期刊
VACCINES
卷 10, 期 11, 页码 -出版社
MDPI
DOI: 10.3390/vaccines10111892
关键词
tuberculosis; ageing; infection; mycobacterium tuberculosis; immune; mTOR; autophagy; mitophagy; susceptibility
资金
- NIH
- [RHL143545-01A1]
Several reports suggest that ageing negatively affects the human immune system and increases susceptibility to infections like Mycobacterium tuberculosis (M. tb). This article explores how ageing decreases T-cell immune response, reduces glutathione production, over activates the mTORC1 pathway, inhibits autophagy and mitophagy, and alters protective genes/transcription factors. It also highlights a potential defect in antigen presenting by dendritic cells and the role of inflammaging in increasing susceptibility to M. tb infection. Possible preventative strategies, such as immunomodulators and antioxidant supplementation, are proposed.
Several reports have suggested that ageing negatively affects the human body resulting in the alteration of various parameters important for sufficient immune health. Although, the breakdown of innate and adaptive immunity has been hypothesized to increase an individual's susceptibility to infections including Mycobacterium tuberculosis (M. tb), little research has been done to bridge this gap and understand the pathophysiology underlying how ageing increases the pathogenesis of M. tb infection. Our objective was to study research from a plethora of resources to better understand the pathogenesis of ageing and its link to the human immune system. To achieve this goal, this article explores how ageing decreases the collective T-cell immune response, reduces glutathione (GSH) production, over activates the mammalian target of rapamycin (mTORC1) pathway, inhibits autophagy and mitophagy, and alters various protective genes/transcription factors. Specifically highlighting how each of these pathways cripple an individual's immune system and increases their susceptibility from M. tb infection. Furthermore, research summarized in this article gives rise to an additional mechanism of susceptibility to M. tb infection which includes a potential defect in antigen presenting by dendritic cells rather than the T-cells response. Inflammaging has also been shown to play a role in the ageing of the immune system and can also potentially be a driving factor for increased susceptibility to M. tb infection in the elderly. In addition, this article features possible preventative strategies that could decrease infections like M. tb in this population. These strategies would need to be further explored and range from immunomodulators, like Everolimus to antioxidant supplementation through GSH intake. We have also proposed the need to research these therapies in conjunction with the administration of the BCG vaccine, especially in endemic populations, to better understand the risk contracting M. tb infection as well as ways to prevent infection in the first place.
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