key: cord-0037133-ci5wx26t authors: Di Benedetto, Svetlana; Müller, Ludmila title: Aging, Immunity, and Neuroinflammation: The Modulatory Potential of Nutrition date: 2019-07-31 journal: Nutrition and Immunity DOI: 10.1007/978-3-030-16073-9_14 sha: 19e02c46134425487becf1ff1750b38fd8b22bfd doc_id: 37133 cord_uid: ci5wx26t Aging influences an organism’s entire physiology, affecting functions at the molecular, cellular, and systemic levels and increasing susceptibility to many major chronic diseases. The changes in the immune system that accompany human aging are very complex and are generally referred to as immunosenescence. The factors and mechanisms of immunosenescence are multiple and include, among others, defects in the bone marrow, thymic involution, and intrinsic defects in the formation, maturation, homeostasis, and migration of peripheral lymphocytes. Aging affects both the innate and adaptive arms of the immune system. The process of aging is commonly accompanied by low-grade inflammation thought to contribute to neuroinflammation and to many age-related diseases. Numerous attempts to define the role of chronic inflammation in aging have implicated chronic oxidative stress, mitochondrial damage, immunosenescence, epigenetic modifications, and other phenomena. Several lifestyle strategies, such as intervening to provide an adequate diet and physical and mental activity, have been shown to result in improved immune and neuroprotective functions, a decrease in oxidative stress and inflammation, and a potential increase in individual longevity. The studies published thus far describe a critical role for nutrition in maintaining the immune response of the aged, but they also indicate the need for a more in-depth, holistic approach to determining the optimal nutritional and behavioral strategies that would maintain immune and other physiological systems in elderly people. In this chapter, we focus first on the age-related changes of the immune system. Further, we discuss possible deleterious influences of immunosenescence and low-grade inflammation (inflammaging) on neurodegenerative processes in the normally aging brain. Finally, we consider our current understanding of the modulatory potential of nutrition that may mediate anti-inflammatory effects and thus positively affect immunity and the aging brain. It is now clear that a variety of genetic and environmental factors impact upon health in old age, including effects on immunity. However, the relative contribution of these factors to immunosenescence will have to be more accurately established. These variables clearly include nutrition (micro and macro), physical activity, mental well-being, as well as gender and ethnicity, genetic background, psychosocial parameters (including stress), socioeconomic status, earlylife events, and different chronic infections [1, 2] . contributing to immune competence, since undernutrition impairs the immune system, suppressing immune functions that are fundamental to host protection. Undernutrition leading to an impairment of immune function can be due either to insufficient intake of energy and macronutrients or to specific deficiencies in some particular micronutrients, although often these occur in combination [4] . Among other micronutrients, zinc, for instance, has an essential significance to health; its deficiency is responsible for various diseases. Zinc is one of the most important trace elements in the organism, with three major biological roles, as a catalyst, structural, and regulatory ion. It plays a critical role in organism homeostasis, in immune function, in oxidative stress, in apoptosis, and in other physiological activities [2, 5] . Thus, zinc deficiency may adversely affect the immunological status, increase oxidative stress, lead to the generation of inflammatory cytokines, and influence the progression of many chronic diseases, including atherosclerosis, neurological disorders, autoimmune diseases, age-related degenerative diseases, and various malignancies [5] . Zinc deficiency is known to decrease innate immune function. It particularly impairs the lytic activity of natural killer (NK) cells, reduces natural killer T (NKT)-cell cytotoxicity and immune signaling, influences the neuroendocrine-immune pathway, and alters cytokine generation in mast cells [6, 7] . However, excessive amounts of some nutrients may also impair immune function. Overnutrition, combined with an inactive lifestyle and sedentary behavior, promotes the accumulation of visceral fat and leads to obesity. Accumulating evidence indicates that obesity causes chronic low-grade inflammation and the development of systemic metabolic dysfunction that appears to be aetiologically associated with obesity-linked disorders [2, 8] . Adipose tissue acts as a key endocrine organ by releasing bioactive substances, known as adipokines, that may have either pro-or anti-inflammatory activities [9] . The production of pro-inflammatory adipokines, such as tumor necrosis factor (TNF), leptin, retinol-binding protein 4, lipocalin 2, IL-6, IL-18, and angiopoietin-like protein 2, in expanding fat tissue increases, while the concentrations of anti-inflammatory cytokines are reduced [9] . This process is accompanied by an infiltration of adipose tissue with pro-inflammatory mediators and the induction of a low-grade inflammatory state, which is characterized by elevated levels of circulating inflammation markers, such as IL-6, TNF, and C-reactive protein (CRP). Adipose tissue is infiltrated with macrophages in two separate polarization states: M1, which produces pro-inflammatory cytokines, and M2, which produces anti-inflammatory cytokines. Therefore, it has been proposed that in the adipose tissue, a phenotypic switch takes place toward the macrophages of M1-phenotype, promoting the inflammatory state. This low-grade systemic inflammation is known to be associated with the development of atherosclerosis, neurodegeneration, insulin resistance, and the promotion of tumor growth [10] . It was also demonstrated that diet-induced obesity recruits monocytes from the periphery to the brain following herpes simplex virus (HSV)-1 latency in mice [11] , leading to an exaggerated neuroinflammatory response and the promotion of neurodegeneration. While these phenomena are not limited to the elderly, they often tend to be exacerbated in older people who, for one reason or another, exercise less than the young [2] . Thus, many chronic and neurodegenerative diseases can be prevented by changing lifestyle and behavioral habits, particularly dietary habits, and exercise. For example, a positive effect of a 3-month regimen of comprehensive lifestyle changes (plant-based diet, moderate exercise, stress management, and improved social support) on increased telomerase activity was demonstrated in men with low-risk prostate cancer. After a 5-year follow-up, relative telomere lengths of lymphocytes were increased in the lifestyle intervention group and decreased in the control group [12] . According to the findings of another study on more than 23,000 adults, a healthy lifestyle alone lowered the risk of developing chronic diseases with known inflammatory etiology by 78% [13] . Although such changes are thought to be beneficial, more investigations are needed to confirm whether this is really the case, and the full biological implications remain to be determined in large RCTs [2, 14] . Thus, recent studies indicate the need for a more in-depth, holistic approach to determine the optimal nutritional and behavioral strategies that would maintain immune and other physiological systems in the elderly people. Superimposed on chronological age alone, the remodeling of immunity as a result of interactions with the environment over the life course is instrumental in shaping immune status in later life. In addition to interactions with pathogens, host microbiome and nutrition, exercise and stress, and many other extrinsic factors are crucial modulators of this immunosenescence process [2] . In the next sections, we briefly describe the observed agerelated changes in the immune system and then outline the possible contribution of inflammaging and immunosenescence to neuroinflammation and finally discuss the modulatory potential of nutrition and active lifestyle thereon. Human immune aging represents a universal and multifaceted process characterized by progressive immunodeficiency, chronic inflammation, and autoimmunity [15, 16] . The complex regulatory circuits required for maintaining appropriate physiological homeostasis may become compromised with aging [17, 18] . Age-related immune dysfunction (in combination with other mechanisms) may at least in part explain the process of aging itself [19] , as originally proposed by Walford in 1969 [20] . In the course of aging, our immune system undergoes an imprecisely defined process of immunosenescence that affects both adaptive and innate immune systems. The most marked changes in adaptive immunity are decreased numbers of peripheral naïve T cells and the concomitant accumulation of late-stage differentiated memory T cells [18, [21] [22] [23] [24] [25] [26] [27] [28] with reduced antigen receptor repertoire diversity [26, [29] [30] [31] (Figs. 14.1 and 14.2). This phenomenon results from poorly understood age-related impairments in the hematopoietic stem cell (HSC) compartment which generates fewer T-cell precursors in adult and later life, on the one hand, and thymic involution at puberty which markedly reduces the production of mature T cells from their precursors, on the other hand [32] . The HSC compartment (Fig. 14.1 ) is negatively modulated and functionally affected by aging [33] and is increasingly substituted by adipose tissue [18, 34, 35] . Age-related modification within the HSC compartment may be partly due to the "intrinsic cellular aging" of HSCs themselves. Aged HSCs demonstrate more accumulated DNA damage, telomere attrition, and epigenetic deregulation, often in combination with an increase in intracellular reactive oxygen species (ROS) [2, 36] . Such events may also lead to progressive myeloproliferative disorders and the malignant transformation of HSCs. In addition to such "intrinsic" HSC age effects, the extracellular and stromal matrix of the aging bone marrow (which normally nurtures and drives stem cell production) also undergoes dramatic structural changes in terms of the numbers of stromal cells and osteoblasts and reduced production of IL-7 ( Fig. 14.1 ). The aged pool of HSCs is often characterized by a marked shift in lymphoid and myeloid lineage output. Such age-associated myeloid skewing of the differentiation potential, together with decreased homing efficiency, contributes to changes in the cellular composition of the HSC compartment and is believed to be an important contributor to the decline of immune competence in the elderly [2, 37, 38] . Given the age-associated alterations at the level of immune cell production in the bone marrow and the skewing toward myeloid differentiation in the cells exported to the periphery, it is not surprising that immune functioning also changes with age. Not only are fewer B cells produced and fewer T-cell progenitors, but in the case of the latter, their development in the thymus is compromised by the universal process of thymic involution ( Fig. 14.1 ). Although this may be viewed as a developmental event and not truly a senescence effect, it is thought to have dramatic consequences for immunity over the lifespan [18] . Both extrinsic and intrinsic factors are considered ( Fig. 14.1 ) to be involved in causing thymic involution, including the thymic microenvironment as well as the impaired development of aged thymocytes themselves [39] . During this ongoing process, beginning even before puberty, as in the bone marrow, a progressive replacement of lymphoid tissue by fatty tissue takes place, accompanied by a reduction of the active areas of thymopoiesis [40] . Most elderly people do retain some residual thymic function, which may act to provide a continuous low-level input of new naïve T cells (Fig. 14.1 ) to the periphery [41] at least until extreme old age [18] . The end result of thymic involution is that the individual is equipped with a set of naïve T cells early in life, but which are not constantly replaced at the same level throughout life. Thus, elderly people have vanishingly small numbers of naïve T cells and accumulations of memory T cells (Figs. 14.1 and 14.2), mostly specific for the pathogens that they have previously encountered [18] . Aged individuals have decreased protection against newly arising infections as well as difficulties in controlling endogenous persistent viral infections [42] . According to a current paradigm, the age-associated shrinkage of compartment size and diminution in T-and B-cell receptor diversity ( Fig. 14 .1) appears