Normal aging and to a greater degree degenerative brain diseases such as Alzheimer's disease (AD), cause changes in the brain's structure and function. Degenerative changes in brain structure and decline in its function are associated with declines in cognitive ability. Early detection of AD is a key priority in dementia services and research. However, depending on the disease progression, neurodegenerative manifestations, such as cerebral atrophy, are detected late in course of AD. Functional changes in the brain may be an indirect indicator of trans-synaptic activity and they usually appear prior to structural changes in AD. Resting-state functional magnetic resonance imaging (RS-fMRI) has recently been highlighted as a new technique for interrogating intrinsic functional connectivity networks. Among the majority of RS-fMRI studies, the default mode network (DMN), salience network (SN), and central executive network (CEN) gained particular focus because alterations to their functional connectivity were observed in subjects who had AD, who had mild cognitive impairment (MCI), or who were at high risk for AD. Herein, we present a review of the current research on changes in functional connectivity, as measured by RS-fMRI. We focus on the DMN, SN, and CEN to describe RS-fMRI results from three groups: normal healthy aging, MCI and AD.
Worldwide, the elderly population is growing, increasing the concern over age-related cognitive decline. Cognitive decline has a negative impact on quality of life and, healthy brain aging is an essential component of overall well-being. Because of the nearly global rise in life expectancy and the concomitant emphasis on quality of life, healthy brain aging has become an important focus.1
Normal aging and to a greater degree degenerative brain diseases such as Alzheimer's disease (AD), cause changes in the brain's structure and function. Degenerative changes in brain structure and decline in its function are associated with declines in cognitive ability. Mild-to-moderate age-dependent brain volume loss, enlarged periventricular (Virchow-Robin) spaces, punctiform or minor white matter abnormalities, and iron accumulation in the basal ganglia are examples of normal age-related brain changes that can be seen on structural brain imaging.2 These changes, which are associated with cognitive decline, most often affect the domains of attention, memory, and executive function.3,4 AD is accompanied by atrophy in the bilateral medial temporal, parietal, and frontal lobes.2 These changes are associated with serious cognitive decline and a number of neuropsychiatric symptoms.
However, depending on the disease progression, neurodegenerative manifestations, such as cerebral atrophy, are detected late in course of AD. Though CSF amyloid-β(Aβ) 1-42 levels may begin decreasing 25 years before the onset of symptoms and brain amyloid deposition occurs in preclinical stage of AD,5 the gap between early amyloid detection and structural brain changes is wide.6 Early detection of AD is a key priority in dementia services and research. Therefore, additional biomarkers in the pathophysiological cascade of AD are needed, such as functional brain changes. Functional changes in the brain may be an indirect indicator of trans-synaptic activity and they usually appear prior to structural changes in AD.7 Resting-state functional magnetic resonance imaging (RS-fMRI) has recently been highlighted as a new technique for interrogating intrinsic functional connectivity networks (ICN) without an experimentally determined context.8 Previous studies have shown that ICN changes are sensitive to functional brain changes related to Alzheimer's disease pathology across the clinical spectrum.9
Herein, we present a review of the current research on changes in functional connectivity, as measured by RS-fMRI. We compare researcher's outcomes from studies that examine normal healthy aging, patients with MCI, and AD.
RESTING-STATE FMRI BASIC PRINCIPLES AND CORE LARGE-SCALE NETWORKS
Recently, fMRI has largely replaced nuclear medicine techniques because it is non-invasive and does not require use of radioactive contrast media, instead, fMRI uses blood-oxygen-level-dependent (BOLD) contrast.2 In BOLD fMRI, the difference in magnetic susceptibility between oxygenated and deoxygenated blood serves as an intrinsic contrast medium through which to compare conditions.
Initially, fMRI was developed to measure two conditions (e.g., task or no task) using an activation paradigm, so-called task-based fMRI.6 In recent years, there has been an increased interest in applying the technique to at-rest conditions, termed RS-fMRI.10 RS-fMRI focuses on spontaneous low-frequency fluctuations (<0.1 Hz) in the BOLD signal.10 This has led to the description of 10-20 RS networks, the most commonly observed of which are: the default mode network (DMN), the salience network (SN), the central executive network (CEN), the visual processing network, the sensorymotor network, the dorsal attention network, and auditory network, to name a few.
