Alzheimer’s disease

A substantial proportion of large-scale, double-blind RCT have focused on slowing cognitive decline in those afflicted with AD or another dementia, with the results being largely disappointing (for a review, see Otaegui-Arrazola et al. ⁽Reference Otaegui-Arrazola, Amiano and Elbusto²⁸⁾). For instance, trials investigating the efficacy of B vitamins or n-3 fatty acids in mild-to-moderate AD patients found no beneficial effect of these compounds on slowing disease progression, despite ample evidence from non-RCT studies suggesting a role for these nutrients in cognition late in life⁽Reference Aisen, Schneider and Sano^16, Reference Kwok, Lee and Law^19, Reference Quinn, Raman and Thomas^22, Reference Sun, Lu and Chien^23, Reference Freund-Levi, Eriksdotter-Jönhagen and Cederholm²⁹⁾. One possible reason for the preponderance of null results in clinical trials with AD patients is that it may be too late to intervene nutritionally when AD becomes clinically apparent. It is widely appreciated that before even the earliest symptoms of AD becoming manifest, pathological changes are occurring in the brain which give rise to ‘preclinical AD’ and ‘MCI’. Thus, the disease process of AD certainly begins years, if not decades, before the emergence of the clinical syndrome of AD⁽Reference Sperling, Aisen and Beckett³⁰⁾. During the preclinical AD and MCI phases, pathology in the form of amyloid-β and hyperphosphorylated tau proteins accumulates in the brain, followed by synaptic dysfunction and neuronal injury and loss⁽Reference Sperling, Aisen and Beckett^30, Reference Jack, Knopman and Jagust³¹⁾. These processes must occur in sufficient magnitude for the development of any clinically relevant cognitive abnormalities. By the time notable cognitive change that is indicative of the mildest stage of AD begins to occur, considerable deleterious changes in the brain have taken place. In two of the studies above, the mean Mini-Mental State Examination (MMSE) score of the participants was approximately 21 out of 30, such that the average participant in these trials was just outside of the moderate stage of AD; by the time the disease has reached this stage, substantial brain damage has occurred. (The MMSE is a global cognitive screening tool for dementia on a scale of 0–30. Generally, scores of 21–25 are indicative of mild AD, 11–20 moderate AD, and 0–10 severe AD⁽Reference Perneczky, Wagenpfeil and Komossa³²⁾. However, individuals with scores above 25 can still be diagnosed with AD, especially in the earliest stages of the disorder.)

Given the years- to decades-long head start of AD, implementing a nutritional intervention at the mild-to-moderate stages of AD in order to affect cognition seems unlikely to succeed. Furthermore, when considering the notion that pharmaceutical approaches such as acetylcholinesterase inhibitors offer only palliative effects⁽Reference Aisen, Cummings and Schneider³³⁾, it is perhaps unsurprising that single-nutrient interventions tend to fail in this population. Therefore, in order to offer a role for nutrition to modify cognition in older adults, researchers must focus on areas of the ageing spectrum where brain function is less impaired. Supporting this notion, Freund-Levi et al. ⁽Reference Freund-Levi, Eriksdotter-Jönhagen and Cederholm²⁹⁾ evaluated a range of AD patients with MMSE scores from 15 to 30. Across the full spectrum of patients, they found no effect of n-3 fatty acids on the rate of cognitive decline over 12 months. However, when selectively looking at the most mildly affected patients (MMSE≥28), n-3 fatty acid supplementation attenuated cognitive decline in this small sample⁽Reference Freund-Levi, Eriksdotter-Jönhagen and Cederholm²⁹⁾. The fact that Freund-Levi et al. ⁽Reference Freund-Levi, Eriksdotter-Jönhagen and Cederholm²⁹⁾ found a positive effect of n-3 fatty acids in patients with MMSE scores between 28 and 30, which more likely reflects a cognitive state akin to MCI rather than AD, underscores the notion that initiating a nutritional intervention before the onset of dementia is more likely to influence cognition in late life. Nonetheless, two other studies that supplemented n-3 fatty acids to participants in the same MMSE range did not see beneficial cognitive effects⁽Reference Dangour, Allen and Elbourne^17, Reference Van de Rest, Geleijnse and Kok²⁴⁾, furthering the complexity of this area.

