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Small Molecules Targeting the RNA-Binding Protein HuR Inhibit Tumor Growth in Xenografts.

Xiaoqing WuRemya RameshJinan WangYouguang ZhengAhlam M ArmalyLanjing WeiMinli XingSudeshna RoyLan LanFei Philip GaoYinglong MiaoLiang XuJeffrey Aube
Published in: Journal of medicinal chemistry (2023)
The RNA-binding protein Hu antigen R (HuR) is a post-transcriptional regulator critical in several types of diseases, including cancer, making it a promising therapeutic target. We have identified small-molecule inhibitors of HuR through a screening approach used in combination with fragment analysis. A total of 36 new compounds originating from fragment linking or structural optimization were studied to establish structure-activity relationships in the set. Two top inhibitors, 1c and 7c , were further validated by binding assays and cellular functional assays. Both block HuR function by directly binding to the RNA-binding pocket, inhibit cancer cell growth dependence of HuR, and suppress cancer cell invasion. Intraperitoneal administration of inhibitor 1c inhibits tumor growth as a single agent and shows a synergistic effect in combination with chemotherapy docetaxel in breast cancer xenograft models. Mechanistically, 1c interferes with the HuR-TGFB/THBS1 axis.
Keyphrases
  • binding protein
  • papillary thyroid
  • small molecule
  • squamous cell
  • transcription factor
  • gene expression
  • lymph node metastasis
  • childhood cancer
  • radiation therapy
  • dna binding