Triple Negative Breast Cancer Clinical Trial
Official title:
An International, Multicenter, Phase II, Randomized, Parallel-arm Trial Investigating the Role of Two Different Metronomic Chemotherapy Regimens in Locally Advanced or Metastatic Triple Negative Breast Cancer Patients (TNBC) as Maintenance Therapy After First Line Treatment
TNBC, defined by the lack of immunohistochemical staining for oestrogen receptors,
progesterone receptors, and lack of overexpression or amplification of HER2/neu, has an
aggressive biological behaviour, marked by increased risk of recurrence and poorer survival
compared with hormone receptor-positive subtypes.
The key points for the rationale of the present study are:
1. Despite different efforts for improving the outcome of TNBC patients, the median
distant-disease free interval for relapsed triple-negative breast cancer is about 1-2
years, and the median survival for metastatic TNBC is approximately one year.
2. International guidelines currently recommend polychemotherapy instead of sequential
single agents as first-line treatment in this subgroup of patients, but no data is
available at the moment regarding the optimal duration of chemotherapy.
3. There is growing evidence to suggest that platinum-based therapy may have a role in both
advanced and early-stage TNBC, though results are not definitive. Three randomized phase
II neoadjuvant trials have been reported, two of which demonstrated an improvement in
pathological complete response (pCR) rates when carboplatin is added to anthracycline
and taxane-based chemotherapy, though this pCR improvement came at the cost of an
increase in toxicity. Definitive results from phase III trials demonstrating improvement
in long-term outcomes such as event-free and overall survival are not yet available, and
it remains unclear how to optimally incorporate platinums into neoadjuvant therapy, as
toxicity is enhanced when platinum is incorporated as an add-on to standard combination
chemotherapy backbones. A randomized phase III trial comparing cisplatin plus
gemcitabine to paclitaxel plus gemcitabine has been published recently. After a median
follow-up of 16.3 months in the cisplatin plus gemcitabine group and 15.9 months in the
paclitaxel plus gemcitabine group, the hazard ratio for progression-free survival was
0.692 (95% CI 0•523-0•915; pnon-inferiority<0•0001, superiority=0•009. Thus cisplatin
plus gemcitabine was both non-inferior to and superior to paclitaxel plus gemcitabine.
Median progression-free survival was 7.7 months (95% CI 6.2-9.3) in the cisplatin plus
gemcitabine group and 6.5 months (5.8-7.2) in the paclitaxel plus gemcitabine group.
4. In both early and advanced disease settings, response rates appear to be influenced by
germ line BRCA1 and BRCA2 mutation status, and BRCA1 and BRCA2 mutation status has
emerged as an important potential biomarker for platinum therapy. Outside of the BRCA
mutant setting, there is certainly good reason to believe that there are patients with
sporadic TNBC who stand to benefit greatly from a platinum-based approach. Tumour-based
assays that detect levels of genomic scarring caused by the accumulation of DNA damage
over time secondary to underlying DNA repair defects, such as the Myriad HRD assay, have
potential to identify non carriers of BRCA1 or BRCA2 mutations with "BRCA-like" breast
cancer, who may respond to DNA repair- targeted treatment strategies, such as platinum
agents.
One of the most promising way to improve clinical outcome in poor-risk patients is
represented by maintenance therapy with a non-cross resistant regimen after an induction
treatment, until disease progression. Nevertheless, the main limit to such a strategy is the
choice of chemotherapy agents, considering that patients could be treated for a long period
of time The results of the VICTOR-1 study was recently published, the aim of this study was
the determination of the maximum tolerated dose of oral metronomic schedule of vinorelbine
(VNR) in combination with fixed doses of capecitabine (CAPE), as well as to confirm the
safety profile of the combination in a cohort of HER2-negative metastatic breast cancer
patients. The results demonstrated a lower incidence of hematological grade 3-4 adverse
events (1.1%), in comparison to what published in other series, using the standard schedules
of the two drugs. The present study is designed to select the best arm between oral
metronomic schedule of vinorelbine (VNR) and combination of oral metronomic schedule VNR with
fixed doses of capecitabine (CAPE) as maintenance therapy in advanced TNBC patients
responders after an induction treatment.
n/a
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