Veterans Affairs San Diego Healthcare System, San Diego, CA, USA.
Department of Neurosciences, University of California San Diego, San Diego, La Jolla, CA, USA.
J Neuroinflammation. 2020 Apr 11;17(1):112. doi: 10.1186/s12974-020-01781-w.
HIV-associated neurocognitive disorders (HAND) persist in the era of combined antiretroviral therapy (ART) despite reductions in viral load (VL) and overall disease severity. The mechanisms underlying HAND in the ART era are not well understood but are likely multifactorial, involving alterations in common pathways such as inflammation, autophagy, neurogenesis, and mitochondrial function. Newly developed omics approaches hold potential to identify mechanisms driving neuropathogenesis of HIV in the ART era.
In this study, using 33 postmortem frontal cortex (FC) tissues, neuropathological, molecular, and biochemical analyses were used to determine cellular localization and validate expression levels of the prolific transcription factor (TF), CCAAT enhancer binding protein (C/EBP) β, in brain tissues from HIV+ cognitively normal and HAND cases. RNA sequencing (seq) and transcriptomic analyses were performed on FC tissues including 24 specimens from well-characterized people with HIV that had undergone neurocognitive assessments. In vitro models for brain cells were used to investigate the role of C/EBPβ in mediating gene expression.
The most robust signal for TF dysregulation was observed in cases diagnosed with minor neurocognitive disorder (MND) compared to cognitive normal (CN) cases. Of particular interest, due to its role in inflammation, autophagy and neurogenesis, C/EBPβ was significantly upregulated in MND compared to CN brains. C/EBPβ was increased at the protein level in HAND brains. C/EBPβ levels were significantly reduced in neurons and increased in astroglia in HAND brains compared to CN. Transfection of human astroglial cells with a plasmid expressing C/EBPβ induced expression of multiple targets identified in the transcriptomic analysis of HAND brains, including dynamin-1-like protein (DNM1L) and interleukin-1 receptor-associated kinase 1. Recombinant HIV-Tat reduced and increased C/EBPβ levels in neuronal and astroglial cells, respectively.
These findings are the first to present RNAseq-based transcriptomic analyses of HIV+ brain tissues, providing further evidence of altered neuroinflammation, neurogenesis, mitochondrial function, and autophagy in HAND. Interestingly, these studies confirm a role for CEBPβ in regulating inflammation, metabolism, and autophagy in astroglia. Therapeutic strategies aimed at transcriptional regulation of astroglia or downstream pathways may provide relief to HIV+ patients at risk for HAND and other neurological disorders.
尽管病毒载量(VL)和整体疾病严重程度降低,但在联合抗逆转录病毒治疗(ART)时代,仍存在与 HIV 相关的神经认知障碍(HAND)。HAND 在 ART 时代的发病机制尚不清楚,但可能是多因素的,涉及炎症、自噬、神经发生和线粒体功能等常见途径的改变。新开发的组学方法有可能确定 HIV 在 ART 时代导致神经发病机制的机制。
在这项研究中,使用 33 个死后额皮质(FC)组织,通过神经病理学、分子和生化分析,确定 HIV+认知正常和 HAND 病例脑组织中丰富的转录因子(TF)CCAAT 增强子结合蛋白(C/EBP)β的细胞定位和验证表达水平。对包括 24 名经过神经认知评估的 HIV 特征明确的人的 FC 组织进行 RNA 测序(seq)和转录组分析。体外脑细胞模型用于研究 C/EBPβ 在介导基因表达中的作用。
在诊断为轻度认知障碍(MND)的病例中观察到 TF 失调的最强信号,与认知正常(CN)病例相比。特别有趣的是,由于其在炎症、自噬和神经发生中的作用,C/EBPβ 在 MND 脑与 CN 脑相比显著上调。HAND 脑蛋白水平的 C/EBPβ 增加。与 CN 脑相比,HAND 脑神经元中的 C/EBPβ 水平显著降低,星形胶质细胞中的 C/EBPβ 水平增加。用表达 C/EBPβ 的质粒转染人星形胶质细胞,可诱导 HAND 脑转录组分析中多个靶基因的表达,包括动力蛋白 1 样蛋白(DNM1L)和白细胞介素 1 受体相关激酶 1。重组 HIV-Tat 分别降低和增加神经元和星形胶质细胞中的 C/EBPβ 水平。
这些发现是首次对 HIV+脑组织进行基于 RNAseq 的转录组分析,进一步证明 HAND 中存在神经炎症、神经发生、线粒体功能和自噬改变。有趣的是,这些研究证实了 C/EBPβ 在调节星形胶质细胞中的炎症、代谢和自噬中的作用。针对星形胶质细胞或下游途径的转录调控的治疗策略可能为 HAND 和其他神经障碍的 HIV+患者提供缓解。
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