Department of Obstetrics and Gynecology, University of Washington, Seattle, Washington, USA.
Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Research Center, Seattle, Washington, USA.
J Virol. 2020 Apr 16;94(9). doi: 10.1128/JVI.01904-19.
Pharmacological HIV-1 reactivation to reverse latent infection has been extensively studied. However, HIV-1 reactivation also occurs naturally, as evidenced by occasional low-level viremia ("viral blips") during antiretroviral treatment (ART). Clarifying where blips originate from and how they happen could provide clues to stimulate latency reversal more effectively and safely or to prevent viral rebound following ART cessation. We studied HIV-1 reactivation in the female genital tract, a dynamic anatomical target for HIV-1 infection throughout all disease stages. We found that primary endocervical epithelial cells from several women reactivated HIV-1 from latently infected T cells. The endocervical cells' HIV-1 reactivation capacity further increased upon Toll-like receptor 3 stimulation with poly(I·C) double-stranded RNA or infection with herpes simplex virus 2 (HSV-2). Notably, acyclovir did not eliminate HSV-2-induced HIV-1 reactivation. While endocervical epithelial cells secreted large amounts of several cytokines and chemokines, especially tumor necrosis factor alpha (TNF-α), CCL3, CCL4, and CCL20, their HIV-1 reactivation capacity was almost completely blocked by TNF-α neutralization alone. Thus, immunosurveillance activities by columnar epithelial cells in the endocervix can cause endogenous HIV-1 reactivation, which may contribute to viral blips during ART or rebound following ART interruption. A reason that there is no universal cure for HIV-1 is that the virus can hide in the genome of infected cells in the form of latent proviral DNA. This hidden provirus is protected from antiviral drugs until it eventually reactivates to produce new virions. It is not well understood where in the body or how this reactivation occurs. We studied HIV-1 reactivation in the female genital tract, which is often the portal of HIV-1 entry and which remains a site of infection throughout the disease. We found that the columnar epithelial cells lining the endocervix, the lower part of the uterus, are particularly effective in reactivating HIV-1 from infected T cells. This activity was enhanced by certain microbial stimuli, including herpes simplex virus 2, and blocked by antibodies against the inflammatory cytokine TNF-α. Avoiding HIV-1 reactivation could be important for maintaining a functional HIV-1 cure when antiviral therapy is stopped.
HIV-1 的药理学再激活已被广泛研究,以逆转潜伏感染。然而,HIV-1 的再激活也会自然发生,这可以从抗逆转录病毒治疗 (ART) 期间偶尔出现的低水平病毒血症 ("病毒闪烁") 中得到证明。阐明病毒闪烁的起源和发生方式可能为更有效地和安全地刺激潜伏期逆转提供线索,或防止 ART 停止后病毒反弹。我们研究了女性生殖道中的 HIV-1 再激活,这是 HIV-1 感染在所有疾病阶段的一个动态解剖靶标。我们发现,来自几名女性的原发性宫颈上皮细胞可以从潜伏感染的 T 细胞中再激活 HIV-1。在用 Toll 样受体 3 刺激 poly(I·C) 双链 RNA 或感染单纯疱疹病毒 2 (HSV-2) 后,宫颈上皮细胞的 HIV-1 再激活能力进一步增加。值得注意的是,阿昔洛韦并不能消除 HSV-2 诱导的 HIV-1 再激活。虽然宫颈上皮细胞大量分泌多种细胞因子和趋化因子,特别是肿瘤坏死因子 α(TNF-α)、CCL3、CCL4 和 CCL20,但它们的 HIV-1 再激活能力几乎完全被 TNF-α 中和单独阻断。因此,柱状上皮细胞的免疫监视活动可能导致内源性 HIV-1 再激活,这可能导致 ART 期间的病毒闪烁或 ART 中断后的病毒反弹。HIV-1 没有通用治愈方法的一个原因是,病毒可以以潜伏前病毒 DNA 的形式隐藏在受感染细胞的基因组中。这种隐藏的前病毒可以免受抗病毒药物的影响,直到它最终重新激活产生新的病毒粒子。目前还不清楚这种再激活发生在体内的何处或如何发生。我们研究了女性生殖道中的 HIV-1 再激活,女性生殖道通常是 HIV-1 进入的门户,并且在整个疾病过程中仍然是感染部位。我们发现,衬里子宫颈的柱状上皮细胞特别有效地从感染的 T 细胞中再激活 HIV-1。这种活性被某些微生物刺激物增强,包括单纯疱疹病毒 2,并被针对炎症细胞因子 TNF-α的抗体阻断。当抗病毒治疗停止时,避免 HIV-1 再激活对于维持功能性 HIV-1 治愈可能很重要。