In many task-based fMRI studies, reversed contrasts revealed consistent deactivation of specific regions,11 including the medial prefrontal cortex (mPFC), the posterior cingulate cortex (PCC), the precuneus, the anterior cingulate cortex (ACC), the parietal cortex, and, in a minority of studies, the hippocampus.12 The default mode network (DMN) is so named because it is the most active network in the absence of a task.13 Among the majority of RS-fMRI studies, the DMN gained particular focus because alterations to its functional connectivity were observed in subjects who had AD, who had MCI, or who were at high risk for AD. The DMN is known to be involved in the retrieval of autobiographical episodic memory as well as self-referential mental processing.14,15
Besides the DMN, other stable ICNs, such as the SN and the CEN, have been known to play crucial roles in cognitive processing.16 The CEN includes the dorsolateral prefrontal cortex (DLPFC) and the posterior parietal cortex (PPC).17 It plays a key role in active maintenance and manipulation of information in working memory, and in judgment and decision-making in the context of goal-directed behavior.18,19,20 Additionally, the SN mainly consists of the dorsal ACC and the frontoinsular cortices (FIC). It serves to identify the most relevant stimuli for guiding behavior in response to several internal and external stimuli.21,22 The right FIC is a core node of the SN and plays a critical role in switching between the CEN and the DMN,23 which are known to interact competitively during cognitive information processing.24,25 Once a salient stimulus is detected, the FIC initiates the appropriate transient control signals to engage the CEN to mediate attention, working memory and other higher-order cognitive processes, all while disengaging the DMN.22 This switching mechanism helps to focus attention on external stimuli and eventually allows the stimuli to take on added significance or saliency.22
In this review, we focus on the DMN, SN, and CEN to describe RS-fMRI results from three groups: normal healthy aging, MCI and AD.
ANALYTIC TECHNIQUES
There are three main analytic techniques used to assess functional connectivity: the seed-based approach, independent components analysis (ICA), and graph theory.
In the seed-based approach, the researcher selects a "seed" of interest (region of interest, ROI) and extracts the time course of activation at that ROI. This time course is then tested for correlation with the time courses of the rest of the voxels of the brain to search for matches.26 Brain regions that are positively correlated with each other are thought to belong to functionally coupled networks.27
In contrast, in ICA, the researcher does not need to select a reference region. Instead, the entire set of four-dimensional fMRI data can be decomposed into time courses and associated spatial maps that describe the temporal and spatial characteristics of the data components.28 ICA seeks underlying components of activation that are statistically independent of each other. Both seed-based and ICA approaches tend to reveal the same networks. However, seed-based analyses are sometimes preferred because they can make group comparisons easier.27
Studies using graph theory with RS-fMRI are emerging. In graph theory, ROIs can be represented as nodes.10 Nodes define anatomically homogeneous brain regions or individual voxels.29 The fMRI data is spatially parcellated according to a structural map of the brain, and correlations are computed between activations in all region pairs.27 Typical measurements taken under graph theory include average path length and global connectedness, which is the average length of the shortest connections between all pairs of nodes.30 Another measure of interest is the clustering coefficient, which is related to the connectedness of neighboring nodes and reflects the presence of small world structures.30
RESTING-STATE FUNCTIONAL MRI ALTERATIONS IN THE NORMAL HEALTHY AGING
RS-fMRI allows for the investigation of the neural bases of age-related cognitive changes, such as attention, information processing, and working memory.31,32 To date, the DMN has been the main focus of aging-related RS-fMRI research. Many studies reported that this network's activity during rest is necessary for memory consolidation.26 Additionally, amyloid deposition associated with AD is seen initially and most prominently in DMN hubs.12,33,34
Most of the RS-fMRI studies that focused on the DMN showed that aging are associated with decreased connectivity within this system. After assessing functional connectivity within the network, the seed-based and ICA studies produced similar results. Several studies reported reduced functional connectivity between anterior and posterior components of the DMN with advanced age.35,36 Wu et al.37 found greater integrity and greater preparation of DMN components in younger subjects compared to elderly subjects. The reduced RS-fMRI activity seen in the DMN in normal healthy aging subjects was correlated with executive dysfunction and decreased processing speed.2 Graph analysis studies further showed that decreased global connectivity and decreased nodal efficiency in several major brain hubs became more common during the aging process.38 Studies that focused on the modularity of functional networks reported that modularity decreased with age, indicating changes in size, composition, and the topological roles of the networks.39
Age-related resting-state functional connectivity changes have been reported not only in the DMN but also in the SN and the CEN. Because there are fewer studies of the SN and the CEN, age-related resting-state functional connectivity changes in these regions are not yet well understood. Onoda et al.40 reported that connectivity within the SN decreased and certain internetwork connectivities (e.g., SN to auditory network, DMN to visual processing network, etc.) also decreased with aging. He et al.41 found age-related decreases in the positive functional connectivities between the right FIC in SN and the CEN and in the negative functional connectivities between the right FIC and the DMN, with and without atrophy correction. In a later study, He et al.42 also found that functional impairments of the SN may occur as early as in normal aging.
