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HIF-1α inhibition by MO-2097, a novel chiral-free benzofuran targeting hnRNPA2B1open access
- Authors
- Han, Ho Jin; Sivaraman, Aneesh; Kim, Minkyoung; Min, Kyoung Ho; Song, Mo Eun; Choi, Yongseok; Choi, Won-Jun; Han, Hyo-Kyung; Han, Junyeol; Jang, Jun-Pil; Ryoo, In-Ja; Lee, Kyeong; Soung, Nak-Kyun
- Issue Date
- Oct-2024
- Publisher
- Elsevier B.V.
- Keywords
- HIF-1α inhibition; hnRNPA2B1; Nature-inspired chiral-free benzofuran; Patient-derived cancer organoid; RNA-binding protein
- Citation
- Journal of Advanced Research, v.64, pp 67 - 81
- Pages
- 15
- Indexed
- SCIE
SCOPUS
- Journal Title
- Journal of Advanced Research
- Volume
- 64
- Start Page
- 67
- End Page
- 81
- ISSN
- 2090-1232
2090-1224
- Abstract
- Introduction: Hypoxia-inducible factor 1 (HIF-1) is a transcriptional activator mediating adaptive responses to hypoxia. It is up-regulated in the tumor microenvironment and recognized as an effective anticancer drug target. Previously, we discovered that the natural compound moracin-O and its synthetic derivative MO-460 inhibited HIF-1α via hnRNPA2B1. Objectives: This study aimed to develop novel HIF-1 inhibitors for cancer chemotherapy by harnessing the potential of the natural products moracins-O and P. Methods: In an ongoing search for novel HIF-1 inhibitors, a series of nature-inspired benzofurans with modifications on the chiral rings of moracins-O and P were synthesized. They showed improved chemical tractability and were evaluated for their inhibitory activity on HIF-1α accumulation under hypoxic conditions in HeLa CCL2 cells. The most potent derivative's chemical-based toxicities, binding affinities, and in vivo anti-tumorigenic effects were evaluated. Further, we examined whether our compound, MO-2097, exhibited anticancer effects in three-dimensional cultured organoids. Results: Herein, we identified a novel synthetic chiral-free compound, MO-2097, with reduced structural complexity and increased efficiency. MO-2097 exhibited inhibitory effects on hypoxia-induced HIF-1α accumulation in HeLa CCL2 cells via inhibition of hnRNPA2B1 protein, whose binding affinities were confirmed by isothermal titration calorimetry analysis. In addition, MO-2097 demonstrated in vivo efficacy and biocompatibility in a BALB/c mice xenograft model. The immunohistochemistry staining of MO-2097-treated tissues showed decreased expression of HIF-1α and increased levels of apoptosis marker cleaved caspase 3, confirming in vivo efficacy. Furthermore, we confirmed that MO-2097 works effectively in cancer patient-based organoid models. Conclusion: MO-2097 represents a promising new generation of chemotherapeutic agents targeting HIF-1α inhibition via hnRNPA2B1, requiring further investigation. © 2023
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Related Researcher
- Lee, Kyeong
- College of Pharmacy (Department of Pharmacy)