Nature Communications (Oct 2024)

Aberrant cytoplasmic expression of UHRF1 restrains the MHC-I-mediated anti-tumor immune response

  • Lianmei Tan,
  • Tao Yin,
  • Handan Xiang,
  • Liuyang Wang,
  • Poorva Mudgal,
  • Junying Chen,
  • Yi Ding,
  • Guoping Wang,
  • Bryan Jian Wei Lim,
  • Yuqi Huang,
  • De Huang,
  • Yaosi Liang,
  • Peter B. Alexander,
  • Kun Xiang,
  • Ergang Wang,
  • Chengsong Yan,
  • Zhehao Ma,
  • Minjia Tan,
  • Qi-Jing Li,
  • Xiao-Fan Wang

DOI
https://doi.org/10.1038/s41467-024-52902-5
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 15

Abstract

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Abstract Immunotherapy successfully complements traditional cancer treatment. However, primary and acquired resistance might limit efficacy. Reduced antigen presentation by MHC-I has been identified as potential resistance factor. Here we show that the epigenetic regulator ubiquitin-like with PHD and ring finger domains 1 (UHRF1), exhibits altered expression and aberrant cytosolic localization in cancerous tissues, where it promotes MHC-I ubiquitination and degradation. Cytoplasmic translocation of UHRF1 is induced by its phosphorylation on a specific serine in response to signals provided by factors present in the tumor microenvironment (TME), such as TGF-β, enabling UHRF1 to bind MHC-I. Downregulation of MHC-I results in suppression of the antigen presentation pathway to establish an immune hostile TME. UHRF1 inactivation by genetic deletion synergizes with immune checkpoint blockade (ICB) treatment and induces an anti-tumour memory response by evoking low-affinity T cells. Our study adds to the understanding of UHRF1 in cancer immune evasion and provides a potential target to synergize with immunotherapy and overcome immunotherapeutic resistance.