1. Academic Validation
  2. Rational discovery of novel type-III FTF antagonists to competitively suppress TIF-2 coactivation in liver cancer

Rational discovery of novel type-III FTF antagonists to competitively suppress TIF-2 coactivation in liver cancer

  • J Recept Signal Transduct Res. 2019 Aug;39(4):304-311. doi: 10.1080/10799893.2019.1690513.
Linlin Xu 1 Zhongming Chen 1 Keke Shao 1 Yungang Wang 1 Leilei Cui 1 Naizhou Guo 1
Affiliations

Affiliation

  • 1 Department of Laboratory Medicine, The First People's Hospital of Yancheng City, the Fourth Affiliated Hospital of Nantong University, Yancheng, China.
Abstract

The α-fetoprotein transcription factor (FTF) is a member of the nuclear receptor NR5A subfamily, which is involved in the pathogenesis of liver Cancer and some Other gastrointestinal cancers. The protein's transcriptional activity is regulated by binding TIF-2 coactivator at its coactivator-interacting site (CIS); suppression of the transcriptional activity has been recognized as a potential therapeutic strategy against Cancer. Previously, small-molecule antagonists have been developed to target the ligand-binding site (LBS) of FTF ligand-binding domain, which simply occupy the site to exclusively block natural ligand entry (type-I antagonists) or destabilize the agonist conformation of activation helix 12 of the domain (type-II antagonists). Here, we describe the use of small-molecule competitors (type-III antagonists) to directly disrupt FTF-TIF-2 interaction by competitively targeting FTF CIS site. High-throughput virtual screening is performed against a structurally diverse, commercially available compound library to identify FTF CIS Binders as competitor candidates, from which 12 hits are manually selected and their competitive potency with TIF-2 core binding sequence for FTF CIS site is tested with CC50 values up to 2.5 μM. Structural modeling analysis revealed that the competitive ligands can form a complicated network of noncovalent interactions to specifically or nonspecifically pack against FTF CIS site, thus preventing TIF-2 from binding to the site.

Keywords

coactivator; liver cancer; transcriptional mediator/intermediary factor 2; type-III antagonist; α-fetoprotein transcription factor.

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