH Gabriella Miller Kids First funds [U2CHL138346]
- Swiss National Science Foundation (SNF) [CRSII5_198739] Funding Source: Swiss National Science Foundation (SNF)
The imipridone ONC201 and its derivative ONC206 significantly reduce cell viability in pediatric diffuse midline gliomas (DMGs) and prolong the survival of DMG PDX models. Both drugs impair tumor cell growth and survival by activating mitochondrial metabolism and the integrative stress response (ISR), and trigger cell lineage differentiation. These findings are of great importance for the treatment of pediatric DMGs.
Background Pediatric diffuse midline gliomas (DMGs) are incurable childhood cancers. The imipridone ONC201 has shown early clinical efficacy in a subset of DMGs. However, the anticancer mechanisms of ONC201 and its derivative ONC206 have not been fully described in DMGs. Methods DMG models including primary human in vitro (n = 18) and in vivo (murine and zebrafish) models, and patient (n = 20) frozen and FFPE specimens were used. Drug-target engagement was evaluated using in silico ChemPLP and in vitro thermal shift assay. Drug toxicity and neurotoxicity were assessed in zebrafish models. Seahorse XF Cell Mito Stress Test, MitoSOX and TMRM assays, and electron microscopy imaging were used to assess metabolic signatures. Cell lineage differentiation and drug-altered pathways were defined using bulk and single-cell RNA-seq. Results ONC201 and ONC206 reduce viability of DMG cells in nM concentrations and extend survival of DMG PDX models (ONC201: 117 days, P = .01; ONC206: 113 days, P = .001). ONC206 is 10X more potent than ONC201 in vitro and combination treatment was the most efficacious at prolonging survival in vivo (125 days, P = .02). Thermal shift assay confirmed that both drugs bind to ClpP, with ONC206 exhibiting a higher binding affinity as assessed by in silico ChemPLP. ClpP activation by both drugs results in impaired tumor cell metabolism, mitochondrial damage, ROS production, activation of integrative stress response (ISR), and apoptosis in vitro and in vivo. Strikingly, imipridone treatment triggered a lineage shift from a proliferative, oligodendrocyte precursor-like state to a mature, astrocyte-like state. Conclusion Targeting mitochondrial metabolism and ISR activation effectively impairs DMG tumorigenicity. These results supported the initiation of two pediatric clinical trials (NCT05009992, NCT04732065).
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