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Open Access 02-10-2023 | Type 1 Diabetes | Article

A first-in-human, open-label Phase 1b and a randomised, double-blind Phase 2a clinical trial in recent-onset type 1 diabetes with AG019 as monotherapy and in combination with teplizumab

Authors: Chantal Mathieu, Alice Wiedeman, Karen Cerosaletti, S. Alice Long, Elisavet Serti, Laura Cooney, Joan Vermeiren, Silvia Caluwaerts, Karolien Van Huynegem, Lothar Steidler, Sven Blomme, Pieter Rottiers, Gerald T. Nepom, Kevan C. Herold, on behalf of the AG019-T1D-101 Trial Investigators

Published in: Diabetologia | Issue 1/2024

Abstract

Aims/hypothesis

We hypothesised that islet beta cell antigen presentation in the gut along with a tolerising cytokine would lead to antigen-specific tolerance in type 1 diabetes. We evaluated this in a parallel open-label Phase 1b study using oral AG019, food-grade Lactococcus lactis bacteria genetically modified to express human proinsulin and human IL-10, as a monotherapy and in a parallel, randomised, double-blind Phase 2a study using AG019 in combination with teplizumab.

Methods

Adults (18–42 years) and adolescents (12–17 years) with type 1 diabetes diagnosed within 150 days were enrolled, with documented evidence of at least one autoantibody and a stimulated peak C-peptide level >0.2 nmol/l. Participants were allocated to interventions using interactive response technology. We treated 42 people aged 12–42 years with recent-onset type 1 diabetes, 24 with Phase 1b monotherapy (open-label) and 18 with Phase 2a combination therapy. In the Phase 2a study, after treatment of the first two open-label participants, all people involved were blinded to group assignment, except for the Data Safety Monitoring Board members and the unblinded statistician. The primary endpoint was safety and tolerability based on the incidence of treatment-emergent adverse events, collected up to 6 months post treatment initiation. The secondary endpoints were pharmacokinetics, based on AG019 detection in blood and faeces, and pharmacodynamic activity. Metabolic and immune endpoints included stimulated C-peptide levels during a mixed meal tolerance test, HbA_1c levels, insulin use, and antigen-specific CD4⁺ and CD8⁺ T cell responses using an activation-induced marker assay and pooled tetramers, respectively.

Results

Data from 24 Phase 1b participants and 18 Phase 2a participants were analysed. No serious adverse events were reported and none of the participants discontinued AG019 due to treatment-emergent adverse events. No systemic exposure to AG019 bacteria, proinsulin or human IL-10 was demonstrated. In AG019 monotherapy-treated adults, metabolic variables were stabilised up to 6 months (C-peptide, insulin use) or 12 months (HbA_1c) post treatment initiation. In participants treated with AG019/teplizumab combination therapy, all measured metabolic variables stabilised or improved up to 12 months and CD8⁺ T cells with a partially exhausted phenotype were significantly increased at 6 months. Circulating preproinsulin-specific CD4⁺ and CD8⁺ T cells were detected before and after treatment, with a reduction in the frequency of preproinsulin-specific CD8⁺ T cells after treatment with monotherapy or combination therapy.

Conclusions/interpretation

Oral delivery of AG019 was well tolerated and safe as monotherapy and in combination with teplizumab. AG019 was not shown to interfere with the safety profile of teplizumab and may have additional biological effects, including changes in preproinsulin-specific T cells. These preliminary data support continuing studies with this agent alone and in combination with teplizumab or other systemic immunotherapies in type 1 diabetes.

Trial registration

ClinicalTrials.gov NCT03751007, EudraCT 2017-002871-24

Funding

This study was funded by Precigen ActoBio

Graphical Abstract

Available only for authorised users

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Title: A first-in-human, open-label Phase 1b and a randomised, double-blind Phase 2a clinical trial in recent-onset type 1 diabetes with AG019 as monotherapy and in combination with teplizumab
Authors: Chantal Mathieu
Alice Wiedeman
Karen Cerosaletti
S. Alice Long
Elisavet Serti
Laura Cooney
Joan Vermeiren
Silvia Caluwaerts
Karolien Van Huynegem
Lothar Steidler
Sven Blomme
Pieter Rottiers
Gerald T. Nepom
Kevan C. Herold
on behalf of the AG019-T1D-101 Trial Investigators
Publication date: 02-10-2023
Publisher: Springer Berlin Heidelberg
Keywords: Type 1 Diabetes
Anti-CD3 Antibody
Published in: Diabetologia / Issue 1/2024
Print ISSN: 0012-186X
Electronic ISSN: 1432-0428
DOI: https://doi.org/10.1007/s00125-023-06014-2

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