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S0333 Combination Chemotherapy in Treating Patients With Newly Diagnosed Acute Lymphoblastic Leukemia

A Phase II Study of Double Induction Chemotherapy for Newly Diagnosed Non-L3 Adult Acute Lymphoblastic Leukemia With Investigation of Minimal Residual Disease and Risk of Relapse Following Maintenance Chemotherapy

Status
Completed
Phases
Phase 2
Study type
Interventional
Source
ClinicalTrials.gov
Registry ID
NCT00109837
Enrollment
79
Registered
2005-05-04
Start date
2005-04-30
Completion date
2014-11-30
Last updated
2015-03-25

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Leukemia

Keywords

L1 adult acute lymphoblastic leukemia, L2 adult acute lymphoblastic leukemia, untreated adult acute lymphoblastic leukemia

Brief summary

RATIONALE: Drugs used in chemotherapy work in different ways to stop the growth of cancer cells, either by killing the cells or by stopping them from dividing. Giving more than one drug (combination chemotherapy), and giving the drugs in different combinations may kill more cancer cells. PURPOSE: This phase II trial is studying how well combination chemotherapy works in treating patients with newly diagnosed acute lymphoblastic leukemia.

Detailed description

OBJECTIVES: Primary * Determine the probability of 1-year continuous complete remission in patients with newly diagnosed acute lymphoblastic leukemia treated with first induction chemotherapy comprising daunorubicin, vincristine, prednisone, and pegaspargase; and second induction chemotherapy comprising high-dose cytarabine and mitoxantrone. Secondary * Determine the frequency and severity of toxic effects of these induction regimens followed by consolidation therapy comprising cyclophosphamide, cytarabine, mercaptopurine, and methotrexate and maintenance chemotherapy comprising mercaptopurine, methotrexate, vincristine, doxorubicin, dexamethasone, cyclophosphamide, thioguanine, and cytarabine in these patients. Other objectives (if funding allows): * To evaluate in a preliminary manner the significance of detecting minimal residual disease as a prognostic factor for survival and relapse-free survival of patients receiving chemotherapy * To evaluate in a preliminary manner the pattern of gene expression of patients entered onto the trial and its relationship to cytogenetics/FISH risk classification, overall survival, and relapse-free survival OUTLINE: This is a multicenter study. * First induction chemotherapy: Patients receive daunorubicin IV on days 1-3; vincristine IV on days 1, 8, 15, and 22; prednisone IV or orally on days 1-28, followed by a taper to day 35; and pegaspargase IV or subcutaneously (SC) on day 15. Patients with CNS leukemia also receive methotrexate intrathecally (IT) or intraventricularly twice weekly and oral leucovorin calcium four times daily for 4 doses after each administration of methotrexate. When blasts are no longer present in the spinal fluid, patients receive methotrexate IT or intraventricularly once weekly for 4 weeks and then once monthly for 1 year. Patients are reevaluated on day 28. Patients who achieve A1 bone marrow status and B1 peripheral blood status or those with resistant disease proceed to second induction therapy. * Second induction chemotherapy: Patients receive high-dose cytarabine IV on days 1-5; mitoxantrone IV on day 3; and filgrastim (G-CSF) SC or IV beginning on day 7 and continuing until blood counts recover. Patients with CNS leukemia also receive methotrexate and leucovorin calcium as in first induction chemotherapy. Patients are reevaluated on day 28. Patients who achieve A1 bone marrow status and B1 peripheral blood status with no extramedullary disease (other than CNS involvement) proceed to consolidation chemotherapy. Patients with resistant disease OR Philadelphia chromosome- or BCR/ABL-positive disease are removed from the study after receiving double induction chemotherapy. * Consolidation chemotherapy: Patients receive cyclophosphamide IV on days 1, 15, and 29; cytarabine IV on days 2-5 and 16-19; oral mercaptopurine on days 1-28; and methotrexate IT or intraventricularly on days 2, 9, 16, and 23. Patients with CNS leukemia also undergo cranial radiotherapy once daily, 5 days a week, for 2 weeks. Patients in complete remission proceed to maintenance chemotherapy. * Maintenance chemotherapy: * Course 1: Patients receive oral mercaptopurine on days 1-63 and oral methotrexate on days 1, 8, 15, 22, 29, 36, 43, 50, and 57. Patients proceed to course 2 after blood counts recover. * Course 2: Patients receive vincristine IV and doxorubicin IV on days 1, 8, 15, and 22 and oral dexamethasone on days 1-28. Patients proceed to course 3 after blood counts recover. * Course 3: Patients receive cyclophosphamide IV on day 1; oral thioguanine on days 1-14; and cytarabine IV on days 3-6 and 10-13. Patients proceed to course 4 after blood counts recover. * Course 4: Patients receive oral mercaptopurine once daily for 2 years and oral methotrexate once weekly for 2 years. Treatment continues in the absence of disease relapse or unacceptable toxicity. After completion of study therapy, patients are followed every 3 months for 1 year, every 6 months for 1 year, and then annually for 3 years.

