This is an open-labelled and non-controlled Phase I/II clinical trial, evaluating the safety and the efficacy of Human T Lymphoid Progenitor (HTLP) injection to accelerate immune reconstitution after umbilical cord blood (UCB) transplantation in adult patients with hematologic malignancies. The dose limiting toxicity of HTLP injection will be evaluated using a model-based design.
Allogeneic bone marrow transplantation (AlloSCT) is the treatment of choice for high- risk acute myeloid leukemias in complete first remission after induction therapy and other high-risk hematological malignancies. Umbilical cord blood grafts are frequently used for patients lacking an HLA- matched family donor (Matched-sibling donor, MSD) as well as in the absence of an appropriate unrelated donor (10/10 MUD). As any HSCT, UCB transplantations are associated with the risk of acute and chronic GVHD, post- transplant immunodeficiency with increased risk of infections as well as relapse. Especially the risk of infection and therefore non- relapse mortality (NRM) or transplant- related mortality (TRM) is significantly higher in UCB transplantations as compared to MSD or 10/10 MUD transplantations. All of these risks have been linked to a significant delay in immune reconstitution including various immune cell populations like CD4 and CD8 T cells, Treg, NK, iNKT, pDC and others. The investigators therefore make the hypothesis that if T-cell-mediated immunity was rapidly generated after a partially HLA-compatible UCB transplantation will reduce the risk of infection and to prevent relapse without increasing the risk of GVHD.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
TREATMENT
Masking
NONE
Enrollment
10
The HTLP cell suspension will be injected intravenously at the time of UCB HSCT on D0
Hôpital Saint Louis
Paris, France
RECRUITINGService d'Hématologie et thérapie cellulaire / CHU of Bordeaux
Pessac, France
RECRUITINGIUCT Oncopole Toulouse
Toulouse, France
RECRUITINGInstitut Gustave Roussy
Villejuif, France
NOT_YET_RECRUITINGHematology department / Necker Children's Hospital
Paris, Île-de-France Region, France
RECRUITINGCumulative incidence of grade III-IV graft-versus-host disease (GvHD)
according to Glucksberg grading system, to define toxicity
Time frame: Within 100 Days following HSCT
CD4 + T cells analysis
Efficacy defined by the presence of \>50/μl CD4+ CD3+ TCRαβ+ T cells at 2 consecutive measures \< within 4 months post HSCT.
Time frame: Within 100 days following HSCT
Time to hematologic engraftment
ANC \> 0.5G/L and platelets \> 20G/L on 3 consecutive days
Time frame: Up to 24 months post-transplantation
Last transfusion of platelets and red blood cell
Time frame: During the follow-up
Absolute numbers of neutrophils
Time frame: Month 1, 2, 3, 6 and 12 post -transplantation
Time course of T cell immune reconstitution
by immunophenotyping (flow cytometry analysis) - with a focus on time needed to exceed a count of 100 naive CD4+ and \>100 total CD8+ cells per μL
Time frame: Month 1, 2, 3, 6 and 12 post -transplantation
Immune phenotype (flow-cytometry analysis) of the different TCRαβ+ cell subpopulations
TCD4 naive/memory population (CD31+CD45RA+/CD4+, CD45RO/CD4+; CD31+CD4+); TCD8 naive/memory population (CD45RA+CCR7+/CD8+, CD45RA-CCR7+/ CD8+, CD45RA- CCR7+/ CD8+, CD45RA-CCR7-/CD8+) , CD8 effector memory RA+ (TEMRA) (CD45RA+CCR7- /CD8+ ); Regulatory T cells (CD4+CD25+CD127lowCD25+). • Analysis of CD3, CD4, CD8 numbers will be performed if total lymphocytes ≥ 500/μL and analysis of T cell subpopulations if CD3+ cells ≥ 1000/μL
Time frame: Month 1, 2, 3, 6 and 12 post -transplantation
B-cell reconstitution
(B CD19 naive/memory population (CD27-IgD+/CD19+, CD27+IgD+/CD19+, CD27+IgD-/CD19 and Ig levels) at 1, 2, 3, 6 and 12 months post HSCT with focus on time needed for cessation of intravenously IgG replacement therapy
Time frame: Month 1, 2, 3, 6 and 12 post -transplantation
Reconstitution of the NK cell
compartment (CD16+CD56+)
Time frame: Month 1, 2, 3, 6 and 12 post -transplantation
Assessment of engraftment of each UCB unit over time by hematological monitoring and chimerism analysis
at 1, 2, 3, 6 and 12 months following HSCT and between M1 and M2 post-transplantation if necessary according to the result of the chimerism at M1 on neutrophils, T, B, NK, pDC and macrophages. • The chimerism is studied on whole blood and on mononuclear cells (i.e. cells reconditioning after Ficoll) until the total number of lymphocyte is ≥ 100/μL. When lymphocyte count is ≥ 100/μL, the chimerism will be analysed on immunoselected cell populations (CD15+/CD3+/NK, CD19+)
Time frame: at 1, 2, 3, 6 and 12 months following HSCT.
Graft failure/rejection rate
detected by hematological monitoring of each UCB unit
Time frame: at 3 months following HSCT
Cumulative incidence of infections
Time frame: at 3, 6 and 12 months post- transplantation
Cumulative incidence of acute and chronic episodes of GVHD and their grade according to Glucksberg GvHD staging.
Time frame: at 3, 6, 12 and 24 months post-transplantation
Relapse rate
Time frame: 2 years
Overall survival
Time frame: 2 years
Disease-free survival
Time frame: 2 years
Progression-free survival
Time frame: 2 years
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