Cytomegalovirus Infections Clinical Trial
Official title:
Injection of CD4 and CD8 + T Cells Anti-CMV or Anti-adenovirus for the Treatment of Viral Infections Occurring After Allogenic Hematopoietic Stem Cell Transplantation (HSCT)
The main purpose of this project is to evaluate the efficiency of the injection of CD4 and CD8+ T cell anti-Cytomegalovirus (CMV) on blood viral replication of CMV, 21 days after the first injection (adenovirus infection is not enough usual, especially in adults, to be used for the primary purpose and is measured in the secondary endpoints).
Cytomegalovirus (CMV) and adenoviruses infections are a major source of morbidity and
mortality after allogenic haematopoietic stem cell transplantation (HSC). Conventional
antiviral therapy have sometimes insufficient efficiency and a significant potential
toxicity. Over the last ten years, adoptive immunotherapy has demonstrated its efficiency in
treatment of viral infections in this context. Different methods have been used but
organizational and technological barriers have prevented a wide use of this therapeutic
approach.
This protocol aims to assess the efficiency of treatment by injection of donor CD4 + and CD8
+ T cells specifically directed against cytomegalovirus or adenovirus, to patients receiving
allogenic transplant with infection of one of these two viruses, and in conventional
antiviral treatment failure. Donor memory T cells will be obtained from an aphaeresis of
mononuclear cells and will be selected on the basis of their ability to produce
interferon-gamma (IFN-g) after stimulation with viral peptides. The speed (48 hours) and the
reproducibility of this method let hope a better feasibility for clinical use compared to
previously developed technologies. Given epidemiology different after allogenic transplant
of HSC of these two viruses, and the relative low expected number of patients with
adenovirus infection, statistical analysis will focus exclusively on patients who received T
cells for CMV infection. The study of efficiency and tolerance of this adoptive
immunotherapy for adenovirus will be considered as a secondary purpose.
This is a multicenter non-comparative phase I/II protocol, which predicts the inclusion of
30 patients with 25 patients infected with CMV, to demonstrate efficiency of 55% with a
minimum required efficiency of 30%, an alpha risk of 10% and a strength of 90%. The main
purpose of the study is to evaluate the efficiency of this treatment on the level of CMV
viral replication 21 days after the first injection. A positive response is defined by a
viral load became undetectable or reduced by at least 2 log10. A negative response is
defined on the basis of unchanged or increased viral load after injection of T cells; a
partial response is defined as a significant decrease (greater than 0.3log10 copies / ml but
less than 2 log10) of the viral load, which still remains above the detection threshold. For
patients with an isolated organ damage (patient without PCR), a positive response is defined
by the healing of the affected organ. In case of negative or partial response 21 days after
the first injection, a second injection if available can be programmed in the absence of
clinical signs of graft versus host or aggravation of pre-existing GVHa. The secondary
purposes are: a) assess the tolerance, in terms of occurrence of acute reaction graft versus
host (GVHa) directly due to the injection of T cells ; b) evaluation of indirect biological
parameters of efficiency such as injected T cells expansion studied using tetramers specific
secretion of IFN-g; c) the study of efficiency and tolerance of this immunotherapy against
adenovirus. Inclusion criteria concern children and adults who have received allogenic
transplant of HSC, which donor is CMV + and having an active viral infection: 1) in
conventional antiviral treatment failure, with a persistent viral load and/or increased
after 15 days of treatment or with CMV or ADV disease with organ damage documented without
systemic replication (if possible, with a CMV PCR or ADV PCR positive in the organ), or 2)
in intolerance or toxicity situation of this treatment which prevents its pursuit. Donor T
cells will be injected if the following conditions are observed : 1) donor chimerism > 10%,
2) absence of GvHa ≥ grade II 3) absence of severe organ failure. The antiviral drug therapy
may eventually be continued jointly with cellular immunotherapy.
Number of participating centers: grafter centers of Ile-de-France and Hospital Edouard
HERRIOT to Lyon, CHU of Nantes, CHU of Poitiers (so 10 centers). The study duration will be
42 months, with an inclusion period of 36 months and a follow-up period of 6 months from the
last inclusion. If the study gives expected results, a compared phase III trial will be
considered for the treatment of CMV infections and a Phase I/II for the treatment of
adenoviral infection.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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