Several hypotheses have been formulated to explain the functional connectivity deficits associated with non-pathological brain aging. Age-related changes in resting state functional connectivity are thought to reflect declines in structural connectivity, especially in white matter integrity, dopaminergic deficit, and amyloid deposition in the brain.43
RESTING-STATE FMRI ALTERATIONS IN PATIENTS WITH MCI AND AD
Most seed-based and ICA studies indicate that there is decreased connectivity in the DMN and other networks in subjects with MCI and AD. The majority of RS-fMRI studies found reduced DMN connectivity across widespread regions in the frontal, parietal, temporal and occipital regions of AD patients.44,45 Using graph analysis, major hubs in the brain seem to be affected by MCI and AD. Supkar et al.46 observed the loss of small-world organization in the functional brain network, characterized by a significantly lower clustering coefficient, which is indicative of disrupted local connectivity. Brier et al.47 also found that the clustering coefficient and modularity were lower in AD patients. In the same study, cognitively normal participants who harbor AD pathologies also showed reduced functional connectivity, demonstrating brain changes similar to, but smaller than, those seen in AD.47
However, results regarding aberrant functions in the DMN from MCI patients were different in patterns from those of AD patients. Damoiseaux et al.9 reported decreased connectivity in the posterior DMN alongside increased connectivity in the ventral and anterior DMN using ICA. Also using ICA, Qi et al.48 found that MCI patients showed a trend toward reduced hippocampus activity compared to healthy elderly. They also found that reduced functional activity in the bilateral precuneus/posterior cingulate cortex, the right inferior parietal lobule, and the left fusiform gyrus indicated network deficiency, while increased activity in the left prefrontal cortex, the inferior parietal lobule, and the middle temporal gyrus suggested network compensation in MCI patients. Using a seed-based approach, the most recent study of MCI patients reported increased DMN connectivity between the medial prefrontal regions and the posterior cingulate and between the posterior cingulated, the parahippocampus and the anterior hippocampus.49 These results suggest that the DMN functions aberrantly in MCI patients, which might be due to neuronal loss in the initial phase of neurodegeneration. Increased functional connectivity between the PCC, the parahippocampus, and the anterior hippocampus in MCI patients may reflect a maladaptive mechanism.49
Decreased DMN connectivity was even found in unaffected carriers of familial AD who have pathogenic presenilin-1 (PSEN1), presenilin-2 (PSEN2), or amyloid precursor protein (APP) mutations,50 as well as among subjects with cognitive complaints, but normal neuropsychological performance.51 Also, APOE ɛ4 carriers showed decreased connectivity of the posterior DMN and relatively increased connectivity of the SN.52 However, PSEN1-mutation carriers who are between 9 to 17 years old demonstrated increased functional connectivity between the posterior cingulate cortex and the medial temporal lobe regions, as well as high gray-matter volume in their temporal regions.53
There are several studies that look into the association between amyloid-β deposition and functional brain connectivity. Several previous studies reported that reduced functional connectivity of the DMN can be found in cognitively normal subjects with brain amyloid burden.33,34,54 Using graph analysis, a decreased number of hubs and reduced connectivity within the DMN were found both MCI and AD, as well as in healthy elderly with amyloid-β deposition on positron emission tomography (PET) images.33,55 However, Lim et al.56 reported that the functional connectivity of the DMN among older adults with normal cognition was greater, while the SN was not different, and the CEN was lower in among the Pittsburgh compound B-positive group, compared to the Pittsburgh compound B-negative group. The authors explained that the discrepancy in DMN result might be attributed to the "acceleration" and "brain reserve" hypotheses. The acceleration hypothesis predicts that the initiation of amyloid-β deposition by independent events instigates a milieu of higher functional connectivity that accelerates this deposition, which eventually leads to functional disconnection or metabolic deterioration in subjects with amyloid burden.57,58 The brain reserve hypothesis states that higher brain metabolism and functional connectivity represent stable traits that impart the capacity to withstand amyloid-β deposition and maintain normal cognition.57
