Dose-effect Relationship of Low-dose IL-2 in Type 1 Diabetes
NCT ID: NCT01353833
Last Updated: 2012-04-23
Study Results
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Basic Information
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COMPLETED
PHASE1/PHASE2
25 participants
INTERVENTIONAL
2011-05-31
2012-04-30
Brief Summary
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Detailed Description
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Type 1 diabetes (T1D) results from an autoimmune destruction of beta-pancreatic cells that regulatory T cells (Treg) fail to control. This is in part due to a deficit in production of, or response to, interleukin 2 (IL-2). This cytokine is essential to Treg development, survival and function. Importantly, while IL-2 also contributes to the activation of effector T cells (Teff), IL-2/IL-2 receptor signal transduction threshold is much lower for Treg than Teff. Thus low-dose IL-2 could be a specific Treg inducer/stimulator.
The investigators then recently showed that low-dose IL-2 could cure recent onset diabetes in NOD mice that develop spontaneous diabetes considered as the best model of human T1D. A 5-day treatment with IL-2 could cure over 30% of the mice versus 0% for controls.
With these premises, the investigators propose to explore if Treg induction could be obtained in patients who may have a deficit in production of, or response to, IL-2. Defining the dose effect relationship of low dose IL-2 for Treg induction will optimize the risk benefit ratio for IL-2 in T1D.
Principal objective:
To define the dose-effect relationship of low dose IL-2 for Treg induction in patient with recent onset diabetes
Evaluation Criteria:
* Efficacy Kinetic variation of Treg proportions within CD4+ T cells in peripheral blood from Day+0 to Day+60.
* Tolerance Evaluation by clinical exams, laboratory tests and monitoring of side effects. The criterion for terminating the study will be the occurrence of one serious unexpected side effect in the month following IL-2 first administration in at least 2 patients.
Study plan:
After inclusion (Day0), the patient receives a 5-day course of IL-2 or placebo. Patients are randomized in 4 arms receiving either a placebo, or IL-2 doses of 0,33 - 1 or 3 millions UI/day. Laboratory follow-up of peripheral blood T cell subsets will be performed at D0 to D6 (daily), D15, D22 and D60 by immunophenotyping and transcriptomics.
Tolerance will be evaluated at D0-6, D15, D22 and D60.
Methodology:
Double blind placebo controlled randomized study, with 4 parallel groups. Patients will have T1D of autoimmune origin attested by the presence of auto-antibodies (at least one of: anti-islet, anti-GAD, anti-IA2 or anti-ZnT8), with a diagnostic inferior or equal to 24 months.
Study length:
Study length = 9 months Patient participation = 2 months Inclusion period = 6 months
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
DOUBLE
Study Groups
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IL2-4
Aldesleukin
0.33 ; 1 ; 3 ; 0 millions IU of IL-2 per day for arm 1 to 4, respectively. 1 s.c. injection per day for 5 days.
IL2-2
1 millions IU of IL-2 per day
Aldesleukin
0.33 ; 1 ; 3 ; 0 millions IU of IL-2 per day for arm 1 to 4, respectively. 1 s.c. injection per day for 5 days.
IL2-3
3 millions IU of IL-2 per day
Aldesleukin
0.33 ; 1 ; 3 ; 0 millions IU of IL-2 per day for arm 1 to 4, respectively. 1 s.c. injection per day for 5 days.
IL2-1
0.33 millions IU of IL-2 per day
Aldesleukin
0.33 ; 1 ; 3 ; 0 millions IU of IL-2 per day for arm 1 to 4, respectively. 1 s.c. injection per day for 5 days.
Interventions
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Aldesleukin
0.33 ; 1 ; 3 ; 0 millions IU of IL-2 per day for arm 1 to 4, respectively. 1 s.c. injection per day for 5 days.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* With a T1D:
* Treated with insulin for ≤ 2 years,
* With at least one auto-antibody among: anti-islet, anti-GAD, anti-IA2, anti-ZnT8 ;
* No clinically relevant abnormal value for hematology, biochemistry, liver and kidney function
* Lymphocyte \[1000-4000\]/ mm3
* Informed consent signed by the patient and the investigator before any intervention necessary for the trial.
Exclusion Criteria
* Hypersensibility to IL-2 or its excipients,
* Severe cardiopathy
* Ongoing infection requiring antibiotherapy,
* O2 Saturation ≤ 90 %
* Severe impairment of a vital organ
* Previous organ allograft
* Non authorized concomitant treatment : i.e. immuno-modulators, cytotoxic, drug modifying glycemia
* Cancer progressing or cured for less than 5 years except for primary basal cell carcinoma or carcinoma in situ of the uterine cervix.
* Participation to another clinical investigation in \< 3 months
* Pregnant or lactating women
* Male or female in age of procreation without efficient contraception during the study
* No affiliation to National Health Insurance
18 Years
50 Years
ALL
No
Sponsors
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Assistance Publique - Hôpitaux de Paris
OTHER
Responsible Party
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Principal Investigators
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Davis Klatzmann, MD, PhD
Role: PRINCIPAL_INVESTIGATOR
Assistance Publique - Hôpitaux de Paris
Locations
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Hôpital Pitié-Salpêtrière
Paris, , France
Countries
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References
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Hartemann A, Bensimon G, Payan CA, Jacqueminet S, Bourron O, Nicolas N, Fonfrede M, Rosenzwajg M, Bernard C, Klatzmann D. Low-dose interleukin 2 in patients with type 1 diabetes: a phase 1/2 randomised, double-blind, placebo-controlled trial. Lancet Diabetes Endocrinol. 2013 Dec;1(4):295-305. doi: 10.1016/S2213-8587(13)70113-X. Epub 2013 Oct 8.
Other Identifiers
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2010-024499-24
Identifier Type: EUDRACT_NUMBER
Identifier Source: secondary_id
P101101
Identifier Type: -
Identifier Source: org_study_id
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