Citation

  • Authors: Sun Z. et al.
  • Year: 2022
  • Journal: Carcinogenesis 43 243-253
  • Applications: in vitro / siRNA / INTERFERin
  • Cell type: DU 145
    Description: Human prostate carcinoma cells

Method

To knockdown PD-L1, 20 nM PD-L1 siRNA was transfected into cells using INTERFERin® (Polyplus-transfection) according to manufacturer's instructions.

Abstract

Numerous studies have shown that the different isoforms vitamin E have distinct activity on carcinogenesis. α-Tocopherol (α-T), the most abundant vitamin E in certain types of food and animal tissues, has demonstrated a cancer-promoting effect in a number of human clinical trials and pre-clinical studies, whereas the γ- and δ- forms of Tocopherols and Tocotrienols have exhibited significant anticancer effect in various pre-clinical studies. However, the mechanisms underlying the tumorigenic effect of α-T have not yet been fully understood. In the present study, we found that α-T was able to activate programmed death-ligand 1 (PD-L1)-mediated tumor-intrinsic signaling and immune suppression via JAK/STAT3-dependent transcriptional and ERK-dependent post-transcriptional mechanism. In line with PD-L1 induction, α-T treatment increased cancer cell viability in vitro and promoted tumor growth in LLC xenograft mouse model. The findings of the present study for the first time provided evidence that PD-L1-mediated tumor-intrinsic and immune escape mechanism contributed to the tumorigenic effect of α-T.

Go to