Please use this identifier to cite or link to this item: https://dora.health.qld.gov.au/qldresearchjspui/handle/1/1473
Title: A safety and pharmacodynamics study of temelimab, an antipathogenic human endogenous retrovirus type W envelope monoclonal antibody, in patients with type 1 diabetes
Authors: Curtin, Francois
Champion, Bernard
Davoren, Peter 
Duke, Sally
Ekinci, Elif I
Gilfillan, Chris
Morbey, Claire
Nathow, Thomas
O'Moore-Sullivan, Trisha
O'Neal, David
Roberts, Adam
Stranks, Stephen
Stuckey, Bronwyn
Vora, Parind
Malpass, Sam
Lloyd, David
Maëstracci-Beard, Nicole
Buffet, Bénédicte
Kornmann, Gabrielle
Bernard, Corinne
Porchet, Hervé
Simpson, Richard
Issue Date: Jul-2020
Publisher: Wiley-Blackwell Publishing Ltd.
Source: Curtin F, Champion B, Davoren P, Duke S, Ekinci EI, Gilfillan C, Morbey C, Nathow T, O'Moore-Sullivan T, O'Neal D, Roberts A, Stranks S, Stuckey B, Vora P, Malpass S, Lloyd D, Maëstracci-Beard N, Buffet B, Kornmann G, Bernard C, Porchet H, Simpson R. A safety and pharmacodynamics study of temelimab, an antipathogenic human endogenous retrovirus type W envelope monoclonal antibody, in patients with type 1 diabetes. Diabetes Obes Metab. 2020 Jul;22(7):1111-1121. doi: 10.1111/dom.14010
Journal: Diabetes, obesity & metabolism
Abstract: To report the first study of temelimab, a monoclonal antibody neutralizing the pathogenic human endogenous retrovirus type W envelope, in patients with type 1 diabetes (T1D). This double-blind, placebo-controlled, randomized clinical trial recruited adult patients with T1D within 4 years postdiagnosis and remaining C-peptide secretion. Sixty-four patients were randomized (2:1) to monthly temelimab 6 mg/kg or placebo during 24 weeks followed by a 24-week, open-label extension, during which all patients received temelimab. The primary objective was the safety and tolerability of temelimab. The secondary objective was to assess the pharmacodynamics response such as C-peptide levels, insulin use, HbA1c, hypoglycaemia and autoantibodies. Temelimab was well tolerated without any group difference in the frequency or severity of adverse events. Concerning exploratory endpoints, there was no difference in the levels of C-peptide, insulin use or HbA1c between treatment groups at weeks 24 and 48. The frequency of hypoglycaemia events was reduced with temelimab (P = 0.0004) at week 24 and the level of anti-insulin antibodies was lower with temelimab (P < 0.01); the other autoantibodies did not differ between groups. Temelimab appeared safe in patients with T1D. Pharmacodynamics signals (hypoglycaemia and anti-insulin antibodies) under temelimab were observed. Markers of β-cell functions were not modified by treatment. These results need to be further explored in younger patients with T1D with earlier disease onset.
DOI: 10.1111/dom.14010
Keywords: Antibodies;Diabetes Mellitus;Double-Blind Method;Monoclonal;Endogenous Retroviruses;Hypoglycemic Agents;Endogenous;Temelimab;Type 1 diabetes
Type: Article
Appears in Sites:Gold Coast Health Publications

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