Interventions

BIOLOGICALfilgrastim

As needed per physician discretion

DRUGcyclophosphamide

Cyclophosphamide Consolidation: 650 mg/m2; IV; days 1, 15, 29 Post-consolidation course 3: 650 mg/m2; IV; day 1

DRUGcytarabine

Induction 2: 3 g/m2; IV over 3 hrs; days 1-5 Consolidation: 75 mg/m2/d; IV push; days 2-5 and 16-19 Post-consolidation course 3: 75 mg/m2/d; IV push; days 3-6 and 10-13

DRUGdaunorubicin

Induction: 60 mg/m2/d; IV; days 1, 2, and 3

DRUGdexamethasone

Induction 2: 0.1% QID; eye drops; days 1-6 Post consolidation course 2: 10 mg/m2/d; PO; days 1-28

DRUGdoxorubicin

Post consolidation: 25 mg/m2; IV; days 1, 8, 15, and 22

DRUGleucovorin

For CNS during induction: 5 mg every 6 hrs for 4 doses; PO; days 1, 4, 8, 11, etx.; after methotrexate if WBC \< 3,000

DRUGmercaptopurine

Consolidation: 60 mg/m2; PO; days 1-28 Post-consolidation course 1: 60 mg/m2/d; PO; days 1-63 Post-consolidation course 4: 60 mg/m2/d; PO; daily for 2 yrs

DRUGmethotrexate

Consolidation: 12 mg; intrathecal or intraventricularly; days 2, 9, 16, and 23 Post-consolidation course 1: 20 mg/m2/wk; PO; days 1, 8 15, 22, 29, 36, 43, 50, 57 Post-consolidation course 4: 20 mg/m2; PO; weekly for 2 yrs

DRUGmitoxantrone

Induction 2: 80 mg/m2; IV; day 3

DRUGAsparaginase

Induction: 2,000 IU/m2; IM or IV; day 15

DRUGprednisone

Induction: 60 mg/m2/d; PO or IV; days 1-35

DRUGthioguanine

Post-consolidation course 3: 60 mg/m2/d; PO; days 1-14

DRUGvincristine

Induction: 1.4 mg/m2/d (2 mg max); IV; days 1, 8, 15, 22

RADIATIONradiation therapy

For CNS during consolidation: cranial radiation after blasts are no longer present in spinal fluid. Total dose of 1800 cGy over 2 wks in 10 fractions of 180 cGy 5 days/wk.

DRUGallopurinol

300 mg/d PO Days 1-7

DRUGbactrim

1 double strenth tablet 2x/d, 2x/wk, PO, begin with prednisone

Sponsors

National Cancer Institute (NCI)
CollaboratorNIH
SWOG Cancer Research Network
Lead SponsorNETWORK

Study design

Allocation
NA
Intervention model
SINGLE_GROUP
Primary purpose
TREATMENT
Masking
NONE

Eligibility

Sex/Gender
ALL
Age
18 Years to 64 Years
Healthy volunteers
No

Inclusion criteria

DISEASE CHARACTERISTICS: * Morphologically confirmed acute lymphoblastic leukemia (ALL), meeting any of the following criteria: * FAB class L1 or L2 disease * Mixed lineage ALL * Ph-negative/BCR/ABL-negative * Newly diagnosed disease * Patients with the following diagnoses are not eligible: * FAB class L3 ALL * Non-Hodgkin's lymphoma * Chronic myelogenous leukemia in lymphoid blast crisis * Mixed lineage acute myeloid leukemia * Acute minimally differentiated myeloid leukemia (M0) * Must be registered on protocols SWOG-9007 AND SWOG-S9910 PATIENT CHARACTERISTICS: Age * 18 to 64 Performance status * Zubrod 0-3 Life expectancy * Not specified Hematopoietic * Not specified Hepatic * No chronic liver disease * Hepatitis panel, including hepatitis B and C, negative * History of hepatitis A with positive antibody allowed Renal * Creatinine ≤ 1.5 times upper limit of normal OR * Creatinine clearance \> 60 mL/min Cardiovascular * Left ventricular function normal * Ejection fraction ≥ 50% by MUGA or 2-dimensional echocardiogram * No symptomatic congestive heart failure * No coronary artery disease * No cardiomyopathy * No uncontrolled arrhythmia Other * Not pregnant or nursing * Fertile patients must use effective contraception * HIV negative * No other malignancy within the past 5 years except adequately treated basal cell or squamous cell skin cancer, carcinoma in situ of the cervix, or adequately treated stage I or II cancer in complete remission PRIOR CONCURRENT THERAPY: Biologic therapy * Not specified Chemotherapy * No prior remission induction chemotherapy for ALL * Prior hydroxyurea to control WBC count allowed Endocrine therapy * Not specified Radiotherapy * Not specified Surgery * Not specified Other * No other prior treatment for ALL

