Late-life Attenuation of Cytomegalovirus-mediated CD8 T Cell Memory Inflation: Shrinking of the Cytomegalovirus Latency Niche.

IF 3.6 3区 医学 Q2 IMMUNOLOGY
Christopher P Coplen, Sandip Ashok Sonar, Janko Ž Nikolich
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Abstract

CMV drives the accumulation of virus-specific, highly differentiated CD8 memory T cells (memory inflation [MI]). In mice, MI was shown to directly correlate with the CMV infection dose, yet the CMV-associated CD8 MI plateaus over time. It is unclear how MI is regulated with aging. We infected young mice with 102, 104, and 106 PFU of murine CMV and confirmed that MI magnitude was directly proportional to the infectious dose, reaching a setpoint by midlife. By old age, MI subsided, most prominently in mice infected with 106 PFU, and reached statistical parity between groups in 26-mo-old mice. This corresponded to an age-related loss in lymphatic endothelial cells in lymph nodes, recently shown to be sufficient to drive MI in mice. We propose that MI size and persistence over the lifespan is controlled by the size of the lymphatic endothelial cell niche, whose shrinking leads to reduced MI with aging.

晚期巨细胞病毒介导的 CD8 T 细胞记忆性炎症衰减:巨细胞病毒潜伏龛缩小。
CMV 可促使病毒特异性、高度分化的 CD8 记忆 T 细胞(记忆膨胀 [MI])积累。在小鼠中,MI 与 CMV 感染剂量直接相关,但随着时间的推移,CMV 相关的 CD8 记忆 T 细胞的 MI 会趋于平稳。目前还不清楚随着年龄的增长,MI 是如何调节的。我们用 102、104 和 106 PFU 的小鼠 CMV 感染了年轻的小鼠,结果证实,MI 的大小与感染剂量成正比,到中年时达到一个设定点。到了老年,MI 有所减弱,在感染了 106 PFU 的小鼠中最为明显,在 26 个月大的小鼠中,各组之间达到了统计学上的均等。这与淋巴结中与年龄相关的淋巴内皮细胞的损失相对应,最近的研究表明,淋巴内皮细胞的损失足以驱动小鼠的MI。我们认为,MI 的大小和持续时间受淋巴内皮细胞生态位大小的控制,而淋巴内皮细胞生态位的萎缩会导致 MI 随年龄增长而减少。
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来源期刊
Journal of immunology
Journal of immunology 医学-免疫学
CiteScore
8.20
自引率
2.30%
发文量
495
审稿时长
1 months
期刊介绍: The JI publishes novel, peer-reviewed findings in all areas of experimental immunology, including innate and adaptive immunity, inflammation, host defense, clinical immunology, autoimmunity and more. Special sections include Cutting Edge articles, Brief Reviews and Pillars of Immunology. The JI is published by The American Association of Immunologists (AAI)
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