Multiple Myeloma Clinical Trial
— MoTDOfficial title:
A Multi-centre Phase II Trial of GVHD Prophylaxis Following Unrelated Donor Stem Cell Transplantation Comparing Thymoglobulin vs. Calcineurin Inhibitor or Sirolimus-based Post-transplant Cyclophosphamide
A multi-centre phase II trial of GvHD prophylaxis following unrelated donor stem cell transplantation comparing Thymoglobulin vs. Calcineurin inhibitor or Sirolimus-based post-transplant cyclophosphamide.
Status | Recruiting |
Enrollment | 400 |
Est. completion date | January 2026 |
Est. primary completion date | January 2026 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 16 Years to 70 Years |
Eligibility | Inclusion Criteria: - Availability of suitably matched unrelated donor (9/10 or 10/10) - Planned to receive one of the following RIC protocols: - Fludarabine-Melphalan (Fludarabine 120-180mg/m2 IV; melphalan = 150mg/m2 IV) - BEAM or LEAM (carmustine 300mg/m2 IV or lomustine 200mg/m2 IV with: etoposide 800 mg/m2 IV; cytarabine 1600mg/m2 IV; melphalan 140mg/m2 IV) - Fludarabine-Busulphan (Fludarabine 120-180mg/m2 IV; Busulphan = 8mg/kg PO or 6.4mg/kg IV) - Fludarabine- Treosulfan (Fludarabine 150mg/m2 IV; Treosulfan 30g/m2 IV) - Planned use of PBSCs for transplantation - Planned allo-SCT for one of the following haematological malignancies: - AML in CR (patients enrolled onto the COSI trial are not eligible for this study) - ALL in CR (patients enrolled onto the ALL-RIC trial are not eligible for this study) - CMML <10% blasts - MDS <10% blasts (patients enrolled onto the COSI trial are not eligible for this study) - NHL in CR/PR - HL in CR/PR - MM in CR/PR - CLL in CR/PR - CML in 1st or 2nd chronic phase - Myelofibrosis - Age 16-70 years - Females of and male patients of reproductive potential (i.e., not post-menopausal or surgically sterilised) must agree to use appropriate, highly effective, contraception from the point of commencing therapy until 12 months after transplant Exclusion Criteria: - Use of any method of graft manipulation (excluding storage of future DLI) - Use of alemtuzumab or any method of T cell depletion except those that are protocol-defined - Known hypersensitivity to study drugs or history of hypersensitivity to rabbits - Pregnant or lactating women - Adults of reproductive potential not willing to use appropriate, highly effective, contraception during the specified period - Life expectancy <8 weeks - Active HBV or HCV infection - Organ dysfunction defined as: - LVEF <45% - GFR <50ml/min - Bilirubin >50µmol/l - AST/ALT>3 x ULN - Participation in COSI or ALL-RIC trials - Contraindication to treatment with the study drugs (Thymoglobulin, cyclophosphamide, sirolimus, ciclosporin and mycophenolate mofetil) as detailed in each study drug SPC. - Patient has any other systemic dysfunction (e.g., gastrointestinal, renal, respiratory, cardiovascular) or significant disorder which, in the opinion of the investigator would jeopardise the safety of the patient by taking part in the trial. |
Country | Name | City | State |
---|---|---|---|
United Kingdom | Queen Elizabeth Hospital | Birmingham | |
United Kingdom | Bristol Haematology and Oncology Centre | Bristol | |
United Kingdom | Addenbrookes Hospital | Cambridge | |
United Kingdom | University Hospital of Wales | Cardiff | Wales |
United Kingdom | Queen Elizabeth Hospital Glasgow | Glasgow | |
United Kingdom | St Jame's University Hospital | Leeds | |
United Kingdom | Hammersmith Hospital | London | |
United Kingdom | King's College Hospital | London | |
United Kingdom | University College London Hospital | London | |
United Kingdom | Manchester Royal Infirmary | Manchester | |
United Kingdom | The Christie | Manchester | |
United Kingdom | Freeman Hospital | Newcastle Upon Tyne | |
United Kingdom | Nottingham City Hospital | Nottingham | |
United Kingdom | Churchill Hospital | Oxford | |
United Kingdom | Derriford Hospital | Plymouth |
Lead Sponsor | Collaborator |
---|---|
University of Birmingham | IMPACT (funded by NHS Blood & Transplant, Anthony Nolan and Leukaemia UK) |
United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | GVHD-free, relapse-free survival | GVHD assessment scoring will be performed as per the modified Glucksberg criteria (revised by MAGIC) and the National Institutes of Health (NIH) criteria. GvHD-free, relapse-free survival (GRFS) defined as the time from date of day 0 (defined as the day of stem cell infusion) to the date of first event or death from any cause. An event is defined as GvHD (both acute and chronic), relapse or progression. Patients who are alive and event free at the end of the trial will be censored at their date of last follow-up | at 1 year | |
Secondary | Cumulative incidence of acute grade II-IV and III-IV GvHD | GVHD assessment scoring will be performed as per the modified Glucksberg criteria (revised by MAGIC) and the National Institutes of Health (NIH) criteria. GvHD-free | at 1 year | |
Secondary | Cumulative incidence of moderate and severe chronic GvHD | GVHD assessment scoring will be performed as per the modified Glucksberg criteria (revised by MAGIC) and the National Institutes of Health (NIH) criteria. GvHD-free | at 1 year | |
