Department of Pathology and Laboratory Medicine, University of Wisconsin-Madison, Madison, Wisconsin, USA.
Department of Microbiology and Molecular Genetics, University of Pittsburghgrid.21925.3d, Pittsburgh, Pennsylvania, USA.
Microbiol Spectr. 2022 Jun 29;10(3):e0172421. doi: 10.1128/spectrum.01724-21. Epub 2022 Apr 25.
Individuals co-infected with HIV and Mycobacterium tuberculosis (Mtb) are more likely to develop severe tuberculosis (TB) disease than HIV-naive individuals. To understand how a chronic pre-existing Simian immunodeficiency virus (SIV) infection impairs the early immune response to Mtb, we used the Mauritian cynomolgus macaque (MCM) model of SIV/Mtb co-infection. We examined the relationship between peripheral viral control and Mtb burden, Mtb dissemination, and T cell function between SIV+ spontaneous controllers, SIV+ non-controllers, and SIV-naive MCM who were challenged with a barcoded Mtb Erdman strain 6 months post-SIV infection and necropsied 6 weeks post-Mtb infection. Mycobacterial burden was highest in the SIV+ non-controllers in all assessed tissues. In lung granulomas, the frequency of TNF-α-producing CD4 T cells was reduced in all SIV+ MCM, but IFNγ-producing CD4 T cells were only lower in the SIV+ non-controllers. Further, while all SIV+ MCM had more PD1+ and TIGIT+ T cells in the lung granulomas relative to SIV-naive MCM, SIV+ controllers exhibited the highest frequency of cells expressing these markers. To measure the effect of SIV infection on within-host bacterial dissemination, we sequenced the molecular barcodes of Mtb present in each tissue and characterized the Mtb population complexity. While Mtb population complexity was not associated with SIV infection group, lymph nodes had increased complexity when compared with lung granulomas across all groups. These results provide evidence that SIV+ animals, independent of viral control, exhibit a dysregulated T cell immune response and enhanced dissemination of Mtb, likely contributing to the poor TB disease course across all SIV/Mtb co-infected animals. HIV and TB remain significant global health issues, despite the availability of treatments. Individuals with HIV, including those who are virally suppressed, are at an increased risk to develop and succumb to severe TB disease when compared with HIV-naive individuals. Our study aims to understand the relationship between the extent of SIV replication, mycobacterial growth, and T cell function in the tissues of co-infected Mauritian cynomolgus macaques during the first 6 weeks of Mtb infection. Here we demonstrate that increased viral replication is associated with increased bacterial burden in the tissues and impaired T cell responses, and that the immunological damage attributed to virus infection is not fully eliminated when animals spontaneously control virus replication.
个体同时感染 HIV 和结核分枝杆菌(Mtb)比 HIV 未感染者更易发展为严重结核病(TB)。为了了解慢性前期存在的猴免疫缺陷病毒(SIV)感染如何损害对 Mtb 的早期免疫反应,我们使用感染 SIV/Mtb 的毛里求斯食蟹猕猴(MCM)模型。我们研究了外周病毒控制与 Mtb 负担、Mtb 传播和 T 细胞功能之间的关系,这些关系存在于 SIV+自发性控制器、SIV+非控制器和 SIV 感染 6 个月后接受条形码 Mtb Erdman 菌株挑战并在 Mtb 感染后 6 周剖检的 SIV 未感染 MCM 之间。在所有评估的组织中,SIV+非控制器中的 Mtb 负担最高。在肺肉芽肿中,所有 SIV+MCM 中 TNF-α 产生的 CD4 T 细胞频率降低,但 IFNγ 产生的 CD4 T 细胞仅在 SIV+非控制器中降低。此外,虽然所有 SIV+MCM 的肺肉芽肿中 PD1+和 TIGIT+T 细胞数量都高于 SIV 未感染的 MCM,但 SIV+控制器表现出这些标记物表达频率最高。为了测量 SIV 感染对体内细菌传播的影响,我们对存在于每种组织中的 Mtb 的分子条码进行了测序,并对 Mtb 种群复杂性进行了特征描述。虽然 Mtb 种群复杂性与 SIV 感染组无关,但与所有组的肺肉芽肿相比,淋巴结的复杂性增加。这些结果提供了证据表明,无论病毒控制情况如何,SIV+动物都表现出失调的 T 细胞免疫反应和 Mtb 的增强传播,这可能导致所有 SIV/Mtb 共感染动物的 TB 疾病过程恶化。HIV 和 TB 仍然是全球重大健康问题,尽管有治疗方法。与 HIV 未感染者相比,HIV 感染者,包括病毒抑制者,发展和死于严重 TB 疾病的风险增加。我们的研究旨在了解在 Mtb 感染的前 6 周内,感染 SIV 的毛里求斯食蟹猕猴组织中 SIV 复制程度、分枝杆菌生长和 T 细胞功能之间的关系。在这里,我们证明了病毒复制增加与组织中的细菌负担增加和 T 细胞反应受损有关,并且当动物自发控制病毒复制时,归因于病毒感染的免疫损伤并未完全消除。