Results in the SN and CEN appear to be less consistent. Sorg et al.59 found reduced connectivity in the DMN and central executive network (CEN) hubs of MCI patients. Agosta et al.60 reported decreased connectivity in the DMN among MCI and AD patients, as well as increased mean connectivity in the CEN among AD patients. Balachandar et al.7 reported decreased connectivity in the DMN and increased connectivity in CEN in mild AD patients. Zhou et al.61 reported increased functional connectivity in the SN of AD patients. However, He et al.42 found that both the structural and functional organizations of the SN are impaired in MCI and AD patients.
The summary of the main group differences in RS-fMRI obtained using both the seed-based and independent components analysis (ICA) methods is provided in Table 1.
CONCLUSIONS
According to a number of empirical studies, subjects who are aging healthfully, those who have MCI and those who have AD all show changes in functional connectivity in three large-scale networks-the DMN, SN, and CEN-based on RS-fMRI results. These findings help build an understanding of the neural substrates in the aging brain and during pathological degenerative processes.
Previous studies have shown that the ICN changes that are observable in RS-fMRI are sensitive to the functional brain changes that are often seen across the spectrum of AD pathology.9 The ICN changes seen on RS-fMRI are potentially sensitive, non-invasive biomarkers of AD. Among the ICNs, the DMN, SN and CEN have turned out to be particularly important for maintaining higher cognitive function; hence, the use of the term "core" neurocognitive networks. In particular, the DMN has been the most investigated resting-state network. And most RS-fMRI studies report reduced DMN connectivity in normally aging, MCI and AD subjects. However, reduced DMN connectivity has also been reported to be associated with a variety of other diseases, such as Parkinson's disease and multiple sclerosis, and is by no means specific to AD.6 Besides, DMN, SN and CEN abnormalities are wide-spread in psychiatric, as well as in neurological disorders.16 Different studies have revealed that there are both consistencies and discrepancies in ICN changes among normally aging, MCI and AD subjects, possibly due to methodological differences and/or clinical heterogeneity among subjects.62 These limitations have recently been overcome and it is expected that clinical applications of RS-fMRI in normal aging, MCI and AD will continue to increase.
WilliamsKNKemperSInterventions to reduce cognitive decline in aging201048425120415290BarkhofFFoxNCBastos-LeiteAJScheltensPNew YorkSpringer-Verlag Berlin Heidelberg2011HeddenTGabrieliJDInsights into the ageing mind: a view from cognitive neuroscience20045879614735112WhalleyLJDearyIJAppletonCLStarrJMCognitive reserve and the neurobiology of cognitive aging2004336938215541707BatemanRJXiongCBenzingerTLFaganAMGoateAFoxNCClinical and biomarker changes in dominantly inherited Alzheimer's disease201236779580422784036BarkhofFHallerSRomboutsSAResting-state functional MR imaging: a new window to the brain2014272294924956047BalachandarRJohnJPSainiJKumarKJJoshiHSadanandSA study of structural and functional connectivity in early Alzheimer's disease using rest fMRI and diffusion tensor imaging20153049750424990445VemuriPJonesDTJackCRJrResting state functional MRI in Alzheimer's disease20124222236691DamoiseauxJSPraterKEMillerBLGreiciusMDFunctional connectivity tracks clinical deterioration in Alzheimer's disease201233828.e19828.e3021840627LeeMHSmyserCDShimonyJSResting-state