Design outcomes

Primary

MeasureTime frameDescription
Continuous Complete Remission at 1 YearAfter induction, after consolidation, every 3 months during maintenance, and every three months after off treatment for up to a yearA patient has a continuous complete remission at 1 year if they achieve a CR and are alive 365 days after registering to the study.

Secondary

MeasureTime frameDescription
ToxicityPatients were assessed for adverse events after the induction cycleNumber of patients with Grade 3-5 adverse events that are related to study drug by given type of adverse event

Countries

United States

Participant flow

Participants by arm

ArmCount
Treatment
Treatment included: Induc 1: Allo; Dauno; Vin; Pred; asparag; Bactrim Induc 2: Allo; AraC; Dex; GCSF; Mitx; Meth; leuc; Meth Consol: cyclo; AraC; 6-mercapto; Meth; GCSF Maint:Course 1: 6-mercapto; Meth 20 Course 2: Vincristine; Adriamycin; Dex Course 3: Cyclo; 6-thio; AraC Course 4: 6-mercapto; meth
60
Total60

Withdrawals & dropouts

PeriodReasonFG000
Overall StudyAdverse Event2
Overall StudyBCR/ABL+ or Ph+17
Overall StudyDeath1
Overall StudyIneligible1
Overall StudyNot treated1
Overall StudyRefusal unrelated to adverse effects1

Baseline characteristics

CharacteristicTreatment
Age, Continuous42 years
Region of Enrollment
United States
60 participants
Sex: Female, Male
Female
20 Participants
Sex: Female, Male
Male
40 Participants

Adverse events

Event typeEG000
affected / at risk
EG001
affected / at risk
EG002
affected / at risk
EG003
affected / at risk
deaths
Total, all-cause mortality
— / —— / —— / —— / —
other
Total, other adverse events
71 / 7554 / 5633 / 3311 / 12
serious
Total, serious adverse events
2 / 752 / 561 / 330 / 12

Outcome results

Primary

Continuous Complete Remission at 1 Year

A patient has a continuous complete remission at 1 year if they achieve a CR and are alive 365 days after registering to the study.

Time frame: After induction, after consolidation, every 3 months during maintenance, and every three months after off treatment for up to a year

Population: Eligible, Ph-, treated, and evaluable patients

ArmMeasureValue (NUMBER)
TreatmentContinuous Complete Remission at 1 Year21 participants
Comparison: The regimen would be of no further interest if the true 1-year continuous complete remission (CCR) rate was less than 45% (null). Sample size was chosen for an alternative of 65%, power of 92% and type-1 error of 4.6%.
Secondary

Toxicity

Number of patients with Grade 3-5 adverse events that are related to study drug by given type of adverse event

