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NCT00222612 Clinical Trial

Medical Research Council (MRC) Working Party on Leukaemia in Children UK National Acute Lymphoblastic Leukaemia (ALL) Trial: UKALL 2003

Acute Lymphoblastic Leukemia Clinical Trial

Official title:
Medical Research Council Working Party on Leukaemia in Children UK National Acute Lymphoblastic Leukaemia (ALL) Trial: UKALL 2003

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT00222612
Other study ID # UKALL2003
Secondary ID
Status Recruiting
Phase Phase 4
First received September 13, 2005
Last updated February 2, 2010
Start date October 2003
Est. completion date August 2013

Study information
Verified date February 2010
Source University of Oxford
Contact Susan Richards, D Phil
Email Sue.Richards@ctsu.ox.ac.uk
Is FDA regulated No
Health authority United Kingdom: National Health Service
Study type Interventional

Clinical Trial Summary

A randomised trial for children with acute lymphoblastic leukemia, using the detection of minimal residual disease to define risk groups, aiming to answer the questions:

1. Can treatment be reduced without compromising efficacy in a MRD-defined low risk group?

2. Does further post-remission intensification improve outcome for a MRD-defined high risk group?

3. Measure the Quality of Life impact of the different treatment arms on the children and their families.

Description:

Randomisations

Patients will be assigned to MRD risk groups based on day 29 and post consolidation MRD results and randomised as follows:

1. MRD Low Risk Group (MRD negative at day 29 and week 11 or positive <1 x 10-4 at day 28 and negative at week 11) will continue on previously assigned Regimens (A or B) but randomised between two delayed intensifications and one delayed intensification.

2. MRD High Risk Group (MRD positive > 1 x 10-4 at day 29) randomised between previously assigned Regimen (A or B) and Regimen C.

3. MRD Indeterminate Group (No MRD result or MRD positive <1 x 10-4 at day 29 and at week 11) will continue on previously assigned Regimen (A or B) and received two delayed intensifications

Recruitment information / eligibility
Status Recruiting
Enrollment 2100
Est. completion date August 2013
Est. primary completion date August 2013
Accepts healthy volunteers No
Gender Both
Age group 1 Year to 18 Years
Eligibility Inclusion criteria:

Children aged 1 - 18 years with ALL except the following:

Exclusion criteria:

1. Infants less than a year old should be entered onto the Interfant ALL study.

2. Children with B-ALL (Burkitt-like, t(8;14), L3 morphology, SMIg positive). Patients with this disease will be eligible for the current UKCCSG B cell NHL/ALL trial.

3. Children with Philadelphia-positive ALL (t(9;22) or BCR/ABL positive) will start induction therapy on this protocol but transfer to the European Intergroup Protocol as soon as their Philadelphia status is known.

Initially, eligible patients will be stratified into three risk groups based on the following criteria:

1. Standard risk: all children >1<10 years with a highest white cell count before starting treatment of <50x109/l, and who do not have BCR-ABL, hypodiploidy (=44 chromosomes), or an MLL gene rearrangement.

2. Intermediate risk: all children =10 years old, or with a diagnostic WBC =50x109/l (or both) and who do not have BCR-ABL, hypodiploidy (=44 chromosomes), or an MLL gene rearrangement.

3. High Risk: all children, irrespective of initial risk category, who have a slow early response (SER) as defined below - see section 6 - together with those who have BCR-ABL (induction only), hypodiploidy (=44 chromosomes), or an MLL gene rearrangement. These patients will not be eligible for MRD randomisation.

Patients will then start treatment according to their risk group as follows:

1. Standard risk, (around 60-65% of the total): regimen A - three-drug induction.

2. Intermediate risk, (around 20- 30% of the total): regimen B - four-drug induction.

3. High risk (around 10-12% of the total): These patients will not be eligible for MRD randomisation. They will be allocated regimen C - four drug induction, augmented BFM consolidation, Capizzi interim maintenance, and two further BFM-style intensification periods of extended duration.

Inclusion criteria for entry into the randomisations:

1. Standard or Intermediate Risk as defined above.

2. Morphological Complete Remission (BM1 Marrow) at Day 29 of Induction.

3. Availability of MRD results at Day 28 and after consolidation therapy.

4. Informed consent obtained.

5. Induction given as protocol.

Exclusion criteria for entry into the MRD randomisation:

1. High Risk as defined above. These patients will receive Regimen C.

2. Day 28 non-remitters. These patients will receive Regimen C if BM2 or go off-protocol if BM3 (see below for definitions of BM2 and BM3).

3. MRD Indeterminate Group (No result or MRD positive < 1 x 10-4 at day 28 and after consolidation therapy) will continue on previously assigned therapy.

4. Sub-optimal induction therapy. The clinical significance of day 28 MRD is uncertain in patients who have received sub-optimal induction therapy. Please discuss these patients with a co-ordinator.

Study Design

Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment

Related Conditions & MeSH terms

Intervention

Other:
Reduced intensification
Deletion of one 7 week treatment block containing dexamethasone, vincristine, doxorubicin, Peg-asparaginase, intrathecal methotrexate, cyclophosphamide, cytarabine.
Drug:
Standard childhood UK ALL protocol
No additional treatment to standard protocol.
Intensified treatment including Capizzi maintenance
Augmented consolidation: vincristine, Peg-asparaginase. Capizzi maintenance: iv methotrexate and peg-asparaginase

Locations
Country Name City State
United Kingdom Sheffield Children's Hospital Sheffield

Sponsors (2)
Lead Sponsor Collaborator
University of Oxford Medical Research Council

Country where clinical trial is conducted

United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary Event free survival 5 years No
Secondary Survival 5 years No
Secondary Quality of life 3 years No
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