Mild cognitive impairment

Individuals with a diagnosis of MCI display heterogeneous cognitive impairments that are exacerbated for their age. However, these decrements in cognition have not progressed to the level observed in AD or other dementias. Importantly though, the clinical development of MCI symptoms is preceded by a protracted period of brain damage⁽Reference Sperling, Aisen and Beckett³⁰⁾ occurring in the medial temporal lobe (including the hippocampus) as well as portions of the prefrontal cortex (PFC) and parietal lobe. Therefore, these underlying pathological changes that have developed may make successful nutritional intervention at this stage difficult.

There have been some studies indicative of a cognitive benefit via nutritional supplementation in MCI populations. For instance, cognitive impairment was attenuated in an MCI population with elevated homocysteine levels when receiving B vitamin supplementation (vitamins B₆, B₁₂, folic acid) relative to the control group⁽Reference De Jager, Oulhaj and Jacoby³⁴⁾. The focus on homocysteine reduction directly addresses previous findings linking high levels of this compound to dementia and white matter damage in the elderly⁽Reference Dufouil, Alpérovitch and Ducros^35, Reference Seshadri, Beiser and Selhub³⁶⁾. Further, a few smaller-scale studies have observed an improvement in cognition when providing n-3 fatty acid supplementation to those with MCI⁽Reference Chiu, Su and Cheng^37–Reference Lee, Shahar and Chin³⁹⁾, and it will be important for larger trials to replicate these beneficial effects.

Despite these successes, not all vitamin trials in MCI patients report positive results, as van Uffelen et al. ⁽Reference Van Uffelen, Chinapaw and van Mechelen⁴⁰⁾ did not find an improvement following vitamin B supplementation. One possibility explaining these opposing findings concerns dosage, as vitamin B₁₂ and folic acid/folate in too high of a dose may actually worsen cognitive outcomes⁽Reference Eussen, de Groot and Joosten^41–Reference Morris, Evans and Schneider⁴³⁾. Similarly administration (in supplement form) of the antioxidant vitamin E in a double-blind RCT in MCI patients did not reduce the rate at which these participants converted to AD⁽Reference Petersen, Thomas and Grundman²¹⁾. These results seem at odds with prospective cohort investigations indicating a protective role of dietary vitamin E intake and cognitive ageing⁽Reference Engelhart, Geerlings and Ruitenberg^44, Reference Morris, Evans and Bienias⁴⁵⁾.

One explanation for these mixed results may be revealed by an investigation of the changes occurring in the brain that give rise to MCI. Similar to AD but on a lesser scale, in order for the clinical symptoms of MCI to become apparent (at least when due to an AD-like aetiology), substantial brain pathology, along with synapse and neuron dysfunction or loss, must accumulate in a ‘preclinical phase’, which typically occurs on a timescale of years⁽Reference Sperling, Aisen and Beckett³⁰⁾. Thus, any nutritional intervention initiated when MCI is clinically apparent faces a disease process with a years-long head start, thereby decreasing the likelihood of success. It is clear from some of the above studies that this head start is not insurmountable (perhaps unlike AD), but including these patients in RCT investigating nutrition and cognitive ageing may mask the beneficial effects of certain nutrients (for example, vitamin E) on brain health, as the nutrient cannot fully or successfully act on the brain in this diminished state. Moreover, while any intervention that can prevent patients from converting to dementia from MCI is highly valuable, when considering quality-of-life issues and overall public health, it would be even more valuable to find approaches that reduce the risk of a healthy older adult from developing MCI. Though not as impaired as an AD patient, the patient with MCI may lose his/her ability to work or drive, and he/she also faces an increased risk of developing AD. Therefore, identifying roles for nutrition in cognitive ageing that can lower the risk of developing MCI or AD, rather than attempting to use nutrition to treat these disorders outright, is of paramount importance. By focusing efforts on healthy older adults (and even in middle-aged populations), it may be possible to further achieve this goal.

