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Influence of Cytokines on HIV-Specific Antibody-Dependent Cellular Cytotoxicity Activation Profile of Natural Killer Cells

机译:细胞因子对天然杀伤细胞的HIV特异性抗体依赖性细胞毒性作用的影响

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摘要

There is growing interest in HIV-specific antibody-dependent cellular cytotoxicity (ADCC) as an effective immune response to prevent or control HIV infection. ADCC relies on innate immune effector cells, particularly NK cells, to mediate control of virus-infected cells. The activation of NK cells (i.e., expression of cytokines and/or degranulation) by ADCC antibodies in serum is likely subject to the influence of other factors that are also present. We observed that the HIV-specific ADCC antibodies, within serum samples from a panel of HIV-infected individuals induced divergent activation profiles of NK cells from the same donor. Some serum samples primarily induced NK cell cytokine expression (i.e., IFNγ), some primarily initiated NK cell expression of a degranulation marker (CD107a) and others initiated a similar magnitude of responses across both effector functions. We therefore evaluated a number of HIV-relevant soluble factors for their influence on the activation of NK cells by HIV-specific ADCC antibodies. Key findings were that the cytokines IL-15 and IL-10 consistently enhanced the ability of NK cells to respond to HIV-specific ADCC antibodies. Furthermore, IL-15 was demonstrated to potently activate “educated” KIR3DL1+ NK cells from individuals carrying its HLA-Bw4 ligand. The cytokine was also demonstrated to activate “uneducated” KIR3DL1+ NK cells from HLA-Bw6 homozygotes, but to a lesser extent. Our results show that cytokines influence the ability of NK cells to respond to ADCC antibodies in vitro. Manipulating the immunological environment to enhance the potency of NK cell-mediated HIV-specific ADCC effector functions could be a promising immunotherapy or vaccine strategy.
机译:作为预防或控制HIV感染的有效免疫应答,HIV特异性抗体依赖性细胞毒性(ADCC)引起了越来越多的关注。 ADCC依靠先天性免疫效应细胞,特别是NK细胞来介导病毒感染细胞的控制。血清中ADCC抗体对NK细胞的激活(即细胞因子的表达和/或脱粒)可能受到其他因素的影响。我们观察到,一组HIV感染者的血清样本中的HIV特异性ADCC抗体诱导了来自同一供体的NK细胞的不同激活特征。一些血清样品主要诱导NK细胞细胞因子表达(即IFNγ),一些样品主要引发脱颗粒标志物(CD107a)的NK细胞表达,而另一些样品则在两种效应子功能之间引发相似的反应幅度。因此,我们评估了许多与HIV相关的可溶性因子对它们对HIV特异性ADCC抗体激活NK细胞的影响。关键发现是细胞因子IL-15和IL-10持续增强了NK细胞对HIV特异性ADCC抗体的反应能力。此外,IL-15被证明可以有效地激活携带HLA-Bw4配体的个体的“受过教育”的KIR3DL1 + NK细胞。还证明了该细胞因子可激活HLA-Bw6纯合子的“未受教育的” KIR3DL1 + NK细胞,但程度较小。我们的结果表明,细胞因子会影响NK细胞在体外对ADCC抗体的反应能力。操纵免疫环境以增强NK细胞介导的HIV特异性ADCC效应子功能的效力可能是一种有前途的免疫疗法或疫苗策略。

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