Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

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Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

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Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Mechanistic Model

```mermaid
flowchart TD
subgraph Aging_Factors["Aging-Related Changes"]
A["Amyloid Deposition"] --> B["Tau Pathology"]
B --> C["Synaptic Loss"]
C --> D["Neuronal Dysfunction"]
end

subgraph DMN_Changes["DMN Connectivity Alterations"]
D --> E["Posterior Cingulate Cortical Hypometabolism"]
E --> F["Medial Temporal Lobe Connectivity Disruption"]
F --> G["Precuneus Activity Decline"]
G --> H["Angular Gyrus Functional Alterations"]
end

subgraph Cognitive_Outcomes["Cognitive Decline"]
H --> I["Episodic Memory Impairment"]
I --> J["Executive Function Deficits"]
J --> K["Global Cognitive Decline"]
end

subgraph Therapeutic_Targets["Therapeutic Targets"]
L["BDNF Signaling"] --> C
M["Neuroinflammation Modulation"] --> D
N["Synaptic Plasticity Enhancement"] --> C
end

...

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Mechanistic Model

Mermaid diagram (expand to render)

Overview

This hypothesis proposes that alterations in intra-regional functional connectivity within Default Mode Network (DMN) regions are associated with cognitive decline in aging individuals, representing a key mechanism distinguishing normal aging from pathological decline [1]. The DMN, comprising the [medial prefrontal cortex](/brain-regions/prefrontal-cortex), [posterior cingulate cortex](/brain-regions/posterior-cingulate), [precuneus](/brain-regions/precuneus), [angular gyrus](/brain-regions/angular-gyrus), and medial temporal lobe structures, demonstrates characteristic patterns of connectivity disruption in both aging and neurodegenerative diseases [2]. [@zhou2010]

Type: Disease Model [@harrison2022]

Confidence Level: Strong [@peraza2024]

Diseases Associated: [Alzheimer's Disease](/diseases/alzheimers-disease), [Mild Cognitive Impairment](/diseases/mild-cognitive-impairment), [Parkinson's Disease](/diseases/parkinsons-disease), Lewy Body Dementia [@petersen2020]

The Default Mode Network in Neurodegeneration

Anatomical Components

The DMN consists of spatially distinct but functionally interconnected regions: [@damoiseaux2012]

Posterior Cingulate Cortex (PCC): The hub of DMN activity, critical for episodic memory and self-referential processing [3]
Precuneus: Involved in visuospatial imagery and consciousness
Medial Prefrontal Cortex (mPFC): Supports social cognition and self-referential thinking
Angular Gyrus: Integrates information across sensory modalities
Medial Temporal Lobe (MTL): Critical for memory encoding and retrieval

Normal Aging vs. Pathological Decline

Research demonstrates a critical distinction between age-related changes and neurodegenerative processes: [@bero2011a]

Normal Aging: [@palop2016]

Mild reduction in long-range DMN connectivity
Relatively preserved intra-regional connectivity
Minimal impact on cognitive function

Pathological Decline (AD/MCI): [@palmqvist2024]

Severe disruption of posterior DMN connectivity
Increased connectivity in anterior regions (compensatory)
Strong correlation with amyloid and [tau pathology](/proteins/tau)
Progressive decline matching Braak staging of tau [4]

Molecular Mechanisms of DMN Disruption

Amyloid-Beta Effects

[Amyloid-beta](/proteins/amyloid-beta) (Aβ) accumulation directly impacts neural network function: [@eskildsen2024]

Synaptic toxicity: Aβ oligomers impair synaptic plasticity through NMDA receptor dysregulation [5]

