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在自组装疫苗中滴定T细胞表位可优化CD4+辅助性T细胞和抗体的产出。

Titrating T-cell epitopes within self-assembled vaccines optimizes CD4+ helper T cell and antibody outputs.

作者信息

Pompano Rebecca R, Chen Jianjun, Verbus Emily A, Han Huifang, Fridman Arthur, McNeely Tessie, Collier Joel H, Chong Anita S

机构信息

Department of Surgery, Committee of Immunology, University of Chicago, 5841 S. Maryland Avenue, MC5032, Chicago, IL, 60637, USA.

出版信息

Adv Healthc Mater. 2014 Nov;3(11):1898-908. doi: 10.1002/adhm.201400137. Epub 2014 Jun 13.

Abstract

Epitope content plays a critical role in determining T-cell and antibody responses to vaccines, biomaterials, and protein therapeutics, but its effects are nonlinear and difficult to isolate. Here, molecular self-assembly is used to build a vaccine with precise control over epitope content, in order to finely tune the magnitude and phenotype of T helper and antibody responses. Self-adjuvanting peptide nanofibers are formed by co-assembling a high-affinity universal CD4+ T-cell epitope (PADRE) and a B-cell epitope from Staphylococcus aureus at specifiable concentrations. Increasing the PADRE concentration from micromolar to millimolar elicited bell-shaped dose-responses that are unique to different T-cell populations. Notably, the epitope ratios that maximize T follicular helper and antibody responses differed by an order of magnitude from those that maximized Th1 or Th2 responses. Thus, modular materials assembly provides a means of controlling epitope content and efficiently skewing the adaptive immune response in the absence of exogenous adjuvant; this approach may contribute to the development of improved vaccines and immunotherapies.

摘要

表位含量在决定对疫苗、生物材料和蛋白质疗法的T细胞及抗体反应中起着关键作用,但其作用是非线性的且难以分离。在此,利用分子自组装构建了一种能精确控制表位含量的疫苗,以便精确调节辅助性T细胞反应的强度和表型以及抗体反应。通过将高亲和力的通用CD4+ T细胞表位(PADRE)与来自金黄色葡萄球菌的B细胞表位以可指定的浓度共同组装,形成了自佐剂化肽纳米纤维。将PADRE浓度从微摩尔增加到毫摩尔引发了钟形剂量反应,这对不同的T细胞群体而言是独特的。值得注意的是,使滤泡辅助性T细胞和抗体反应最大化的表位比例与使Th1或Th2反应最大化的表位比例相差一个数量级。因此,模块化材料组装提供了一种在无外源性佐剂的情况下控制表位含量并有效偏向适应性免疫反应的方法;这种方法可能有助于改进疫苗和免疫疗法的开发。

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