Effect of CFP-10/ESAT-6 secretory proteins on long-term non-specific immunological memory in mouse macrophages

Q4 Medicine

Medical Immunology (Russia) Pub Date : 2023-06-01 DOI:10.15789/1563-0625-eoe-2663

А. P. Lykov, S. Belogorodtsev, Е. К. Nemkova, А. Vetlugina, Т. М. Terekhova, Y. Schwartz

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Abstract

Innate immune cells (monocytes/macrophages, NK) can also develop immune memory, which means that these cells are trained after their first encounter with pathogens so that they exhibit a nonspecific immunological response to the same or another pathogen. Bacilli Calmette–Gu rin (BCG) induces nonspecific innate memory (trained immunity) in innate immune cells. We examined nonspecific innate memory in macrophages of BALB/c mice in response to mycobacteria with or without the RD1 region in the genome. Mice were immunized with BCG vaccine, and peritoneal macrophages were isolated on day 7, and then stimulated with bacterial lipopolysaccharide, CFP-10, or ESAT-6. In addition, mice were immunized with Mycobacterium tuberculosis uro-BCG vaccine (RD1-) and Mycobacterium tuberculosis strain H37Rv (RD1+) subcutaneously or intravenously; peritoneal macrophages were isolated and stimulated with lipopolysaccharide on day 4. Alveolar macrophages were obtained from lung explants of mice infected with Mycobacterium tuberculosis strain H37Rv mice, were expanded to confluence 70-80% and further stimulated with lipopolysaccharide. Lactate, cytokines, and glucose levels were examined in conditioned macrophage medium. Peritoneal macrophages from mice primed with BCG vaccine were shown to increase IL-1b, TNFa, and lactate production in response to CFP-6 and ESAT-10 (p < 0.05). Of note is the fact that lipopolysaccharide also increased production of IL-1b, TNFa, and also increased glucose uptake by peritoneal macrophages primed with BCG vaccine (p < 0.05). Peritoneal macrophages primed with Uro-BCG were shown to increase spontaneous production of IL-1b and decrease spontaneous production of TNFa (p < 0.05). When macrophages were primed by subcutaneous or intravenous administration of Mycobacterium tuberculosis strain H37Rv differentially affected cytokine production, by decreasing IL-1b production and increasing TNFa and IL-10, was observed. In response to lipopolysaccharide, peritoneal macrophages increased IL-1b, TNFa, IL-10 production and glucose consumption (p < 0.05). The mode of priming of macrophages with Mycobacterium tuberculosis strain H37Rv also led to multidirectional levels of cytokine production. Alveolar macrophages were shown to retain trained immunity, as they produced elevated levels of IL-1b, TNFa, and IL-10 (p < 0.05). Thus, mouse macrophages formed a trained immunity phenotype in response to different types of mycobacteria, which persists for a long time after primary contact with the pathogen, particularly in alveolar macrophages.

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CFP-10/ESAT-6分泌蛋白对小鼠巨噬细胞长期非特异性免疫记忆的影响

先天免疫细胞(单核/巨噬细胞，NK细胞)也可以发展免疫记忆，这意味着这些细胞在第一次遇到病原体后受到训练，因此它们对相同或另一种病原体表现出非特异性免疫反应。卡介苗诱导先天免疫细胞的非特异性先天记忆(训练免疫)。我们检测了BALB/c小鼠巨噬细胞对基因组中有或没有RD1区域的分枝杆菌的非特异性先天记忆。用卡介苗免疫小鼠，第7天分离腹腔巨噬细胞，然后用细菌脂多糖、CFP-10或ESAT-6刺激。此外，小鼠皮下或静脉注射结核分枝杆菌尿卡介苗(RD1-)和结核分枝杆菌H37Rv株(RD1+)免疫;第4天分离腹腔巨噬细胞，用脂多糖刺激。从感染结核分枝杆菌H37Rv小鼠的肺外植体中获得肺泡巨噬细胞，扩增至融合70-80%，并进一步用脂多糖刺激。在条件巨噬细胞培养基中检测乳酸、细胞因子和葡萄糖水平。接种卡介苗的小鼠腹腔巨噬细胞对CFP-6和ESAT-10的反应显示IL-1b、TNFa和乳酸的产生增加(p < 0.05)。值得注意的是，脂多糖也增加了IL-1b、TNFa的产生，并增加了接种卡介苗的腹膜巨噬细胞对葡萄糖的摄取(p < 0.05)。经urobcg诱导的巨噬细胞可增加IL-1b的自发生成，降低TNFa的自发生成(p < 0.05)。皮下或静脉注射结核分枝杆菌H37Rv诱导巨噬细胞时，观察到细胞因子产生的差异，IL-1b产生减少，TNFa和IL-10产生增加。腹腔巨噬细胞对脂多糖的反应增加了IL-1b、TNFa、IL-10的产生和葡萄糖消耗(p < 0.05)。用结核分枝杆菌H37Rv菌株引发巨噬细胞的模式也导致细胞因子的多向水平产生。肺泡巨噬细胞可以产生高水平的IL-1b、TNFa和IL-10，从而保持训练后的免疫力(p < 0.05)。因此，小鼠巨噬细胞对不同类型的分枝杆菌形成了一种经过训练的免疫表型，这种免疫表型在与病原体初次接触后持续很长时间，尤其是在肺泡巨噬细胞中。

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来源期刊

Medical Immunology (Russia) Medicine-Immunology and Allergy

CiteScore

0.70

自引率

0.00%

发文量

审稿时长

12 weeks

期刊介绍： The journal mission is to promote scientific achievements in fundamental and applied immunology to various medical fields, the publication of reviews, lectures, essays by leading domestic and foreign experts in the field of fundamental and experimental immunology, clinical immunology, allergology, immunodiagnostics and immunotherapy of infectious, allergy, autoimmune diseases and cancer.