Pandiyan Pushpa, Younes Souheil-Antoine, Ribeiro Susan Pereira, Talla Aarthi, McDonald David, Bhaskaran Natarajan, Levine Alan D, Weinberg Aaron, Sekaly Rafick P
Department of Biological Sciences, School of Dental Medicine, Case Western Reserve University , Cleveland, OH , USA.
Department of Medicine, Division of Infectious Diseases, University Hospitals, Case Western Reserve University , Cleveland, OH , USA.
Front Immunol. 2016 Jun 20;7:228. doi: 10.3389/fimmu.2016.00228. eCollection 2016.
Residual mucosal inflammation along with chronic systemic immune activation is an important feature in individuals infected with human immunodeficiency virus (HIV), and has been linked to a wide range of co-morbidities, including malignancy, opportunistic infections, immunopathology, and cardiovascular complications. Although combined antiretroviral therapy (cART) can reduce plasma viral loads to undetectable levels, reservoirs of virus persist, and increased mortality is associated with immune dysbiosis in mucosal lymphoid tissues. Immune-based therapies are pursued with the goal of improving CD4(+) T-cell restoration, as well as reducing chronic immune activation in cART-treated patients. However, the majority of research on immune activation has been derived from analysis of circulating T cells. How immune cell alterations in mucosal tissues contribute to HIV immune dysregulation and the associated risk of non-infectious chronic complications is less studied. Given the significant differences between mucosal T cells and circulating T cells, and the immediate interactions of mucosal T cells with the microbiome, more attention should be devoted to mucosal immune cells and their contribution to systemic immune activation in HIV-infected individuals. Here, we will focus on mucosal immune cells with a specific emphasis on CD4(+) T lymphocytes, such as T helper 17 cells and CD4(+)Foxp3(+) regulatory T cells (Tregs), which play crucial roles in maintaining mucosal barrier integrity and preventing inflammation, respectively. We hypothesize that pro-inflammatory milieu in cART-treated patients with immune activation significantly contributes to enhanced loss of Th17 cells and increased frequency of dysregulated Tregs in the mucosa, which in turn may exacerbate immune dysfunction in HIV-infected patients. We also present initial evidence to support this hypothesis. A better comprehension of how pro-inflammatory milieu impacts these two types of cells in the mucosa will shed light on mucosal immune dysfunction and HIV reservoirs, and lead to novel ways to restore immune functions in HIV(+) patients.
残余的黏膜炎症以及慢性全身免疫激活是感染人类免疫缺陷病毒(HIV)个体的一个重要特征,并且与多种合并症相关,包括恶性肿瘤、机会性感染、免疫病理学和心血管并发症。尽管联合抗逆转录病毒疗法(cART)可将血浆病毒载量降低到检测不到的水平,但病毒库仍然存在,并且黏膜淋巴组织中的免疫失调与死亡率增加有关。基于免疫的疗法旨在改善CD4(+) T细胞恢复,并减少接受cART治疗患者的慢性免疫激活。然而,大多数关于免疫激活的研究都来自对循环T细胞的分析。黏膜组织中的免疫细胞改变如何导致HIV免疫失调以及相关的非感染性慢性并发症风险,这方面的研究较少。鉴于黏膜T细胞和循环T细胞之间存在显著差异,以及黏膜T细胞与微生物群的直接相互作用,应更多关注HIV感染个体的黏膜免疫细胞及其对全身免疫激活的作用。在此,我们将重点关注黏膜免疫细胞,特别强调CD4(+) T淋巴细胞,如辅助性T细胞17(Th17)和CD4(+)Foxp3(+)调节性T细胞(Tregs),它们分别在维持黏膜屏障完整性和预防炎症方面发挥关键作用。我们假设,在接受cART治疗且有免疫激活的患者中,促炎环境显著导致黏膜中Th17细胞的损失增加以及失调的Tregs频率升高,这反过来可能会加剧HIV感染患者的免疫功能障碍。我们还提供了初步证据来支持这一假设。更好地理解促炎环境如何影响黏膜中的这两种细胞,将有助于揭示黏膜免疫功能障碍和HIV病毒库,并为恢复HIV(+)患者的免疫功能带来新方法。
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