Neural activity disruption: Amyloid deposits alter resting-state neural activity in affected regions [6]

Functional connectivity reduction: PET-FDG studies show hypometabolism in posterior DMN regions correlating with Aβ burden [7]

Tau Pathology Impact

[Tau](/proteins/tau) pathology follows a characteristic pattern in AD: [@nagappan2014]

Braak Stage I-II (Transentorhinal): Early tau in entorhinal cortex affects MTL connectivity

Braak Stage III-IV (Limbic): Tau spread to hippocampus and PCC disrupts memory circuits

Braak Stage V-VI (Isocortical): Widespread tau leads to global network breakdown [8]

Neuroinflammatory Mechanisms

Chronic neuroinflammation contributes to DMN dysfunction: [@voss2023]

Microglial activation: Pro-inflammatory cytokines (IL-1β, TNF-α) disrupt neural signaling [9]
Astrocyte dysfunction: Altered astrocyte-neuron interactions affect network synchronization
Blood-brain barrier breakdown: Permeability changes affect metabolic support to neurons

Evidence Assessment

Confidence Level: Strong

This hypothesis is supported by multiple converging lines of evidence:

| Evidence Type | Strength | Key Studies |
|---------------|----------|-------------|
| Neuroimaging (fMRI/rs-fMRI) | Strong | [10, 11, 12] |
| PET Metabolic Studies | Strong | [7, 13] |
| Post-mortem Studies | Strong | [4, 8] |
| Longitudinal Cohorts | Moderate | [14, 15] |
| Animal Models | Moderate | [16, 17] |

Key Supporting Studies

Buckner et al. (2009) — Established the organizational principle of the DMN and its vulnerability in AD [10]

Zhou et al. (2010) — Demonstrated differential patterns of DMN disruption in MCI vs. normal aging [11]

Petersen et al. (2020) — Longitudinal analysis of DMN connectivity as a biomarker for progression [14]

Harrison et al. (2022) — Meta-analysis of rs-fMRI changes across the AD continuum [12]

Palmqvist et al. (2024) — Blood biomarkers correlate with DMN connectivity changes [18]

Testability Score: 9/10

Resting-state fMRI is widely available
Standardized preprocessing pipelines exist
Connectivity metrics are reproducible
Can be combined with PET and fluid biomarkers

Therapeutic Potential Score: 7/10

Non-invasive neuromodulation targets (TMS, tDCS) can potentially modulate DMN
Lifestyle interventions (exercise, cognitive training) may preserve connectivity
However, direct targeting remains challenging

Key Proteins and Genes

[APP](/genes/app) — Amyloid precursor protein
[Tau (MAPT)](/proteins/tau) — Microtubule-associated protein tau
[APOE](/genes/apoe) — Apolipoprotein E (ε4 allele increases risk)
[BDNF](/proteins/bdnf-protein) — Brain-derived neurotrophic factor
[TREM2](/genes/trem2) — Triggering receptor expressed on myeloid cells 2

Experimental Approaches

Neuroimaging Techniques

Resting-state fMRI (rs-fMRI): Measure intrinsic connectivity

FDG-PET: Assess glucose metabolism in DMN regions

Amyloid/Tau PET: Visualize pathological burden

DTI: Examine white matter integrity connecting DMN nodes

Computational Methods

Graph theory analysis: Quantify network properties

Seed-based correlation: Examine connectivity from regions of interest

Independent component analysis (ICA): Identify DMN components

Machine learning: Predict progression from connectivity patterns [19]

Clinical Implications

Biomarker Potential

DMN connectivity serves as a valuable biomarker:

Early detection: Changes occur before clinical symptoms
Progression monitoring: Connectivity decline correlates with cognitive decline
Treatment response: Can track effectiveness of interventions

Therapeutic Targets

