Department of Microbiology and Physiological Systems, University of Massachusetts Chan Medical Schoolgrid.168645.8, Worcester, Massachusetts, USA.
Immunology and Microbiology Program, Graduate School of Biomedical Science, University of Massachusetts Chan Medical Schoolgrid.168645.8, Worcester, Massachusetts, USA.
mBio. 2022 Dec 20;13(6):e0302022. doi: 10.1128/mbio.03020-22. Epub 2022 Nov 21.
The cytotoxic granules of human NK and CD8 T cells contain the effector molecule granulysin. Although studies indicate that granulysin is bactericidal to Mycobacterium tuberculosis and human CD8 T cells restrict intracellular M. tuberculosis by granule exocytosis, the role of granulysin in cell-mediated immunity against infection is incompletely understood, in part because a granulysin gene ortholog is absent in mice. Transgenic mice that express human granulysin (GNLY-Tg) under the control of human regulatory DNA sequences permit the study of granulysin . We assessed whether granulysin expression by murine CD8 T cells enhances their control of M. tuberculosis infection. GNLY-Tg mice did not control pulmonary M. tuberculosis infection better than non-Tg control mice, and purified GNLY-Tg and non-Tg CD8 T cells had a similar ability to transfer protection to T cell deficient mice. Lung CD8 T cells from infected control and GNLY-transgenic mice similarly controlled intracellular M. tuberculosis growth in macrophages . Importantly, after M. tuberculosis infection of GNLY-Tg mice, granulysin was detected in NK cells but not in CD8 T cells. Only after prolonged stimulation could granulysin expression be detected in antigen-specific CD8 T cells. GNLY-Tg mice are an imperfect model to determine whether granulysin expression by CD8 T cells enhances immunity against M. tuberculosis. Better models expressing granulysin are needed to explore the role of this antimicrobial effector molecule . Human CD8 T cells express the antimicrobial peptide granulysin in their cytotoxic granules, and analysis suggest that it restricts growth of Mycobacterium tuberculosis and other intracellular pathogens. The murine model of tuberculosis cannot assess granulysin's role , as rodents lack the granulysin gene. A long-held hypothesis is that murine CD8 T cells inefficiently control M. tuberculosis infection because they lack granulysin. We used human granulysin transgenic (GNLY-Tg) mice to test this hypothesis. GNLY-Tg mice did not differ in their susceptibility to tuberculosis. However, granulysin expression by pulmonary CD8 T cells could not be detected after M. tuberculosis infection. As the pattern of granulysin expression in human CD8 T cells and GNLY-Tg mice seem to differ, GNLY-Tg mice are an imperfect model to study the role of granulysin. An improved model is needed to answer the importance of granulysin expression by CD8 T cells in different diseases.
人 NK 和 CD8 T 细胞的细胞毒性颗粒含有效应分子颗粒酶。虽然研究表明颗粒酶对结核分枝杆菌具有杀菌作用,并且人类 CD8 T 细胞通过颗粒外排来限制分枝杆菌的胞内生长,但颗粒酶在细胞介导的抗感染免疫中的作用尚未完全了解,部分原因是小鼠中缺乏颗粒酶基因的同源物。在人类调控 DNA 序列的控制下表达人颗粒酶的转基因小鼠(GNLY-Tg)允许研究颗粒酶。我们评估了鼠 CD8 T 细胞表达颗粒酶是否增强了它们对结核分枝杆菌感染的控制。与非 Tg 对照小鼠相比,GNLY-Tg 小鼠并未更好地控制肺部结核分枝杆菌感染,并且纯化的 GNLY-Tg 和非 Tg CD8 T 细胞具有向 T 细胞缺陷小鼠转移保护的相似能力。感染对照和 GNLY 转基因小鼠的肺 CD8 T 细胞同样控制了巨噬细胞内结核分枝杆菌的生长。重要的是,在 GNLY-Tg 小鼠感染结核分枝杆菌后,NK 细胞中检测到颗粒酶,但在 CD8 T 细胞中未检测到。只有在长期刺激后,才能在抗原特异性 CD8 T 细胞中检测到颗粒酶表达。GNLY-Tg 小鼠不是确定 CD8 T 细胞表达颗粒酶是否增强对结核分枝杆菌免疫力的理想模型。需要更好地表达颗粒酶的模型来探索这种抗菌效应分子的作用。人 CD8 T 细胞在其细胞毒性颗粒中表达抗菌肽颗粒酶,分析表明它限制了结核分枝杆菌和其他胞内病原体的生长。由于啮齿动物缺乏颗粒酶基因,因此结核分枝杆菌的小鼠模型无法评估颗粒酶的作用。一个长期存在的假设是,由于缺乏颗粒酶,鼠 CD8 T 细胞不能有效地控制结核分枝杆菌感染。我们使用人颗粒酶转基因(GNLY-Tg)小鼠来测试这一假设。GNLY-Tg 小鼠在对结核病的易感性方面没有差异。然而,在结核分枝杆菌感染后,不能检测到肺部 CD8 T 细胞中的颗粒酶表达。由于人 CD8 T 细胞和 GNLY-Tg 小鼠中颗粒酶表达的模式似乎不同,因此 GNLY-Tg 小鼠是研究颗粒酶作用的不完美模型。需要一种改进的模型来回答 CD8 T 细胞表达颗粒酶在不同疾病中的重要性。
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