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PMID-35862873 – Twenty-Year Benefit From Adjuvant Goserelin in Breast Cancer

PMID-35862873 – Twenty-Year Benefit From Adjuvant Goserelin in Breast Cancer

Johansson A, Dar H, van 't Veer LJ, Tobin NP, Perez-Tenorio G, Nordenskjold A, Johansson U, Hartman J, Skoog L, Yau C, Benz CC, Esserman LJ, Stal O, Nordenskjold B, Fornander T, Lindstrom LS. Twenty-Year Benefit From Adjuvant Goserelin and Tamoxifen in Premenopausal Patients With Breast Cancer in a Controlled Randomized Clinical Trial. J Clin Oncol. 2022;40(35):4071-4082.

Quick Reference

Property Value
PMID 35862873
DOI 10.1200/JCO.21.02844
Year 2022
Journal Journal of Clinical Oncology
Study Type RCT (20-year follow-up)
Evidence Level I
Sample Premenopausal breast cancer patients
Peptide(s) Studied Goserelin

Key Findings

  • Goserelin significantly improved long-term distant recurrence-free interval in ER-positive patients (HR 0.49)
  • Genomic high-risk patients derived the greatest benefit from goserelin monotherapy (HR 0.24)
  • Genomic low-risk patients responded better to tamoxifen alone
  • Combining tamoxifen with goserelin paradoxically increased risk in genomic high-risk patients
  • Twenty-year follow-up demonstrates durable, sustained benefit from ovarian suppression with goserelin

Study Design

Long-term follow-up (20 years) of a controlled randomized clinical trial evaluating adjuvant goserelin, tamoxifen, or their combination in premenopausal patients with ER-positive breast cancer. Genomic risk stratification was applied retrospectively to identify differential treatment responses.

Limitations

  • Retrospective genomic risk analysis was not pre-specified
  • Treatment paradigms have evolved significantly since the trial began
  • Combination therapy results may reflect specific dosing/scheduling that differs from current practice
  • No comparison with aromatase inhibitors or modern endocrine regimens

Clinical Relevance

This study provides the strongest long-term evidence for goserelin's role in premenopausal breast cancer, demonstrating that ovarian suppression alone can produce dramatic reductions in recurrence for genomic high-risk patients. The finding that combination therapy may be counterproductive in some subgroups challenges assumptions about escalating endocrine therapy and supports personalized treatment selection based on tumor genomics.

Related

#research #RCT #peptide #sexual-health #reproductive #evidence-level-I