Healthy older adults

Healthy older adults without a diagnosis of AD or MCI do not have an objective cognitive impairment for their age, as measured by current neuropsychological tests. Importantly, this does not indicate that they are operating at the same cognitive level as someone 40 years their junior. Ageing research demonstrates that healthy older adults exhibit decline in several areas of cognition relative to younger adults, including episodic and working memory, as well as processing speed. Interestingly, some cognitive aspects, such as semantic knowledge, stay the same or even improve with age⁽Reference Park, Lautenschlager and Hedden⁴⁶⁾. Furthermore, advancing age is a major risk factor for the development of MCI or AD, so a healthy older adult at age 70 years may still develop MCI or AD by the age of 75 years. Therefore, despite normal cognition for his/her age, any given healthy older adult still has: (a) room for improvement in certain cognitive domains; and (b) an increasing risk of objective cognitive impairment stemming from MCI, AD or another dementia as he/she increases in age. By intervening to address these two related points, nutrition has great potential to maintain or improve healthy cognitive ageing; however, the research to date paints a murky picture as to whether nutrition has a role in cognition and brain health for healthy older adults.

The tension between prospective longitudinal and epidemiological studies on the one hand, and RCT on the other, is perhaps greatest when considering the available data from healthy older adults. Though not without controversy, numerous prospective longitudinal and epidemiological studies indicate that dietary intake of n-3 fatty acids, various vitamins, flavonoids and/or adherence to a Mediterranean-type diet reduces AD risk and/or improves cognition (for a review, see Otaegui-Arrazola et al. ⁽Reference Otaegui-Arrazola, Amiano and Elbusto²⁸⁾). Despite this, the preponderance of data from nutritional RCT in healthy older adults tilts towards these nutrients not having a modulatory effect in cognitive ageing.

With regard to RCT indicating positive effects, an enhancement for memory was observed in healthy older adult males undergoing long-term β-carotene supplementation⁽Reference Grodstein, Kang and Glynn⁴⁷⁾. Another report assessed the effect of 24 weeks of DHA administration in older adults who were free of dementia or MCI, but had subjective complaints about their memory. In this population, there was an improvement in memory for the DHA group compared with those receiving the placebo⁽Reference Yurko-Mauro, McCarthy and Rom⁴⁸⁾. Also, a study investigating 3-year folic acid supplementation in participants aged 50–70 years with elevated (>13 µmol/l) homocysteine levels found that the folic acid group had better scores on memory and information processing speed tasks relative to the placebo group⁽Reference Durga, van Boxtel and Schouten⁴⁹⁾. This study had some unique characteristics that may shed light on the proper population and length of time necessary for a nutrition intervention. The study by Durga et al. ⁽Reference Durga, van Boxtel and Schouten⁴⁹⁾ included younger participants than many studies on ageing and nutrition, as in most studies the youngest included age is 65 years, with the mean age being much higher. The inclusion of a sample of individuals in their fifties may provide a population in which the negative brain changes accruing from ageing are in a more benign state and thus more responsive to nutritional intervention, thereby allowing for a greater preservation of cognitive function that is in turn more readily detectable on cognitive tests. The supplementation period was also 3 years, which is also longer than most studies. Yet the larger examination of the literature paints a more complex picture. A recent meta-analysis of homocysteine-lowering B vitamin supplementation and cognition in the elderly did not find support for the role of B vitamins on cognition, even when looking at younger subpopulations and including studies of long duration (up to 8 years⁽Reference Clarke, Bennett and Parish⁵⁰⁾). It should be noted that this meta-analysis did include studies investigating cerebrovascular patients, and the primary variable in many trials was not cognition but rather lowering of homocysteine. Nonetheless, these null results are seemingly reinforced by the lack of an effect found by van der Zwaluw et al. ⁽Reference van der Zwaluw, Dhonukshe-Rutten and Van Wijngaarden⁵¹⁾, who studied the effect of B vitamin treatment and cognition in older adults with elevated homocysteine. As described below, one explanation for these inconsistent findings centres on the neurocognitive domains studied and the tools used to assess these domains.

A final note that warrants discussion in the study of nutrition and cognition in healthy adults concerns the length of time necessary for intervention studies. Ideally, studies should be long enough to capture natural deterioration in cognitive abilities over time and/or of sufficient duration for nutrition to have a biological effect on the brain to improve cognitive performance. When studying healthy adults, especially if the study population includes individuals closer to middle-aged, multi-year longitudinal studies would be the ideal norm. This must be balanced with the pragmatic realities that work against multi-year studies such as cost, dropout rate, etc. Below we advocate for the use of assessment tools more appropriate for a healthy population in including more challenging cognitive tests that may potentially reveal subtle cognitive change over time. Therefore, this may shorten the length of interventions, though studies that seek to understand the role of nutrition on the trajectory of cognitive decline in healthy adults still need to be of sufficient length for that decline to occur.

