Enhertu early breast cancer treatments have secured a groundbreaking double regulatory approval from the U.S. Food and Drug Administration (FDA). Announced on May 15, 2026, this landmark clearance expands the use of fam-trastuzumab deruxtecan-nxki into both the neoadjuvant (pre-surgery) and adjuvant (post-surgery) settings for patients with HER2-positive early-stage disease. This development introduces a highly potent antibody-drug conjugate (ADC) into early therapeutic lines where the primary goal is a definitive cure.
Developed jointly by AstraZeneca and Daiichi Sankyo, the therapeutic regimen provides a targeted alternative to standard chemotherapy configurations. By attacking HER2-expressing cells earlier in the disease cycle, this intervention aims to intercept microscopic residual disease before it can metastasize. Consequently, the dual approval addresses a critical medical need for patients facing an aggressive diagnosis who require maximum systemic protection.
The clinical community has anticipated these transitions as data from large-scale clinical trials matured over the last year. As detailed in our comprehensive Oncology Innovation Hub, incorporating advanced ADCs into early-stage protocols represents a massive paradigm shift away from traditional, less-targeted cytostatic options. Medical institutions are already revising their internal guidance documents to incorporate these newly validated treatment pathways.
Dual Indications: Reshaping Enhertu Early Breast Cancer Treatment Pathways
In the preoperative neoadjuvant setting, the FDA approved the drug followed by a taxane, trastuzumab, and pertuzumab (THP) regimen for Stage II and Stage III disease. Data from the Phase III DESTINY-Breast11 trial demonstrated a pathological complete response (pCR) rate of 67.3% for patients receiving this updated protocol. Achieving pCR serves as an essential clinical milestone, correlates strongly with long-term survival, and minimizes the extent of required surgical resection.
Conversely, the adjuvant approval transforms care for individuals who continue to show residual invasive disease after completing initial preoperative HER2-targeted therapies. The landmark Phase III The New England Journal of Medicine published DESTINY-Breast05 trial revealed that the drug slashed the risk of invasive disease recurrence or death by 53% compared to trastuzumab emtansine (T-DM1). This profound reduction establishes a new benchmark for high-risk, post-neoadjuvant patient populations.
While the efficacy data represents a historic win for patient care, the safety profile demands proactive, rigorous clinical oversight. The therapeutic agent carries a boxed warning for interstitial lung disease (ILD) and pneumonitis, meaning that transitioning into early-stage curative settings requires careful patient screening and diagnostic surveillance. Clinicians must balance these high-impact efficacy outcomes against the necessity of early detection and management of pulmonary toxicities.
Clinical Trial Data of Enhertu Early Breast Cancer Trials
DESTINY-Breast11 Neoadjuvant Patient Outcomes
| Regimen Arm | Pathological Complete Response (pCR) | Statistical Significance |
| Enhertu-Containing Protocol | 67.3% | p = 0.003 |
| Standard Control (ddAC-THP) | 56.3% | Reference Baseline |
DESTINY-Breast05 Adjuvant Survival Parameters
| Clinical Endpoint Metric | Hazard Ratio (HR) | Risk Reduction | 3-Year IDFS Rate |
| Invasive Disease-Free Survival | 0.47 | 53% Reduction | 92.4% (vs. 83.7% with T-DM1) |
| Distant Recurrence Free Interval | 0.49 | 51% Reduction | Statistically Significant |
| Central Nervous System Relapse | 0.64 | 36% Reduction | Key Secondary Discovery |