to be responsible for the impaired protective ability of the immune system to respond to a universe of antigens [25, 26, 42] . Particularly, dramatic changes with age are seen in the repertoire diversity that declines dramatically [29, 31] . Lifelong exposure to different pathogens (Figs. 14.1 and 14.2) is regarded as a major driving factor of the phenotypic changes in the distribution of T-cell subsets over the life course. For unclear reasons, especially a latent infection with cytomegalovirus (CMV), but not with any other herpes viruses, with recurrent episodes of reactivation has been found to promote memory T-cell "inflation" and drive T cells to a late stage of differentiation. In aged individuals, oligoclonally expanded CD8 + T cells show an increased expression of late-stage differentiation markers. The accumulation of these highly differentiated T cells, at least some of which may be truly senescent, contributes to the age-associated increased production of pro-inflammatory cytokines and low-grade inflammation and could thus possibly also contribute to age-related morbidity and mortality [24, [43] [44] [45] [46] [47] . Regulatory T cells (Tregs) play a central role in immune regulation ( Fig. 14. 1), providing a delicate balance between protective and patho- The aging immune system. The HSC compartment is negatively modulated and functionally affected by aging (a). Age-related modification within the HSC compartment may be partly due to "intrinsic cellular aging" of HSCs themselves, with accumulated DNA damage, telomere attrition, and epigenetic deregulation. The extracellular and stromal matrix also undergoes dramatic structural changes in terms of the numbers of stromal cells and osteoblasts and the reduced production of IL-7. The aged pool of HSC shows a marked shift in lymphoid and myeloid lineage output. Thymic involution (b) involves both extrinsic and intrinsic factors, including the thymic microenvironment as well as the impaired development of aged thymocytes themselves. A progressive replacement of lymphoid tissue by fatty tissue takes place, accompanied by a reduction of the active areas of thymopoiesis. The end result of thymic involution is vanishingly small numbers of naïve TC and accumulations of memory TC (c), mostly specific for the pathogens that they have previously encountered. Age-affected Tregs (d) can induce chronic inflammation, an increased risk of autoimmunity, but also be responsible for diminished immunity. Elevated inflammatory immune mediators, SARS (e), are responsible for the activation of self-reactive memory BC, producing increased levels of auto-Ab (f), which are frequent in aged individuals as a result of tissue damage and apoptosis. Repetitive antigenic challenges over the lifetime (g) may stimulate pro-inflammatory cytokines, contributing to the maintenance of persistent chronic inflammation. Self-reactive B and T cells (h) recognize a self-antigen and differentiate into memory and effector cells due to a breakdown of the control of autoreactivity. Chronic inflammation additionally resulting in tissue injury and apoptosis attracts DCs, which in elderly people have impaired the ability to take up apoptotic cells (i). Instead, they induce a vicious circle with a further pro-inflammatory response and increased reactivity to self-DNA, which may be more immunogenic in the elderly. Additionally, DAMPs (I), present in proteins released during cell necrosis, promote sterile inflammation. ECM, extracellular matrix; HSC, hematopoietic stem cell; TEC, thymic epithelial cells; ADPC, adipocytes; OB, osteoblasts; DC, dendritic cells; FB, fibroblasts; BM, bone marrow; BC, B cells; TC, T cells; auto-TC, autoreactive T cells; Tregs, regulatory TC; MDSCs, myeloid-derived suppressor cells; ApoptB, apoptotic bodies; DNA, deoxyribonucleic acid; DAMPs, damage-associated molecular patterns; SASP, senescence-associated secretory phenotype; IL, interleukin; Auto-Ab, autoantibodies. (Modified from Müller and Pawelec [18] ) genic immune responses [18] . Early data indicated that younger and older people possessed phenotypically identical Tregs but that suppressive function waned in the latter [48] . More recent data confirm that aging significantly affects the generation, homeostasis, diversity, and functional competence of Tregs. A decline of thymic function disturbs the thymic Treg production and also seems to be compensated for through the peripheral expansion of pre-existing Tregs and/or through the conversion of conventional T cells into Tregs [49] , as had been demonstrated using T-cell clonal culture models much earlier [50] . Thus, due to the leading role of Tregs in immune homeostasis, an age-related deterioration of Tregs ( Fig. 14. 1) might induce either excessive immunity (impacting a chronic inflammation as well as increasing the risk for autoimmunity) or, conversely, an age-related increase of Treg activity might result in failing immunity (raising the risk of malignancies and infectious diseases) in the elderly [49, 51, 52] . As we age, the maintenance of homeostatic conditions may become compromised [18] . The consequence of this imbalance may be that immunity is redirected toward the innate immune responses, characterized by increased levels of systemic inflammatory molecules -a phenomenon dubbed as inflammaging [44] . Large epidemiologic studies commonly report about elevated levels of inflammatory factors such as CRP, IL-6, and TNF in the peripheral blood of elderly people [53] . Elevated inflammatory immune mediators ( Fig. 14.1 ) are thought to be involved in most age-related chronic and neurodegenerative diseases as well as carcinogenesis. Over the life course, inflammatory stimuli from pathogen sources are likely to become increasingly entangled with endogenous stimuli. One possible source of this endogenous "noise" is the senescence-associated secretory phenotype (SASP) characterizing the accumulating "senescent" cells in the elderly that can affect the behavior of neighboring cells [54, 55] . The SASP is a spectrum of pro-inflammatory proteins and cytokines secreted by such cells, which have permanently exited the cell cycle and are known to accumulate in the periphery to significant numbers with advancing age [56, 57] . This process is also associated with the activation of self-reactive memory B cells, producing increased levels of autoantibodies ( Fig. 14.1) , which are frequent in aged individuals as a