Metastatic Lung Adenocarcinomas Clinical Trial
Official title:
Retrospective Analysis of the Expression of the Neurotensin Receptor by Metastatic Lung Adenocarcinomas
Lung cancer is the leading cause of cancer mortality in France and worldwide. 60% of patients
present themselves with a disease diagnosis immediately metastatic non curable.
Adenocarcinomas account for 50% of incident tumors. Treatment is based on the platinum-based
chemotherapy with or without maintenance therapy. When there is to exhaust this first line, a
second line treatment is offered to the patient. Three drugs are allowed in this situation:
docetaxel, erlotinib (inhibitor of the tyrosine kinase activity of the receptor for epidermal
growth factor - TKI-EGFR) and pemetrexed (which in fact has become virtually standard in
first online and in combination with platinum in all patients with non-squamous cancer, so
that his place is in second line reduced facto). There is no recommendation for treatment in
third line situation where only erlotinib is allowed.
Most recently, the nivolumab, anti-PD1 monoclonal antibody (which aims to enable immunutaire
system) saw its demonstrated effectiveness in the second line and beyond in the two Phase 3
trials where it was compared with docetaxel for the treatment of squamous cell carcinoma and
non-squamous. The very recent availability in France of the drug under an ATU fact that it
will most likely become a standard second line, which will tend to place the third line
docetaxel.
Therefore, erlotinib will be in 4th line situation. However, in the absence of an EGFR
mutation (which is only seen in more than 10% of Caucasian patients) use of the drug does not
seem appropriate or even harmful. A selection of patients likely to benefit from the
prescription of EGFR TKI-is essential.
Neurotensin (NTS) is a polypeptide of 13 amino acids present and active in the central
nervous system and the periphery. At the peripheral level, neurotensin is secreted
postprandial by endocrine cells in the intestinal mucosa and is involved in the motor
functions of the gastrointestinal tract. The effects of neurotensin pass through the
activation of three subtypes of receptors which, mainly, NTSR1 and NTSR2 which are receptors
coupled to G proteins in the extra-digestive normal tissues, including lung, torque NTS /
NTSR1 n is not expressed physiologically. Rather, this complex is likely to recur in tumor
tissues.
The mechanism of this effect is derogatory activation torque NTS / NTSR1 of matrix
metalloproteinases which causes the release by the cell membrane ligands "EGF-like" and thus,
activation of HER receptor (EGFR or HER1, HER2 and HER3). Indeed, in experimental tumors
created by subcutaneous injection in athymic mouse cell lines adenocarcinomas NTS + / NTSR1 +
(non-mutated EGFR), treatment with erlotinib - which blocks EGFR pathway - causes a
significant decrease of tumor growth.
Expression of the neurotensin receptor in cancer cells metastatic primary bronchial
adenocarcinoma is not known. Therefore, its pejorative prognostic value is not confirmed in
the metastatic setting.
The objectives of this work purely descriptive, are:
- Evaluate the expression by tumor cells of the neurotensin receptor on a retrospective
series of patients:
- Consecutively treated between 2010 and 2015 at St. Joseph hospital (about a hundred
patients) and the Saint-Antoine hospital (three hundred patients), holders of a
metastatic and primary lung adenocarcinoma having received all even first-line
chemotherapy with a platinum agent (cisplatin or carboplatin) and pemetrexed (Alimta °)
- If possible, the records of patients treated at St. Joseph Hospital and Saint-Antoine
Hospital between 2005 and 2010 as part of clinical trials evaluating the value of
erlotinib will also be sought,
- Develop a score expression NTSR1 taking into account the percentage of tumor cells
expressing the receptor and the intensity of the marking,
- Correlate labeling cells by NTSR1 with the clinical course of patients to see if
expression NTSR1 is a factor of poor prognosis in metastatic patients.
Teams involved:
Services:
- Pharmacy that will establish the list of patients have been treated with the same
chemotherapy,
- Pathological anatomy-to group blades and ensure immunohistochemical staining and
reading,
- Pneumology and Thoracic Oncology to resume the clinical history of patients.
The scientific coordination of the study will be conducted by INSERM UMR-S 1007, cellular
homeostasis and cancer - Reprogramming of biological and alternative therapies responses
(University Center of the Holy Fathers, 45 rue des Saints Pères, 75006 Paris), one team under
the direction of Dr. Patricia Forge, working on the couple NTS / NTSR1.
expected benefits
Beyond two or three conventional chemotherapy line, which will no doubt add - for a
proportion of patients still to be determined - the new immunotherapy drugs, there is no
longer any recommendations for treatment of patients lung cancer metastatic non-small cells.
Erlotinib is an option since there is no limitation in its approval of prescription ond line.
However, in the absence of EGFR mutation, the therapeutic value of the drug appears to be
very low. Preclinical data that investigators obtained in the laboratory are hypothesize that
tumors expressing NTSR1 could meet the same TKI EGFR in the absence of mutation in the
receptor. The planned study will assess the percentage of patients in this situation in order
to prepare the organization of a Phase II study to evaluate the clinical relevance of a TKI
EGFR in this selected population of patients carrying of a non-mutated tumor.
Nature of the data collected
A file will be drawn from the clinical data found in files: all patients are carriers of
metastatic primary lung adenocarcinoma and having all received the same chemotherapy.
The data obtained will be: age, sex, smoking status, number of courses of chemotherapy
received and the response to treatment, the usual chronological parameters for the
establishment of the survival curves. Histological samples will be processed locally in each
of the two hospitals, according to a specific procedure to be determined between laboratories
and INSERM Unit.
Identification of subjects and circulation and processing of data
In this study, the inclusions are carried out within the hospital group Paris Saint-Joseph
and Saint-Antoine hospital. Histological samples will be processed locally in each of the two
hospitals, according to a specific procedure to be determined between pathological anatomy
and INSERM Unit Laboratories.
These histological samples will be stored at the Pathological Anatomy Laboratory Groupe
Hospitalier Paris Sani Joseph.
Each study participant will be identified by a code of inclusion (first name and surname -
year of birth). The concordance table to link the assigned code and the participant's name
will be kept in each of the participating centers, in a file protected by a password specific
to the principal investigator of each center. Data collected from different centers on
anonymous paper media (only the code for inclusion of each patient are included) will be
centralized within the GHPSJ and entered in a database which anonymous access is protected by
the PIN each in the study of GHPSJ. Data processing and statistical analysis will be
performed on the GHPSJ site in collaboration with the Clinical Research Unit of the European
Hospital Georges Pompidou.
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