Relational memory and the hippocampus

One brain structure particularly sensitive to ageing is the hippocampus, a structure located near the middle of the brain, within the medial temporal lobes, that primarily supports aspects of memory function (see below). MRI studies measuring the volume of the hippocampus indicate that it begins to shrink at an accelerated rate during the sixth decade of life⁽Reference Fjell, Westlye and Grydeland⁵⁸⁾; this volumetric decline probably reflects, at least in part, loss and alternation of synapses and a reduction in proliferation of neurons, but little overt neuronal death in individuals free of neurodegenerative disorders⁽Reference Morrison and Baxter⁵⁹⁾. Additionally, nearly all adults over the age of 65 years, even those without a diagnosis of MCI or AD, will have some degree of AD-like pathology in the form of neurofibrillary tangles within the medial temporal lobe, and these tangles are negatively associated with memory performance⁽Reference Bennett, Wilson and Boyle⁶⁰⁾. When occurring in adults without MCI or AD, this pathology is almost always limited to the transentorhinal and entorhinal cortices, which are located adjacent to, and are densely connected with, the hippocampus; this pathology can also be found in portions of the hippocampus proper in healthy older adults⁽Reference Braak, Thal and Ghebremedhin⁶¹⁾.

While the hippocampus contributes to a variety of cognitive abilities, its main function may be to serve as the critical hub for a network underlying relational (associative) memory formation and retrieval. Through its cellular architecture that displays disproportionate and rapid plasticity, and anatomical location, which serves as a convergence zone for cortical afferents, the hippocampus is capable of binding together various pieces of information into lasting representations (for reviews, see Eichenbaum & Cohen⁽Reference Eichenbaum and Cohen⁶²⁾, Cohen & Eichenbaum⁽Reference Cohen and Eichenbaum⁶³⁾ and Konkel & Cohen⁽Reference Konkel and Cohen⁶⁴⁾). This system allows one to later remember what the person who introduced himself as ‘Roger Atwood’ looks like, and that you met him when staying at a hotel the first time you visited Santa Fe. Only the hippocampal memory system can learn such novel relations with just one exposure, making it vital to forming new memories of experience throughout a lifetime. Consequently, tests that maximally engage this function, using novel stimuli and novel relations rather than familiar items, are likely to best tap into hippocampal processing.

Given that the hippocampus deteriorates with age, it is unsurprising that relational memory function declines disproportionately as well⁽Reference Naveh-Benjamin⁶⁵⁾. Relational memory, because it depends upon a network of brain structures interacting with the hippocampus, may be particularly susceptible to ageing and hence particularly useful in the study of nutrition and cognitive ageing. Further, the hippocampus is aided by areas of the PFC and parietal lobe during encoding and retrieval, which serve to modulate functions such as goal-directed behaviour and attention (for reviews, see Cabeza et al. ⁽Reference Cabeza, Ciaramelli and Olson⁶⁶⁾, Simons & Spiers⁽Reference Simons and Spiers⁶⁷⁾ and Wagner et al. ⁽Reference Wagner, Shannon and Kahn⁶⁸⁾), and that these structures, too, are sensitive to age-related effects (see below).

Critically, the literature provides reason to believe that these deleterious effects of hippocampal ageing may be partially ameliorated by nutrition. For instance, animal models indicate that intake of flavonoids increases hippocampal neurogenesis, and it is associated with better spatial memory in rodents⁽Reference Green, Martinez-Coria and Khashwji^10, Reference Casadesus, Shukitt-Hale and Stellwagen^69, Reference Van Praag, Lucero and Yeo⁷⁰⁾. Moreover, DHA administration in rodents also has been linked to higher levels of neurogenesis and enhanced hippocampal memory⁽Reference He, Qu and Cui^71, Reference Petursdottir, Farr and Morley⁷²⁾. In addition to these nutrition-induced changes in gross brain structure that allow for better spatial memory, both DHA and various flavonoids reduce the amount of tau protein deposition in the brain⁽Reference Frautschy, Hu and Kim^9, Reference Wang, Santa-Maria and Ho⁷³⁾. Pertinent to hippocampal health in ageing, the neurofibrillary tangles that form in the medial temporal lobe with ageing are composed of hyperphosphorylated tau protein. Though amyloid-β has a more widespread distribution in the brain, its accumulation is also known to impair the type of memory processes that rely on the hippocampus. Importantly, evidence exists for potential modulation of amyloid-β by diet. In murine models of ageing, DHA and curcumin supplementation reduce the amount of amyloid-β burden, with curcumin also preventing amyloid-associated memory impairment⁽Reference Kim, Son and Park^8, Reference Green, Martinez-Coria and Khashwji^10, Reference Lim, Calon and Morihara⁷⁴⁾. In a canine model of ageing, pleiotropic diets composed of multiple antioxidants can ameliorate amyloid deposition and improve retention of information⁽Reference Milgram, Zicker and Head^14, Reference Pop, Head and Hill¹⁵⁾. Finally in humans with MCI, more hippocampal tissue was spared over a 2-year period in a group receiving vitamins B₆, B₁₂ and folic acid supplementation.

