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A Correlate of HIV-1 Control Consisting of Both Innate and Adaptive Immune Parameters Best Predicts Viral Load by Multivariable Analysis in HIV-1 Infected Viremic Controllers and Chronically-Infected Non-Controllers

机译：通过自然变量和适应性免疫参数组成的HIV-1对照的相关性可以通过HIV-1感染的病毒控制者和慢性感染的非控制者的多变量分析最好地预测病毒载量

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HIV-1 infected viremic controllers maintain durable viral suppression below 2000 copies viral RNA/ml without anti-retroviral therapy (ART), and the immunological factor(s) associated with host control in presence of low but detectable viral replication are of considerable interest. Here, we utilized a multivariable analysis to identify which innate and adaptive immune parameters best correlated with viral control utilizing a cohort of viremic controllers (median 704 viral RNA/ml) and non-controllers (median 21,932 viral RNA/ml) that were matched for similar CD4⁺ T cell counts in the absence of ART. We observed that HIV-1 Gag-specific CD8⁺ T cell responses were preferentially targeted over Pol-specific responses in viremic controllers (p = 0.0137), while Pol-specific responses were positively associated with viral load (rho = 0.7753, p = 0.0001, n = 23). Viremic controllers exhibited significantly higher NK and plasmacytoid dendritic cells (pDC) frequency as well as retained expression of the NK CD16 receptor and strong target cell-induced NK cell IFN-gamma production compared to non-controllers (p<0.05). Despite differences in innate and adaptive immune function however, both viremic controllers (p<0.05) and non-controller subjects (p<0.001) exhibited significantly increased CD8⁺ T cell activation and spontaneous NK cell degranulation compared to uninfected donors. Overall, we identified that a combination of innate (pDC frequency) and adaptive (Pol-specific CD8⁺ T cell responses) immune parameters best predicted viral load (R² = 0.5864, p = 0.0021, n = 17) by a multivariable analysis. Together, this data indicates that preferential Gag-specific over Pol-specific CD8⁺ T cell responses along with a retention of functional innate subsets best predict host control over viral replication in HIV-1 infected viremic controllers compared to chronically-infected non-controllers.

机译：被HIV-1感染的病毒控制者无需抗逆转录病毒疗法（ART），即可在2000拷贝病毒RNA / ml以下维持持久的病毒抑制，并且与宿主控制相关的免疫因素在低但可检测到的病毒复制下引起了人们的极大兴趣。在这里，我们利用多变量分析来确定哪些先天性和适应性免疫参数与病毒控制最相关，这是利用一组病毒控制者（中位数704病毒RNA / ml）和非控制者（中位数21932病毒RNA / ml）匹配的。在没有ART的情况下，CD4 ^{+ T细胞计数相似。我们观察到，在病毒控制者中，HIV-1 Gag特异性CD8 ^{+ T细胞应答优先于Pol特异性应答（p = 0.0137），而Pol特异性应答与病毒载量正相关（ rho = 0.7753，p = 0.0001，n = 23）。与非控制者相比，病毒控制者表现出明显更高的NK和浆细胞样树突状细胞（pDC）频率，以及保留的NK CD16受体表达和强烈的靶细胞诱导的NK细胞IFN-γ产生（p <0.05）。尽管先天和适应性免疫功能存在差异，但是与之相比，病毒控制者（p <0.05）和非控制者（p <0.001）均表现出显着增加的CD8 ^{+ T细胞活化和自发性NK细胞脱粒未感染的捐助者。总体而言，我们确定先天性（pDC频率）和适应性（Pol特异性CD8 ^{+ T细胞应答）免疫参数的组合可以最好地预测病毒载量（R ^{2 = 0.5864 ，p = 0.0021，n = 17）。总的来说，这些数据表明，优先于Gag特异性而不是Pol特异性CD8 ^{+ T细胞应答以及功能性先天亚型的保留最能预测宿主对HIV-1感染的病毒控制者中病毒复制的控制。慢性感染的非控制者。}}}}}}

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作者
Costin Tomescu; Qin Liu; Brian N. Ross; Xiangfan Yin; Kenneth Lynn; Karam C. Mounzer; Jay R. Kostman; Luis J. Montaner;
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年(卷),期 -1(9),7
年度 -1
页码 e103209
总页数 10
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入库时间 2022-08-21 11:18:06

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专利

1. Association of HIV-1 Gag-Specific IgG Antibodies With Natural Control of HIV-1 Infection in Individuals Not Carrying HLA-B*57:01 Is Only Observed in Viremic Controllers [J] . Tjiam M. Christian, Morshidi Mazmah A., Sariputra Lucy, JAIDS: Journal of acquired immune deficiency syndromes . 2017,第3期

机译：HIV-1 GAG特异性IgG抗体的缔合具有HIV-1感染的自然对照，仅在雌激素控制器中仅观察到HIV-1感染中的单独感染
2. Rate and predictors of progression in elite and viremic HIV-1 controllers [J] . Leon Agathe, Perez Ignacio, Ruiz-Mateos Ezequiel, AIDS . 2016,第8期

机译：精英和病毒血症HIV-1控制者的进展率和预测指标
3. Transcriptomics and Targeted Proteomics Analysis to Gain Insights Into the Immune-control Mechanisms of HIV-1 Infected Elite Controllers [J] . Wang Zhang, Anoop T. Ambikan, Maike Sperk, EBioMedicine . 2018,第4期

机译：转录组学和靶向蛋白质组学分析可深入了解HIV-1感染的精英控制者的免疫控制机制。
4. Passive repression of HIV-1 long terminal repeat enhancer controlled viral transcription in HIV-1 infected cells [C] . S.R.K.Hoffmann, L.Bisset, J.Schupbach, the International Peptide Symposium . 2001

机译：HIV-1长末端重复增强剂受控病毒转录的被动压制在HIV-1感染细胞中
5. HIV-1 immunity: Innate immune correlates and vaccine responses. [D] . Pine, Samuel O'Neill. 2009

机译：HIV-1免疫：先天免疫相关性和疫苗反应。
6. The association of HIV-1 Gag-specific IgG antibodies with natural control of HIV-1 infection in individuals not carrying HLA-B*57:01 is only observed in viremic controllers [O] . M. Christian TJIAM, Mazmah A. MORSHIDI, Lucy SARIPUTRA, -1

机译：仅在病毒血症控制者中观察到HIV-1 Gag特异性IgG抗体与不携带HLA-B * 57：01的个体对HIV-1感染的自然控制的关联
7. A correlate of HIV-1 control consisting of both innate and adaptive immune parameters best predicts viral load by multivariable analysis in HIV-1 infected viremic controllers and chronically-infected non-controllers. [O] . Costin Tomescu, Qin Liu, Brian N Ross, 2014

机译：由先天性和适应性免疫参数组成的HIV-1对照的相关性通过HIV-1感染的病毒血症控制器和慢性感染的非控制者的多变量分析最好地预测病毒载量。

A Correlate of HIV-1 Control Consisting of Both Innate and Adaptive Immune Parameters Best Predicts Viral Load by Multivariable Analysis in HIV-1 Infected Viremic Controllers and Chronically-Infected Non-Controllers

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