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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 :
Large Granular Lymphocyte (LGL) leukemia is a clonal disorder involving tissue invasion of marrow, spleen and liver. Clinical presentation is dominated by recurrent infections associated with neutropenia, anemia, splenomegaly, and auto-immune diseases, particularly rheumatoid arthritis. Both T cell and NK cell subtypes of LGL leukemia are indolent disease and considered as a chronic illness and lead to a treatment in more than 60% of patients.
LGL leukemia displays a chronic clinical course. Recommendations regarding therapy are similar for both subtypes. Indications for treatment include 1) severe neutropenia (ANC <500 mm3); 2) neutropenia (ANC <1500mm3) with symptomatic recurrent infections; 3) symptomatic or transfusion-dependent anemia and 4) associated autoimmune conditions requiring therapy, most often rheumatoid arthritis.
There is no standard treatment for patients with LGL leukemia. The numerous case reports published do not provide a consensus for a particular treatment. All the six largest series published in the literature so far (collecting data on more than 40 patients) are retrospective.
Immunosuppressive therapy remains the foundation of treatment including single three agents i.e. methotrexate, oral cyclophosphamide and ciclosporin A. However prospective trials involving large numbers of patients have not been performed and no molecule has proven superiority over others.
Invetigators 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. Combining the results of our series with those of the literature, invetigators estimate that overall response rate and complete response rate are 55% and 30% with methotrexate, 60% and 50% with cyclophosphamide, and 55% and less than 20% with ciclosporine A, respectively.
Thus, there are four objective in this study :
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| METHOTREXATE | Active Comparator | In step 1, 55 patients will receive methotrexate 10mg / m² orally once a week, (at split doses of 5 mg/m2 in the morning and 5 mg/m2 at night), that is to say 2 tablets of 2.5 mg at each take In step 2, responders at Month 4 (CR or PR) will be treated during 8 additional months with methotrexate at the same dosage. Non responders at Month 4 will be randomized and treated either by:
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| CYCLOPHOSPHAMIDE | Active Comparator | In step 1, 55 patients will receive cyclophosphamide 100 mg orally once daily, that is to say 2 tablets of 50 mg at each take. In step 2, responders at Month 4 (CR or PR) will be treated during 8 additional months with cyclophosphamide (at 50 mg orally once daily); Non responders at Month 4 will be randomized and treated either by:
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| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Methotrexate | Drug | methotrexate 10mg / m² orally once a week, (at split doses of 5 mg/m2 in the morning and 5 mg/m2 at night), that is to say 2 tablets of 2.5 mg at each take, during 4 months. |
| Measure | Description | Time Frame |
|---|---|---|
| Complete response (CR) | The main endpoint will be the hematological CR rate evaluated after 4 months of treatment (binary endpoint). Complete response (CR) is defined as a normalization of clinical examination (disappearance of splenomegaly) and a complete normalization of blood counts (i.e., hemoglobin >12g/dL, platelets >150x109/L, ANC >1.5x109/L), lymphocytosis <4x109/L and circulating LGL in the normal range (<0.3x109/L). The number of LGL will be quantitated on blood smears. | at Month 4 |
| Measure | Description | Time Frame |
|---|---|---|
| overall response rate (ORR) | Hematological overall response rate (ORR) defined as the sum of complete responses and partial responses over the total number of patients. | at Month 4, and at Month 8 and Month 12 in non-responders at Month 4 |
| Complete response (CR) |
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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:
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.
