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Frequent and Strong Antibody-Mediated Natural Killer Cell Activation in Response to HIV-1 Env in Individuals with Chronic HIV-1 Infection

机译:频繁和强大的抗体介导的自然杀伤细胞活化对患有慢性HIV-1感染者的HIV-1 Env的反应

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摘要

Natural killer (NK) cells play a critical role in the control of HIV-1 infection, and NK cells that respond to HIV-1 peptides have been recently described. However, the mechanisms by which NK cells recognize HIV-1 antigens are not fully understood. We investigated NK cell activation in response to HIV-1 peptides during early and chronic HIV-1 clade B infection using a whole-blood assay and multiparameter flow cytometry. Antibody-mediated NK cell activation in response to HIV-1 peptides was not detected in HIV-1-uninfected individuals. In contrast, 79% of individuals with chronic infection and 22% of individuals with early infection had detectable gamma interferon (IFN-γ) NK cell responses to HIV-1 antigens (P < 0.00001). IFN-γ- and tumor necrosis factor alpha (TNF-α)-producing NK cells most frequently targeted Env gp120 (median of 4% and range of 0 to 31% of all NK cells). NK cells rarely targeted other HIV-1 proteins such as Gag, Pol, and Nef. Antibody-mediated NK cell responses to peptides mapped predominantly to Env protein, required the presence of plasma or plasma IgG, and resulted in lower CD16 expression on NK cells, suggesting an antibody-mediated activation of NK cells. Further studies are needed to assess the consequences of these antibody-mediated NK cell responses for HIV-1 disease progression and vaccine-induced protection from infection.
机译:天然杀伤(NK)细胞在控制HIV-1感染中起着关键作用,最近已经描述了对HIV-1肽有反应的NK细胞。但是,尚未完全了解NK细胞识别HIV-1抗原的机制。我们使用全血分析和多参数流式细胞术研究了早期和慢性HIV-1进化枝B感染过程中NK细胞对HIV-1肽的反应。在未感染HIV-1的个体中未检测到响应HIV-1肽的抗体介导的NK细胞活化。相反,有79%的慢性感染患者和22%的早期感染患者对HIV-1抗原具有可检测到的γ-干扰素(IFN-γ)NK细胞应答(P <0.00001)。产生IFN-γ和肿瘤坏死因子α(TNF-α)的NK细胞最常靶向Env gp120(中位数为4%,范围为所有NK细胞的0至31%)。 NK细胞很少靶向其他HIV-1蛋白,例如Gag,Pol和Nef。抗体介导的NK细胞对主要映射到Env蛋白的肽的反应,需要血浆或血浆IgG的存在,并导致NK细胞上CD16的表达降低,提示抗体介导的NK细胞活化。需要进一步的研究来评估这些抗体介导的NK细胞应答对HIV-1疾病进展和疫苗诱导的预防感染的后果。

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