Expression of neurotensin receptor-1 (NTS1) in primary breast tumors, cellular distribution, and association with clinical and biological factors

Purpose: Neurotensin receptor-1 (NTS₁) is increasingly recognized as a potential target in diverse tumors including breast cancer, but factors associated with NTS₁ expression have not been fully clarified.

Methods: We studied NTS₁ expression using the Tissue MicroArray (TMA) of primary breast tumors from Institut Bergonié. We also studied association between NTS₁ expression and clinical, pathological, and biological parameters, as well as patient outcomes.

Results: Out of 1419 primary breast tumors, moderate to strong positivity for NTS₁ (≥ 10% of tumoral cells stained) was seen in 459 samples (32.4%). NTS₁ staining was cytoplasmic in 304 tumors and nuclear in 155 tumors, a distribution which appeared mutually exclusive. Cytoplasmic overexpression of NTS₁ was present in 21.5% of all breast tumors. In multivariate analysis, factors associated with cytoplasmic overexpression of NTS₁ in breast cancer samples were higher tumor grade, Ki67 ≥ 20%, and higher pT stage. Cytoplasmic NTS₁ was more frequent in tumors other than luminal A (30% versus 17.3%; p < 0.0001). Contrastingly, the main « correlates » of a nuclear location of NTS₁ were estrogen receptor (ER) positivity, low E&E (Elston and Ellis) grade, Ki67 < 20%, and lower pT stage. In NTS₁-positive samples, cytoplasmic expression of NTS₁ was associated with shorter 10-year metastasis-free interval (p = 0.033) compared to NTS₁ nuclear staining. Ancillary analysis showed NTS₁ expression in 73% of invaded lymph nodes from NTS₁-positive primaries.

Conclusion: NTS₁ overexpression was found in about one-third of breast tumors from patients undergoing primary surgery with two distinct patterns of distribution, cytoplasmic distribution being more frequent in aggressive subtypes. These findings encourage the development of NTS₁-targeting strategy, including radiopharmaceuticals for imaging and therapy.