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Synthesis and biological evaluation of α-D-tocopherol derivatives as anticancer agents targeting mitochondrial metabolism
- Authors
- Kim, Younghoon ; Kim, Jungmin ; Hwang, Kyubin ; Park, Ki Cheong ; Cheong, Jae-Ho ; Sim, Taebo
- Citation
- EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY, Vol.299, 2025-12
- Article Number
- 118081
- Journal Title
- EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY
- ISSN
- 0223-5234
- Issue Date
- 2025-12
- MeSH
- Animals ; Antineoplastic Agents* / chemical synthesis ; Antineoplastic Agents* / chemistry ; Antineoplastic Agents* / pharmacology ; Apoptosis / drug effects ; Cell Line, Tumor ; Cell Proliferation / drug effects ; Dose-Response Relationship, Drug ; Drug Screening Assays, Antitumor ; Humans ; Mice ; Mitochondria* / drug effects ; Mitochondria* / metabolism ; Molecular Structure ; Stomach Neoplasms* / drug therapy ; Stomach Neoplasms* / metabolism ; Stomach Neoplasms* / pathology ; Structure-Activity Relationship ; Succinate Dehydrogenase / antagonists & inhibitors ; Succinate Dehydrogenase / metabolism ; alpha-Tocopherol* / chemical synthesis ; alpha-Tocopherol* / chemistry ; alpha-Tocopherol* / pharmacology
- Keywords
- Complex II ; Mitochondrial metabolism ; Succinate dehydrogenase (SDH) inhibitor ; Gastric cancer (GC) ; Cancer stemness ; SEM-Type GC ; Molecular targeted therapy
- Abstract
- Cancer, driven by mitochondrial and nuclear DNA mutations, presents opportunities for targeted therapies. Gastric cancer (GC), the 4th leading cause of cancer-related deaths, has poor prognosis due to cancer stem cells (CSCs), which depend on mitochondrial complex II (CII) respiration. Among CSC-enriched subtypes, the aggressive stem-like/EMT/Mesenchymal (SEM) GC subtype exhibits high plasticity, chemotherapy resistance, and metabolic adaptations that promote tumor survival. This study explores alpha-D-tocopherol derivatives targeting GC cells with enriched cancer stemness (S-cells) by inhibiting succinate dehydrogenase (SDH), also known as the CII complex. Malonate (10) and primary amide (17) derivatives of alpha-D-tocopherol showed potent anti-proliferative activities in S-cells, with GI50 values of 0.203 mu M (SSNU638) and 0.156 mu M (SSK4), respectively, over 10-fold more potent than alpha-TOS (6). Mechanistic studies showed that both 10 and 17 inhibit SDHC activity, reduce CII-specific oxygen consumption rates (OCR), and induce increased ROS production, leading to apoptosis. Furthermore, in patient-derived organoid (PDO) models, derivative 10 (GA265T GI50 = 5.623 mu M) and 17 (GA265T GI50 = 6.347 mu M) exhibited enhanced anti-proliferative activity in SEM-type GC PDOs (SDHC-high) compared to non-SEM-type PDOs (SDHC-low), with over a 2-fold increase in anti-proliferative activity against the GA265T SEM-type PDO model compared to alpha-TOS (6; GA265T GI50 = 12.660 mu M). In vivo studies further demonstrated that compound markedly inhibited tumor growth in SSK4 xenograft models with miniaml systemic toxicity, outperforming the reference compound alpha-TOS. These results support that selective targeting of SDHC by alpha-TOS derivatives 10 and 17 disrupts mitochondrial complex II function and redox homeostasis, thereby inducing apoptosis in SEM-type gastric cancer both in vitro and in vivo.
- Appears in Collections:
- 1. College of Medicine (의과대학) > BioMedical Science Institute (의생명과학부) > 1. Journal Papers
1. College of Medicine (의과대학) > Dept. of Surgery (외과학교실) > 1. Journal Papers
- Yonsei Authors
-
Kim, Jung Min(김정민)
Park, Ki Cheong(박기청)
https://orcid.org/0000-0002-3435-3985
Sim, Taebo(심태보)
Cheong, Jae Ho(정재호) https://orcid.org/0000-0002-1703-1781
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