Metastatic Breast Cancer Clinical Trial
Official title:
Randomized, Double-Blind, Placebo-Controlled Phase II Trial of Fulvestrant (Faslodex) Plus Everolimus in Post-Menopausal Patients With Hormone-Receptor Positive Metastatic Breast Cancer Resistant to Aromatase Inhibitor Therapy
Post-menopausal women with hormone-receptor positive (HR+) metastatic breast cancer resistant
to aromatase inhibitor (AI) therapy will be randomized to receive Fulvestrant (Faslodex) with
Everolimus or Fulvestrant (Faslodex) with a placebo (no active ingredients).
Fulvestrant has demonstrated activity when used as first, second, or third line endocrine
therapy, making it an attractive therapy for combination with other agents. In addition, it
is commonly reserved for use following disease progression on AI therapy.
Everolimus is an orally administered drug that blocks a signaling pathway called "mTOR".
"mTOR" acts as a regulator for many processes in the body, including cell growth. Blocking
this pathway may have an effect on cell growth.
The combination of a novel class of agents (mTOR inhibitors) and an established standard
treatment for metastatic HR+ breast cancer may potentially increase the clinical benefit by
targeting multiple different biological pathways.
Breast cancer is the most commonly diagnosed malignancy in women worldwide. In the United
States, an estimated 230,480 new cases of invasive breast cancer were diagnosed in 2011, with
39,520 breast cancer deaths. In 40-80% of women with node-positive disease at diagnosis,
their breast cancer will recur. When distant metastases occur, median survival is 18 to 36
months from time of recurrence. Among the 60-70% of women with HR+ breast cancer, 40-60% of
them will benefit from endocrine therapy. Endocrine therapy has shown to yield similar
survival rates in hormone-sensitive disease as compared to chemotherapy; although response
rates are lower and responses develop more slowly. Endocrine therapy is considerably less
toxic than chemotherapy, and is therefore the preferred treatment option for patients with
HR+ disease.
Endocrine therapy represents the foundation of treatment for HR+ metastatic and locally
advanced breast cancer. Multiple compounds in varying classes exist, and those most widely
used include the selective estrogen receptor modulators (SERMs), aromatase inhibitors (AIs),
and the selective estrogen receptor down-regulators (SERDs). Although the utility of these
drugs is well established, as many as 50% of women with HR+ breast cancer will fail to
respond to endocrine treatment. Moreover, those who do respond will inevitably develop
acquired resistance.
Fulvestrant is the first drug which acts as a pure estrogen receptor (ER) antagonist without
known agonist effects. It competitively binds to the ERs with an approximately 100 times
greater affinity than that of tamoxifen. Fulvestrant promotes the degradation of ERs and
subsequently prevents ER-mediated gene transcription.
Everolimus (RAD001) is an oral derivative of rapamycin that is an m-TOR inhibitor. At
cellular and molecular levels, everolimus acts as a signal transduction inhibitor. Everolimus
selectively inhibits mTOR (mammalian target of rapamycin); a key and highly conserved
serine-threonine kinase which is present in all cells and is a central regulator of protein
synthesis and ultimately cell growth, cell proliferation, angiogenesis and cell survival.
mTOR is the only currently known target of everolimus.
In oncology, everolimus has been in clinical development since 2002 for patients with various
hematologic and non-hematologic malignancies as a single agent or in combination with
antitumor agents, including cytotoxic chemotherapeutic agents, targeted therapies, antibodies
and hormonal agents.
Patients will be randomized (1:1) to receive everolimus or placebo with fulvestrant after
consideration of stratification factors of performance status (0 vs. 1), measurable disease
(yes vs. no), and prior chemotherapy for metastatic disease (yes vs. no).
Patients will be evaluated for disease response every 12 weeks, and treated until disease
progression or unacceptable toxicity or withdrawal of consent for a maximum of 12 cycles (48
weeks).
Patients with no evidence of progressive disease who remain on study after completing 12
cycles are unblinded and continue to receive fulvestrant alone (if originally randomized to
placebo) or in combination with everolimus (if originally randomized to everolimus) at the
same dose and schedule. Patients will continue to be evaluated for disease response every 12
weeks and continue until disease progression or unacceptable toxicity.
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