4.8 Article

Trained Immunity Enhances Human Monocyte Function in Aging and Sepsis

Journal

FRONTIERS IN IMMUNOLOGY
Volume 13, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fimmu.2022.872652

Keywords

trained immunity; aging; immunosenescence; innate immunity; monocytes

Categories

Funding

  1. National Institutes of Health (NIH) [R01GM122934, RO1 AI151210, R01GM119197, RO1GM083016, C0RR036551]

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Aging and infection severity are closely related, with age as an independent predictor of mortality in sepsis. Trained immunity can improve immune function in aging and/or sepsis patients, but there is limited data on trained immunity in the aging immune system or in the presence of sepsis. This study found that trained immunity can be induced in aging monocytes and monocytes from sepsis patients, resulting in enhanced metabolic capacity and cytokine production.
Aging plays a critical role in the incidence and severity of infection, with age emerging as an independent predictor of mortality in sepsis. Trained immunity reprograms immunocytes to respond more rapidly and effectively to pathogens and serves as a potential approach to improve immune function in aging and/or sepsis. However, there is very little data on trained immunity in the aging immune system or in the presence of sepsis. We examined the impact of beta-glucan induced innate immune training on monocytes from aging healthy humans (>60 years old) as well as sepsis patients. We observed increased metabolic capacity, upregulated cytokine secretion, increased H3K27 acetylation, and upregulation of crucial intracellular signaling pathways in trained monocytes from healthy aging subjects. The response to trained immunity in healthy aging monocytes was equivalent to the response of monocytes from younger, i.e., 18 - 59 years, individuals. Additionally, we found that trained immunity induced a unique expression pattern of cell surface markers in monocytes that was consistent across age groups. Trained monocytes from sepsis patients also displayed enhanced metabolic capacity and increased cytokine production. These results indicate that immune training can be induced in aging monocytes as well as monocytes from critically ill sepsis patients.

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