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:
Written informed consent
Exclusion Criteria:
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| CHU Sud | Amiens | 80054 | France | |||
| CHU Angers |
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| Cyclophosphamide | Drug | cyclophosphamide 100 mg orally once daily, that is to say 2 tablets of 50 mg at each take, during 4 months. |
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Complete response (CR) is defined as a normalization of clinical examination (disappearance of splenomegaly) and a complete normalization of blood counts (i.e., hemoglobin >12g/dL, platelets >150x109/L, ANC >1.5x109/L), lymphocytosis <4x109/L and circulating LGL in the normal range (<0.3x109/L). The number of LGL will be quantitated on blood smears. |
| at Month 8 and Month 12 |
| Hematological partial response (PR) | Hematological partial response (PR) defined as an improvement in blood counts which do not meet criteria for complete remission (e.g., ANC increasing more than 50% and reaching more than 0.5 but less than 1.5x109/L with non-recurrence of infections, or hemoglobin level increasing more than 2 g/dL from baseline and transfusion requirements stopping without normalization of the hemoglobin level defined as hemoglobin >12g/dL). | at Month 4, Month 8 and Month 12 |
| Progressive disease | Progressive disease defined as worsening of cytopenia or organomegaly or incidence of infections. | at Month 4, Month 8 and Month 12 |
| Time-to-relapse | Time-to-relapse (censored variable). Relapse is defined as re-occurrence of either neutropenia or anemia (ANC <1x109/L and/or hemoglobin <10g/dL) or clonal LGL >0.5x109/L in complete responders, or as a return to baseline values of either ANC or hemoglobin in partial responders, at two monthly consecutive blood tests. | from Month 4 to endpoint (in first-line treatment responders) |
| Time-to-relapse | Time-to-relapse (censored variable). Relapse is defined as re-occurrence of either neutropenia or anemia (ANC <1x109/L and/or hemoglobin <10g/dL) or clonal LGL >0.5x109/L in complete responders, or as a return to baseline values of either ANC or hemoglobin in partial responders, at two monthly consecutive blood tests. | from Month 8 to endpoint (in second-line treatment responders) |
| Molecular remission | Molecular remission defined as the disappearance of the clonal pattern of TCR gamma multiplex rearrangement and Phenotypic remission is defined as :
| at Month 4 and Month 12 for hematological complete responders |
| Adverse events rate | Adverse events rate | Month 2, Month 4, Month 6, Month 8, Month 10, Month 12 |
| Compliance | Compliance | Month 2, Month 4, Month 6, Month 8, Month 10, Month 12 |
| relationship between the response to treatment and the phenotypic subtype | Identification of a relationship between the response to treatment and the phenotypic subtype characterized by the panel of monoclonal antibodies defined in the ancillary study subsection. | Day 1 |
| Angers |
| 49033 |
| France |
| Intern medecine Service - CH Antibes-Juan-les-Pins | Antibes | France |
| Hematology Service - CH Avignon | Avignon | 84902 | France |
| Hematology Service - CH de la cote basque | Bayonne | France |
| hematology service - CH Beauvais | Beauvais | 60021 | France |
| Hematology Service - CH Jean Minjoz | Besançon | 25030 | France |
| Hematology Service - CH Beziers | Béziers | 34500 | France |
| Hematology Unit - HOpital Avicienne | Bobigny | 93009 | France |
| Hematology Service - CH Docteur Duchenne | Boulogne-sur-Mer | 62321 | France |
| Hematology Service - CH de Brest | Brest | 29609 | France |
| Institut d'Hématologie de Basse Normandie | Caen | 14000 | France |
