S100A8 gene copy number and protein expression in breast cancer: associations with proliferation, histopathological grade and molecular subtypes
Permanent lenke
https://hdl.handle.net/10037/30711Dato
2023-07-14Type
Journal articleTidsskriftartikkel
Peer reviewed
Forfatter
Børkja, Mathieu; Giambelluca, Miriam Soledad; Ytterhus, Borgny; Prestvik, Wenche Slettahjell; Bjørkøy, Geir; Bofin, Anna M.Sammendrag
Methods We examined S100A8 copy number (CN) alterations using fluorescence in situ hybridization in 475 primary breast cancers and 117 corresponding lymph nodes. In addition, we studied S100A8 protein expression using immunohistochemistry in 498 primary breast cancers from the same cohort.
Results We found increased S100A8 CN (≥4) in tumor epithelial cells in 20% of the tumors, increased S100A8 protein expression in 15%, and ≥10 infiltrating S100A8+polymorphonuclear cells in 19%. Both increased S100A8 CN and protein expression in cancer cells were associated with high Ki67 status, high mitotic count and high histopathological grade. We observed no association between increased S100A8 CN and S100A8 protein expression, and only a weak association (p=0.09) between increased CN and number of infiltrating S100A8+immune cells. Only S100A8 protein expression in cancer cells was associated with significantly worse prognosis.
Conclusions Amplification of S100A8 does not appear to be associated with S100A8 protein expression in breast cancer. S100A8 protein expression in tumor epithelial cells identifies a subgroup of predominantly non-luminal tumors with a high mean age at diagnosis and significantly worse prognosis. Finally, S100A8 alone is not a sufficient marker to identify infiltrating immune cells linked to worse prognosis.