Prospective, Sequential Multiple Assignment, Multicentric, Phase II Randomized Controlled Trial on Two Parallel Groups Comparing the Efficacy of Two Immunosuppressive Drugs (Methotrexate, Cyclophosphamide) in Large Granular Lymphocytes Leukemia

LGL

LGL leukemia represents a rare subtype of chronic T or NK lymphoproliferative disorders. It is an indolent disease, the main hematological or autoimmune complications lead to a treatment in more than 60% of patients. Investigators set up at the University Hospital of Rennes, a database of more than 300 patients with LGL leukemia from major French services that support this disease, and published in 2010 the largest series of patients in the world (n = 229). However, the limited heterogeneity and retrospective data collected, as all previously released, makes it difficult the proposal of consensual treatment options. If first and second line treatments are based on the use of immunosuppression with methotrexate, cyclophosphamide, or cyclosporin A, no molecule has proven superiority over others. Methotrexate and cyclophosphamide are mainly used in the first line. Invetigators just have in the literature data on about 100 patients treated with either of these drugs. Combining the results of our series with those in the literature, invetigators estimate the respective overall response rate (RG) and complete response rate (CR) in 55% and 30% for methotrexate, and 60% and 50% for cyclophosphamide. Thus, there are four objective in this study : 1. to compare the respective efficacies of methotrexate and cyclophosphamide when administered as first-line therapies in patients suffering from T/NK LGL leukemia with severe neutropenia or neutropenia associated with infections, and/or anemia requiring transfusions, and/or auto-immune associated disease 2. to evaluate the percentage of patients refractory to methotrexate or cyclophosphamide for which a second line treatment is efficacious 3. to explore, in case of non-response to the first-line therapy, the efficacy of ciclosporine A, the comparison being performed with the treatment which was not administered in the first-line therapy 4. to evaluate the response rate according to the phenotypic subtype of LGL leukemia.

2013-11-26

2024-02-05

2027-05-26

Active (not recruiting)

Early phase I

166

Inclusion Criteria: * Common criteria of LGL leukemia: the diagnosis is based on a chronic LGL peripheral blood expansion (\>0.5x109/L), usually lasting more than 6 months * Specific criteria for T-LGL leukemia or NK-LGL lymphocytosis or chronic NK-LGL leukemia: * Specific criteria for T-LGL leukemia: * Expression of LGL surface markers compatible with an activated T-cell (commonly alpha-beta+/CD3+/CD8+/CD57+ and/or CD16+) phenotype or gamma-delta+ T cells; * Clonal rearrangement of TCRγ gene using PCR or specific and clonal Vβ expression using FCM. * Specific criteria for NK-LGL lymphocytosis or chronic NK LGL leukemia: * Expression of LGL surface markers compatible with a NK cell (commonly CD3-/CD8+/CD16+ and/or CD16+/CD56+) phenotype; * CD56+ or CD16+ NK cells greater than 0.75x109/L; * The term of chronic NK-LGL lymphocytosis is used for patients with chronic illness (NB: patients with massive tissue LGL infiltration of the spleen, liver and bone marrow and presenting aggressive clinical behavior are considered as having aggressive NK-LGL leukemia and should not be included). * Age above 18 years * ECOG performance status of 0-2 * Life expectancy of at least 1 year * Lack of previous treatment (except with G-CSF or transfusions) * At least one indication of treatment: * Isolated severe neutropenia (ANC \<0.5x109/L) or neutropenia (ANC \<1.5x109/L) with two or more infections requiring antibiotics; * Anemia (whatever the underlying mechanism: pure red cell aplasia or marrow infiltration) requiring transfusions greater than 2 units for two months prior to inclusion, or symptomatic anemia (hemoglobin \<10g/dl) with impairment of the quality of life; * Associated complications such as systemic diseases or auto-immune diseases (i.e. recurrent uveitis, cutaneous vasculitis, autoimmune hemolytic anemia, idiopathic thrombocytopenic purpura, rheumatoid arthritis resistant to steroids and/or immunomodulator agents (colchicin, disulone, hydrochloroquine)) and justifying a treatment with methotrexate or cyclophosphamide * Written informed consent Exclusion Criteria: * Inability to understand or to follow study procedures * Prior or concurrent malignancy within the past 5 years except inactive nonmelanomatous skin cancer or carcinoma in situ of the cervix * Other serious medical illnesses, such as hepatic, renal, cardiac, pulmonary, neurologic, or metabolic disease that would preclude the patient's ability to tolerate methotrexate, cyclophosphamide, or ciclosporine A * Reactive LGL lymphocytosis (i.e. after viral infection) * ALAT/ASAT or alkalin phosphatases \>3 times normal values * Creatinine clairance \<50 ml/min * Serologic evidence of HIV, hepatitis C or hepatitis B infection * Non effective contraception * Positive pregnancy test * Nursing woman

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2024-02-14