Adverse prognostic value of peritumoral vascular invasion: is it abrogated by adequate endocrine adjuvant therapy? Results from two International Breast Cancer Study Group randomized trials of chemoendocrine adjuvant therapy for early breast cancer
Articolo
Data di Pubblicazione:
2010
Citazione:
Adverse prognostic value of peritumoral vascular invasion: is it abrogated by adequate endocrine adjuvant therapy? Results from two International Breast Cancer Study Group randomized trials of chemoendocrine adjuvant therapy for early breast cancer / Viale, G; GIOBBIE-HARDER, A; Gusterson, B; Maiorano, E; Mastropasqua, Mg; Sonzogni, A; Mallon, E; Colleoni, M; CASTIGLIONE-GERTSCH, M; Regan, Mm; Price, Kn; Brown, Rw; Golouh, R; Crivellari, D; Karlsson, P; Öhlschlegel, C; Gelber, Rd; Goldhirsch, A; Coates, As. - In: ANNALS OF ONCOLOGY. - ISSN 0923-7534. - 21:2(2010), pp. 245-254. [10.1093/annonc/mdp317]
Abstract:
Abstract
Background
Peritumoral vascular invasion (PVI) may assist in assigning optimal adjuvant systemic therapy for women with early breast cancer.
Patients and methods
Patients participated in two International Breast Cancer Study Group randomized trials testing chemoendocrine adjuvant therapies in premenopausal (trial VIII) or postmenopausal (trial IX) node-negative breast cancer. PVI was assessed by institutional pathologists and/or central review on hematoxylin–eosin-stained slides in 99% of patients (analysis cohort 2754 patients, median follow-up >9 years).
Results
PVI, present in 23% of the tumors, was associated with higher grade tumors and larger tumor size (trial IX only). Presence of PVI increased locoregional and distant recurrence and was significantly associated with poorer disease-free survival. The adverse prognostic impact of PVI in trial VIII was limited to premenopausal patients with endocrine-responsive tumors randomized to therapies not containing goserelin, and conversely the beneficial effect of goserelin was limited to patients whose tumors showed PVI. In trial IX, all patients received tamoxifen: the adverse prognostic impact of PVI was limited to patients with receptor-negative tumors regardless of chemotherapy.
Conclusion
Adequate endocrine adjuvant therapy appears to abrogate the adverse impact of PVI in node-negative disease, while PVI may identify patients who will benefit particularly from adjuvant therapy.
Background
Peritumoral vascular invasion (PVI) may assist in assigning optimal adjuvant systemic therapy for women with early breast cancer.
Patients and methods
Patients participated in two International Breast Cancer Study Group randomized trials testing chemoendocrine adjuvant therapies in premenopausal (trial VIII) or postmenopausal (trial IX) node-negative breast cancer. PVI was assessed by institutional pathologists and/or central review on hematoxylin–eosin-stained slides in 99% of patients (analysis cohort 2754 patients, median follow-up >9 years).
Results
PVI, present in 23% of the tumors, was associated with higher grade tumors and larger tumor size (trial IX only). Presence of PVI increased locoregional and distant recurrence and was significantly associated with poorer disease-free survival. The adverse prognostic impact of PVI in trial VIII was limited to premenopausal patients with endocrine-responsive tumors randomized to therapies not containing goserelin, and conversely the beneficial effect of goserelin was limited to patients whose tumors showed PVI. In trial IX, all patients received tamoxifen: the adverse prognostic impact of PVI was limited to patients with receptor-negative tumors regardless of chemotherapy.
Conclusion
Adequate endocrine adjuvant therapy appears to abrogate the adverse impact of PVI in node-negative disease, while PVI may identify patients who will benefit particularly from adjuvant therapy.
Tipologia CRIS:
1.1 Articolo in rivista
Keywords:
Adjuvant therapy; breast cancer; endocrine responsiveness; metastasis; prognosis; vascular invasion
Elenco autori:
Viale, G; GIOBBIE-HARDER, A; Gusterson, B; Maiorano, E; Mastropasqua, Mg; Sonzogni, A; Mallon, E; Colleoni, M; CASTIGLIONE-GERTSCH, M; Regan, Mm; Price, Kn; Brown, Rw; Golouh, R; Crivellari, D; Karlsson, P; Öhlschlegel, C; Gelber, Rd; Goldhirsch, A; Coates, As
Link alla scheda completa:
Pubblicato in: