Cotugno Nicola, De Armas Lesley, Pallikkuth Suresh, Rinaldi Stefano, Issac Biju, Cagigi Alberto, Rossi Paolo, Palma Paolo, Pahwa Savita
Research Unit in Congenital and Perinatal Infection, Immune and Infectious Diseases Division, Academic Department of Pediatrics, Bambino Gesù Children's Hospital, Rome, Italy.
Miami Center for AIDS Research, Department of Microbiology and Immunology, Miller School of Medicine, University of Miami, Miami, FL, United States.
Front Immunol. 2017 Sep 11;8:1083. doi: 10.3389/fimmu.2017.01083. eCollection 2017.
Despite effective antiretroviral therapy (ART), HIV-infected individuals with apparently similar clinical and immunological characteristics can vary in responsiveness to vaccinations. However, molecular mechanisms responsible for such impairment, as well as biomarkers able to predict vaccine responsiveness in HIV-infected children, remain unknown. Following the hypothesis that a B cell qualitative impairment persists in HIV-infected children (HIV) despite effective ART and phenotypic B cell immune reconstitution, the aim of the current study was to investigate B cell gene expression of HIV compared to age-matched healthy controls (HCs) and to determine whether distinct gene expression patterns could predict the ability to respond to influenza vaccine. To do so, we analyzed prevaccination transcriptional levels of a 96-gene panel in equal numbers of sort-purified B cell subsets (SPBS) isolated from peripheral blood mononuclear cells using multiplexed RT-PCR. Immune responses to H1N1 antigen were determined by hemaglutination inhibition and memory B cell ELISpot assays following trivalent-inactivated influenza vaccination (TIV) for all study participants. Although there were no differences in terms of cell frequencies of SPBS between HIV and HC, the groups were distinguishable based upon gene expression analyses. Indeed, a 28-gene signature, characterized by higher expression of genes involved in the inflammatory response and immune activation was observed in activated memory B cells (CD27CD21) from HIV when compared to HC despite long-term viral control (>24 months). Further analysis, taking into account H1N1 responses after TIV in HIV participants, revealed that a 25-gene signature in resting memory (RM) B cells (CD27CD21) was able to distinguish vaccine responders from non-responders (NR). In fact, prevaccination RM B cells of responders showed a higher expression of gene sets involved in B cell adaptive immune responses () and BCR signaling () when compared to NR. Overall, these data suggest that a perturbation at a transcriptional level in the B cell compartment persists despite stable virus control achieved through ART in HIV-infected children. Additionally, the present study demonstrates the potential utility of transcriptional evaluation of RM B cells before vaccination for identifying predictive correlates of vaccine responses in this population.
尽管有有效的抗逆转录病毒疗法(ART),但具有明显相似临床和免疫学特征的HIV感染者对疫苗接种的反应性可能存在差异。然而,导致这种损害的分子机制以及能够预测HIV感染儿童疫苗反应性的生物标志物仍然未知。基于这样的假设,即尽管有有效的ART和表型B细胞免疫重建,但HIV感染儿童(HIV)中仍存在B细胞质量损害,本研究的目的是调查HIV与年龄匹配的健康对照(HC)相比的B细胞基因表达,并确定不同的基因表达模式是否可以预测对流感疫苗的反应能力。为此,我们使用多重逆转录聚合酶链反应分析了从外周血单个核细胞中分离出的等量分选纯化B细胞亚群(SPBS)中96个基因面板的接种前转录水平。对所有研究参与者进行三价灭活流感疫苗接种(TIV)后,通过血凝抑制和记忆B细胞酶联免疫斑点试验确定对H1N1抗原的免疫反应。尽管HIV和HC之间的SPBS细胞频率没有差异,但根据基因表达分析,这两组是可区分的。事实上,与HC相比,尽管有长期病毒控制(>24个月),但在HIV的活化记忆B细胞(CD27CD21)中观察到一个由炎症反应和免疫激活相关基因高表达所表征的28个基因特征。进一步分析,考虑到HIV参与者在TIV后的H1N1反应,发现静息记忆(RM)B细胞(CD27CD21)中的一个25个基因特征能够区分疫苗应答者和无应答者(NR)。事实上,与NR相比,应答者接种前的RM B细胞显示出参与B细胞适应性免疫反应()和BCR信号传导()的基因集表达更高。总体而言,这些数据表明,尽管通过ART在HIV感染儿童中实现了稳定的病毒控制,但B细胞区室在转录水平上仍存在扰动。此外,本研究证明了接种前对RM B细胞进行转录评估在识别该人群疫苗反应预测相关性方面的潜在效用。
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