Working memory, executive function and the frontoparietal network

In addition to relational memory, several other cognitive constructs may prove amenable to nutritional intervention due to their reliance on brain networks that are disproportionately affected by ageing processes. One good candidate is working memory, which involves the ability to temporarily maintain information in one’s head, especially in the face of interference, and/or to manipulate the temporarily maintained information to achieve a goal. An example of working memory entails recalling the spatial layout and furniture placement of your living room, and then mentally rearranging the furniture to produce a new design. Working memory processes are thought to rely heavily on frontal and parietal regions of the brain⁽Reference Gazzaley and Nobre^75, Reference Kane and Engle⁷⁶⁾, and older adults frequently experience reductions in working memory capabilities⁽Reference Park, Lautenschlager and Hedden⁴⁶⁾. A closely related cognitive construct to working memory is executive function, which is even sometimes thought of as a parent category to working memory. Executive function processes entail abilities such as planning, inhibition and fluid reasoning; these abilities largely rely on a fronto-parietal network⁽Reference Barbey, Colom and Solomon⁷⁷⁾, and it is common to observe age-related deficits in executive function⁽Reference Buckner⁷⁸⁾.

Biological mechanisms accounting for these deficits in working memory and executive function centre on age-related changes that occur with the PFC and parietal lobe. Normal ageing is associated with a reduction in synapses in the PFC⁽Reference Morrison and Baxter⁵⁹⁾, and it is additionally known that both the PFC and posterior parietal lobe undergo volume loss with ageing⁽Reference Raz, Ghisletta and Rodrigue⁵⁵⁾. Similar to the hippocampus, intake of B vitamins has been associated with more grey matter volume⁽Reference Erickson, Suever and Prakash⁷⁹⁾, suggesting the possibility of B vitamins to spare cortical grey matter volume, which may in turn have an effect on working memory. Additionally, amyloid-β accumulates in a substantial proportion of older adults presumed to be free of MCI or AD, with particular concentration in the PFC and in areas of the medial parietal lobe, such as the precuneus⁽Reference Rodrigue, Kennedy and Devous^80, Reference Sperling, Laviolette and O’Keefe⁸¹⁾. The level of amyloid-β in these areas is inversely related to multiple cognitive abilities, including various forms of memory, attention and processing speed⁽Reference Kennedy, Rodrigue and Devous^82, Reference Rentz, Amariglio and Becker⁸³⁾. One intriguing study that manipulated dietary macronutrient proportions over a 4-week period indicated that a diet low in saturated fat and a low glycaemic index led to reduced levels of amyloid-β 42 in the cerebrospinal fluid (a biomarker for amyloid-β in the brain) of healthy older adults⁽Reference Bayer-Carter, Green and Montine⁸⁴⁾. Future studies are needed to further discern how macronutrient profiles may mediate amyloid-β clearance in humans.

Processing speed and white matter

A major area of decline in ageing is speed of processing, which refers to how quickly one can process information of multiple modalities⁽Reference Park, Lautenschlager and Hedden^46, Reference Salthouse⁸⁵⁾. In fact, some have argued that speed of processing may underlie many of the cognitive deficits observed in ageing⁽Reference Salthouse^86, Reference Salthouse⁸⁷⁾. In the brain, processing speed ability is largely dependent on whole-brain white matter integrity⁽Reference Borghesani, Madhyastha and Aylward^88, Reference Wen, Zhu and He⁸⁹⁾. Normal ageing is also associated with deterioration of the white matter. These changes in the white matter are more pronounced in the PFC⁽Reference Wen and Sachdev⁹⁰⁾. The aetiology of this pathology in the white matter among healthy older adults is most often due to subtle cerebrovascular-related changes, such as arterial stiffening or microscopic bleeding within the brain⁽Reference Jagust⁵⁴⁾. Moreover, white matter damage is mitigated by n-3 fatty acid intake and adherence to a Mediterranean-type diet⁽Reference Bowman, Silbert and Howieson^91, Reference Scarmeas, Luchsinger and Stern⁹²⁾, potentially due to the salutary cardiovascular effects of this type of diet and the relationship between white matter integrity and cerebrovascular integrity.

