Clinical Trial: Differentiation Therapy With Decitabine in Treating Patients With Myelodysplastic Syndrome

Study Status: Completed
Recruit Status: Completed
Study Type: Interventional

Official Title: A Proof of Concept Study of Non-DNA Damaging DNMT1 Depletion Therapy for Myelodysplastic Syndrome

Brief Summary: RATIONALE: Decitabine may help myelodysplastic cells become more like normal stem cells. PURPOSE: This clinical trial studies differentiation therapy with decitabine in treating patients with myelodysplastic syndrome.

Detailed Summary:

PRIMARY OBJECTIVES:

I. Demonstrate that differentiation therapy with DNMT1 depleting but non-DNA damaging doses of decitabine is efficacious and can be administered weekly for > = 12 months. SECONDARY OBJECTIVES: I. Assess safety of the regimen.

II. Retrospectively compare study and standard regimen clinical responses. III. Assess the ability of a pharmacodynamic assay that measures DNMT1 depletion in peripheral blood white blood cells to predict clinical responses to decitabine.

IV. Assess PCR for aberrant methylation signature as an early marker of relapse. V. Identify biologic features of MDS that correlate with response to decitabine, thereby facilitating future patient selection.

VI. In cases of relapse or resistance, assess the role of the enzyme CDA in altering decitabine metabolism and preventing DNMT1 depletion.

OUTLINE:

INDUCTION PHASE: Patients receive decitabine subcutaneously (SC) twice weekly for 4 weeks or thrice weekly until achieving bone marrow blasts < 5%.

MAINTENANCE PHASE: Patients then receive decitabine SC twice weekly for up to 52 weeks in the absence of disease progression or unacceptable toxicity. After completion of study treatment, patients are followed periodically.


Sponsor: Case Comprehensive Cancer Center

Current Primary Outcome: Number of Patients With Response as Defined by IWG (International Working Group) Criteria for Myelodysplasia [ Time Frame: Formal assessment at week 12 for study primary end-point (hematologic improvement). ]

The criteria for complete remission (CR) and partial remission (PR) involve specific improvements in marrow and peripheral blood measurements obtained on 2 or more successive assessments. The response parameters in peripheral blood must be maintained for at least 8 weeks. Responses designated as CR include less than 5% marrow blasts without evidence of dysplasia and normalization of peripheral blood counts, including a hemoglobin level of 110 g/L (11 g/dL) or more, a neutrophil count of 1.5 × 109/L or more, and a platelet count of 100 × 109/L or more. For PR, patients must demonstrate all CR criteria if abnormal before treatment except that marrow blasts should decrease by 50% or more compared with pretreatment levels, or patients may demonstrate a less-advanced MDS disease classification category than prior to treatment.


Original Primary Outcome: Hematologic Improvement as defined by IWG Criteria for Response in Clinical Trials [ Time Frame: Formal assessment at week 12 for study primary end-point (hematologic improvement). ]

Current Secondary Outcome:

  • Number of Patients That Experience > Grade 2 Non-hematologic Toxicity by National Cancer Institute (NCI)/Cancer Therapy Evaluation Program (CTEP) v4 Criteria [ Time Frame: up to 12 months of treatment ]
    Incidence of treatment-emergent adverse events (AEs) will be presented in tables that include causality, seriousness, severity/grade, and whether the AE resulted in death or discontinuation of treatment, Laboratory data will be summarized in tables that show changes from pre-treatment values and frequencies of abnormal values. Descriptive statistics will also be provided.
  • Cytogenetic Response as Per IWG Criteria [ Time Frame: at 12 months ]
    Described as the number of patients with a major cytogenetic response (refers to disappearance of a cytogenetic abnormality) or a minor cytogenetic response (50% or more reduction of abnormal metaphases).
  • Proportion of Patients With Pharmacodynamic Evidence of Drug Effect. [ Time Frame: Day 0, 42, 84 ]
    Evidence of pharmacodynamic effect will be correlated with clinical response criteria.
  • Proportion of Patients With Bone Marrow Evidence of Cytotoxicity. [ Time Frame: Day 0, 42, 84 ]
    Cytotoxicity will be correlated with clinical response criteria
  • Proportion of Patients With Bone Marrow Evidence of Terminal Differentiation Response to Therapy. [ Time Frame: Day 0,42,84 ]
    Bone marrow evidence of terminal differentiation will be correlated with response criteria
  • Proportion of Patients With Particular Genetic Abnormalities Detected by Whole Exome Sequencing Correlation With Clinical Response [ Time Frame: Baseline ]
    Proportion of patients with particular genetic abnormalities detected by whole exome sequencing correlation with clinical response


Original Secondary Outcome:

  • NCI Common Toxicity Criteria for Adverse Events (CTCAE), Version 4.0 [ Time Frame: Blood counts are CBC with differential and reticulocyte count, every week from week 1-12 then every 2 weeks. Drug dose and schedule is interrupted or modified based on peripheral blood counts as described in detail in 'Dose Modification for Toxicity'. ]
  • Complete hematologic remission, and other measures of response and duration as per IWG criteria [ Time Frame: Protocol treatment will continue for 52 weeks or until disease progression, relapse or failure, whichever comes first. ]
  • Correlation of DNMT1 depletion with clinical response criteria [ Time Frame: D42 (w6), D84, 168, 365 & relapse, Q56 day ]
  • Response by aberrant methylation signature [ Time Frame: Day 84, 168, 365 & relapse, Q56 day ]
  • Correlation of cytogenetic and methylome profile (measured by microarray) with clinical response criteria [ Time Frame: Day 42(cytogenetic), 84, 168, 365 & relapse ]
  • Correlation of CDA genotype and expression with clinical response criteria [ Time Frame: Day 84, 168, 365 & relapse ]


Information By: Case Comprehensive Cancer Center

Dates:
Date Received: July 14, 2010
Date Started: July 2010
Date Completion:
Last Updated: February 25, 2013
Last Verified: February 2013