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外周髓样细胞中干扰素调节因子-8 表达降低与治疗后 HIV 感染的不良中枢神经系统结局相关。

Lower Interferon Regulatory Factor-8 Expression in Peripheral Myeloid Cells Tracks With Adverse Central Nervous System Outcomes in Treated HIV Infection.

机构信息

Department of Tropical Medicine, University of Hawai'i, Honolulu, HI, United States.

Hawaii Center for AIDS, University of Hawai'i, Honolulu, HI, United States.

出版信息

Front Immunol. 2019 Nov 29;10:2789. doi: 10.3389/fimmu.2019.02789. eCollection 2019.

Abstract

Cognitive dysfunction persists in 30-50% of chronically HIV-infected individuals despite combination antiretroviral therapy (ART). Although monocytes are implicated in poor cognitive performance, distinct biological mechanisms associated with cognitive dysfunction in HIV infection are unclear. We previously showed that a regulatory region of the () gene is hyper-methylated in HIV-infected individuals with cognitive impairment compared to those with normal cognition. Here, we investigated IRF-8 protein expression and assessed relationships with multiple parameters associated with brain health. Intracellular IRF-8 expression was measured in cryopreserved peripheral blood mononuclear cells from chronically HIV-infected individuals on ART using flow cytometry. Neuropsychological performance was assessed by generating domain-specific standardized (NPZ) scores, with a global score defined by aggregating individual domain scores. Regional brain volumes were obtained by magnetic resonance imaging and soluble inflammatory factors were assessed by immunosorbent assays. Non-parametric analyses were conducted and statistical significance was defined as < 0.05. Twenty aviremic (HIV RNA<50 copies/ml) participants, 84% male, median age 51 [interquartile range (IQR) 46, 55], median CD4 count 548 [439, 700] were evaluated. IRF-8 expression was highest in plasmacytoid dendritic cells (pDCs). Assessing cognitive function, lower IRF-8 density in classical monocytes significantly correlated with worse NPZ_learning memory (LM; rho = 0.556) and NPZ_working memory (WM; rho = 0.612) scores, in intermediate monocytes with worse NPZ_LM (rho = 0.532) scores, and in non-classical monocytes, lower IRF-8 correlated with worse global NPZ (rho = 0.646), NPZ_LM (rho = 0.536), NPZ_WM (rho = 0.647), and NPZ_executive function (rho = 0.605) scores. In myeloid DCs (mDCs) lower IRF-8 correlated with worse NPZ_WM (rho = 0.48) scores and in pDCs with worse NPZ_WM (rho = 0.561) scores. Declines in IRF-8 in classical monocytes significantly correlated with smaller hippocampal volume (rho = 0.573) and in intermediate and non-classical monocytes with smaller cerebral white matter volume (rho = 0.509 and rho = 0.473, respectively). IRF-8 density in DCs did not significantly correlate with brain volumes. Among biomarkers tested, higher soluble ICAM-1 levels significantly correlated with higher IRF-8 in all monocyte and DC subsets. These data may implicate IRF-8 as a novel transcription factor in the neuropathophysiology of brain abnormalities in treated HIV and serve as a potential therapeutic target to decrease the burden of cognitive dysfunction in this population.

摘要

认知功能障碍在接受联合抗逆转录病毒治疗 (ART) 的慢性 HIV 感染者中仍持续存在 30-50%。尽管单核细胞与认知障碍有关,但与 HIV 感染相关的认知障碍的独特生物学机制尚不清楚。我们之前表明,与认知正常的个体相比,HIV 感染的个体中 ()基因的一个调节区域存在超甲基化。在这里,我们研究了 IRF-8 蛋白表达,并评估了与与大脑健康相关的多个参数的关系。使用流式细胞术测量了接受 ART 的慢性 HIV 感染者冷冻保存的外周血单核细胞中的细胞内 IRF-8 表达。通过生成特定于域的标准化 (NPZ) 评分来评估神经心理学表现,通过聚合个体域评分来定义总体评分。通过磁共振成像获得脑区体积,通过免疫吸附测定法评估可溶性炎症因子。进行了非参数分析,定义统计学意义为 < 0.05。评估了 20 名无病毒血症 (HIV RNA<50 拷贝/ml) 参与者,其中 84%为男性,中位年龄 51 [四分位间距 (IQR) 46, 55],中位 CD4 计数 548 [439, 700]。IRF-8 表达在浆细胞样树突状细胞 (pDCs) 中最高。评估认知功能时,经典单核细胞中 IRF-8 密度降低与 NPZ_学习记忆 (LM; rho = 0.556) 和 NPZ_工作记忆 (WM; rho = 0.612) 评分更差相关,在中间单核细胞中与 NPZ_LM (rho = 0.532) 评分更差相关,在非经典单核细胞中,IRF-8 与 NPZ 总评分 (rho = 0.646)、NPZ_LM (rho = 0.536)、NPZ_WM (rho = 0.647) 和 NPZ 执行功能 (rho = 0.605) 评分更差相关。在髓样树突状细胞 (mDCs) 中,IRF-8 与 NPZ_WM (rho = 0.48) 评分更差相关,在 pDCs 中与 NPZ_WM (rho = 0.561) 评分更差相关。经典单核细胞中 IRF-8 表达的下降与海马体积减小显著相关 (rho = 0.573),而中间和非经典单核细胞中与脑白质体积减小相关 (rho = 0.509 和 rho = 0.473)。DC 中 IRF-8 密度与脑体积无显著相关性。在测试的生物标志物中,较高的可溶性 ICAM-1 水平与所有单核细胞和 DC 亚群中更高的 IRF-8 显著相关。这些数据可能表明 IRF-8 是治疗 HIV 中脑异常神经发病机制的一种新型转录因子,并可能成为降低该人群认知功能障碍负担的潜在治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2732/6895026/0425ed5b938e/fimmu-10-02789-g0001.jpg

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