4.7 Article

High-Throughput/High Content Imaging Screen Identifies Novel Small Molecule Inhibitors and Immunoproteasomes as Therapeutic Targets for Chordoma

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PHARMACEUTICS
卷 15, 期 4, 页码 -

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MDPI
DOI: 10.3390/pharmaceutics15041274

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chordoma; proteasome; high-throughput screening; rare disease; cell proliferation

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Chordomas are rare bone tumors, accounting for approximately 1-4% of all malignant bone tumors and 20% of primary tumors of the spinal column. The underlying mechanism of chordoma is unknown, making it challenging to treat. In this study, a small molecule screening identified potential compounds that can inhibit chordoma cell proliferation, and proteasomal inhibitors were discovered as promising molecules for targeted therapy.
Chordomas account for approximately 1-4% of all malignant bone tumors and 20% of primary tumors of the spinal column. It is a rare disease, with an incidence estimated to be approximately 1 per 1,000,000 people. The underlying causative mechanism of chordoma is unknown, which makes it challenging to treat. Chordomas have been linked to the T-box transcription factor T (TBXT) gene located on chromosome 6. The TBXT gene encodes a protein transcription factor TBXT, or brachyury homolog. Currently, there is no approved targeted therapy for chordoma. Here, we performed a small molecule screening to identify small chemical molecules and therapeutic targets for treating chordoma. We screened 3730 unique compounds and selected 50 potential hits. The top three hits were Ribociclib, Ingenol-3-angelate, and Duvelisib. Among the top 10 hits, we found a novel class of small molecules, including proteasomal inhibitors, as promising molecules that reduce the proliferation of human chordoma cells. Furthermore, we discovered that proteasomal subunits PSMB5 and PSMB8 are increased in human chordoma cell lines U-CH1 and U-CH2, confirming that the proteasome may serve as a molecular target whose specific inhibition may lead to better therapeutic strategies for chordoma.

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