result of tissue damage and apoptosis [58] . Repetitive antigenic challenges over a lifetime (Figs. 14.1 and 14.2) may stimulate pro-inflammatory cytokines, contributing to the maintenance of persistent chronic inflammation [59] . Such persistent age-related chronic inflammation represents an extreme stress factor for the immune system, causing eventual exhaustion. Autoimmunity is associated with what could be considered premature immune aging, demonstrating the relationship between chronic immune stimulation and progressive immunosenescence [18, 60] . According to the current paradigm, autoimmunity develops when self-reactive B and T cells (Fig. 14.1 ) recognize a self-antigen and differentiate into memory and effector cells due to the breakdown of the control of autoreactivity [15] . It can occur by a selection of T cells with an elevated affinity for self-antigens or latent viruses, which are at the same time also pro-inflammatory. The chronic inflammation additionally resulting in tissue injury and apoptosis attracts dendritic cells (DC), which in elderly people have an impaired ability to take up apoptotic cells (Fig. 14.1) . Instead, they induce a vicious circle with a further pro-inflammatory response and increased reactivity to self-DNA, which may be more immunogenic in the elderly due to increased hypomethylation [16] . Additionally, damageassociated molecular patterns (DAMPs), present on proteins released during cell necrosis and promoting sterile inflammation, also become more frequent with advancing age [17, 18] . It has been suggested that aging is associated with chronic innate immune activation and significant changes in the functions of monocytes and macrophages, which may have implications for increased low-grade chronic inflammation and for the development of age-related diseases [61] . Monocytes are known to be mediators of the inflammatory response and comprise at least three different subsets, namely, classical, intermediate, and nonclassical monocytes. An age-related increase in frequencies of intermediate and nonclassical monocytes has been reported [62, 61] . Our results from the Berlin Aging Study II confirmed these findings, where we also found an age-related increase in frequencies of intermediate and nonclassical monocytes [63] . Together with age-related macrophage activation, inflammatory monocytes contribute to the subclinical chronic inflammatory process [44, 64, 65] . The immune and central nervous systems represent two adaptive physiological systems of the body, which extensively communicate with each other throughout the lifespan. Given the multifaceted interactions between these systems and their tight interdependency, it is to be expected that peripheral immunosenescence and inflammaging contribute to neuroinflammation. Peripheral low-grade inflammation may promote inflammatory processes in the aged brain ( Fig. 14. 2) by modulating glial cells toward a more active pro-inflammatory state, leading to the loss of neuroprotective function, to neuronal dysfunction, and to the accumulation of brain tissue damage [65] [66] [67] . Systemic inflammation may, therefore, increase the risk of developing cognitive impairment, neurological disorders, and neurodegeneration [68] [69] [70] . In the next section, we will have a closer look at how inflammaging may contribute to the process of neuroinflammation during aging. Human aging is characterized by an impairment of cognitive abilities. Although no agreement exists on the basic mechanisms involved in this process, neuroinflammation appears to be the main contributor that links together many factors associated with cognitive aging [65, 71] . As we age, we experience greater susceptibility to memory impairments following an immune challenge that is characterized by an increased and prolonged production of pro-inflammatory cytokines in the otherwise healthy aged brain [65, 72] . It is widely established that both aging and stress can affect the neuroendocrine system, activate the hypothalamic-pituitary-adrenal (HPA) axis to release corticotropin-releasing hormone (CRH) from the paraventricular nucleus of the hypothalamus, and cause the anterior pituitary gland to secrete adrenocorticotropin (ACTH) (Fig. 14.3) . This, in turn, induces the release of glucocorti-coids from the adrenal gland into the circulation [73] . Cortisol affects the immune system in different ways by regulating the expression of cytokines [74] , chemokines, and adhesion molecules and by affecting immune cell migration, maturation, and differentiation [65, 72, 75] . High levels of cortisol can negatively influence hippocampal neurogenesis directly or indirectly through the regulation of the expression of cytokines and their receptors on the brain and immune cells. Recent ultrastructural analyses have uncovered a new player in the age-related remodeling of neuronal circuits, especially at the synapse level, that is rare under homeostatic conditions but becomes abundant during aging, neurodegeneration, and chronic stress [76] . These hyperactive "dark microglia" (Fig. 14. 3) frequently reach into synaptic clefts with their highly ramified and thin processes, extensively encircle axon terminals and dendritic spines, and engulf them [76, 77] . Aging and neurodegeneration are characterized by dysregulated interactions with synapses, resulting in neuronal loss, which, in turn, represents the best pathological correlate of cognitive decline [77] . These conditions can sensitize the aged brain to produce an exaggerated response following exposure to a stressor or to the presence of an immune stimulus in the periphery [78] . Altered microglia profiles together with impairments in key regulatory systems can lead to prolonged neuroinflammation and age-related neurobehavioral complications [65, 79] . On the systemic level, peripheral immunosenescence and inflammaging lead to age-related changes in the blood (Fig. 14. 