fMRI: a review of methods and clinical applications2013341866187222936095GusnardDARaichleMERaichleMESearching for a baseline: functional imaging and the resting human brain2001268569411584306BucknerRLAndrews-HannaJRSchacterDLThe brain's default network: anatomy, function, and relevance to disease2008112413818400922RaichleMEMacLeodAMSnyderAZPowersWJGusnardDAShulmanGLA default mode of brain function200198676682SprengRNMarRAKimASThe common neural basis of autobiographical memory, prospection, navigation, theory of mind, and the default mode: a quantitative meta-analysis20092148951018510452Whitfield-GabrieliSMoranJMNieto-CastanonATriantafyllouCSaxeRGabrieliJDAssociations and dissociations between default and self-reference networks in the human brain20115522523221111832MenonVLarge-scale brain networks and psychopathology: a unifying triple network model20111548350621908230DamoiseauxJSRomboutsSABarkhofFScheltensPStamCJSmithSMConsistent resting-state networks across healthy subjects2006103138481385316945915PetridesMLateral prefrontal cortex: architectonic and functional organization200536078179515937012MullerNGKnightRTThe functional neuroanatomy of working memory: contributions of human brain lesion studies2006139515816352402KoechlinESummerfieldCAn information theoretical approach to prefrontal executive function20071122923517475536SeeleyWWMenonVSchatzbergAFKellerJGloverGHKennaHDissociable intrinsic connectivity networks for salience processing and executive control2007272349235617329432MenonVUddinLQSaliency, switching, attention and control: a network model of insula function201021465566720512370SridharanDLevitinDJMenonVA critical role for the right fronto-insular cortex in switching between central-executive and default-mode networks2008105125691257418723676GreiciusMDKrasnowBReissALMenonVFunctional connectivity in the resting brain: a network analysis of the default mode hypothesis200310025325812506194FoxMDSnyderAZVincentJLCorbettaMVan EssenDCRaichleMEThe human brain is intrinsically organized into dynamic, anticorrelated functional networks20051029673967815976020FoxMDRaichleMESpontaneous fluctuations in brain activity observed with functional magnetic resonance imaging2007870071117704812DennisELThompsonPMFunctional brain connectivity using fMRI in aging and Alzheimer's disease201424496224562737BeckmannCFDeLucaMDevlinJTSmithSMInvestigations into resting-state connectivity using independent component analysis20053601001101316087444StamCJde HaanWDaffertshoferAJonesBFManshandenIvan Cappellen van WalsumAMGraph theoretical analysis of magnetoencephalographic functional connectivity in Alzheimer's disease200913221322418952674van den HeuvelMPStamCJBoersmaMHulshoff PolHESmall-world and scale-free organization of voxel-based resting-state functional connectivity in the human brain20084352853918786642ParkDCSmithADLautenschlagerGEarlesJLFrieskeDZwahrMMediators of long-term memory performance across the life span1996116216379000294SalthouseTAFerrer-CajaEWhat needs to be explained to account for age-related effects on multiple cognitive variables?2003189111012641315HeddenTVan DijkKRBeckerJAMehtaASperlingRAJohnsonKADisruption of functional connectivity in clinically normal older adults harboring amyloid burden200929126861269419812343MorminoECSmiljicAHayengaAOOnamiSHGreiciusMDRabinoviciGDRelationships between β-amyloid and functional connectivity in different components of the default mode network in aging2011212399240721383234Andrews-HannaJRSnyderAZVincentJLLustigCHeadDRaichleMEDisruption of large-scale brain systems in advanced aging20075692493518054866DamoiseauxJSBeckmannCFArigitaEJBarkhofFScheltensPStamCJReduced resting-state brain activity in the "default network" in normal aging2008181856186418063564WuJTWuHZYanCGChenWXZhangHYHeYAging-related changes in the default mode network and its anti-correlated networks: a resting-state fMRI study2011504626721925236AchardSBullmoreEEfficiency and cost of economical brain functional networks20073e1717274684MeunierDAchardSMorcomABullmoreEAge-related changes in modular organization of human brain functional networks20094471572319027073OnodaKIshiharaMYamaguchiSDecreased