与HIV控制相关的HLA-B35分子分类的分子见解。

IF 3.2 4区 医学 Q3 CELL BIOLOGY Immunology & Cell Biology Pub Date : 2023-10-09 DOI:10.1111/imcb.12698
Christian A Lobos, Demetra SM Chatzileontiadou, Bonin Sok, Coral-Ann Almedia, Hanim Halim, Lloyd D'Orsogna, Stephanie Gras
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摘要

人类白细胞抗原(HLA)I类分子已被证明影响对HIV感染和获得性免疫缺陷综合征进展的免疫反应。HLA-B35分子的多态性将该家族分为两组,即Px和PY。Px组与HIV+患者的有害影响和加速疾病进展有关,而PY组则不然。该分类基于PY组肽C末端部分的酪氨酸和Px组中的非酪氨酸残基的优先结合。然而,对这两个群体之间的分子差异缺乏了解。在此,我们研究了三种HLA-B35分子,即HLA-B*35:01(PY)、HLA-B*35:03(Px)和HLA-B*350:05(未分类)。我们选择了一种HIV衍生肽NY9,并证明它可以在HLA-B*35:01+/HIV/患者中触发多功能CD8+T细胞反应。我们确定,在与NY9肽的复合物中,PY分子比Px分子更稳定。我们解决了与NY9肽复合的三种HLA分子的晶体结构,并且与HLA-B*35:01的结构相似性将HLA-B*350:05归类为PY组。有趣的是,我们发现HLA-B*35:05也可以在其缝隙中结合一个小分子,这表明小药物也可以结合。
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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Molecular insights into the HLA-B35 molecules' classification associated with HIV control

Human leukocyte antigen (HLA) class I molecules have been shown to influence the immune response to HIV infection and acquired immunodeficiency syndrome progression. Polymorphisms within the HLA-B35 molecules divide the family into two groups, namely, Px and PY. The Px group is associated with deleterious effects and accelerated disease progression in HIV+ patients, whereas the PY group is not. The classification is based on the preferential binding of a tyrosine at the C-terminal part of the peptide in the PY group, and a nontyrosine residue in the Px group. However, there is a lack of knowledge on the molecular differences between the two groups. Here, we have investigated three HLA-B35 molecules, namely, HLA-B*35:01 (PY), HLA-B*35:03 (Px) and HLA-B*35:05 (unclassified). We selected an HIV-derived peptide, NY9, and demonstrated that it can trigger a polyfunctional CD8+ T-cell response in HLA-B*35:01+/HIV+ patients. We determined that in the complex with the NY9 peptide, the PY molecule was more stable than the Px molecule. We solved the crystal structures of the three HLA molecules in complex with the NY9 peptide, and structural similarities with HLA-B*35:01 would classify the HLA-B*35:05 within the PY group. Interestingly, we found that HLA-B*35:05 can also bind a small molecule in its cleft, suggesting that small drugs could bind as well.

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来源期刊
Immunology & Cell Biology
Immunology & Cell Biology 医学-免疫学
CiteScore
7.50
自引率
2.50%
发文量
98
审稿时长
4-8 weeks
期刊介绍: The Australasian Society for Immunology Incorporated (ASI) was created by the amalgamation in 1991 of the Australian Society for Immunology, formed in 1970, and the New Zealand Society for Immunology, formed in 1975. The aim of the Society is to encourage and support the discipline of immunology in the Australasian region. It is a broadly based Society, embracing clinical and experimental, cellular and molecular immunology in humans and animals. The Society provides a network for the exchange of information and for collaboration within Australia, New Zealand and overseas. ASI members have been prominent in advancing biological and medical research worldwide. We seek to encourage the study of immunology in Australia and New Zealand and are active in introducing young scientists to the discipline.
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