Your search keyword '"Elia, Andrés"' showing total 2 results

1. Progesterone receptor isoform ratio dictates antiprogestin/progestin effects on breast cancer growth and metastases: A role for NDRG1.

Author

Abascal, María Florencia, Elia, Andrés, Alvarez, Michelle, Pataccini, Gabriela, Sequeira, Gonzalo, Riggio, Marina, Figueroa, Virginia, Lamb, Caroline A., Rojas, Paola A., Spengler, Eunice, Martínez‐Vazquez, Paula, Burruchaga, Javier, Liguori, Marcos, Sahores, Ana, Wargon, Victoria, Molinolo, Alfredo, Hewitt, Stephen, Lombes, Marc, Sartorius, Carol, and Vanzulli, Silvia Inés

Subjects

PROGESTATIONAL hormones, PROGESTERONE receptors, TUMOR suppressor proteins, LYMPHATIC metastasis, PROGESTERONE antagonists

Abstract

Progesterone receptors (PRs) ligands are being tested in luminal breast cancer. There are mainly two PR isoforms, PRA and PRB, and their ratio (PRA/PRB) may be predictive of antiprogestin response. Our aim was to investigate: the impact of the PR isoform ratio on metastatic behaviour, the PR isoform ratio in paired primary tumours and lymph node metastases (LNM) and, the effect of antiprogestin/progestins on metastatic growth. Using murine and human metastatic models, we demonstrated that tumours with PRB > PRA (PRB‐H) have a higher proliferation index but less metastatic ability than those with PRA > PRB (PRA‐H). Antiprogestins and progestins inhibited metastatic burden in PRA‐H and PRB‐H models, respectively. In breast cancer samples, LNM retained the same PRA/PRB ratio as their matched primary tumours. Moreover, PRA‐H LNM expressed higher total PR levels than the primary tumours. The expression of NDRG1, a metastasis suppressor protein, was higher in PRB‐H compared to PRA‐H tumours and was inversely regulated by antiprogestins/progestins. The binding of the corepressor SMRT at the progesterone responsive elements of the NDRG1 regulatory sequences, together with PRA, impeded its expression in PRA‐H cells. Antiprogestins modulate the interplay between SMRT and AIB1 recruitment in PRA‐H or PRB‐H contexts regulating NDRG1 expression and thus, metastasis. In conclusion, we provide a mechanistic interpretation to explain the differential role of PR isoforms in metastatic growth and highlight the therapeutic benefit of using antiprogestins in PRA‐H tumours. The therapeutic effect of progestins in PRB‐H tumours is suggested. [ABSTRACT FROM AUTHOR]

Published

2022

2. Progesterone Receptor Isoform Ratio: A Breast Cancer Prognostic and Predictive Factor for Antiprogestin Responsiveness.

Author

Rojas, Paola A., May, María, Sequeira, Gonzalo R., Elia, Andrés, Alvarez, Michelle, Martínez, Paula, Gonzalez, Pedro, Hewitt, Stephen, Xiaping He, Perou, Charles M., Molinolo, Alfredo, Gibbons, Luz, Abba, Martin C., Gass, Hugo, Lanari, Claudia, and He, Xiaping

Subjects

PROGESTERONE receptors, BREAST cancer, IMMUNOBLOTTING, IMMUNOASSAY, CHEST (Anatomy), MIFEPRISTONE, HORMONE antagonists, BREAST tumors, CELL physiology, CELL receptors, GENES, IMMUNOHISTOCHEMISTRY, PROGESTATIONAL hormones, PROGNOSIS, TREATMENT effectiveness, PREDICTIVE tests, OLIGONUCLEOTIDE arrays, TISSUE arrays, GENE expression profiling, CANCER cell culture, CHEMICAL inhibitors, THERAPEUTICS

Abstract

Background: Compelling evidence shows that progestins regulate breast cancer growth. Using preclinical models, we demonstrated that antiprogestins are inhibitory when the level of progesterone receptor isoform A (PR-A) is higher than that of isoform B (PR-B) and that they might stimulate growth when PR-B is predominant. The aims of this study were to investigate ex vivo responses to mifepristone (MFP) in breast carcinomas with different PR isoform ratios and to examine their clinical and molecular characteristics.Methods: We performed human breast cancer tissue culture assays (n = 36) to evaluate the effect of MFP on cell proliferation. PR isoform expression was determined by immunoblotting (n = 282). Tumors were categorized as PRA-H (PR-A/PR-B ≥ 1.2) or PRB-H (PR-A/PR-B ≤ 0.83). RNA was extracted for Ribo-Zero-Seq sequencing to evaluate differentially expressed genes. Subtypes and risk scores were predicted using the PAM50 gene set, the data analyzed using The Cancer Genome Atlas RNA-seq gene analysis and other publicly available gene expression data. Tissue microarrays were performed using paraffin-embedded tissues (PRA-H n = 53, PRB-H n = 24), and protein expression analyzed by immunohistochemistry. All statistical tests were two-sided.Results: One hundred sixteen out of 222 (52.3%) PR+ tumors were PRA-H, and 64 (28.8%) PRB-H. Cell proliferation was inhibited by MFP in 19 of 19 tissue cultures from PRA-H tumors. A total of 139 transcripts related to proliferative pathways were differentially expressed in nine PRA-H and seven PRB-H tumors. PRB-H and PRA-H tumors were either luminal B or A phenotypes, respectively ( P = .03). PRB-H cases were associated with shorter relapse-free survival (hazard ratio [HR] = 2.70, 95% confidence interval [CI] = 1.71 to 6.20, P = .02) and distant metastasis-free survival (HR = 4.17, 95% CI = 2.18 to 7.97, P <  .001). PRB-H tumors showed increased tumor size ( P <  .001), Ki-67 levels ( P <  .001), human epidermal growth factor receptor 2 expression ( P =  .04), high grades ( P =  .03), and decreased total PR ( P =  .004) compared with PRA-H tumors. MUC-2 ( P <  .001) and KRT6A ( P =  .02) were also overexpressed in PRB-H tumors.Conclusion: The PRA/PRB ratio is a prognostic and predictive factor for antiprogestin responsiveness in breast cancer. [ABSTRACT FROM AUTHOR]

Published

2017