Estrogen Receptor Positive Breast Cancer Clinical Trial
Official title:
A Randomized Phase II Study of Fulvestrant in Combination With the Dual mTOR Inhibitor AZD2014 or Everolimus or Fulvestrant Alone in Estrogen Receptor-positive Advanced or Metastatic Breast Cancer
This is an open-label, multicentre, 4-arm randomised phase II trial of fulvestrant + AZD2014
versus fulvestrant + everolimus versus fulvestrant alone in patients with ER-positive,
HER2-negative advanced or metastatic breast cancer, whose disease relapsed during treatment
with (or within 12 months after discontinuation of) an AI in the adjuvant setting or
progressed during treatment with an AI in the metastatic setting. Patients will be randomised
(2:3:3:2) to one of the four treatment arms:
- Fulvestrant
- Fulvestrant + AZD2014 (continuous daily schedule)
- Fulvestrant + AZD2014 (intermittent schedule - 2 days on, 5 days off)
- Fulvestrant + everolimus
Randomization will be stratified by the following criteria:
- Measurable disease (vs. non-measurable).
- Sensitivity to prior endocrine therapy (sensitive versus resistant)
This is an open-label, multicentre, 4-arm randomised phase II trial of fulvestrant + AZD2014
versus fulvestrant + everolimus versus fulvestrant alone in patients with ER-positive,
HER2-negative advanced or metastatic breast cancer, whose disease relapsed during treatment
with (or within 12 months after discontinuation of) an AI in the adjuvant setting or
progressed during treatment with an AI in the metastatic setting. Patients will be randomised
(2:3:3:2) to one of the four treatment arms:
- Fulvestrant
- Fulvestrant + AZD2014 (continuous daily schedule)
- Fulvestrant + AZD2014 (intermittent schedule - 2 days on, 5 days off)
- Fulvestrant + everolimus
Randomization will be stratified by the following criteria:
- Measurable disease (vs. non-measurable).
- Sensitivity to prior endocrine therapy (sensitive versus resistant) Sensitivity to prior
endocrine therapy is defined as (i) at least 24 months of endocrine therapy before
recurrence in the adjuvant setting or (ii) a complete or partial response to prior
metastatic endocrine treatment, or (iii) stabilization for at least 24 weeks of
endocrine therapy for advanced disease.
Treatment will be continued until disease progression unless there is evidence of
unacceptable toxicity or if the patient requests to be withdrawn from the study. If one of
the treatments (fulvestrant or mTOR inhibitor) is discontinued prior to disease progression,
patients should be continued on single agent treatment until progression, evidence of
unacceptable toxicity or if the patient requests to be withdrawn from the study.
At the time of documented disease progression (using RECIST 1.1), patients randomised to
receive fulvestrant + everolimus who still meet eligibility criteria may be permitted to
receive open-label crossover treatment with fulvestrant + AZD2014. Crossover therapy must
begin no later than 28 days after the clinic visit at which progression was determined.
Patients will receive crossover therapy until progression, intolerable toxicity, elective
withdrawal from the study, or until the completion or termination of the study, whichever
occurs first.
Tumour evaluations will be performed before the initiation of treatment, every 8 weeks during
the first 40 weeks and every 12 weeks thereafter until disease progression.
The study will also assess the relationship between the anticipated anti-tumour activity of
the treatment regimen and biological characteristics of patients' tumour at baseline
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