functional connectivity by aging is associated with cognitive decline2012242186219822784277HeXQinWLiuYZhangXDuanYSongJAge-related decrease in functional connectivity of the right fronto-insular cortex with the central executive and default-mode networks in adults from young to middle age2013544747923583587HeXQinWLiuYZhangXDuanYSongJAbnormal salience network in normal aging and in amnestic mild cognitive impairment and Alzheimer's disease2014353446346424222384FerreiraLKBusattoGFResting-state functional connectivity in normal brain aging20133738440023333262BrierMRThomasJBSnyderAZBenzingerTLZhangDRaichleMELoss of intranetwork and internetwork resting state functional connections with Alzheimer's disease progression2012328890889922745490ZhangHYWangSJXingJLiuBMaZLYangMDetection of PCC functional connectivity characteristics in resting-state fMRI in mild Alzheimer's disease200919710310818786570SupekarKMenonVRubinDMusenMGreiciusMDNetwork analysis of intrinsic functional brain connectivity in Alzheimer's disease20084e100010018584043BrierMRThomasJBFaganAMHassenstabJHoltzmanDMBenzingerTLFunctional connectivity and graph theory in preclinical Alzheimer's disease20143575776824216223QiZWuXWangZZhangNDongHYaoLImpairment and compensation coexist in amnestic MCI default mode network201050485520006713GardiniSVenneriASambataroFCuetosFFasanoFMarchiMIncreased functional connectivity in the default mode network in mild cognitive impairment: a maladaptive compensatory mechanism associated with poor semantic memory performance20154545747025547636ChhatwalJPSchultzAPJohnsonKBenzingerTLJackCJrAncesBMImpaired default network functional connectivity in autosomal dominant Alzheimer disease20138173674423884042WangYRisacherSLWestJDMcDonaldBCMageeTRFarlowMRAltered default mode network connectivity in older adults with cognitive complaints and amnestic mild cognitive impairment20133575176023481685MachuldaMMJonesDTVemuriPMcDadeEAvulaRPrzybelskiSEffect of APOE epsilon4 status on intrinsic network connectivity in cognitively normal elderly subjects2011681131113621555604QuirozYTSchultzAPChenKProtasHDBrickhouseMFleisherASBrain imaging and blood biomarker abnormalities in children with autosomal dominant Alzheimer disease: a cross-sectional study20157291291926121081ShelineYIRaichleMESnyderAZMorrisJCHeadDWangSAmyloid plaques disrupt resting state default mode network connectivity in cognitively normal elderly20106758458719833321ShelineYIRaichleMEResting state functional connectivity in preclinical Alzheimer's disease20137434034723290495LimHKNebesRSnitzBCohenAMathisCPriceJRegional amyloid burden and intrinsic connectivity networks in cognitively normal elderly subjects20141373327333825266592CohenADPriceJCWeissfeldLAJamesJRosarioBLBiWBasal cerebral metabolism may modulate the cognitive effects of Abeta in mild cognitive impairment: an example of brain reserve200929147701477819940172JohnsonSCChristianBTOkonkwoOCOhJMHardingSXuGAmyloid burden and neural function in people at risk for Alzheimer's disease20143557658424269021SorgCRiedlVMuhlauMCalhounVDEicheleTLaerLSelective changes of resting-state networks in individuals at risk for Alzheimer's disease2007104187601876518003904AgostaFPievaniMGeroldiCCopettiMFrisoniGBFilippiMResting state fMRI in Alzheimer's disease: beyond the default mode network2012331564157821813210ZhouJGreiciusMDGennatasEDGrowdonMEJangJYRabinoviciGDDivergent network connectivity changes in behavioural variant frontotemporal dementia and Alzheimer's disease20101331352136720410145BaiFZhangZYuHShiYYuanYZhuWDefault-mode network activity distinguishes amnestic type mild cognitive impairment from healthy aging: a combined structural and resting-state functional MRI study200843811111518455308
Schematic summary of the main group differences in RS-fMRI obtained using both the seed-based and independent components analysis (ICA) methods
DMN: default mode network, SN: salience network, CEN: central executive network, ↓: decreased functional connectivity, ↑: increased functional connectivity, -: not different, NA: not applicable, PCC: posterior cingulate cortex, PFC: prefrontal cortex. RS-fMRI: Resting-state functional magnetic resonance imaging