3) [65] . Chronic exposure to inflammatory mediators may disrupt the endothelial barrier and allow for the transfer of immune cells and numerous pro-inflammatory cytokines into the brain parenchyma that, in turn, can modulate microglial phenotype and reactivity and drive low-grade brain inflammation. Brain cells, such as microglia, astrocytes, and neurons, as well as peripheral immune cells, such as T cells, monocytes, and macrophages, participate in inflammation (Fig. 14.3) . It would provide an inflammatory milieu that is populated by all these resident and additional infiltrating immune cells that participate in a complex inter- Fig. 14.3 The aging brain and neuroinflammation. Aging and stress activate the HPA axis to release CRH from the paraventricular nucleus of the hypothalamus and cause the anterior pituitary gland to secrete ACTH. This, in turn, induces the release of glucocorticoids from the adrenal gland into the circulation. High levels of cortisol can negatively influence hippocampal neurogenesis directly or indirectly through the regulation of an expression of cytokines and their receptors on the brain and immune cells. Peripheral immunosenescence and inflammaging lead to age-related changes in the blood. Chronic exposure to inflammatory mediators may disrupt the endothelial barrier and allow for the transfer of immune cells and numerous pro-inflammatory cytokines into the brain parenchyma that, in turn, can modulate microglial phenotype and reactivity and drive low-grade brain inflammation. Activated microglia and astrocytes change their morphology and function and produce pro-inflammatory cytokines, such as IL-1 β, IL-6, and TNF. Macrophages change their protective M2-phenotype to the pro-inflammatory M1-phenotype, thus contributing to further neuroinflammation. This overproduction of proinflammatory mediators disrupts the delicate balance needed for LTP induction, impairs synaptic plasticity, and reduces the production of BDNF and IGF-1, thus having detrimental consequences for neural precursor cells as well as for the normal neuronal functioning. HPA, hypothalamic-pituitary-adrenal axis; CRH, corticotropin-releasing hormone; ACTH, adrenocorticotropin; IL, interleukin; IFN, interferon; TNF, tumor necrosis factor; LTP, long-term memory potentiation; BDNF, brainderived neurotrophic factor; IGF, insulin-like growth factor. (Modified from Di Benedetto et al. [65] . https:// doi.org/10.1016/j.neubiorev.2017.01.044) play between secreted inflammatory modulators and activated cell surface receptors, such as Tolllike receptors (TLRs) [65] . These receptors are primarily expressed on cells that play central roles in inflammatory response, including macrophages and microglia [80] . Activated microglia and astrocytes change their morphology and function and produce proinflammatory cytokines such as IL-1β, IL-6, and TNF [65] . Recent work suggests that microglia undergo a process of senescence, similar to the one in peripheral immune cells. Senescent and hyperactive microglia have been detected in the aged and diseased brain [81] . The aging brain, in turn, is apparently able to modulate the immune system and to support the recruitment of immune cells from the periphery, thereby contributing further to immunosenescence and neuroinflammation [82] . In addition, macrophages change their protective M2-phenotype to the proinflammatory M1-phenotype, thus contributing to further neuroinflammation [65] . As the aged brain is already "primed" to respond to inflammatory stimuli, additional stress or infection may induce more detrimental changes in the cognitive functioning of aged individuals [78, 83] . Furthermore, the age-related concurrent reduction of anti-inflammatory molecules also contributes to a sensitization to extrinsic and intrinsic stressors. T cells produce less IL-4 and IL-10 and more interferon gamma (IFN-γ), thereby promoting microglial activation. This has detrimental consequences for neural precursor cells, leading to a decrease of neurogenesis (Fig. 14. 3) as well as increased decrements in learning and memory [84, 85] . Taken together, the overproduction of proinflammatory mediators in the periphery may induce a progressive increase in neuroinflammation, characterized by increased glial activation, elevated steady-state levels of inflammatory cytokines, and a decreased production of antiinflammatory molecules, even in neurologically intact aged individuals [65] . In the next section, we consider the modulatory potential of nutrition in its ability, in combination with physical activity, to mediate anti-inflammatory effects and thus positively influence immunity and the aging brain. Evidence that long-term behavioral changes, including nutritional intervention and reduced energy intake together with physical activity, may prevent, improve, or even reverse age-related impairments in immune function continues to accumulate [2] . Lifestyle factors, such as diet and exercise, have been established as playing an important role in immunosenescence, and the practice of "healthy" behavior may minimize the age-associated decline of immune function (Figs. 14.4 and 14.5). Accumulating data strongly suggest that inflammation and oxidative stress are the main inducers of cellular aging (Fig. 14.5) . The cross talk between oxidative stress and inflammation is a complex process, and there are studies reporting that ROS can stimulate inflammation via the activation of inflammasomes and the production of cytokines such as IL-1β and IL-18, which subsequently trigger inflammatory responses [86] . At least in the context of adiposity and inflammation mentioned above, as well as via multiple other postulated physiological effects, caloric restriction (CR) in humans might have beneficial effects in terms of lowering metabolism, a reduction of visceral fat, and weight loss [2] . CR has been shown to delay signs of immunosenescence in animals and is considered today as the only known method to prolong median as well as maximal lifespan in several tested species, from invertebrates to rodents and even including nonhuman primates [32, 87] . Thus, in rodents and nonhuman primates, CR leads to an attenuation of the age-related shift from naïve to memoryphenotype T cells and maintains a higher number of naïve T cells in aged animals [88] . Furthermore, the age-associated rise of pro-inflammatory cytokines, such as IL-6, IFN-γ, and TNF, and the resulting pro-inflammatory state of an aged immune system can be reversed by CR. It has been reported that the age-related decrease in the proliferative capacity of T cells (due to the shift from naïve to memory-phenotype T cells) can be reversed by CR [2, 32] . Nevertheless, there are still many open questions concerning CR, which has been shown to be effective in improving the immune response in unchallenged animals, although it might compromise the host's defense against pathogenic infection and result in higher morbidity and mortality