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首页> 美国卫生研究院文献>The Journal of General Virology >Pre-infection transcript levels of FAM26F in peripheral blood mononuclear cells inform about overall plasma viral load in acute and post-acute phase after simian immunodeficiency virus infection
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Pre-infection transcript levels of FAM26F in peripheral blood mononuclear cells inform about overall plasma viral load in acute and post-acute phase after simian immunodeficiency virus infection

机译:猿猴免疫缺陷病毒感染后外周血单个核细胞中FAM26F的感染前转录本水平可反映急性和急性后阶段的总体血浆病毒载量

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CD8+ cells from simian immunodeficiency virus (SIV)-infected long-term non-progressors and some uninfected macaques can suppress viral replication in vitro without killing the infected cells. The aim of this study was to identify factors responsible for non-cytolytic viral suppression by transcriptional profiling and to investigate their potential impact on SIV replication. Results of microarray experiments and further validation with cells from infected and uninfected macaques revealed that FAM26F RNA levels distinguished CD8+ cells of controllers and non-controllers (P=0.001). However, FAM26F was also expressed in CD4+ T-cells and B-cells. FAM26F expression increased in lymphocytes after in vitro IFN-γ treatment on average 40-fold, and ex vivo FAM26F RNA levels in peripheral blood mononuclear cells correlated with plasma IFN-γ but not with IFN-α. Baseline FAM26F expression appeared to be stable for months, albeit the individual expression levels varied up to tenfold. Investigating its role in SIV-infection revealed that FAM26F was upregulated after infection (P<0.0008), but did not directly correlate with viral load in contrast to MX1 and CXCL10. However, pre-infection levels of FAM26F correlated inversely with overall plasma viral load (AUC) during the acute and post-acute phases of infection (e.g. AUC weeks post infection 0–8; no AIDS vaccine: P<0.0001, Spearman rank correlation coefficient (rs)=−0.89, n=16; immunized with an AIDS vaccine: P=0.033, rs=−0.43; n=25). FAM26F transcript levels prior to infection can provide information about the pace and strength of the antiviral immune response during the early stage of infection. FAM26F expression represented, in our experiments, one of the earliest prognostic markers, and could supplement major histocompatibility complex (MHC)-typing to predict disease progression before SIV-infection.
机译:猿猴免疫缺陷病毒(SIV)感染的长期非进展者和某些未感染的猕猴的CD8 + 细胞可以在不杀死感染细胞的情况下抑制体外病毒复制。这项研究的目的是通过转录谱分析确定负责非溶细胞病毒抑制的因素,并研究它们对SIV复制的潜在影响。微阵列实验的结果以及对感染和未感染猕猴细胞的进一步验证表明,FAM26F RNA水平区分了控制者和非控制者的CD8 + 细胞(P = 0.001)。然而,FAM26F也在CD4 + T细胞和B细胞中表达。在体外IFN-γ处理后,淋巴细胞中FAM26F表达平均增加40倍,而外周血单核细胞中离体FAM26F RNA水平与血浆IFN-γ相关,但与IFN-α不相关。基线FAM26F表达似乎稳定了几个月,尽管单个表达水平变化了十倍。研究其在SIV感染中的作用表明,FAM26F在感染后被上调(P <0.0008),但与MX1和CXCL10相比,它与病毒载量没有直接关系。但是,在感染的急性期和急性期(例如感染后0至8周的AUC);感染前FAM26F的水平与总血浆病毒载量(AUC)呈反比关系;无AIDS疫苗:P <0.0001,Spearman等级相关系数(rs)=-0.89,n = 16;用AIDS疫苗免疫:P = 0.033,rs = -0.43; n = 25)。感染前的 FAM26F 转录水平可以提供有关感染初期抗病毒免疫反应的步伐和强度的信息。在我们的实验中, FAM26F 表达代表了最早的预后标记之一,并且可以补充主要组织相容性复合物(MHC)分型以预测SIV感染前的疾病进展。

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