Up-front Matched Unrelated Donor Transplantation in Pediatric Patients With Idiopathic Aplastic Anemia

Severe Aplastic Anemia Clinical Trial

— UPFRONT-MUD  

Official title:

Up-front Matched Unrelated Donor Transplantation in Pediatric Patients With Idiopathic Aplastic Anemia: a Phase II Feasibility Study

Clinical Trial Details — Status: Not yet recruiting

Administrative data

• NCT number: NCT05419843
• Other study ID #: APHP 200005
• Status: Not yet recruiting
• Phase: Phase 2
• Start date: June 2022
• Est. completion date: June 2027

Study information

• Verified date: May 2022
• Source: Assistance Publique - Hôpitaux de Paris
• Contact: Jean-Hugues Pr DALLES
• Phone: +33140035388
• Email: jean-hugues.dalle[@]aphp.fr
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

Pediatric patients with idiopathic aplastic anemia (AA) respond better than adults to immunosuppressive therapy (IST) but the long-term risks of relapse, ciclosporine dependence, and clonal evolution are high. UK investigators reported a 5-year estimated failure-free survival (FFS) after IST of 13.3%. In contrast, in 44 successive children who received a matched unrelated donor (MUD), hematopoietic stem cell transplantation (HSCT), there was an excellent estimated 5-year FFS of 95%. Forty of these children had previously failed IST. Because of those excellent results, up-front fully matched unrelated donor (MUD) hematopoietic stem cell transplantation (HSCT) became an attractive first-line option. In 2005 to 2014, a UK cohort of 29 children with idiopathic AA thus received MUD HSCTs as first-line therapy (they did not receive IST prior to HSCT). Results were excellent, with low Graft versus Host Disease rates and only 1 death (idiopathic pneumonia). This cohort was then compared with historical matched controls, transplanted or not. Outcomes for the up-front unrelated cohort HSCT were similar to Matched Related Donor HSCT and superior to IST and unrelated HSCT post-IST failure. Since then, many investigators are offering up-front MUD HSCT in pediatric patients worldwide. However, those results should be treated with extreme caution: 1) the design is retrospective; 2) the excellent up-front MUD HSCT may arise from the use of alemtuzumab in the conditioning regimen (alemtuzumab is not easily available worldwide) and 3) there was no formal quality-of-life assessment. Moreover, this strategy is highly dependent on donor identification (Caucasian patients have the highest likelihood of having a MUD) and donor not eventually receive HSCT because of the risk of infections/complications caused by unexpected donor delays or cancellation. Prospective trials are thus urgently needed to address the feasibility of such procedure, in term of timing (delay to offer MUD HSCT) and conditioning regimen (nothing is known of the use of other regimens, non alemtuzumab-based, in this setting).

The main objective of this Two-Stage Phase 2 multicenter study is to realize up-front HSCT within 2 months once a MUD has been identified.

Recruitment information / eligibility

• Status: Not yet recruiting
• Enrollment: 25
• Est. completion date: June 2027
• Est. primary completion date: August 2025
• Accepts healthy volunteers: No
• Gender: All
• Age group: N/A to 18 Years

Eligibility

Inclusion Criteria:

• age<18years old

• Pediatric patients aged less than 18 years with idiopathic aplastic anemia and an indication for treatment (severe aplastic anemia or moderate aplastic anemia requiring transfusions)

• With a good probability to have a HLA-10/10 matched unrelated donor available (the patient needs to have at least 3 MUD identified within the book BMDW (Bone Marrow Donors Worldwide) or using the easy match software to be included)

• With usual criteria for allo-SCT:

• Lansky >70% for those below 16 years and Karnofsky > 70% for those above 16 years

• No severe and uncontrolled infection

• Adequate organ function: ASAT and ALAT = 5N*, total bilirubin = 2N, creatinine clearance > 70% of higher normal values for age.

• With health insurance coverage

• Contraception methods** for young girl and men of childbearing age must be prescribed during all the duration of the research.

• Parents having read and understand the information note and signed a written informed consent (the patient's agreement depending on his age will be sought)

*because typical presentation of aplastic anemia post-hepatitis

** NB : The authorized contraceptive methods are:

• For women of childbearing age and in absence of permanent sterilization: oral, intravaginal or transdermal combined hormonal contraception, oral, injectable or transdermal progestogen-only hormonal contraception, intrauterine hormonal-releasing system (IUS).

• For man in absence of permanent sterilization: condoms

Exclusion Criteria:

Patients :

• With a matched related donor available

• With uncontrolled infection

• With seropositivity for HIV or HTLV-1 or active hepatitis B or C defined by a positive PCR HBV or HCV and associated hepatic cytolysis

• Renal failure with creatinine clearance below 70% of higher normal values for age

• Pregnant (ßHCG positive) or breast-feeding

• With Heart failure according to NYHA (II or more)

• Preexisting acute hemorrhagic cystitis

• Urinary tract obstruction

• Yellow fever vaccine within 2 months before transplantation

• Who have any debilitating medical or psychiatric illness, which preclude understanding the inform consent as well as optimal treatment and follow-up (depending of his age and understanding).

• With Contraindication to treatments used during the research

Related Conditions & MeSH terms

• Anemia
• Anemia, Aplastic
• Severe Aplastic Anemia

Intervention

Other:
• HSCT Arm group
Conditioning regimen Stem cell source Only Bone Marrow With a minimal target dose of 4x108 nucleated cells/kg recipient ideal body weight. If the graft is less rich than the minimum target dose, it can be administered at the discretion to the physician. GVHD Prophylaxis Prevention of EBV reactivation : Rituximab 150mg/m2 IV at Day+5 post HSCT.