outside the laboratory. Moreover, CR has been shown to delay immunosenescence in animals, but this effect needs to be verified in humans. Furthermore, short-term CR may well be feasible, whereas long-term dietary restriction might have detrimental psychological and other effects in humans, especially in the older population, making its practicality questionable [2, 89, 90] . Nevertheless, the recent results from a multicentered, randomized clinical trial have demonstrated that long-term moderate CR without malnutrition induces a significant and persistent inhibition of inflammation in young and middle-aged healthy nonobese adults without impairing the cell-mediated immunity [91] . The optimization of nutrition may represent one of the first and theoretically easiest and cheapest strategies that can be employed to preserve health during aging [2] . The development of "elderly specific," functional foods, containing probiotics and/or prebiotics, may help in preventing the age-related disruption of the gut environment [92] . In fact, it has been demonstrated that the maintenance of a "healthy" gut microbiota during aging could help to delay or prevent the inflammaging process [93] . Immunostimulatory properties, such as the modulation of cytokine production or adjuvant effects on T-lymphocytes and NK activity, have been demonstrated for various health-promot- ing Lactobacillus and Bifidobacterium strains [94] [95] [96] . It has been shown that 3-and 6-week interventions in elderly people can have positive effects, such as measurable increases of NK cells, tumoricidal activity, and monocyte phagocytic capacity [97] . A probiotic yogurt supplementation tested on elderly persons affected intestinal bacterial overgrowth. This intervention was able to normalize the response to endotoxin and modulate inflammatory markers in blood [98] as well as decrease the incidence of infections in this group of elderly people. Furthermore, a significant increase of phagocytosis, NK-cell activity, and production of IL-10 was also demonstrated following the probiotic supplementation in the elderly as well as the reduced production of the proinflammatory cytokines IL-6, IL-1β, and TNF [92, 99] . Boge et al. showed in two clinical trials that the consumption of a probiotic drink (containing L. casei) by elderly subjects for several weeks before and after an influenza vaccination led to a significant increase in the influenza-specific antibody titer, demonstrating the potential of probiotics in improving the protective efficacy of vaccination in the elderly population, in which it is usually considerably reduced [100, 101] . A seminal advance has been the realization that probiotic supplementation is likely to require "tailor-made" mixtures of different bacteria in order to achieve the desired effect. Atarashi et al. identified 17 strains of bacteria preferentially inducing colonic Tregs which reduced symptoms in models of colitis and allergic diarrhea in mice [102] . Thus, supplementation with tailor-made mixtures of probiotics may be effective in modulating immune responses where the use of single strains is ineffective. This may be one reason why the results of the many human probiotics supplementation trials have often been equivocal since mostly a single strain was used even if it was the "right" strain [2] . The mechanism of action of the mixed bacterial strains is the induction of CD4 + CD25 + FOXP3 + Tregs by bacterial antigens, which in turn stimulate the intestinal epithelial cells to produce TGF-ß1, but not inflammatory IL-6, and TNF. Fecal samples from patients with inflammatory bowel disease and atopy have been reported to contain relatively low amounts of some of the same bacterial strains, suggesting their relevance to human disease as well as in the animal model. In the context of supporting the "right" balance of gut bacteria, reversing our nutritional habits "back to mother nature" might represent an additional solution for the modulation of agerelated inflammatory status and associated chronic and neurodegenerative diseases [2] . The accumulating data from in vitro, animal, and clinical studies provide evidence that a greater consumption of fruits, cereals, vegetables, legumes, and spices is associated with a lower risk of many diseases [103] [104] [105] [106] [107] [108] . Consumption of diets consisting of natural foods can also raise the amounts of plant-based nutraceuticals in the body, such as antioxidants and anti-inflammatory agents. These nutraceuticals are known to cope with free radicals and to modulate the inflammatory signaling pathways in cells, suppressing the onset of age-related chronic conditions [2, 107, [109] [110] [111] . Several studies demonstrate that dietary polyphenols are able to repress inflammation by the inhibition of nuclear factor kappa-light-chain enhancer of activated B-cell (NF-κB) signaling [112] [113] [114] [115] [116] . Remarkably, plant extracts from strawberry, mulberry, and blueberry were shown to contain antioxidants that are able to activate the antioxidant defense system and to counter the deleterious effects of irradiation by reducing oxidative stress and inflammation [117] . A significant decrease in the levels of inflammatory cytokines was demonstrated by the administration of the diet supplements containing pomegranates, figs, or dates [118] . Nutritional intervention including micronutrients and vitamins has also been recognized as a practical, cost-effective approach to attenuate age-associated declines in immune function, vaccination efficiency, and resistance to infectious and neoplastic diseases. The importance of micronutrients, trace elements, and vitamins in proper immune functioning is clear, and deficiencies in one or more of these nutrients may impair practically all forms of immunity [2] . Among them, zinc is an essential element of which the significance to health is indisputable, as discussed above [119] . It has been shown that zinc supplementation enhances the innate immune responses by increasing phagocytosis and T-cell functionality [120] . An increase in serum zinc concentration was associated with an increase in the number of T cells [119] . Zinc supplementation was also able to improve the generation of NK cells from CD34 + cell progenitors through the increased expression of the GATA-3 transcription factor [7] . Vitamin C has also been found to positively modulate immunosenescence and