The present hypothesis is that anti-EGFR agents are active in tumors with low-level RAS mutation when the majority of tumor cells is still sensitive. While response rate may be high and may reflect sensitivity to anti-EGFR agents, PFS is anticipated to be shorter than in RAS wild-type patients due to the faster development of resistance when sensitive cells are eradicated and when the RAS-mutant anti-EGFR resistant clones become predominant. The characteristics of low-level RAS mutant tumors would be: * Objective response rate (ORR) high (reflecting the sensitive clone) * Progression-free survival (PFS) short (reflecting the more rapid outgrowth of RAS mutant clones)
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
120
Panitumumab 6 mg/kg BW as 60-min i.v. infusion\* D1 \*If the 1st infusion is well tolerated, all subsequent infusions can be applied over 30-60 minutes.
Irinotecan 180 mg/m² BSA i.v., 30 - 90 min D1
Folinic acid (racemic) 400 mg/m²BSA i.v., 120 min D1
5-FU 400 mg/m² BSA, bolus, D1 5-FU 2400 mg/m² BSA i.v. infusion over a period of 46 h D1-2
Ludwigs Maximialians University
Munich, Germany
Overall Response Rate
As primary endpoint ORR according to RECIST 1.1 will be evaluated separately for each arm of patients with defined low-frequency RAS mutation
Time frame: up to 60 months
Progression free survival (PFS)
PFS, separately for each arm of patients with defined low-frequency RAS mutation
Time frame: up to 60 months
Overall Survival (OS)
OS, separately for each arm of patients with defined low-frequency RAS mutation
Time frame: up to 60 months
Investigation of Early Tumor shrinkage (ETS) as an alternative early-on-treatment predictor of treatment efficacy
ETS, separately for each group of patients with defined low-frequency RAS mutation
Time frame: up to 48 months
Investigation of Depth of Response (DpR) to define the nadir of tumour response
DpR, separately for each arm of patients with defined low-frequency RAS Mutation.
Time frame: up to 48 months
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