Locations

Country	Name	City	State
n/a

Sponsors (1)

Lead Sponsor	Collaborator
Assistance Publique - Hôpitaux de Paris

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Proportion of patients with upfront matched unrelated donor (MUD) hematopoietic stem cell transplantation (HSCT) effectively performed	Proportion of patients with upfront matched unrelated donor (MUD) hematopoietic stem cell transplantation (HSCT) effectively performed in the first two months after unrelated donor search.	within 2 months (60 days) after identification of a MUD
Secondary	Graft failure incidence		up to 24 months
Secondary	Neutrophils engraftment	Neutrophils engraftment will be defined as first day of 3 consecutive days with neutrophils >0.5 G/L	at day 100
Secondary	Platelets engraftment	Platelets engraftment will be defined as first day of 7 consecutive days with platelets >20 G/L	at day 100
Secondary	Absolute number of neutrophils		at 1 month
Secondary	Absolute number of neutrophils		at 2 months
Secondary	Absolute number of neutrophils		at 3 months
Secondary	Absolute number of neutrophils		at 6 months
Secondary	Absolute number of neutrophils		at 12 months
Secondary	Absolute number of neutrophils		at day of last platelet and red blood cell transfusions (assessed up to 24 months)
Secondary	Absolute numbers of platelets		at 1 month
Secondary	Absolute numbers of platelets		at 2 months
Secondary	Absolute numbers of platelets		at 3 months
Secondary	Absolute numbers of platelets		at 6 months
Secondary	Absolute numbers of platelets		at 12 months
Secondary	Absolute numbers of platelets		up to 24 months
Secondary	Acute GvHD incidence		at month 3
Secondary	Chronic GvHD incidence		at 24 months
Secondary	Relapse incidence		at 12 months
Secondary	Relapse incidence		at 24 months
Secondary	Progression free survival		at 12 months
Secondary	Progression free survival		at 24 months
Secondary	Incidence of CMV infection		at 12 months
Secondary	Incidence of EBV infection		at 12 months
Secondary	Incidence of severe infections	Severe infections will be defined as CTACE grade 3-4	at 3 months
Secondary	Incidence of severe infections	Severe infections will be defined as CTACE grade 3-4	at 6 months
Secondary	Incidence of severe infections	Severe infections will be defined as CTACE grade 3-4	at 12 months
Secondary	Incidence of severe infections	Severe infections will be defined as CTACE grade 3-4	at 24 months
Secondary	Non-relapse mortality		at 24 months
Secondary	Overall survival		at 24 months
Secondary	Quality of life questionnaires PedsQL	Quality of life will be evaluated using PedsQL questionnaire. Scores varies from 0 to100, with higher scores associated with better health-related quality of life.	at inclusion
Secondary	Quality of life questionnaires PedsQL	Quality of life will be evaluated using PedQQL questionnaire.Higher scores associated with better health-related quality of life. Scores varies from 0 to100, with higher scores associated with better health-related quality of life.	at 1 month
Secondary	Quality of life questionnaires PedsQL	Quality of life will be evaluated using PedQQL questionnaire.Higher scores associated with better health-related quality of life. Scores varies from 0 to100, with higher scores associated with better health-related quality of life.	at 3 months
Secondary	Quality of life questionnaires PedsQL	Quality of life will be evaluated using PedsQL questionnaire. Higher scores associated with better health-related quality of life. Scores varies from 0 to100, with higher scores associated with better health-related quality of life.	at 6 months
Secondary	Quality of life questionnaires PedsQL	Quality of life will be evaluated using PedsQL questionnaire.Scores varies from 0 to100, with higher scores associated with better health-related quality of life.	at 12 months
Secondary	Quality of life questionnaires PedsQL	Quality of life will be evaluated using PedsQL questionnaire.Scores varies from 0 to100, with higher scores associated with better health-related quality of life.	at 24 months
Secondary	Proportion of patients with a donor chimerism of 90% or more		at 1 month
Secondary	Proportion of patients with a donor chimerism of 90% or more		at 3 months
Secondary	Proportion of patients with a donor chimerism of 90% or more		at 6 months
Secondary	Proportion of patients with a donor chimerism of 90% or more		at 12 months
Secondary	Immune reconstitution	Immune reconstitution will be done by analyzing T, B, NK, regulatory T cell levels in the peripheral blood. All have the same unit measure namely absolute numbers/microL	at 3 months
Secondary	Immune reconstitution	Immune reconstitution will be done by analyzing T, B, NK, regulatory T cell levels in the peripheral blood. All have the same unit measure namely absolute numbers/microL	at 6 months
Secondary	Immune reconstitution	Immune reconstitution will be done by analyzing T, B, NK, regulatory T cell levels in the peripheral blood. All have the same unit measure namely absolute numbers/microL.	at 12 months
Secondary	Immune reconstitution	Immune reconstitution will be done by analyzing T, B, NK, regulatory T cell levels in the peripheral blood. All have the same unit measure namely absolute numbers/microL.	at 24 months
Secondary	Ferritin levels		at 3 months
Secondary	Ferritin levels		at 6 months
Secondary	Ferritin levels		at 12 months
Secondary	Ferritin levels		at 24 months