inflammaging, representing two main hallmarks of human aging. Moreover, it has been shown to epigenetically regulate genome integrity and stability, indicating a key role of vitamin C in healthy aging [121] . Vitamin E supplementation has been demonstrated to improve immune responsiveness in healthy elderly individuals by the enhancement of cell-mediated immunity [122] . It was also able to reverse many of the T-cell age-associated defects, including reduced levels of phosphorylation of critical signaling proteins, as well as to improve defective immune synapse formation. Vitamin E also enhances the production of IL-2, the expression of several cell cycle control proteins, and T-cell proliferation [123] . Intake of vitamin E above recommended levels has been shown to enhance T-cell function in aged animals and humans. This effect is believed to contribute to an improved resistance to influenza infection and to a reduced incidence of upper respiratory infections in elderly people [1, 124] . Here, we can provide only a few examples, limited to spices and fruits and their bioactive components, known to modulate different stages of tumorigenesis, including tumor cell survival, proliferation, invasion, and angiogenesis. The anticancer activities of spices are mediated primarily through the suppression of inflammation. Bioactive components of spices, such as eugenol and 6-gingerol, prevent the release of TNF and IL-1β [125] in vitro stimulated macrophages [126] . Curcumin has been shown to suppress the inflammatory mediators NF-κβ and COX-2 [127] , anethole inhibits NF-κβ activation and cytokine production [128] , and cinnamaldehyde blocks the age-related activation of NF-κβ and targets inflammatory COX-2 as well as induces nitric oxide synthase (NOS) [129] . Ursolic acid, which is present in many fruits, including apples, pears, plums, bearberries, loquat, jamun, and rosemary, has been found to exert antitumor activity against colon cancer [130] , breast cancer [131] , nonsmall cell lung cancer [132] , pancreatic cancer [105] , melanoma [133] , multiple myeloma [134] , cervical cancer [135] , and prostate cancer [108] . Also, several other nutraceuticals have been shown to exert antitumor and anti-inflammatory activities. Since oxidative stress and inflammation are two of the major triggers of age-related pathologies and neurodegeneration, the consumption of phytochemicals from fruits, vegetables, herbs, and spices may exert relevant immunomodulatory and anti-inflammatory activities also in the context of the aging brain [86] . Compelling evidence has shown that dietary phytochemicals, particularly polyphenols, have properties that may suppress neuroinflammation and prevent toxic and degenerative effects in the brain. The mechanisms by which polyphenols exert their action are not fully understood, but it is clear that they have a direct effect through their antioxidant activities. They have also been shown to modulate intracellular signaling cascades, including the PI3K-Akt, MAPK, Nrf2, and MEK pathways. Polyphenols also interact with a range of neurotransmitters, illustrating that these compounds can promote their health benefits in the brain through a direct, indirect, or complex action [136] . Approaches with multiple antioxidant nutrients to block the oxidative stress related to the systemic and brain inflammation pathways may, therefore, prevent or delay the cognitive impairments by preventing microglia aging [137] . As a framework of balanced multicomponent diet strategy, adherence to a Mediterranean diet enriched with fruits, vegetables, nuts, and unsaturated fatty acids promotes neuroprotection by decreasing inflammation, restoring cerebral blood flow and volume, inhibiting neurodegeneration, and enhancing neural plasticity by increasing neurogenesis [138] . Flavonoids, plant polyphenolic compounds, which are abundant in fruits and vegetables, exhibit a wide variety of biological effects, including antioxidant, free-radical scavenging, and anti-inflammatory properties. Luteolin, a flavonoid found in high concentrations in celery and green pepper, has been shown to reduce the production of pro-inflammatory mediators and to inhibit the JNK and AP-1 signaling pathway in mice [139] . It was therefore suggested that luteolin may inhibit neuroinflammation and improve cognition in the otherwise healthy aged by constraining brain microglia [140] . Phenolic acids, an important class of polyphenols, are abundantly present in berries, nuts, coffee, tea, and whole grains. They exert their antioxidant and anti-inflammatory activities by the attenuation of microglial activation; the significant inhibition of the production of TNF, IL-6, IL-1β, and NO; and the reduction of mRNA and protein levels of COX-2 and iNOS [141] . Also, retinoids and carotenoids are known as potent antioxidants and anti-inflammatory agents having neuroprotective properties [142] . Sesamol, a phenolic lignan from sesame supplementation, prevents systemic inflammation-induced memory impairment [143] . Recently, much interest has focused on the suggested anti-inflammatory and neuroprotective effects of dietary-derived polyphenols and the long-chain n-3 polyunsaturated fatty acids (PUFA), eicosapentaenoic acid (EPA), and docosahexaenoic acid (DHA), rendering these molecules as potential candidates for use in preventative and therapeutic strategies to reduce the risk of age-related chronic neurodegenerative diseases [144] [145] [146] . Both DHA and EPA can reduce neuroinflammation and cognitive decline. In particular, it has been demonstrated that EPA positively influences mood disorders and DHA maintains normal brain structure [147] . Supplementation with EPA may attenuate neuroinflammation by inhibiting microglial activation and microgliaproduced pro-inflammatory cytokines and by enhancing the expression of astrocyte-produced neurotrophins and their receptors [148] . In general, many studies with animal models support the protective effects of n-3 PUFA supplementation under different conditions. However, studies to demonstrate clear benefits on human subjects toward a particular disease have not been conclusive, probably due to heterogeneous dietary habits and the population being in different demographic conditions. Since many botanical polyphenols can also up-and downregulate the same pathways, future studies may need to include testing for combined effects of DHA and these polyphenols [149] . Thus, more