Design of TCR Structural Variants That Retain or Invert the Normal Activation Signal.

计算机科学 生物
作者
Jee-Young Mock,Julyun Oh,Jason J. Yi,Mark E. Daris,Agnes E. Hamburger,Alexander Kamb
出处
期刊:ImmunoHorizons [The American Association of Immunologists]
卷期号:5 (5): 349-359 被引量:1
标识
DOI:10.4049/immunohorizons.2100033
摘要

We designed variant human TCRs composed of the full-length TCRα/β or extracellular and transmembrane domains of the associated CD3 subunits fused to polypeptides derived from proteins thought to either enhance or inhibit normal T cell function. First, we showed that the C termini of both the TCR α- and β-chains can accommodate specific additional sequences, without abrogating complex formation or acute sensitivity of the receptor. Replacement of ITAMs with ITIM-containing intracellular domains inverted the TCR signal (i.e., created a ligand-dependent inhibitory receptor). The normal signaling function of the CD3 complex was transferable to the TCR by eliminating all CD3 ITAMs and grafting three to six ITAMs onto the C termini of the α/β-chains, with no effect on acute sensitivity. The observation that TCR variants of such diverse C-terminal composition can fold and function as signaling receptors demonstrates substantial structural and functional malleability of TCRs. These results add to knowledge about TCR structure-function with regard to acute signaling and may provide a route to use TCRs in different ways for T cell therapy.

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