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Post-diagnostic beta blocker use and breast cancer-specific mortality: a population-based cohort study

Oliver William Scott, Sandar Tin Tin, Mark Elwood, Alana Cavadino, Laurel A. Habel, Marion Kuper‐Hommel, Ian Campbell, Ross Lawrenson

2022Breast Cancer Research and Treatment17 citationsDOIOpen Access PDF

Abstract

PURPOSE: Beta blockers (BB) have been associated with improved, worsened, or unchanged breast cancer outcomes in previous studies. This study examines the association between the post-diagnostic use of BBs and death from breast cancer in a large, representative sample of New Zealand (NZ) women with breast cancer. METHODS: Women diagnosed with a first primary breast cancer between 2007 and 2016 were identified from four population-based regional NZ breast cancer registries and linked to national pharmaceutical data, hospital discharges, and death records. The median follow-up time was 4.51 years. Cox proportional hazard models were used to estimate the hazard of breast cancer-specific death (BCD) associated with any post-diagnostic BB use. RESULTS: Of the 14,976 women included in analyses, 21% used a BB after diagnosis. BB use (vs non-use) was associated with a small and nonstatistically significant increased risk of BCD (adjusted hazard ratio: 1.11; 95% CI 0.95-1.29). A statistically significant increased risk confined to short-term use (0-3 months) was seen (HR = 1.40; 1.14-1.73), and this risk steadily decreased with increasing duration of use and became a statistically significant protective effect at 3 + years of use (HR = 0.55; 0.34-0.88). CONCLUSION: Our findings suggest that any increased risk associated with BB use may be driven by risk in the initial few months of use. Long-term BB use may be associated with a reduction in BCD.

Topics & Concepts

MedicineBreast cancerHazard ratioProportional hazards modelCancerInternal medicinePopulationCohortOncologyCohort studyCause of deathGynecologyConfidence intervalDiseaseEnvironmental healthCancer, Stress, Anesthesia, and Immune ResponseInflammatory mediators and NSAID effectsReceptor Mechanisms and Signaling
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