Cognitive measurements

Through the excellent work of those in the field of neuropsychology, there exists an array of behavioural assessment tools available to measure aspects of cognitive function. Most often, these tests are deployed when evaluating clinical populations, such as those who have sustained a traumatic brain injury or those suspected of having AD. As an example, when measuring hippocampal-dependent memory, the most commonly used tasks involve asking a participant to memorise a list of common words, and then assessing his/her retention for the material after a delay of approximately 20–30 min⁽Reference Lezak, Howieson and Loring⁹³⁾. In the case of a patient with damage relatively circumscribed to the hippocampus, this type of test (for example, California Verbal Learning Test) works well in detecting the gross memory impairment that follows this injury. Similarly, the current hallmark indication of early clinical AD is a primary deficit on this type of task with relative preservation in other cognitive domains⁽Reference Weintraub, Wicklund and Salmon⁹⁴⁾.

Though these tests have worked well in the characterisation of large impairments due to dementia or brain injury, they may not fare as well in detecting the variance in hippocampal-dependent memory performance among those within the so-called ‘normal range’ of cognitive ability. The idea that the classic neuropsychological tests may be insensitive to subtle changes or early pathology is not new, as demonstrated by the classification of individuals with subjective memory impairment. These individuals do not have an objective memory impairment as measured by a delayed-recall test, but they subjectively report, and are often concerned about, their perceived failing memory ability. Interestingly, those who are concerned about the memory lapses they are experiencing are more likely to develop AD⁽Reference Jessen, Wiese and Bachmann⁹⁵⁾. Thus, it is conceivable that these individuals may have preclinical AD, and that their memory deficit is too subtle to be detected by standard measures; nonetheless, the deficit is real and it could indicate the earliest stages of AD.

The issue of subtle, yet meaningful, effects bears directly on the study of nutrition, brain health, and cognitive ageing. It is unlikely that nutritional modulation of brain function will be on the same magnitude as the effects of brain damage; therefore, just as more sensitive tests may be needed to detect the earliest stages of AD, there may also be the need to develop sensitive tests to demonstrate the effects of nutrition on the ageing brain. Indeed, it may be the case that some studies have failed to detect a nutritional enhancement in memory, not because nutrition does not benefit memory, but rather that the tool used could not detect the effects of nutrition. To date, the vast majority of RCT assessing cognitive function following nutritional intervention have used standardised neuropsychological tests that may be ill-suited for detecting subtle cognitive change. Below we provide examples of types of tasks often used in cognitive neuroscience research that may be more successful in illustrating an effect of nutrition on cognition in an aged population.

MRI

The preceding discussion has emphasised the importance of using sensitive cognitive tasks in order to effectively test nutritional enhancement of cognition in the ageing brain; however, a complimentary tool for assessing how nutrition may alter the health of the ageing brain involves using neuroimaging to gather structural and physiological (for example, functional connectivity, blood flow, metabolites) data on the brain. Even in nutritional interventions where there is a null effect on cognitive task data, a finding indicating the sparing of hippocampal tissue as a result of the intervention would surely be regarded as positive in the context of the ageing brain, and this would probably have downstream behavioural effects, even if they cannot be detected by current neuropsychological tests. Below we highlight successful examples of the deployment of MRI to nutrition and cognitive ageing research, and discuss potentially fruitful MRI techniques not yet applied sufficiently in this field. Though this review only covers MRI, we note that there are other neuroimaging techniques such as electroencephalography or near-IR spectroscopy that may be more suitable for certain questions, particularly due to the high cost of MRI. For a full review on neuroimaging techniques and their application to nutrition, we refer the reader to a recent review by Sizonenko et al. ⁽Reference Sizonenko, Babiloni and Sijben¹¹⁰⁾.