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优特克单抗治疗青少年1型糖尿病:一项多中心、双盲、随机2期试验。

Ustekinumab for type 1 diabetes in adolescents: a multicenter, double-blind, randomized phase 2 trial.

作者信息

Tatovic Danijela, Marwaha Ashish, Taylor Peter, Hanna Stephanie J, Carter Kym, Cheung W Y, Luzio Steve, Dunseath Gareth, Hutchings Hayley A, Holland Gail, Hiles Steve, Fegan Greg, Williams Evangelia, Yang Jennie H M, Domingo-Vila Clara, Pollock Emily, Wadud Muntaha, Ward-Hartstonge Kirsten, Marques-Jones Susie, Bowen-Morris Jane, Stenson Rachel, Levings Megan K, Gregory John W, Tree Timothy I M, Dayan Colin

机构信息

Division of Infection and Immunity, Cardiff University School of Medicine, Cardiff, UK.

University of Calgary, Calgary, Alberta, Canada.

出版信息

Nat Med. 2024 Sep;30(9):2657-2666. doi: 10.1038/s41591-024-03115-2. Epub 2024 Jul 30.

DOI:10.1038/s41591-024-03115-2
PMID:39079992
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11405276/
Abstract

Immunotherapy targeting the autoimmune process in type 1 diabetes (T1D) can delay the loss of β-cells but needs to have minimal adverse effects to be an adjunct to insulin in the management of T1D. Ustekinumab binds to the shared p40 subunit of interleukin (IL)-12 and IL-23, targeting development of T helper 1 cells and T helper 17 cells (T1 and T17 cells) implicated in the pathogenesis of T1D. We conducted a double-blind, randomized controlled trial of ustekinumab in 72 adolescents aged 12-18 years with recent-onset T1D. Treatment was well tolerated with no increase in adverse events. At 12 months, β-cell function, measured by stimulated C-peptide, was 49% higher in the intervention group (P = 0.02), meeting the prespecified primary outcome. Preservation of C-peptide correlated with the reduction of T helper cells co-secreting IL-17A and interferon-γ (T17.1 cells, P = 0.04) and, in particular, with the reduction in a subset of T17.1 cells co-expressing IL-2 and granulocyte-macrophage colony-stimulating factor (IL-2 GM-CSF T17.1 cells, P = 0.04). A significant fall in β-cell-targeted (proinsulin-specific) IL-17A-secreting T cells was also seen (P = 0.0003). Although exploratory, our data suggest a role for an activated subset of T17.1 cells in T1D that can be targeted with minimal adverse effects to reduce C-peptide loss, which requires confirmation in a larger study. (International Standard Randomised Controlled Trial Number Registry: ISRCTN 14274380).

摘要

针对1型糖尿病(T1D)自身免疫过程的免疫疗法可以延缓β细胞的丧失,但作为T1D管理中胰岛素的辅助手段,其副作用必须最小。乌司奴单抗与白细胞介素(IL)-12和IL-23的共享p40亚基结合,靶向参与T1D发病机制的辅助性T1细胞和辅助性T17细胞(T1和T17细胞)的发育。我们对72名12至18岁近期发病的T1D青少年进行了一项乌司奴单抗的双盲随机对照试验。治疗耐受性良好,不良事件没有增加。在12个月时,通过刺激C肽测量的β细胞功能在干预组中高49%(P = 0.02),达到了预先设定的主要结局。C肽的保留与共分泌IL-17A和干扰素-γ的辅助性T细胞(T17.1细胞,P = 0.04)的减少相关,特别是与共表达IL-2和粒细胞-巨噬细胞集落刺激因子的T17.1细胞亚群(IL-2 GM-CSF T17.1细胞,P = 0.04)的减少相关。还观察到靶向β细胞(胰岛素原特异性)分泌IL-17A的T细胞显著减少(P = 0.0003)。尽管是探索性的,但我们的数据表明T17.1细胞的一个活化亚群在T1D中起作用,可以以最小的副作用为靶点来减少C肽丧失,这需要在更大规模的研究中得到证实。(国际标准随机对照试验编号注册:ISRCTN 14274380)

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