Resumen
Breast cancer is a heterogeneous disease and treatment needs to be adapted to individual tumors. Two thirds of breast tumors may benefit from treatment with drugs targeting a specific protein, the estrogen receptor alpha, a regulator of gene expression activated by female sex hormones. However, a significant percentage of tumors will recur and progress. To help detect more accurately the expression status and activity of this protein, a gene that it upregulates, the progesterone receptor (PR), is routinely used in the clinic as an additional marker. Here, we show that PR status is an imperfect reflection of the expression and/or overall activity of estrogen receptor alpha and identify another marker that can perform this task more consistently. Overall, use of CAXII as a marker of ER+ tumors should reinforce the diagnosis of ER status and prediction of its activity and enhance the accuracy of hormonal therapy delivery.