Immune system modulation in aging: Molecular mechanisms and therapeutic targets

The worldwide population is suffering an accelerated growth of old people, bringing formidable healthcare and socioeconomic challenges. From a biological perspective, aging is a complex and multisystemic process that adversely impacts on the organism function, with the nervous, endocrine, hematopoietic, and immune systems being the most affected by this process. Specifically, aging elicits a decline in the immune system, affecting both the innate and adaptive immunity responses (immunosenescence), which result in increased vulnerability to toxins and pathogens and the establishment of a chronic inflammation state (inflammaging). An in-depth study of the immune system has regained relevance due to the public health emergency caused by the coronavirus disease 2019 (COVID-19) pandemic, which preferentially affects older individuals. In this scenario, the present review is focused on the mechanism underlying both immunosenescence and inflammaging, providing also a description of current therapeutic strategies aimed to ameliorate the impact of aging/senescence on immunity.

The term “immunosenescence” comprises several humoral and cellular events that generate age-related dysfunction of the immune system (1). This condition is associated with a higher risk of developing different aged-related pathologies, including infections, cardiovascular and neurodegenerative diseases, autoimmunity, and cancer (2). The main determinants of immunosenescence include genetics, nutrition, sex, race, exercise, and pathogen exposure (2, 3). To better understand immunosenescence, it is necessary to consider the age-driven physiological changes that are related to immunity. Body physical barriers are the first line of defense against pathogens, and in elderly people, the skin becomes thinner and drier, which in turn reduces the amount of fat-soluble defensins. Likewise, the mucosal barrier loses efficiency during aging because the ciliary function is impaired, which consequently facilitates pathogen settlement (4). With respect to the cellular events that underlie immunosenescence, thymic involution, decreased number of T and B lymphocyte cells, impaired telomerase activity, increase of inflammatory mediators, and a weak immune response to vaccination have been consistently observed in aging (5–9). It is worthy to mention that these deficiencies are worsened by exposure to pathogens (2, 3). Furthermore, alterations in the innate immune cells (neutrophils, macrophages, natural killers, dendritic, and mast cells) have been found in aged individuals (Figure 1A). Neutrophils display diminished killing capacity, even though their production in the bone marrow remains unchanged and their number in blood is even slightly higher in aging (10). Similarly, the function of natural killer cells is disturbed in aging, although their turnover in the bone marrow diminishes and their baseline number increases (11). Macrophages and dendritic cells show similar phagocytic activity between young and old people; however, both the total number of these cells in peripheral blood and their ability to present antigens and stimulate T cells are defective in elderly people (12, 13). In addition, macrophages show increased inflammatory response (14). Finally, the activation and function of mast cells are altered in aged individuals (15). On the other hand, the repertoire of naïve T and memory B lymphocytes is abundant during childhood, whereas in old age, a decline in B-cell production in the bone marrow (16) and a reduction in the number of T lymphocytes due to thymic involution occurs (13, 17). Altogether, these events result in an overall reduction of immunity in older individuals (18).

Inflammaging is defined as a systemic proinflammatory state caused by an imbalance between pro- and anti-inflammatory mechanisms, which provokes in turn increased cytokine production (19). This imbalance elicits a prolonged state of low-grade inflammation (19) characterized by augmented levels of pro-inflammatory mediators, including IL-1β, IL-6, TNF-α, IL-8, and CRP (1) (Figure 1B). This phenomenon is a hallmark of aging and is even considered a biomarker of accelerated aging (20). Inflammaging is modulated by multitude interrelated processes; at the physiological level, some relevant factors that can promote inflammaging include physical inactivity, obesity, psychological stress, early life adversity, exposure to xenobiotics, and chronic infections (1, 21). Inflammaging is also considered as a risk factor for several pathologies, including cardiovascular, kidney, and neurodegenerative diseases, type 2 diabetes mellitus, cancer, depression, sarcopenia frailty and infectious diseases (20, 22). Furthermore, several studies correlate inflammaging with the susceptibility of older people to develop COVID-19 with severe complications (1, 23), due to a hyperreactive response to the infectious agent through a massive release of chemical mediators (20, 24, 25). Inflammaging has been recently regarded as an adaptive process that can lead either to healthy aging or to a pathological state, depending on genetic and environmental conditions and lifestyle factors (1, 19, 22). This idea has been reinforced by studies on centenarian populations, in which high levels of inflammatory biomarkers were found to favor longevity via their interaction with anti-inflammatory molecules (26, 27). Inflammaging is a dynamic and complex process driven by several age-related molecular mechanisms, rather than having an exclusive connection with the immune system (22). For instance, oxidative stress induces age-related transcriptional changes in genes encoding key components of inflammatory pathways (19). Specifically, the pro-inflammatory secretome of senescent cells can exert paracrine effects on nearby tissues extending the inflammatory state at the organismal level (19). Finally, dysregulation of the microbiome is another important contributor to inflammaging (21). It is believed that amelioration of age-related dysbiosis by probiotic clinical intervention might in turn alleviate inflammaging (14).

