A Chicken Tapasin ortholog can chaperone empty HLA-B∗37:01 molecules independent of other peptide-loading components.

The Journal of Biological Chemistry Pub Date : 2023-10-01 Epub Date: 2023-08-04 DOI:10.1016/j.jbc.2023.105136
Georgia F Papadaki, Claire H Woodward, Michael C Young, Trenton J Winters, George M Burslem, Nikolaos G Sgourakis
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Abstract

Human Tapasin (hTapasin) is the main chaperone of MHC-I molecules, enabling peptide loading and antigen repertoire optimization across HLA allotypes. However, it is restricted to the endoplasmic reticulum (ER) lumen as part of the protein loading complex (PLC), and therefore is highly unstable when expressed in recombinant form. Additional stabilizing co-factors such as ERp57 are required to catalyze peptide exchange in vitro, limiting uses for the generation of pMHC-I molecules of desired antigen specificities. Here, we show that the chicken Tapasin (chTapasin) ortholog can be expressed recombinantly at high yields in a stable form, independent of co-chaperones. chTapasin can bind the human HLA-B∗37:01 with low micromolar-range affinity to form a stable tertiary complex. Biophysical characterization by methyl-based NMR methods reveals that chTapasin recognizes a conserved β2m epitope on HLA-B∗37:01, consistent with previously solved X-ray structures of hTapasin. Finally, we provide evidence that the B∗37:01/chTapasin complex is peptide-receptive and can be dissociated upon binding of high-affinity peptides. Our results highlight the use of chTapasin as a stable scaffold for protein engineering applications aiming to expand the ligand exchange function on human MHC-I and MHC-like molecules.

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鸡Tapasin直系同源物可以与其他肽负载组分无关地陪伴空的HLA-B*37:01分子。
人类Tapasin(hTapasin)是MHC-I分子的主要伴侣,能够在HLA同种型中优化肽负载和抗原库。然而,作为蛋白质负载复合物(PLC)的一部分,它仅限于内质网(ER)腔,因此在重组形式表达时高度不稳定。需要额外的稳定辅助因子,如ERp57,才能在体外催化肽交换,限制了产生所需抗原特异性的pMHC-I分子的用途。在这里,我们表明鸡Tapasin(chTapasin)同源物可以以稳定的形式以高产率重组表达,而不依赖于共伴侣。chTapasin可以以低微摩尔范围的亲和力与人类HLA-B*37:01结合,形成稳定的三级复合物。通过基于甲基的NMR方法进行的生物物理表征表明,chTapasin识别HLA-B*37:01上的保守β2m表位,与先前解决的hTapasin的X射线结构一致。最后,我们提供了证据,证明B*37:01/chTapasin复合物是肽接受性的,并且可以在结合高亲和力肽时解离。我们的研究结果强调了chTapasin作为蛋白质工程应用的稳定支架的用途,旨在扩大人类MHC-I和MHC-样分子上的配体交换功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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