Time frame: Patients were assessed for adverse events after the induction cycle

Population: Eligible patients who started therapy

ArmMeasureGroupValue (NUMBER)
TreatmentToxicityALT, SGPT (serum glutamic pyruvic transaminase)17 Participants with a given type of AE
TreatmentToxicityAST, SGOT (serum glut oxaloacetic transaminase)13 Participants with a given type of AE
TreatmentToxicityAlbumin, serum-low (hypoalbuminemia)3 Participants with a given type of AE
TreatmentToxicityAlkaline phosphatase2 Participants with a given type of AE
TreatmentToxicityAnorexia2 Participants with a given type of AE
TreatmentToxicityAscites (non-malignant)1 Participants with a given type of AE
TreatmentToxicityBilirubin (hyperbilirubinemia)6 Participants with a given type of AE
TreatmentToxicityCalcium, serum-low (hypocalcemia)7 Participants with a given type of AE
TreatmentToxicityCholecystitis1 Participants with a given type of AE
TreatmentToxicityCholesterol, serum-high (hypercholesterolemia)2 Participants with a given type of AE
TreatmentToxicityCoagulation-Other (Specify)1 Participants with a given type of AE
TreatmentToxicityColitis, infectious (e.g., Clostridium difficile)1 Participants with a given type of AE
TreatmentToxicityConstipation1 Participants with a given type of AE
TreatmentToxicityDIC (disseminated intravascular coagulation)2 Participants with a given type of AE
TreatmentToxicityDeath not assoc with CTCAE term-Multi-organ fail1 Participants with a given type of AE
TreatmentToxicityEdema: limb1 Participants with a given type of AE
TreatmentToxicityFatigue (asthenia, lethargy, malaise)3 Participants with a given type of AE
TreatmentToxicityFebrile neutropenia18 Participants with a given type of AE
TreatmentToxicityFever (in the abs of neutropenia)1 Participants with a given type of AE
TreatmentToxicityFibrinogen11 Participants with a given type of AE
TreatmentToxicityGlucose, serum-high (hyperglycemia)16 Participants with a given type of AE
TreatmentToxicityGlucose, serum-low (hypoglycemia)1 Participants with a given type of AE
TreatmentToxicityHemoglobin33 Participants with a given type of AE
TreatmentToxicityHypertension2 Participants with a given type of AE
TreatmentToxicityHypotension3 Participants with a given type of AE
TreatmentToxicityHypoxia2 Participants with a given type of AE
TreatmentToxicityIleus, GI (functional obstruction of bowel)1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Anal1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Bladder1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Blood11 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Bronchus1 Participants with a given type of AE
TreatmentToxicityIInfec(doc clin or mibio) w/ Gr 3/4 neut-Catheter1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Eye NOS1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Lung1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Nose1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Pharynx1 Participants with a given type of AE
TreatmentToxicityInfec(doc clin or mibio) w/ Gr 3/4 neut-Ur tract2 Participants with a given type of AE
TreatmentToxicityInfec with nor ANC or Gr 1/2 neut-Lung (pneumonia)2 Participants with a given type of AE
TreatmentToxicityInfection-Other (Specify)1 Participants with a given type of AE
TreatmentToxicityLeukocytes (total WBC)43 Participants with a given type of AE
TreatmentToxicityLipase1 Participants with a given type of AE
TreatmentToxicityLiver dysfunction/failure (clinical)2 Participants with a given type of AE
TreatmentToxicityLymphopenia19 Participants with a given type of AE
TreatmentToxicityMagnesium, serum-high (hypermagnesemia)1 Participants with a given type of AE
TreatmentToxicityMucositis/stomatitis (clinical exam) - Oral cavity2 Participants with a given type of AE
TreatmentToxicityMucositis/stomatitis (funct/symp) - Oral cavity1 Participants with a given type of AE
TreatmentToxicityMucositis/stomatitis (func/symp) - Pharynx1 Participants with a given type of AE
TreatmentToxicityMuscle weak,gen spec area-Whole body2 Participants with a given type of AE
TreatmentToxicityNausea3 Participants with a given type of AE
TreatmentToxicityNeuropathy: motor1 Participants with a given type of AE
TreatmentToxicityNeutrophils/granulocytes (ANC/AGC)47 Participants with a given type of AE
TreatmentToxicityPain - Abdomen NOS1 Participants with a given type of AE
TreatmentToxicityPain - Bone1 Participants with a given type of AE
TreatmentToxicityPain - Neck1 Participants with a given type of AE
TreatmentToxicityPancreatic endocrine: glucose intolerance1 Participants with a given type of AE
TreatmentToxicityPancreatitis1 Participants with a given type of AE
TreatmentToxicityPhosphate, serum-low (hypophosphatemia)1 Participants with a given type of AE
TreatmentToxicityPlatelets44 Participants with a given type of AE
TreatmentToxicityPotassium, serum-high (hyperkalemia)1 Participants with a given type of AE
TreatmentToxicityPotassium, serum-low (hypokalemia)7 Participants with a given type of AE
TreatmentToxicityRash/desquamation1 Participants with a given type of AE
TreatmentToxicityRenal failure2 Participants with a given type of AE
TreatmentToxicitySodium, serum-low (hyponatremia)6 Participants with a given type of AE
TreatmentToxicityThrombosis/thrombus/embolism1 Participants with a given type of AE
TreatmentToxicityThrombotic microangiopathy2 Participants with a given type of AE
TreatmentToxicityTriglyceride, serum-high (hypertriglyceridemia)1 Participants with a given type of AE
TreatmentToxicityTumor lysis syndrome5 Participants with a given type of AE
TreatmentToxicityTyphlitis (cecal inflammation)1 Participants with a given type of AE
TreatmentToxicityUric acid, serum-high (hyperuricemia)1 Participants with a given type of AE
TreatmentToxicityVomiting1 Participants with a given type of AE

Source: ClinicalTrials.gov · Data processed: Feb 24, 2026