Characterisation of an Influenza B virus-derived peptide presented by HLA-B*18:01.

IF 4.3 3区生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Biochemical Journal Pub Date : 2025-06-26 DOI:10.1042/bcj20240739

Lawton D Murdolo,Samuel Liwei Leong,Janesha C Maddumage,Nicole Mifsud,Demetra Sm Chatzileontiadou,Emma J Grant,Stephanie Gras

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引用次数: 0

Abstract

The Influenza B virus (IBV) can pose a significant threat to global health. Despite this, IBV is understudied compared to Influenza A virus (IAV). CD8+ T cells have proven highly effective in reducing influenza disease severity. In addition, pre-existing immune responses towards IAV epitopes may provide protection against homologous IBV-derived peptides due to T cell cross-reactivity. To exploit the advantages of T cells for future vaccine developments, a better understanding of the IBV-derived peptide presentation by the highly polymorphic Human Leukocyte Antigen (HLA) is required. We previously determined that the IAV-derived PB1177-A peptide was presented by the HLA-B*18:01 molecule and induced CD8+ T cell responses. Here we assessed the PB1177-A IBV homologue (PB1177-B). Intracellular cytokine staining assays showed that PB1177-B was unable to activate CD8+ T cells from several HLA-B*18:01+ samples tested. We determined that the IAV- and IBV-derived PB1177 adopted different stability and conformation in the cleft of HLA-B*18:01. Molecular dynamics analysis on the crystal structure showed that PB1177-B had a central flexible region with a large hydrophobic patch formed by two phenylalanine residues, not present in PB1177-A. The flexibility and the lower stability of the HLA-B*18:01-PB1177-B complex may hinder CD8+ T cell receptor binding, underpinning the lack of CD8+ T cell activation observed. This provides additional insights into the differences between IAV- and IBV-specific CD8+ T cell responses.

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HLA-B*18:01表达的乙型流感病毒衍生肽的特征

乙型流感病毒（IBV）可对全球健康构成重大威胁。尽管如此，与甲型流感病毒（IAV）相比，IBV的研究不足。CD8+ T细胞已被证明在降低流感疾病严重程度方面非常有效。此外，由于T细胞的交叉反应性，预先存在的针对IAV表位的免疫应答可能对同源ibv衍生肽提供保护。为了在未来的疫苗开发中利用T细胞的优势，需要更好地了解ibv衍生肽由高度多态性的人类白细胞抗原（HLA）呈递。我们之前确定了iav衍生的PB1177-A肽通过HLA-B*18:01分子呈现，并诱导CD8+ T细胞反应。我们对IBV同源物PB1177-A （PB1177-B）进行了鉴定。细胞内细胞因子染色实验表明，PB1177-B不能激活多个HLA-B*18:01+样品中的CD8+ T细胞。我们确定IAV-和ibv -衍生的PB1177在HLA-B*18:01的间隙中具有不同的稳定性和构象。晶体结构的分子动力学分析表明，PB1177-B具有一个由两个苯丙氨酸残基形成的大疏水性斑块的中心柔性区，而PB1177-A不存在。HLA-B*18:01-PB1177-B复合物的灵活性和较低的稳定性可能会阻碍CD8+ T细胞受体的结合，从而支持观察到的CD8+ T细胞缺乏活化。这为IAV特异性和ibv特异性CD8+ T细胞反应之间的差异提供了额外的见解。

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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来源期刊

Biochemical Journal 生物-生化与分子生物学

CiteScore

8.00

自引率

0.00%

发文量

255

审稿时长

1 months

期刊介绍： Exploring the molecular mechanisms that underpin key biological processes, the Biochemical Journal is a leading bioscience journal publishing high-impact scientific research papers and reviews on the latest advances and new mechanistic concepts in the fields of biochemistry, cellular biosciences and molecular biology. The Journal and its Editorial Board are committed to publishing work that provides a significant advance to current understanding or mechanistic insights; studies that go beyond observational work using in vitro and/or in vivo approaches are welcomed. Painless publishing: All papers undergo a rigorous peer review process; however, the Editorial Board is committed to ensuring that, if revisions are recommended, extra experiments not necessary to the paper will not be asked for. Areas covered in the journal include: Cell biology Chemical biology Energy processes Gene expression and regulation Mechanisms of disease Metabolism Molecular structure and function Plant biology Signalling