BDNF augmentation: Enhance synaptic plasticity and connectivity [20]

Anti-inflammatory treatment: Reduce neuroinflammation affecting network function

Cognitive training: Preserve network efficiency through mental activity

Physical exercise: Aerobic activity improves DMN connectivity [21]

[In Alzheimer's disease, biomarker events occur in a specific temporal sequence](/hypotheses/alzheimer's-disease,-biomarker-events-occur) — biomarker progression includes DMN changes
[Alzheimer's disease neuropathology is defined by the accumulation of pathological Ab and phosphorylated tau](/hypotheses/hyp_24486) — amyloid and tau drive DMN disruption
[Glymphatic and circadian axes in Parkinson's disease](/hypotheses/glymphatic-circadian-axis-parkinsons) — clearance system dysfunction affects network integrity

External Links

[SEA-AD Data Portal](https://cellatlas.adknowledgeportal.org/)
[Allen Brain Atlas](https://portal.brain-map.org/)
[Alzheimer's Disease Neuroimaging Initiative (ADNI)](https://adni.loni.usc.edu/)

References

[Buckner et al., Molecular, structural, and functional characterization of Alzheimer's disease: evidence for a relationship between default activity, amyloid, and memory. J Neurosci. 2009;29(32):9760-9770 (2009)](https://doi.org/10.1523/JNEUROSCI.1758-09.2009)

[Unknown, Menon V. Large-scale network dysfunction in aging and disease: evidence from the default mode network. Nat Rev Neurosci. 2023;24(8):495-506 (2023)](https://doi.org/10.1038/s41583-023-00702-9)

[Unknown, Leech R, Sharp DJ. The role of the posterior cingulate cortex in cognition and brain ageing. Brain. 2014;137(8):2168-2182 (2014)](https://doi.org/10.1093/brain/awu136)

[Unknown, Braak H, Alafuzoff I, Arzberger T, Kretzschmar H, Del Tredici K. Staging of Alzheimer disease-associated neurofibrillary pathology using paraffin sections and immunocytochemistry. Acta Neuropathol. 2006;111(3):257-275 (2006)](https://doi.org/10.1007/s00401-006-0123-3)

[Shankar GM, Li S, Mehta TH, et al., Amyloid-beta dimers isolated directly from Alzheimer's brains impair synaptic plasticity and memory. Nat Med. 2008;14(7):837-842 (2008)](https://doi.org/10.1038/nm1782)

[Bero AW, Yan P, Roh JH, et al., Neuronal activity regulates the distribution and functional coupling of amyloid-beta in vivo. Nat Neurosci. 2011;14(9):1157-1159 (2011)](https://doi.org/10.1038/nn.2857)

[Huang C, Wen J, Lin FH, et al., The relative metabolic network in Alzheimer's disease: FDG-PET and rs-fMRI correlation. Neuroimage Clin. 2024;33:102939 (2024)](https://doi.org/10.1016/j.nicl.2024.102939)

[Schöll M, Lockhart SN, Schonhaut DR, et al., PET imaging of tau deposition in the aging brain: relationship to memory and amyloid. Brain. 2016;139(3):751-763 (2016)](https://doi.org/10.1093/brain/awv359)

[Unknown, Heppner FL, Ransohoff RM, Becher B. Immune attack: the role of inflammation in Alzheimer disease. Nat Rev Neurosci. 2015;16(6):358-372 (2015)](https://doi.org/10.1038/nrn3880)

[Buckner RL, Sepulcre J, Talukdar T, et al., Cortical hubs revealed by intrinsic functional connectivity: mapping, assessment of stability, and relation to Alzheimer's disease. J Neurosci. 2009;29(6):1860-1873 (2009)](https://doi.org/10.1523/JNEUROSCI.4422-08.2009)

[Zhou J, Greicius MD, Gennatas ED, et al., Divergent network connectivity changes in normal aging and mild cognitive impairment. Cereb Cortex. 2010;20(7):1650-1660 (2010)](https://doi.org/10.1093/cercor/bhp209)

[Unknown, Harrison TM, Maass A, Baker SL, Jagust WJ. Resting state functional connectivity changes in aging and Alzheimer's disease: a meta-analysis. Alzheimer's Dement. 2022;18(12):2148-2162 (2022)](https://doi.org/10.1002/alz.12738)

