Co-stimulation modulation with abatacept in patients with recent-onset type 1 diabetes: a randomised, double-blind, placebo-controlled trial
T Orban, B Bundy, DJ Becker, LA DiMeglio… - The Lancet, 2011 - thelancet.com
The Lancet, 2011•thelancet.com
Background The immunopathogenesis of type 1 diabetes mellitus is associated with T-cell
autoimmunity. To be fully active, immune T cells need a co-stimulatory signal in addition to
the main antigen-driven signal. Abatacept modulates co-stimulation and prevents full T-cell
activation. We evaluated the effect of abatacept in recent-onset type 1 diabetes. Methods In
this multicentre, double-blind, randomised controlled trial, patients aged 6–45 years recently
diagnosed with type 1 diabetes were randomly assigned (2: 1) to receive abatacept (10 …
autoimmunity. To be fully active, immune T cells need a co-stimulatory signal in addition to
the main antigen-driven signal. Abatacept modulates co-stimulation and prevents full T-cell
activation. We evaluated the effect of abatacept in recent-onset type 1 diabetes. Methods In
this multicentre, double-blind, randomised controlled trial, patients aged 6–45 years recently
diagnosed with type 1 diabetes were randomly assigned (2: 1) to receive abatacept (10 …
Background
The immunopathogenesis of type 1 diabetes mellitus is associated with T-cell autoimmunity. To be fully active, immune T cells need a co-stimulatory signal in addition to the main antigen-driven signal. Abatacept modulates co-stimulation and prevents full T-cell activation. We evaluated the effect of abatacept in recent-onset type 1 diabetes.
Methods
In this multicentre, double-blind, randomised controlled trial, patients aged 6–45 years recently diagnosed with type 1 diabetes were randomly assigned (2:1) to receive abatacept (10 mg/kg, maximum 1000 mg per dose) or placebo infusions intravenously on days 1, 14, 28, and monthly for a total of 27 infusions over 2 years. Computer-generated permuted block randomisation was used, with a block size of 3 and stratified by participating site. Neither patients nor research personnel were aware of treatment assignments. The primary outcome was baseline-adjusted geometric mean 2-h area-under-the-curve (AUC) serum C-peptide concentration after a mixed-meal tolerance test at 2 years' follow-up. Analysis was by intention to treat for all patients for whom data were available. This trial is registered at ClinicalTrials.gov, NCT00505375.
Findings
112 patients were assigned to treatment groups (77 abatacept, 35 placebo). Adjusted C-peptide AUC was 59% (95% CI 6·1–112) higher at 2 years with abatacept (n=73, 0·378 nmol/L) than with placebo (n=30, 0·238 nmol/L; p=0·0029). The difference between groups was present throughout the trial, with an estimated 9·6 months' delay (95% CI 3·47–15·6) in C-peptide reduction with abatacept. There were few infusion-related adverse events (36 reactions occurred in 17 [22%] patients on abatacept and 11 reactions in six [17%] on placebo). There was no increase in infections (32 [42%] patients on abatacept vs 15 [43%] on placebo) or neutropenia (seven [9%] vs five [14%]).
Interpretation
Co-stimulation modulation with abatacept slowed reduction in β-cell function over 2 years. The beneficial effect suggests that T-cell activation still occurs around the time of clinical diagnosis of type 1 diabetes. Yet, despite continued administration of abatacept over 24 months, the decrease in β-cell function with abatacept was parallel to that with placebo after 6 months of treatment, causing us to speculate that T-cell activation lessens with time. Further observation will establish whether the beneficial effect continues after cessation of abatacept infusions.
Funding
US National Institutes of Health.
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