Discovery of Pyrrole-imidazole Polyamides as PD-L1 Expression Inhibitors and Their Anticancer Activity via Immune and Nonimmune Pathways.
Ming WangXudong MaKang ZhouHuijuan MaoJiachun LiuXuqiong XiongXiaoyin ZhaoSuresh NarvaYoshimasa TanakaYanling WuChuanxin GuoHiroshi SugiyamaWen ZhangPublished in: Journal of medicinal chemistry (2021)
In recent years, PD-1 immune checkpoint inhibitors based on monoclonal antibodies have revolutionized cancer therapy, but there still exist unresolved issues, such as the high cost, the relatively low response rates, and so on, compared with small-molecule drugs. Herein a type of pyrrole-imidazole (Py-Im) polyamide as a small-molecule DNA binder was designed and synthesized, which could competitively bind to the same double-stranded DNA stretch in the PD-L1 promoter region as the STAT3 binding site and thus downregulate PD-L1 expression. It was demonstrated that the Py-Im polyamides directly caused apoptosis in tumor cells and retarded cell migration in the absence of T cells through inhibiting the Akt/caspase-3 pathway. Also, in a coculture system, they enhanced the T-cell-mediated killing of tumor cells by the reversal of immune escape. Because such polyamides induced antitumor effects via both immune and nonimmune pathways, they could be further developed as promising PD-L1 gene-targeting antitumor drugs.
Keyphrases
- small molecule
- cancer therapy
- cell migration
- protein protein
- circulating tumor
- signaling pathway
- cell death
- cell proliferation
- cell free
- drug delivery
- single molecule
- oxidative stress
- dna methylation
- nucleic acid
- endoplasmic reticulum stress
- gene expression
- transcription factor
- drug induced
- high glucose
- genome wide
- cell cycle arrest
- binding protein
- genome wide identification