Balancing Trained Immunity with Persistent Immune Activation and the Risk of Simian Immunodeficiency Virus Infection in Infant Macaques Vaccinated with Attenuated Mycobacterium tuberculosis or Mycobacterium bovis BCG Vaccine.

Q2 Biochemistry, Genetics and Molecular Biology

Clinical and Vaccine Immunology Pub Date : 2017-01-05 Print Date: 2017-01-01 DOI:10.1128/CVI.00360-16

Kara Jensen, Myra Grace Dela Pena-Ponce, Michael Piatak, Rebecca Shoemaker, Kelli Oswald, William R Jacobs, Glenn Fennelly, Carissa Lucero, Katie R Mollan, Michael G Hudgens, Angela Amedee, Pamela A Kozlowski, Jacob D Estes, Jeffrey D Lifson, Koen K A Van Rompay, Michelle Larsen, Kristina De Paris

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Abstract

Our goal is to develop a pediatric combination vaccine to protect the vulnerable infant population against human immunodeficiency virus type 1 (HIV-1) and tuberculosis (TB) infections. The vaccine consists of an auxotroph Mycobacterium tuberculosis strain that coexpresses HIV antigens. Utilizing an infant rhesus macaque model, we have previously shown that this attenuated M. tuberculosis (AMtb)-simian immunodeficiency virus (SIV) vaccine is immunogenic, and although the vaccine did not prevent oral SIV infection, a subset of vaccinated animals was able to partially control virus replication. However, unexpectedly, vaccinated infants required fewer SIV exposures to become infected compared to naive controls. Considering that the current TB vaccine, Mycobacterium bovis bacillus Calmette-Guérin (BCG), can induce potent innate immune responses and confer pathogen-unspecific trained immunity, we hypothesized that an imbalance between enhanced myeloid cell function and immune activation might have influenced the outcome of oral SIV challenge in AMtb-SIV-vaccinated infants. To address this question, we used archived samples from unchallenged animals from our previous AMtb-SIV vaccine studies and vaccinated additional infant macaques with BCG or AMtb only. Our results show that vaccinated infants, regardless of vaccine strain or regimen, had enhanced myeloid cell responses. However, CD4⁺ T cells were concurrently activated, and the persistence of these activated target cells in oral and/or gastrointestinal tissues may have facilitated oral SIV infection. Immune activation was more pronounced in BCG-vaccinated infant macaques than in AMtb-vaccinated infant macaques, indicating a role for vaccine attenuation. These findings underline the importance of understanding the interplay of vaccine-induced immunity and immune activation and its effect on HIV acquisition risk and outcome in infants.

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接种减毒结核分枝杆菌或牛分枝杆菌卡介苗的婴幼儿猕猴的训练免疫与持续免疫激活之间的平衡以及感染猿免疫缺陷病毒的风险。

我们的目标是开发一种儿科联合疫苗，以保护易感婴儿群体免受 1 型人类免疫缺陷病毒（HIV-1）和结核病（TB）感染。该疫苗由共表达 HIV 抗原的结核分枝杆菌辅助菌株组成。利用猕猴婴儿模型，我们之前已经证明了这种结核分枝杆菌（AMtb）减毒-西米亚免疫缺陷病毒（SIV）疫苗具有免疫原性，虽然疫苗不能预防口服 SIV 感染，但接种疫苗的动物亚群能够部分控制病毒复制。然而，出乎意料的是，与天真对照组相比，接种疫苗的婴儿需要更少的 SIV 暴露才会感染。考虑到目前的结核病疫苗--牛分枝杆菌卡介苗（BCG）能诱导有效的先天性免疫反应并赋予病原体非特异性训练免疫，我们假设髓系细胞功能增强与免疫激活之间的不平衡可能会影响接种了AMtb-SIV疫苗的婴儿口服SIV挑战的结果。为了解决这个问题，我们使用了以前的 AMtb-SIV 疫苗研究中未受挑战动物的存档样本，并给其他婴儿猕猴只接种了卡介苗或 AMtb 疫苗。我们的研究结果表明，无论疫苗株或接种方案如何，接种疫苗的婴儿都能增强髓系细胞反应。然而，CD4+ T细胞同时被激活，这些激活的靶细胞在口腔和/或胃肠道组织中的持续存在可能会促进口腔SIV感染。接种过卡介苗的猕猴比接种过AMtb疫苗的猕猴的免疫活化更为明显，这表明疫苗的减毒作用。这些发现强调了了解疫苗诱导的免疫和免疫激活的相互作用及其对婴儿感染艾滋病毒的风险和结果的影响的重要性。

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来源期刊

Clinical and Vaccine Immunology 医学-传染病学

CiteScore

2.88

自引率

0.00%

发文量

审稿时长

1.5 months

期刊介绍： Cessation. First launched as Clinical and Diagnostic Laboratory Immunology (CDLI) in 1994, CVI published articles that enhanced the understanding of the immune response in health and disease and after vaccination by showcasing discoveries in clinical, laboratory, and vaccine immunology. CVI was committed to advancing all aspects of vaccine research and immunization, including discovery of new vaccine antigens and vaccine design, development and evaluation of vaccines in animal models and in humans, characterization of immune responses and mechanisms of vaccine action, controlled challenge studies to assess vaccine efficacy, study of vaccine vectors, adjuvants, and immunomodulators, immune correlates of protection, and clinical trials.