| Hematology Service - CH François Baclesse | Caen | 14076 | France |
| hematology Service - CH Louis Pasteur | Chartres | 28018 | France |
| Centre Hospitalier de Cholet | Cholet | 49300 | France |
| Hopital Inter-Armées Percy | Clamart | 92141 | France |
| hematology Service - CHU Estaing | Clermont-Ferrand | 63003 | France |
| Hematology Service - Civils hospital | Colmar | 68024 | France |
| Hematology Service CHSF | Corbeil-Essonnes | 91110 | France |
| CHU Henri Mondor Lymphoid Hemopathy Unit | Créteil | 94000 | France |
| Hematology Unit CH Michalon | Grenoble | 38043 | France |
| Hematology Unit CHD Vendée | La Roche-sur-Yon | 85925 | France |
| Hematology Unit CH LE MANS | Le Mans | 72000 | France |
| CH Robert Boulin | Libourne | 33500 | France |
| Hematology Unit CHRU Lille | Lille | 59037 | France |
| Hematology Unit CHU Dupuytren | Limoges | 87042 | France |
| CH de Bretagne Sud | Lorient | 56322 | France |
| Hematology Unit CHU La Conception | Marseille | 13005 | France |
| Hematology Unit - Institut Paoli-Calmettes | Marseille | 13009 | France |
| Hematology Unit CH Meaux | Meaux | 77100 | France |
| Hematology Unit CH Notre Dame Bon Secours | Metz | 57000 | France |
| Hematogy Unit CHU ST ELOI | Montpellier | 34295 | France |
| Hematology Unit CH E.MULLER | Mulhouse | 68070 | France |
| Internal Medicine - CHU Hotel Dieu | Nantes | France |
| Oncology Unit CH Antoine Lacassagne | Nice | France |
| hematology Unit CHU Caremeau | Nîmes | 30029 | France |
| Hematology Unit - CHR Orleans | Orléans | 45067 | France |
| Hematology Service - Hopital La Pitié Salpetrière | Paris | 75013 | France |
| Hematology Unit - Hopital Hotel Dieu | Paris | 75181 | France |
| Hematology Unit - Hopital Saint Antoine | Paris | 75571 | France |
| AP-HP Hôpital Necker - Enfants Malades | Paris | 75743 | France |
| Hematology Unit - Hopital Saint Louis | Paris | France |
| Hematology Unit Hopital Saint Jean | Perpignan | 66000 | France |
| Hematology Service- CH Haut Leveque | Pessac | 33604 | France |
| Hematology Unit CH LYON SUD | Pierre-Bénite | 69310 | France |
| Hematology Unit CHU La Miletrie | Poitiers | 86000 | France |
| Hematology Unit CH René DUBOS | Pontoise | 95000 | France |
| CH Annecy - Hematology Service | Pringy | 74374 | France |
| Hematology Unit- Hopital Robert Debré | Reims | 51092 | France |
| Hematology Service - CHU of Rennes | Rennes | 35000 | France |
| Hematology Unit - CH Becquerel | Rouen | 76038 | France |
| CH Yves Lefoll | Saint-Brieuc | 22027 | France |
| Oncology Unit - Institut de cancérologie de la Loire | Saint-Priest-en-Jarez | 60008 | France |
| CH Saint Quentin Oncohematology | Saint-Quentin | 21000 | France |
| Hematology Unit CHU Toulouse | Toulouse | 31000 | France |
| Hematology Unit CHU Bretonneau | Tours | 37044 | France |
| Hematology Unit Hopitaux de Brabois | Vandœuvre-lès-Nancy | 54511 | France |
| Intern Medecine Unit CHBA | Vannes | 56017 | France |
| Hôpital André Mignot Centre Hospitalier de Versailles | Versailles | 78157 | France |
| ID | Term |
|---|---|
| D008727 | Methotrexate |
| D003520 | Cyclophosphamide |
| ID | Term |
|---|---|
| D000630 | Aminopterin |
| D011622 | Pterins |
| D011621 | Pteridines |
| D006574 | Heterocyclic Compounds, 2-Ring |
| D000072471 | Heterocyclic Compounds, Fused-Ring |
| D006571 | Heterocyclic Compounds |
| D010752 | Phosphoramide Mustards |
| D009588 | Nitrogen Mustard Compounds |
| D009150 | Mustard Compounds |
| D006846 | Hydrocarbons, Halogenated |
| D006838 | Hydrocarbons |
| D009930 | Organic Chemicals |
| D063088 | Phosphoramides |
| D009943 | Organophosphorus Compounds |
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