Acta Pharmaceutica Sinica B (Oct 2024)

PKCα inhibitors promote breast cancer immune evasion by maintaining PD-L1 stability

  • Jiaojiao Yu,
  • Yujin Xiang,
  • Yuzhen Gao,
  • Shan Chang,
  • Ren Kong,
  • Xiaoxi Lv,
  • Jinmei Yu,
  • Yunjie Jin,
  • Chenxi Li,
  • Yiran Ma,
  • Zhenhe Wang,
  • Jichao Zhou,
  • Hongyu Yuan,
  • Shuang Shang,
  • Fang Hua,
  • Xiaowei Zhang,
  • Bing Cui,
  • Pingping Li

Journal volume & issue
Vol. 14, no. 10
pp. 4378 – 4395

Abstract

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Protein kinase C α (PKCα) regulates diverse biological functions of cancer cells and is a promising therapeutic target. However, clinical trials of PKC-targeted therapies have not yielded satisfactory results. Recent studies have also indicated a tumor-suppressive role of PKCs via unclear molecular mechanisms. In this study, we found that PKCα inhibition enhances CD8+ T-cell-mediated tumor evasion and abolishes antitumor activity in immunocompetent mice. We further identified PKCα as a critical regulator of programmed cell death-ligand 1 (PD-L1) and found that it enhances T-cell-dependent antitumor immunity in breast cancer by interacting with PD-L1 and suppressing PD-L1 expression. We demonstrated that PKCα-mediated PD-L1 phosphorylation promotes PD-L1 degradation through β transducin repeat-containing protein. Notably, the efficacy of PKCα inhibitors was intensified by synergizing with anti-PD-L1 mAb therapy to boost antitumor T-cell immunity in vivo. Clinical analysis revealed that PKCα expression is positively correlated with T-cell function and the interferon-gamma signature in patients with breast cancer. This study demonstrated the antitumor capability of PKCα, identified potential therapeutic strategies to avoid tumor evasion via PKC-targeted therapies, and provided a proof of concept for targeting PKCα in combination with anti-PD-L1 mAb therapy as a potential therapeutic approach against breast cancer, especially TNBC.

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