Chronic infections are a major health problem that affects millions of people worldwide. The innate immune system of aged people loses the ability to respond to viral infections; it initiates a local inflammatory response but fails to eliminate the virally infected cells (28, 29). Chronic infections trigger persistent adaptive immune responses that generate a pro-inflammatory environment. As this state persists, different alterations emerge, such as downregulation of immune responses, which further aggravates the inflammatory response (28, 29) (Figure 1C). This unresponsive immune system, also called immunosenescence, exacerbates the inflammatory response, due to accumulation of inefficient adaptive immune cells, which ultimately causes a physiological decline (30).

Changes in the immune system that occur during aging have just started to be understood. The intricate interplay between inflammaging and immunosenescence requires to be deciphered, in order to develop therapeutic interventions aimed to improve/rejuvenate the immune system. In this section, the most relevant proteins/pathways and immune system cells that modulate the host immune response during aging are described.

During aging, the immune system declines due to dysregulation and overactivation of its innate and adaptive responses, leading to the onset of inflammation-related chronic diseases highly observed in elderly people (72). For that reason, several pharmacological and cellular/genetic strategies have been developed to slow down or reverse the deleterious effects of immunosenescence on health (73): (a) Induced pluripotent stem cells (iPSC) have been employed to generate hematopoietic cells and/or various specific immune cells; (b) administration of cytokine and growth factor cocktails boosted macrophage function; (c) bone marrow transplantation is a widely used therapy for thymus regeneration (74) (Figure 1E); (d) the use of Cdc42 and BATF inhibitors or antioxidants enhances the number and function of lymphoid-biased hematopoietic stem cells (75, 76); (e) inhibition of dual specific phosphatases 4 boosts memory CD4+ T-cell function (77, 78); (f) administration of fibroblast growth factor 7 (FGF7) stimulates naive T-cell production and promotes the removal of dysfunctional cells, thereby restoring thymus function (79, 80); and (g) administration of rapamycin improves CD8+ T-cell function (81, 82) (Figure 1). Finally, a relevant non-pharmacological strategy that has been proven to enhance immunity is caloric restriction; it delays the accumulation of senescent T cells and stimulates thymopoiesis through the activation of IGF-1 and/or PPAR pathways (83, 84). On the other hand, recent studies have unveiled the relevance of functional foods to ameliorate oxidative stress and inflammation and to improve the metabolism of lipids associated with metabolic diseases, via Nrf2 and/or NF-κB signaling pathways (85, 86).

Some of the molecules/pathways that modulate immunosenescence have therapeutic potential. Owing to the crucial role of the activator protein 1 (AP-1) signaling pathway in macrophage-mediated inflammation, targeting of AP-1 has been approached to attenuate inflammation. Transfection of lentiviral siRNA against AP-1 in mice fed with high-fat diet resulted in the alleviation of systemic and hepatic inflammation (87). Interestingly, the use of rosiglitazone, a PPARγ agonist, was found to exert a positive effect on animals with sepsis, decreasing cell death and cardiac inflammation; furthermore, increased fatty acid oxidation and improved insulin resistance were also observed in human skeletal muscle (88). Since aging is a very complex process that involves different biological processes, therapies aimed to modulate inflammaging have to be focused on the synergic effect of more than one compound, to regulate simultaneously different pathways. For instance, a combinatory treatment using three different compounds, rapamycin, acarbose, and 17α-estradiol, converge on the regulation of both ERK1/2 and p38-MAPK pathways (89).

Inflammation is a key factor for the onset and progression of almost all chronic diseases affecting aged individuals, with immunosenescence and inflammaging being two relevant phenomena that modulate the immune system during aging. Therefore, identification and characterization of the molecular and cellular mechanisms underlying the immune system dysfunction will surely help to develop effective therapeutic strategies to prevent the negative outcomes of infectious diseases on aged individuals. Recent scientific evidence indicates that different immune system cells, including hematopoietic stem cells, T cells, B cells, NK cells, thymocytes, macrophages, microglia, granulocytes, and dendritic cells, are suitable targets for cellular and genetic therapies. An effective therapy must combine in a balanced manner immunostimulatory and immunosuppressive strategies, toward a reasonable immune rejuvenation. Given the intricate network of the molecular events involved in the regulation of inflammation/immunosenescence, the therapeutic approaches described herein are focused on the improvement of the immune system in aged individuals rather than longevity.

BC, GL-G, and JM conceptualized the work. BC, IG-A, JU, IA-C, OG-M, JD-L, AT-G, GL-G, and JM wrote the draft manuscript. JU, IG-A, IA-C, OG-M, JD-L and AT-G designed the figure. BC, IA-C, GL-G and JM supervised and edited the final version of manuscript. BC, GL-G and JM obtained funding. All authors contributed to the final version of manuscript and approved the submitted version.

This work was supported by grants from CONACyT CF2019-514879 to BC and 258043 to JM.

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

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