AI Article Synopsis

  • STING (Stimulator of Interferon Genes) signaling plays a vital role in how cancers respond to immunotherapy, but measuring its activation remains challenging.
  • A new immunohistochemistry-based assay reveals that high levels of perinuclear-localized STING (pnSTING) in estrogen receptor-positive breast cancer (ER+) are linked to better patient outcomes and increased immune activity.
  • In contrast, low pnSTING levels in ER+ tumors predict poor prognosis and are associated with chromosomal instability and specific genetic alterations, indicating potential new treatment strategies for this subgroup.

Article Abstract

STING signaling in cancer is a crucial component of response to immunotherapy and other anti-cancer treatments. Currently, there is no robust method of measuring STING activation in cancer. Here, we describe an immunohistochemistry-based assay with digital pathology assessment of STING in tumor cells. Using this novel approach in estrogen receptor-positive (ER+) and ER- breast cancer, we identify perinuclear-localized expression of STING (pnSTING) in ER+ cases as an independent predictor of good prognosis, associated with immune cell infiltration and upregulation of immune checkpoints. Tumors with low pnSTING are immunosuppressed with increased infiltration of "M2"-polarized macrophages. In ER- disease, pnSTING does not appear to have a significant prognostic role with STING uncoupled from interferon responses. Importantly, a gene signature defining low pnSTING expression is predictive of poor prognosis in independent ER+ datasets. Low pnSTING is associated with chromosomal instability, MYC amplification and mTOR signaling, suggesting novel therapeutic approaches for this subgroup.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8233333PMC
http://dx.doi.org/10.1038/s41523-021-00283-zDOI Listing

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