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斩除特洛伊木马:自然杀伤细胞表现出针对异基因 T 细胞的强大抗 HIV-1 抗体依赖性激活和细胞溶解作用。

Slaying the Trojan horse: natural killer cells exhibit robust anti-HIV-1 antibody-dependent activation and cytolysis against allogeneic T cells.

机构信息

Department of Microbiology and Immunology, University of Melbourne, Melbourne, Victoria, Australia.

Centre de Recherche du CHUM, Department of Microbiology, Infectiology and Immunology, Université de Montreal, Montreal, Quebec, Canada.

出版信息

J Virol. 2015 Jan;89(1):97-109. doi: 10.1128/JVI.02461-14. Epub 2014 Oct 15.

Abstract

UNLABELLED

Many attempts to design prophylactic human immunodeficiency virus type 1 (HIV-1) vaccines have focused on the induction of neutralizing antibodies (Abs) that block infection by free virions. Despite the focus on viral particles, virus-infected cells, which can be found within mucosal secretions, are more infectious than free virus both in vitro and in vivo. Furthermore, assessment of human transmission couples suggests infected seminal lymphocytes might be responsible for a proportion of HIV-1 transmissions. Although vaccines that induce neutralizing Abs are sought, only some broadly neutralizing Abs efficiently block cell-to-cell transmission of HIV-1. As HIV-1 vaccines need to elicit immune responses capable of controlling both free and cell-associated virus, we evaluated the potential of natural killer (NK) cells to respond in an Ab-dependent manner to allogeneic T cells bearing HIV-1 antigens. This study presents data measuring Ab-dependent anti-HIV-1 NK cell responses to primary and transformed allogeneic T-cell targets. We found that NK cells are robustly activated in an anti-HIV-1 Ab-dependent manner against allogeneic targets and that tested target cells are subject to Ab-dependent cytolysis. Furthermore, the educated KIR3DL1(+) NK cell subset from HLA-Bw4(+) individuals exhibits an activation advantage over the KIR3DL1(-) subset that contains both NK cells educated through other receptor/ligand combinations and uneducated NK cells. These results are intriguing and important for understanding the regulation of Ab-dependent NK cell responses and are potentially valuable for designing Ab-dependent therapies and/or vaccines.

IMPORTANCE

NK cell-mediated anti-HIV-1 antibody-dependent functions have been associated with protection from infection and disease progression; however, their role in protecting from infection with allogeneic cells infected with HIV-1 is unknown. We found that HIV-1-specific ADCC antibodies bound to allogeneic cells infected with HIV-1 or coated with HIV-1 gp120 were capable of activating NK cells and/or trigging cytolysis of the allogeneic target cells. This suggests ADCC may be able to assist in preventing infection with cell-associated HIV-1. In order to fully utilize NK cell-mediated Ab-dependent effector functions, it might also be important that educated NK cells, which hold the highest activation potential, can become activated against targets bearing HIV-1 antigens and expressing the ligands for self-inhibitory receptors. Here, we show that with Ab-dependent stimulation, NK cells expressing inhibitory receptors can mediate robust activation against targets expressing the ligands for those receptors.

摘要

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许多设计预防性人类免疫缺陷病毒 1 型(HIV-1)疫苗的尝试都集中在诱导能够阻断游离病毒感染的中和抗体(Abs)上。尽管关注的是病毒颗粒,但在体外和体内,感染细胞的病毒比游离病毒更具传染性,这些感染细胞可以在粘膜分泌物中找到。此外,对人类传播对的评估表明,感染的精原淋巴细胞可能负责 HIV-1 传播的一部分。尽管人们正在寻找能够诱导中和 Abs 的疫苗,但只有一些广泛中和 Abs 能够有效地阻断 HIV-1 的细胞间传播。由于 HIV-1 疫苗需要引发能够控制游离病毒和细胞相关病毒的免疫反应,我们评估了自然杀伤(NK)细胞以依赖 Ab 的方式对携带 HIV-1 抗原的同种异体 T 细胞做出反应的潜力。本研究提供了测量针对原发性和转化的同种异体 T 细胞靶标依赖 Ab 的抗 HIV-1 NK 细胞反应的数据。我们发现,NK 细胞以依赖 Ab 的方式针对同种异体靶标被强烈激活,并且经过测试的靶细胞受到依赖 Ab 的细胞溶解作用。此外,来自 HLA-Bw4+个体的受过教育的 KIR3DL1(+)NK 细胞亚群比包含通过其他受体/配体组合受过教育的 NK 细胞和未受过教育的 NK 细胞的 KIR3DL1(-)亚群具有激活优势。这些结果令人着迷,对于理解依赖 Ab 的 NK 细胞反应的调节具有重要意义,并且对于设计依赖 Ab 的治疗方法和/或疫苗可能具有潜在价值。

重要性

NK 细胞介导的抗 HIV-1 抗体依赖性功能与免受感染和疾病进展有关;然而,它们在保护免受感染携带 HIV-1 的同种异体细胞方面的作用尚不清楚。我们发现,HIV-1 特异性 ADCC 抗体与感染 HIV-1 的同种异体细胞结合或与 HIV-1 gp120 包被的同种异体细胞结合,能够激活 NK 细胞并/或触发同种异体靶细胞的细胞溶解。这表明 ADCC 可能能够帮助预防细胞相关 HIV-1 的感染。为了充分利用 NK 细胞介导的依赖 Ab 的效应功能,具有最高激活潜力的受过教育的 NK 细胞能够针对携带 HIV-1 抗原并表达自身抑制性受体配体的靶标激活也可能很重要。在这里,我们表明,通过依赖 Ab 的刺激,表达抑制性受体的 NK 细胞可以针对表达这些受体配体的靶标介导强烈的激活。

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