Data from Elacestrant in ER+, HER2− Metastatic Breast Cancer with ESR1-Mutated Tumors: Subgroup Analyses from the Phase III EMERALD Trial by Prior Duration of Endocrine Therapy plus CDK4/6 Inhibitor and in Clinical Subgroups

Kaklamani, Virginia

Data from Elacestrant in ER⁺, HER2⁻ Metastatic Breast Cancer with ESR1-Mutated Tumors: Subgroup Analyses from the Phase III EMERALD Trial by Prior Duration of Endocrine Therapy plus CDK4/6 Inhibitor and in Clinical Subgroups

Posted on 2024-10-01 - 07:23

AbstractPurpose:

Elacestrant significantly prolonged progression-free survival (PFS) with manageable safety versus standard-of-care (SOC) endocrine therapy (ET) in patients with estrogen receptor–positive (ER⁺), HER2⁻ metastatic breast cancer and tumors harboring estrogen receptor 1 (ESR1) mutation following ET plus a cyclin-dependent kinase 4/6 inhibitor (ET+CDK4/6i). In patients with ESR1-mutated tumors, we evaluated the efficacy and safety of elacestrant versus SOC based on prior ET+CDK4/6i duration and in clinical subgroups with prior ET+CDK4/6i ≥12 months.

Patients and Methods:

EMERALD, an open-label phase III trial, randomly assigned patients with ER⁺, HER2⁻ metastatic breast cancer who had received 1–2 prior lines of ET, mandatory CDK4/6i, and ≤1 chemotherapy to elacestrant (345 mg daily) or SOC (aromatase inhibitor or fulvestrant). PFS was assessed across subgroups in post hoc exploratory analyses without adjustment for multiple testing.

Results:

In patients with ESR1-mutated tumors and prior ET+CDK4/6i ≥12 months, the median PFS for elacestrant versus SOC was 8.6 versus 1.9 months (HR, 0.41; 95% confidence interval, 0.26–0.63). In this population, the median PFS (in months) for elacestrant versus SOC was 9.1 versus 1.9 (bone metastases), 7.3 versus 1.9 (liver and/or lung metastases), 9.0 versus 1.9 (<3 metastatic sites), 10.8 versus 1.8 (≥3 metastatic sites), 5.5 versus 1.9 (PIK3 catalytic subunit α mutation), 8.6 versus 1.9 (tumor protein p53 gene mutation), 9.0 versus 1.9 (HER2-low), 9.0 versus 1.9 (ESR1^D538G-mutated tumors), and 9.0 versus 1.9 (ESR1^Y537S/N-mutated tumors). Subgroup safety was consistent with the overall population.

Conclusions:

The duration of prior ET+CDK4/6i ≥12 months in metastatic breast cancer was associated with a clinically meaningful improvement in PFS for elacestrant compared with SOC and was consistent across all subgroups evaluated in patients with ER⁺, HER2⁻, ESR1-mutated tumors.

CITE THIS COLLECTION

Bardia, Aditya; Cortés, Javier; Bidard, François-Clément; Neven, Patrick; Garcia-Sáenz, José; Aftimos, Phillipe; et al. (2024). Data from Elacestrant in ER⁺, HER2⁻ Metastatic Breast Cancer with ESR1-Mutated Tumors: Subgroup Analyses from the Phase III EMERALD Trial by Prior Duration of Endocrine Therapy plus CDK4/6 Inhibitor and in Clinical Subgroups. American Association for Cancer Research. Collection. https://doi.org/10.1158/1078-0432.c.7474507

https://doi.org/10.1158/1078-0432.c.7474507

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Elacestrant in ER⁺, HER2⁻ Metastatic Breast Cancer with ESR1-Mutated Tumors: Subgroup Analyses from the Phase III EMERALD Trial by Prior Duration of Endocrine Therapy plus CDK4/6 Inhibitor and in Clinical Subgroups

AUTHORS (14)

AB
Aditya Bardia
JC
Javier Cortés
FB
François-Clément Bidard
PN
Patrick Neven
JG
José Garcia-Sáenz
PA
Phillipe Aftimos
JO
Joyce O’Shaughnessy
JL
Janice Lu
GT
Giulia Tonini
SS
Simona Scartoni
AP
Alessandro Paoli
MB
Monica Binaschi
TW
Tomer Wasserman
VK
Virginia Kaklamani

KEYWORDS

Biomarkers Circulating tumor cells/DNA/exosomes Prognostic biomarkers Breast Cancer Clinical Trial Results Phase II clinical trials Drug Resistance Clinical drug resistance Novel mechanisms Precision Medicine Translational Research

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