clinical studies are needed to determine the amounts of dietary agents needed to delay aging and agerelated diseases and to investigate their effects on different age groups [107] . Furthermore, when identifying dietary approaches to promote healthy brain aging, a holistic approach should be considered, including nutrition, exercise, and lifestyle factors, which not only target the brain but also overall cardiovascular, immune, and metabolic health [144] . Several interventions, including different types of exercises, have been proposed to restore immune and neural functions in elderly people. Physical exercise and physical activity in later life might target modifiable risk factors of aging, such as low-grade inflammation, inducing immunoprotective and neuroprotective functions (Fig. 14.5) [150, 151] . Numerous studies have revealed the anti-inflammatory and antioxidative effects following physical activity (Figs. 14.4 and 14.5), which potentially exert beneficial effects on neuroplasticity, affect the expression of neurotrophins, and therefore help to maintain normal neuronal functions [152] . Barrientos and colleagues observed an inhibition of neuroinflammation (caused by infection) in rats performing exercises and an increased induction of BDNF mRNA in the brain of otherwise sedentary animals [153] . Further studies with aged mice revealed that wheel running inhibits the proinflammatory state of microglia and their ability to proliferate, thus inducing a pro-neurogenic phenotype [154] . Certainly, the anti-inflammatory effects of exercise are mediated through multidirectional pathways. Some of them are exerted on adipose tissue, skeletal muscles, immune system cells, and the cardiovascular system (Figs. 14.4 and 14.5). These effects include the modulation of anti-inflammatory and pro-inflammatory cytokine profiles, redox-sensitive transcription factors, and antioxidant and prooxidant enzymes and repair proteins [155] . Regular physical activity combined with nutritional interventions can reduce the size of adipocytes and attenuate inflammation in adipose tissue by phenotype switching from pro-inflammatory M1-type to anti-inflammatory M2-type macrophages (Fig. 14.4) . In addition, a reduction in the numbers of circulating pro-inflammatory-type monocytes and an increase in the numbers of Tregs were found in the peripheral blood of individuals following physical activity [156, 157] . Recent evidence suggests that contracting muscles release myokines [2, [158] [159] [160] [161] [162] , which affect the synthesis of BDNF in the dentate gyrus of the hippocampus [162] . Physical activity may have a buffering role on the hormonal stress-responsive systems (Fig. 14.4) , such as the HPA axis and the sympathetic nervous system [163] , thus maintaining immunoprotective and neuroprotective functions. It has been also shown that regular exercise is associated with an improved immune responsiveness to influenza vaccination in older adults. The exercise-related increase in the antibody titer, T-cell function, macrophage response, improvement of the Th1/Th2 cytokine balance, the level of pro-inflammatory cytokines, and changes in naive/ memory cell ratio have also been reported [164] . Taken together, one might conclude that nutritional intervention in combination with physical activity activates and/or modulates the release of hormones, myokines, and cytokines as well as modulate the expression of various immune-reactive molecules, which all contribute to anti-inflammatory effects and the possible attenuation of immunosenescence and neuroinflammation. Around the world, especially in many European countries, the older segment of the adult population is growing in size and proportion [165] . In dealing with this demographic change, what people make of the added years of their lives will be the most important aspect but will only be advantageous to the individual and to society at large if people can remain active participants in daily life and work [65] . Maintaining immunological and cognitive functions will be paramount, but their performances are known to decrease with increasing age, even in overtly healthy individuals. Preventing and/or attenuating immunosenescence and inflammation and delaying cognitive decline are probably the most effective measures for postponing the point of time at which individuals are no longer able to lead an independent life [65] . Effective pharmacological treatments, especially for cognitive but also for the immune decline, remain unavailable. Therefore, we will need a more holistic view of the aging process, where the dynamics of the interaction between environment, intestinal microbiota, and host must be taken into consideration. We should also take into account the age-associated physiological changes in the gastrointestinal tract as well as age-related modifications in lifestyle, nutritional behavior, and impaired functionality in the immune system of the elderly population [2, 65] . Some modifiable lifestyle factors, such as poor diet and physical and cognitive inactivity, have been identified as being associated with an increased risk of cognitive and immune decline [166] . Encouragingly, exercise can have a protective effect, even if initiated in advanced old age [2, 65, 167] . The intake of antioxidant nutrients reduces both systemic inflammation and neuroinflammation during aging [168] . Due to the fact that diet component targets are different, combining different nutrients acting on convergent antiinflammatory pathways may result in an increased anti-inflammatory efficacy [144, 169, 170] . In this chapter, we have described the potential basic processes underlying age-related decline, namely, immunosenescence and a progressive increase in neuroinflammation characterized by an increased glial activation, elevated steady-state levels of inflammatory cytokines, and a decreased production of neurotrophic molecules as well as potential positive effects of nutrition and physical exercise. It is our hypothesis, as partly summarized here, that a judicious combination of dietary interventions and exercise, cognitive training, and a pharmacological manipulation of immunosenescence and inflammatory processes will eventually deliver an optimal individualized regime for the maintenance of the best possible immune and cognitive functions over the lifespan of every individual. 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