Loss of Nuclear Localized and Tyrosine Phosphorylated Stat5 in Breast Cancer Predicts Poor Clinical Outcome and Increased Risk of Antiestrogen Therapy Failure

Author:

Peck Amy R.1,Witkiewicz Agnieszka K.1,Liu Chengbao1,Stringer Ginger A.1,Klimowicz Alexander C.1,Pequignot Edward1,Freydin Boris1,Tran Thai H.1,Yang Ning1,Rosenberg Anne L.1,Hooke Jeffrey A.1,Kovatich Albert J.1,Nevalainen Marja T.1,Shriver Craig D.1,Hyslop Terry1,Sauter Guido1,Rimm David L.1,Magliocco Anthony M.1,Rui Hallgeir1

Affiliation:

1. From the Kimmel Cancer Center, Thomas Jefferson University, Philadelphia; MDR Global Systems, Windber, PA; Tom Baker Cancer Centre, Alberta Cancer Board, Alberta, Canada; Walter Reed Army Medical Center, Washington, DC; University Medical Center Hamburg-Eppendorf, Hamburg, Germany; and the Yale University School of Medicine, New Haven, CT.

Abstract

Purpose To investigate nuclear localized and tyrosine phosphorylated Stat5 (Nuc-pYStat5) as a marker of prognosis in node-negative breast cancer and as a predictor of response to antiestrogen therapy. Patients and Methods Levels of Nuc-pYStat5 were analyzed in five archival cohorts of breast cancer by traditional diaminobenzidine-chromogen immunostaining and pathologist scoring of whole tissue sections or by immunofluorescence and automated quantitative analysis (AQUA) of tissue microarrays. Results Nuc-pYStat5 was an independent prognostic marker as measured by cancer-specific survival (CSS) in patients with node-negative breast cancer who did not receive systemic adjuvant therapy, when adjusted for common pathology parameters in multivariate analyses both by standard chromogen detection with pathologist scoring of whole tissue sections (cohort I; n = 233) and quantitative immunofluorescence of a tissue microarray (cohort II; n = 291). Two distinct monoclonal antibodies gave concordant results. A progression array (cohort III; n = 180) revealed frequent loss of Nuc-pYStat5 in invasive carcinoma compared to normal breast epithelia or ductal carcinoma in situ, and general loss of Nuc-pYStat5 in lymph node metastases. In cohort IV (n = 221), loss of Nuc-pYStat5 was associated with increased risk of antiestrogen therapy failure as measured by univariate CSS and time to recurrence (TTR). More sensitive AQUA quantification of Nuc-pYStat5 in antiestrogen-treated patients (cohort V; n = 97) identified by multivariate analysis patients with low Nuc-pYStat5 at elevated risk for therapy failure (CSS hazard ratio [HR], 21.55; 95% CI, 5.61 to 82.77; P < .001; TTR HR, 7.30; 95% CI, 2.34 to 22.78; P = .001). Conclusion Nuc-pYStat5 is an independent prognostic marker in node-negative breast cancer. If confirmed in prospective studies, Nuc-pYStat5 may become a useful predictive marker of response to adjuvant hormone therapy.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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