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The efficacy and safety of ustekinumab in adolescents newly diagnosed with type 1 diabetes: the USTEK1D RCT

Kym Carter Orcid Logo, Wai-Yee Cheung Orcid Logo, Hayley Hutchings Orcid Logo, Greg Fegan Orcid Logo, Gail Holland Orcid Logo, Steve Luzio Orcid Logo, Gareth Dunseath Orcid Logo, Stephen Hiles Orcid Logo, Susie Marques-Jones, John W Gregory Orcid Logo, Danijela Tatovic Orcid Logo, Peter Taylor Orcid Logo, Jane Bowen-Morris Orcid Logo, Rachel Stenson Orcid Logo, Stephanie Hanna Orcid Logo, Zainab Mahmood Orcid Logo, Jennie Yang Orcid Logo, Evangelia Williams Orcid Logo, Timothy Tree Orcid Logo, Ashish Marwaha Orcid Logo, Colin M Dayan Orcid Logo, Ivy Cheung, Steve Hiles

Efficacy and Mechanism Evaluation, Volume: 12, Issue: 1, Pages: 1 - 66

Swansea University Authors: Kym Carter Orcid Logo, Hayley Hutchings Orcid Logo, Gail Holland Orcid Logo, Steve Luzio Orcid Logo, Gareth Dunseath Orcid Logo, Ivy Cheung, Steve Hiles

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DOI (Published version): 10.3310/fqln7416

Abstract

Background: Type 1 diabetes is an autoimmune disease affecting over 400,000 children and adults in the United Kingdom for which currently the only available therapy is insulin. Objective(s): To determine the efficacy and safety of the monoclonal antibody ustekinumab targeting the interleukin 12/inte...

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Published in: Efficacy and Mechanism Evaluation
ISSN: 2050-4373
Published: National Institute for Health and Care Research 2025
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URI: https://cronfa.swan.ac.uk/Record/cronfa68939
Abstract: Background: Type 1 diabetes is an autoimmune disease affecting over 400,000 children and adults in the United Kingdom for which currently the only available therapy is insulin. Objective(s): To determine the efficacy and safety of the monoclonal antibody ustekinumab targeting the interleukin 12/interleukin 23 immune pathway that generates T helper 1/T helper 17 T cells to slow down the autoimmune process and preserve beta cell production in type 1 diabetes. Design: Randomised, double-blind, placebo-controlled, parallel-group phase II trial. Setting: Paediatric and young adult diabetes clinics across 16 sites in the United Kingdom. Participants: Newly diagnosed with type 1 diabetes and aged 12–18 years. Eligibility criteria: Type 1 diabetes confirmed by islet autoantibody testing, within 100 days of first insulin injection, and with residual beta cell function (stimulated C-peptide level > 0.2 nmol/l). Interventions: Ustekinumab at the highest approved doses or control (saline) subcutaneously at weeks 0, 4 and 12 and subsequently every 8 weeks to week 44 (seven doses). Main outcome measures: Preservation of Mixed Meal Tolerance Test stimulated 2-hour insulin C-peptide area under the curve at week 52 as compared to control (saline) treatment by analysis of covariance adjusted for baseline parameters. Randomisation: 2 : 1 Remote computerised randomisation with minimisation by age and baseline C-peptide groups. Blinding: Blinding of participants, investigators, laboratory and trial staff. Numbers randomised: Seventy-two participants were randomised, 60% male, 18% aged 16–18 years. Recruitment: Two hundred and eight potentially eligible patients were approached, and 88 patients were screened. Four participants were lost to follow-up (6%). Four participants withdrew from the treatment but attended the primary end-point assessment. Numbers analysed: Six participants were missing baseline data for the primary analysis. The final analysable sample was n = 62. Outcome: Ustekinumab was associated with a 49% higher endogenous stimulated insulin production than control at week 52 after adjustments for baseline factors [geometric ratio of ustekinumab to control was 1.49 (95% confidence interval 1.08 to 2.06; p = 0.02)]. Secondary analyses showed no difference in C-peptide at week 28 suggesting that the effect was ‘late’ or ‘delayed’. Ancillary analysis showed a significant reduction in activated T helper 17.1 T cells (p < 0.001) in the treatment group which was associated with C-peptide preservation from week 28 to week 52. Harms: No severe adverse events were reported and there were no differences between ustekinumab and control groups in the proportion of participants overall experiencing mild (87% vs. 88%) or moderate (32% vs. 32%) events. Limitations: Sensitivity analysis showed the primary end point to be robust to exclusion of small numbers of participants with some protocol deviations and extreme values in key covariates, but not to imputation of all missing data. Conclusions: Ustekinumab appears to slow down the autoimmune process providing the first clinical trial evidence that interleukin 17-secreting T cells play a pathogenic role in type 1 diabetes. Alone, it is insufficient to halt the autoimmune process. Future work: Replication of this result is ongoing in a trial with a similar design in Canada. If confirmed, consideration may be given to testing other drugs targeting the interleukin 17 pathway, using ustekinumab in combination with other agents or using it earlier in the disease pathway (preclinical disease) since it is so well tolerated and simple to use. Study registration: Current Controlled Trials ISRCTN14274380.
College: Faculty of Medicine, Health and Life Sciences
Funders: This award was funded by the National Institute for Health and Care Research (NIHR) Efficacy and Mechanism Evaluation (EME) programme (NIHR award ref: 16/36/01).
Issue: 1
Start Page: 1
End Page: 66

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