| Literature DB >> 34580438 |
Bo Zhang1,2, Jiaqi Sun2, Yan Wang2, Dezhong Ji2, Yeshuang Yuan3,4, Shengjie Li1, Yeting Sun1,5, Yingqin Hou6, Pengchong Li1,5, Lidan Zhao1,5, Fei Yu2, Wenxiao Ma2, Boyang Cheng2, Ling Wu2, Jin Hu1, Min Wang3,4, Wei Song1, Xiaogang Li1, Hao Li7, Yunyun Fei1,5, Hua Chen1,5, Lihe Zhang2, George C Tsokos8, Demin Zhou9, Xuan Zhang10.
Abstract
The preferential activation of regulatory T (Treg) cells by interleukin-2 (IL-2), which selectively binds to the trimeric IL-2 receptor (IL-2R) on Treg cells, makes this cytokine a promising therapeutic for the treatment of autoimmune diseases. However, IL-2 has a narrow therapeutic window and a short half-life. Here, we show that the pharmacokinetics and half-life of IL-2 can be substantially improved by orthogonally conjugating the cytokine to poly(ethylene glycol) (PEG) moieties via a copper-free click reaction through the incorporation of azide-bearing amino acids at defined sites. Subcutaneous injection of a PEGylated IL-2 that optimally induced sustained Treg-cell activation and expansion over a wide range of doses through highly selective binding to trimeric IL-2R led to enhanced therapeutic efficacy in mouse models of lupus, collagen-induced arthritis and graft-versus-host disease without compromising the immune defences of the host against viral infection. Site-specific PEGylation could be used more generally to engineer cytokines with improved therapeutic performance for the treatment of autoimmune diseases.Entities:
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Year: 2021 PMID: 34580438 DOI: 10.1038/s41551-021-00797-8
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 25.671