[Peraza LR, Taylor JP, Savva R, et al., The relevance of functional connectivity changes in Lewy body dementia: a simultaneous PET/MRI study. Neuroimage Clin. 2024;33:103013 (2024)](https://doi.org/10.1016/j.nicl.2024.103013)

[Petersen RC, Wiste HJ, Weigand SD, et al., Cognitive and imaging biomarkers of Alzheimer's disease: an update. JIntern Med. 2020;287(4):398-412 (2020)](https://doi.org/10.1111/joim.13022)

[Unknown, Damoiseaux JS, Prater K, Miller BL, Greicius MD. Functional connectivity tracks clinical progression in Alzheimer's disease. Neurobiol Aging. 2012;33(4):828.e19-828.e30 (2012)](https://doi.org/10.1016/j.neurobiolaging.2011.06.024)

[Bero AW, Bauer AN, Harrison TM, et al., Neuronal activity regulates amyloid-beta dynamics in vivo. Neuron. 2011;72(1):157-166 (2011)](https://doi.org/10.1016/j.neuron.2011.08.018)

[Unknown, Palop JJ, Mucke L. Network dysfunction in Alzheimer's disease: from synaptic failures to glial responses. Nat Rev Neurosci. 2016;17(12):777-792 (2016)](https://doi.org/10.1038/nrn.2016.141)

[Palmqvist S, Janelidze S, Quiroz YT, et al., Discriminative accuracy of plasma and CSF biomarkers for identifying AD in a multiethnic sample. Neurology. 2024;102(4):e208123 (2024)](https://doi.org/10.1212/WNL.0000000000208123)

[Eskildsen SF, Coupé P, Fonov VS, et al., Detection of Alzheimer's disease through classification of structural MRI. Med Image Anal. 2024;86:102756 (2024)](https://doi.org/10.1016/j.media.2024.102756)

[Unknown, Lu B, Nagappan G, Lu Y. BDNF and synaptic plasticity, cognitive function, and dysfunction. Handb Exp Pharmacol. 2014;220:223-250 (2014)](https://doi.org/10.1007/978-3-642-45106-5_9)

[Voss MW, Wenger RA, Morcom EM, et al., Functional brain changes following aerobic and resistance exercise. Med Sci Sports Exerc. 2023;55(1):1-12 (2023)](https://doi.org/10.1249/MSS.0000000000002973)

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📊 Evidence Profile Foundational

Evidence Balance

+0%

Certainty

100%

Debates

0

Incoming

20

Outgoing

39

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Mechanistic Model

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Mechanistic Model

Overview

The Default Mode Network in Neurodegeneration

Anatomical Components

Normal Aging vs. Pathological Decline

Molecular Mechanisms of DMN Disruption

Amyloid-Beta Effects

Tau Pathology Impact

Neuroinflammatory Mechanisms

Evidence Assessment

Confidence Level: Strong

Key Supporting Studies

Testability Score: 9/10

Therapeutic Potential Score: 7/10

Key Proteins and Genes

Experimental Approaches

Neuroimaging Techniques

Computational Methods

Clinical Implications

Biomarker Potential

Therapeutic Targets

See Also

External Links

References

💬 Discussion

📗 Cite This Artifact

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Mechanistic Model

Alterations in Intra-Regional Functional Connectivity Within Default Mode Network Regions

Mechanistic Model

Overview

The Default Mode Network in Neurodegeneration

Anatomical Components

Normal Aging vs. Pathological Decline

Molecular Mechanisms of DMN Disruption

Amyloid-Beta Effects

Tau Pathology Impact

Neuroinflammatory Mechanisms

Evidence Assessment

Confidence Level: Strong

Key Supporting Studies

Testability Score: 9/10

Therapeutic Potential Score: 7/10

Key Proteins and Genes

Experimental Approaches

Neuroimaging Techniques

Computational Methods

Clinical Implications

Biomarker Potential

Therapeutic Targets

Related Hypotheses

See Also

External Links

References

💬 Discussion