The screening of compounds regulating PD‐L1 transcriptional activity in a cell functional high‐throughput manner

Immune checkpoints are protein molecules expressed on the immune cell membrane, which regulate the immune system to kill tumor cells. As an essential immune checkpoint, overexpressed PD‐1 on tumor cells could inhibit T‐cell activation after being bonded to PD‐1. Due to this inhibitory effect, T‐cell...

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Published inCancer medicine (Malden, MA) Vol. 12; no. 8; pp. 9815 - 9825
Main Authors Zhang, Lanxin, Li, Hexin, Liu, Jingchao, Sun, Gaoyuan, Tang, Xiaokun, Xu, Siyuan, Zhang, Lili, Zhang, Wei, Ai, Bin
Format Journal Article
LanguageEnglish
Published United States John Wiley & Sons, Inc 01.04.2023
John Wiley and Sons Inc
Wiley
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Summary:Immune checkpoints are protein molecules expressed on the immune cell membrane, which regulate the immune system to kill tumor cells. As an essential immune checkpoint, overexpressed PD‐1 on tumor cells could inhibit T‐cell activation after being bonded to PD‐1. Due to this inhibitory effect, T‐cell proliferation and cytokine secretion are suppressed, leading to immune escape of tumor cells. Here, we established a high‐throughput method based on cell function screening technology to screen drugs regulating PD‐L1 expression in tumor cells at the transcriptional level. After two screening rounds, 12 compounds that enhanced PD‐L1 transcription while seven weakened were sorted out among 1018 FDA‐approved drugs. Finally, a tumor cell line was used to verify the upregulation of endogenous PD‐L1 expression for a drug named “vorinostat,” a histone deacetylation inhibitor, after the two rounds of optional selection. Therefore, our research provides another perspective for using “vorinostat” in treating tumors and offers a convenient method to detect the transcriptional expression of other intracellular proteins besides PD‐L1. The screening process of small molecular chemical drugs regulating transcriptional PD‐L1 via cell‐based high‐throughput screening system.
Bibliography:Lanxin Zhang and Hexin Li have contributed equally to this work.
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ISSN:2045-7634
2045-7634
DOI:10.1002/cam4.5744