Antineoplastic Agents Clinical Trial
Official title:
Erbitux MEtastatic Colorectal Cancer Strategy Study (ERMES): A Phase III Randomized Two Arm Study With FOLFIRI + Cetuximab Until Disease Progression Compared to FOLFIRI + Cetuximab for 8 Cycles Followed by Cetuximab Alone Until Disease Progression in First Line Treatment of Patients With RAS and BRAF Wild Type Metastatic Colorectal Cancer
- To investigate whether cetuximab alone (given until progression or cumulative toxicity)
after 8 cycles of FOLFIRI + cetuximab results in a non inferior Progression Free
Survival when compared with continuous FOLFIRI + cetuximab (given until progression or
cumulative toxicity).
- To assess whether an improvement in the incidence of grade 3-4 hematological and
non-hematological adverse events (AEs) can be achieved in the experimental arm
(cetuximab alone after 8 cycles FOLFIRI + cetuximab) as compared to the continuous
chemotherapy arm (FOLFIRI plus cetuximab)
- To explore the possibility of using liquid biopsies for molecular profiling as well as
monitoring treatment activity in mCRC pts receiving cetuximab based therapy
Survival of patients undergoing therapy with FOLFIRI + cetuximab seems to be related to the
ability of this treatment to induce a rapid reduction in tumor mass. In the retrospective
analyses of the FIRE-3 trial ETS was significantly associated with PFS and OS, suggesting
that ETS reflects the existence of a selected population of patients highly sensitive to
cetuximab. This permits the assumption that, once this goal has been achieved, further
exposure to combined antineoplastic treatment (cytotoxic drugs and targeted therapy) may not
result in improvement or preservation of the result, but only in an increase of side effects
that will be additional to unavoidable disease progression. In addition, the heavy exposure
to cytotoxic antineoplastic treatments may lead to bone marrow toxicity, hepatic and renal
function decreases that could compromise the sequential treatment plan, negatively affecting
OS. With the availability of an effective treatment such as cetuximab in monotherapy4 without
major side effects on blood counts and liver and kidney function, the use of this treatment
alone after achievement of the deepest clinical response could be a viable strategy to
achieve a good control of the disease, limiting side effects. As shown in several studies
designed to understand the most effective treatment sequence in colorectal carcinoma, the
most important factor that influences the overall survival is the possibility to administer
more lines of effective therapy. As a consequence, a de-intensifying strategy in a subgroup
of highly selected RAS and BRAF WT population might segregate a group of patients with the
largest potential for fast-primary treatment. Joining the best induction treatment with the
expression of patients capability to undergo additional lines of antineoplastic therapy may
be the way to optimize the continuum of care.
Recently, several mechanisms of resistance to anti-EGFR therapy have been described, but
until now none may used early in order to support the treatment choice.Moreover, assessment
of secondary resistance requires further tissue samples and often it is not really feasible.
Therefore, a prospective multiple gene mutation analysis could meet the need of
characterizing primary resistance, whereas liquid biopsy might help to recognize resistance
occurring early during treatment by means of a simple and repeatable assay. Based on all
these considerations, the investigators designed a strategy study: a phase III randomized two
arm study with FOLFIRI + cetuximab until disease progression compared to FOLFIRI + cetuximab
for 8 cycles followed by cetuximab alone until disease progression in the first line
treatment of patients with RAS and BRAF WT metastatic colorectal cancer combined with a
prospective multiple gene mutation analysis of both tumor tissue and blood.
;
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