Retrospective Study in Non Small Cell Lung Cancer (NSCLC) With Epidermal Growth Factor Receptor (EGFR)
NCT ID: NCT02293733
Last Updated: 2014-11-18
Study Results
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Basic Information
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COMPLETED
144 participants
OBSERVATIONAL
2014-01-31
2014-03-31
Brief Summary
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Detailed Description
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• Lung cancer represents the leading cause of death by cancer in France. Significant advances have been made in recent years on knowledge of oncogenesis of NSCLC in particularly the discovery of specific oncogenic drivers playing major role in oncogenic addiction responsible for the occurrence of NSCLC. Activating mutations of the gene encoding the receptor tyrosine kinase EGFR appeared in a subgroup of patients with NSCLC. In 2010, the search for EGFR mutations in patients with lung cancer was performed in 16,834 patients and the mutation rate was 10.5%. The use of specific inhibitors of EGFR tyrosine kinase in patients with activating mutations of EGFR have shown a significant clinical benefit with a response rate more than 70 % ,with PFS ranging from 9 to 13,1 months and median overall survival from 20 to 30 months. Despite these very good results, all patients develop a resistance to EGFR TKI. This progression is usually defined according to RECIST criteria.
These RECIST criteria were established primarily on studies conducted in patients treated with conventional chemotherapy with few or no targeted therapies. In addition, the mode of action of TKI (blocking signalling pathways involved in cell proliferation, angiogenesis, apoptosis, metastasis ..) is very different from the mode of cytotoxic action (action during cell division). Thus, the use of RECIST does not seem to be the most appropriate way to evaluate the response in patients treated by TKI.
Despite this, the RECIST criteria have been used to demonstrate superiority of EGFR TKI compared to chemotherapy in patients with EGFR activating mutations in first line setting.
In 2010, Pr Jackman proposed a clinical definition of acquired resistance to EGFR TKI :
1. Treatment with a single agent EGFR TKI,
2. Presence of EGFR activating mutation, clinical benefit from treatment with an EGFR TKI
3. Systemic progression of disease according to RECIST or WHO criteria while on continuous treatment with EGFR TKI within the last 30 days TKI
4. No intervening systemic therapy between cessation of EGFR TKI and initiation of new therapy.
Tony Mok , in the accompanying editorial, made some criticism to this definition. He argued that it was not uncommon to find new small slow growing tumor nodules after the dramatic initial response to EGFR TKIs. He stated that in this situation, EGFR TKIs could be continued with benefit for the patients.
Since then, others clinical situations have been described, such as the emergence of one or even more new metastasis located in one single organ (like the brain or bones), which can be controlled by a loco-regional treatment. The authors found that the continuation of EGFR TKIs in these cases allowed control of the disease for a considerable length of time.
More recently, it has been suggested that even loco-regional treatment was not mandatory for EGFR TKIs continuation.
Pr Nishino studied retrospectively 56 patients with EGFR activating mutations and acquired resistance. 88% of patients continued EGFR TKI treatment for at least 2 months beyond progressive disease defined according to RECIST criteria. The median time from RECIST progressive disease to termination of TKI for these patients was 10.1 months (range 2.2 to 64.2 months) and the median overall survival was 31.8 months, which is a rather good result.
Pr Oxnard, in a similar study, found that in 45% of 42 patients with acquired resistance to EGFR TKI, alternate systemic therapy could be delayed for three months or more. These 19 patients had more frequently the exon 19 deletion and were free of cancer related symptoms at RECIST progressive disease.
Another recently published retrospective Japanese study suggested that continuous use of EGFR-TKI beyond progressive disease may prolong overall survival compared with switching to cytotoxic chemotherapy in patients with EGFR activating mutations.
A prospective ASIAN phase II study (ASPIRATION) has been recently completed. It compared the continuous use of erlotinib versus stopping erlotinib at progression according to RECIST criteria. Patients could continue erlotinib if progression was slow (\> 6 months stability), asymptomatic minimal increase and/or new cerebral metastasis controlled locally. The patients switch to another systemic treatment if they had rapid progressive disease, extra brain symptomatic metastasis, deterioration of Performance Status (PS) or life threatening complications. The results of this study should be available in December 2014.