Secondary | Cumulative incidence of NRM | Non-relapse mortality (NRM) is defined as the time from day 0 to date of non-relapse death. Patients who die post-relapse from any other cause will be considered a competing risk and patients alive at the end of the trial will be censored at their date last seen. | at 1 year | |
Secondary | Overall survival | Overall survival (OS) is defined as the time from day 0 to date of death, from any cause. Patients who are alive at the end of the trial will be censored at their date last seen. | at 1 year | |
Secondary | Progression-free survival | Progression-free survival (PFS) is defined as the time from day 0 to date of first relapse/progression or death from any cause. Patients who are alive and progression free at the end of the trial will be censored at their date last seen. | at 1 year | |
Secondary | Immune suppression-free survival | Immune suppression-free survival is defined as time from day 0 to the date of first immunosuppressive agent use. Patients who are alive and immune suppression free at the end of the trial will be censored at their date last seen | at 1 year | |
Secondary | Cumulative incidence of engraftment | Cumulative incidence of engraftment defined as time from day 0 to date of engraftment (Neutrophil engraftment defined to be the first of 3 consecutive days a neutrophil count = 0.5×?10?^9/L is reached and platelet engraftment defined to be the first of 3 consecutive days an unsupported platelet count = 20×?10?^9/L is reached). Patients who relapse/progress or die prior to relapse, progression or engraftment will be considered a competing risk at their date of relapse/progression for the former and date of death for the latter. Patients alive and engraftment free at the end of the trial will be censored at their date last seen. | at 1 year | |
Secondary | The incidence of full donor chimerism | Engraftment will be assessed by lineage specific chimerism measurements. Lineage specific chimerism in both whole blood and T-cell compartments (where possible) will be assessed as per local procedure, performed at 3 monthly intervals for the first 12 months post-transplant; at day 100 and then months 6, 9 and 12. Tests should be performed in local laboratories. | at 100 days | |
Secondary | The cumulative incidence of infection requiring inpatient admission | The cumulative incidence of infection requiring inpatient admission measured by blood test and tissue culture at 1 year | at 1 year | |
Secondary | The number of inpatient days | The sum of inpatients days | during first 12 months | |
Secondary | The timing of mixed chimerism, persistent disease or relapse | We will be recording the time (days, post-transplant) whenever mixed chimerism, persistent disease or relapse occurred post transplant | during first 12 months | |
Secondary | Cumulative incidence of EBV-related PTLD | Measured by blood sample, EBV PCR testing. | during first 12 months | |
Secondary | The number of doses of Rituximab administered for EBV reactivation | We will collect the number of doses every time the patient will receive Rituximab whenever there is EBV reactivation | during first 12 months | |
Secondary | QoL measured by FACT-BMT questionnaire | QoL measured by FACT-BMT questionnaire at baseline, 6 months and 12 months. FACT-BMT Questionnaire uses Units on a scale 0-4, higher scores mean a better outcome. | at baseline, 6 months and 12 months | |
Secondary | Cumulative incidence of patients with haemorrhagic cystitis | Cumulative incidence of patients with haemorrhagic cystitis measured by blood and urine sample at 1 year | at 1 year | |
Secondary | Cumulative incidence of CMV viremia and CMV end-organ disease | Cumulative incidence of CMV viremia and CMV end-organ disease measured by blood sample at 1 year | at 1 year | |
Secondary | Safety defined as the incidence of = grade 3 toxicities reported as per the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) V4.0 | . Safety defined as the incidence of = grade 3 toxicities reported as per the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) v4.0. Details of all AEs will be documented and reported from the date of commencement of protocol defined treatment until 28 days after the administration of the last dose of IMP. Serious AEs will be reported from the date of consent. | from the date of commencement of protocol defined treatment until 28 days after the administration of the last dose of IMP. | |
Secondary | Tolerability defined to be the number of patients able to complete therapy as scheduled | Tolerability defined to be the number of patients able to complete therapy as scheduled (excluding any patients who discontinued treatment due to toxicities | during first 12 months | |
Secondary | Dose of Donor lymphocyte infusion (DLI) for mixed chimerism, persistent disease or relapse | We will be collecting the dose of DLI (CD3 Cells/kg) whenever required for mixed chimerism, persistent disease or relapse | during first 12 months |
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