Lung Cancer Clinical Trial
Official title:
Feasibility of New Biological and Histological Samples at Progression for Patients With Advanced or Metastatic Non Small Cell Lung Cancer (NSCLC)
Feasibility of new biological and histological samples at progression in patients with
advanced or metastatic Non Small Cell Lung Cancer (NSCLC).
A recent paper from Professor Sequist and coll. has depicted the resistance mechanisms as
Thréonine790Methionine (T890M) mutation oncogene cMet (CMet) amplification. Re-biopsies
showed in 14% of cases the transition between NSCLC to Small Cells Lung Cancer (SCLC). In 3
patients, resistance mechanisms have disappeared and they became again sensitive to Tyrosine
Kinase Inhibitors (TKIs). It is mandatory to have a better description to natural history of
the disease. This study will be conducted by the French Group of Pneumology-Oncology (Groupe
Français de Pneumo Cancérologie (GFPC)) up to 100 patients during 18 Months. Each center will
have to define if re-biopsies are possible or not and explain why not.
ABSTRACT PROMOTOR GFPC
MAIN INVESTIGATORS Pr Vergnenegre Alain, Dr Dujon Cécile, Pr Rosell Rafael TITLE Feasibility
of new biological and histological samples at progression in patients with advanced or
metastatic Non Small Cell Lung Cancer (NSCLC)
JUSTIFICATION / BACKGROUND In NSCLC, recent progresses have been reached, with better outcome
in terms of survival without relapse, response rate, and improvement of Qualify of Life
(QoL). In the detail, patients with mutations of Epidermal Growth Factor Receptor (EGF-R) are
sensitive to tyrosine kinase inhibitors (TKIs).
1. Patients with EGF-R mutation Response and disease control are frequently achieved on
some long period of time but, in the majority of cases, resistances appear around a
period of 12 months after the diagnosis. One of the major resistance mechanisms is the
onset of T790M mutation, which induces a non sensitivity to TKIs. At the opposite, some
recent papers have depicted that, after a free interval, resistant tumor can be
responder in a second phase to TKIs]. The type of the mutation has different
consequences on the disease evolution. A recent paper from Pr. Sequist and coll. has
depicted the resistance mechanisms as mutation T790M or oncogene cMet (CMet)
amplification. Re-biopsies showed in 14% of cases the transition between NSCLC to SCLC.
In 3 patients, resistance mechanisms have disappeared and they became again sensitive to
TKIs. It is mandatory to have a better description to natural history of the disease.
2. Patients without EGF-R mutation The knowledge of genetic characteristics is currently
needed to perform an inclusion in some research protocol.
TRIAL DESIGN Translational study with iterative biopsies.
OUTCOMES CRITERIA Principal outcome Feasibility of re-biopsies
Secondary outcomes
- analyses and types of resistances,
- time until metastasis disappearance
- correlations with disease management
- biological history of the disease.
INCLUSION CRITERIA All the patient more than 18 years old, with advanced or metastatic NSCLC.
NON INCLUSION CRITERIA
- SCLC, neuroendocrine carcinoma,
- Patients with judicial protection or deprived of liberty
PROCEDURES
A paper CRF will be recorded with data on :
- Patients's characteristics,
- Tumor Node Metastasis classification (TNM) and stage,
- Number of metastasis and location at the diagnosis,
- First line treatment: surgery, radiotherapy, chemotherapy,
- Date of EGF-R status response,
- Date of relapse,
- Type of procedures,
- Treatment for second and third line management
NUMBER OF PATIENTS 100 patients NUMBER OF CENTRES 20 centres DURATION 18 months
PRACTICAL ORGANIZATION IN EACH CENTER Each center will have to define if re-biopsies are
possible or not (and explain why not). Some localisations are difficult to biopsy like bone
metastasis or deep brain metastasis. A bronchial fiberscopy will be systematically performed
to search an endoluminal lesion, which could allow 3 to 5 tissue samples. When possible,
liver, adrenal gland, superficial brain metastases will be analysed after the relapse.
1. For patients with EGF-R mutation The samples will be prepared with the usual technic of
each center. The corresponding slides have to be send to spanish laboratory (Pr R
Rosell, Badalona hospital) A comparison between patients with impossible re-biopsies and
the final patients group will be performed.
2. For patients without EGF-R mutation the usual practice will be used with biological
platforms
BIOLOGICAL PROCEDURES
1. Patients with EGF-R mutation Biological markers analysis will be coordinated by Catalan
Institute of Oncology.
2. Patients without EGF-R mutation: usual biological analysis will be performed in the
local platform.
STATISTICAL ANALYSES A description of each items will be performed in terms of frequence,
range, mean and median. Correlation between biological markers will be assessed by non
parametric tests Wilcoxon or Mann-Whitney.
POSSIBLE APPLICATIONS
- a better knowledge of resistance mechanisms in EGF-R mutated patients
- a better knowledge of genetical and molecular history of these diseases
- a better management according to biological changes and evolution
;
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