Purpose :
The purpose of our retrospective study is to describe which circumstances EGFR TKI is continued despite progression according to the usual RECIST criteria in patients with EGFR activating mutations and acquired resistance to EGFR TKI. This study concerns patients who have began a TKI treatment in first line from 1st JANUARY 2010 to 1st JUNE 2012.We'll collect their social and demographic data (age, sex), first PFS (from start of EGFR TKI: PFS 1) and second (from first progression according to RECIST 1.1 to second progression : PFS2) , OS (from diagnosis OS 1 and from first progression OS2), mutational status, and we will analyze more closely the mode of progression (site), the therapeutic approach at disease progression. We will define two subgroups: those for whom EGFR TKI was continued at least three months despite progression defined according to RECIST criteria, and those for whom a second-line treatment (chemotherapy without EGFR TKI) was chosen at disease progression. It will be individualized the subgroup of patients in whom it was continued TKI after progression.
In this subgroup, it will be searched for a correlation between delaying systemic therapy (second line) by pursuing a EGFR TKI at least 3 months and various parameters:
* Type of EGFR mutation
* Symptoms at disease progression
* Clinical characteristic
* Emergence of new metastases vs increasing size of known targets
* Speed of decay and tumour progression (% per month)
* Delivery of loco-regional treatment when relapse occurs in a single site
* PFS (PFS1 and PFS2) and OS (OS1) from the first progression in this group will be compared to the general population (population for which there was TKI stop to the progression) with EGFR activating mutations.
Conditions
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Study Design
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RETROSPECTIVE
Study Groups
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Patients NSCLC EGFR mutated
This is an observational study, there is no intervention.
No interventions assigned to this group
Eligibility Criteria
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Inclusion Criteria
* First-line treatment with a TKI monotherapy
* Measurable lesion according to RECIST 1.1
* Age\> 18 years
* secondary or acquired resistance of EGFR TKIs according to the jackman criteria
* patients for whom it was started a TKI treatment in first line from January 2010 until June 2012 (patients who received 1 Chemotherapy cycle could be included).
Exclusion Criteria
* Patients without EGFR mutation
* Patients not treated with EGFR TKI in first line treatment
* Not measurable lesion to RECIST 1.1
18 Years
ALL
No
Sponsors
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Groupe Francais De Pneumo-Cancerologie
OTHER
Responsible Party
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Principal Investigators
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AULIAC JA Jean-Bernard, MD
Role: PRINCIPAL_INVESTIGATOR
Hôpital F. Quesnay 2 bd de Sully 78201 MANTES LA JOLIE
GERVAIS RG Radj, MD
Role: STUDY_DIRECTOR
Centre François Baclesse 3 avenue du Général Harris 14076 CAEN CEDEX 05
Locations
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Centre Hospitalier D Argenteuil
Argenteuil, Val D'oise, France
Site 12
Aix-en-Provence, , France
Centre Hospitalier Universitaire
Angers, , France
Centre Hospitalier du Morvan
Brest, , France
Centre François Baclesse
Caen, , France
Centre Hospitalier René Dubos
Cergy-Pontoise, , France
Site 33
Créteil, , France
Site 07
Draguignan, , France
Site 32
Elbeuf, , France
Site 04
Gap, , France
Centre Hospitalier Les Oudairies
La Roche-sur-Yon, , France
Hospital du Cluzeau
Limoges, , France
Site 00
Limoges, , France
Centre Hospitalier Régional
Longjumeau, , France
Site 25
Mantes-la-Jolie, , France
Site 06
Marseille, , France
Site 01
Meaux, , France
Site 19
Périgueux, , France
Site 20
Rennes, , France
Site 18
Rouen, , France
Site 17
Rouen, , France
Hôpital Yves Le Foll
Saint-Brieuc, , France
Site 14
Toulon, , France
Site 11
Villefranche-sur-Saône, , France
Countries
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References
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Auliac JB, Fournier C, Audigier Valette C, Perol M, Bizieux A, Vinas F, Decroisette Phan van Ho C, Bota Ouchlif S, Corre R, Le Garff G, Fournel P, Baize N, Lamy R, Vergnenegre A, Arpin D, Marin B, Chouaid C, Gervais R. Impact of Continuing First-Line EGFR Tyrosine Kinase Inhibitor Therapy Beyond RECIST Disease Progression in Patients with Advanced EGFR-Mutated Non-Small-Cell Lung Cancer (NSCLC): Retrospective GFPC 04-13 Study. Target Oncol. 2016 Apr;11(2):167-74. doi: 10.1007/s11523-015-0387-4.
Other Identifiers
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GFPC 04-2013
Identifier Type: -
Identifier Source: org_study_id