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Engineering an Infectious Treg Biomimetic through Chemoselective Tethering of TGF-β1 to PEG Brush Surfaces

机译:通过将TGF-β1与PEG刷表面化学选择性束缚来设计传染性 Treg仿生物

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摘要

Modulation of immunological responses to allografts following transplantation is of pivotal importance to improving graft outcome and duration. Of the many approaches, harnessing the dominant tolerance induced by regulatory T cells (Treg) holds tremendous promise. Recent studies have highlighted the unique potency of cell surface-bound TGF-β1 on Treg for promoting infectious tolerance, i.e. to confer suppressive capacity from one cell to another. To mimic this characteristic, TGF-β1 was chemoselectively tethered to inert and viable polymer grafting platforms using Staudinger ligation. We report the synthesis and functional characterization of these engineered TGF-β1 surfaces. Inert beads tethered with TGF-β1 were capable of efficiently converting naïve CD4+ CD62Lhi T cells to functional Treg. Concordantly, translation of conjugation scheme from inert surfaces to viable cells also led to efficient generation of functional Treg. Further, the capacity of these platforms to generate antigen-specific Treg was demonstrated. These findings illustrate the unique faculty of tethered TGF-β1 biomaterial platforms to function as an “infectious” Treg and provide a compelling approach for generating tolerogenic microenvironments for allograft transplantation.
机译:移植后对同种异体移植物免疫应答的调节对改善移植物的结果和持续时间至关重要。在许多方法中,利用调节性T细胞(Treg)诱导的显性耐受具有广阔的前景。最近的研究强调了细胞表面结合的TGF-β1在Treg上具有独特的功效,以促进感染耐受,即赋予一种细胞至另一种细胞抑制能力。为了模拟该特性,使用Staudinger结扎法将TGF-β1化学选择性地束缚在惰性和可行的聚合物接枝平台上。我们报告了这些工程化的TGF-β1表面的合成和功能表征。与TGF-β1束缚的惰性珠粒能够将原始CD4 + CD62L hi T细胞有效转化为功能性Treg。相应地,结合方案从惰性表面到活细胞的翻译也导致功能性Treg的有效产生。此外,证明了这些平台产生抗原特异性Treg的能力。这些发现说明了拴系的TGF-β1生物材料平台的独特功能,可充当“传染性” Treg,并为产生同种异体移植的致耐受性微环境提供了引人注目的方法。

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