Synaptic biomarkers in CSF aid in diagnosis, correlate with cognition and predict progression in MCI and Alzheimer's disease

Galasko, Douglas; Xiao, Mei-Fang; Xu, Desheng; Smirnov, Alexander; Salmon, David P.; Dewit, Nele; Vanbrabant, Jeroen; Jacobs, Dirk; Vanderstichele, Hugo; Vanmechelen, Eugeen; Initiative, Alzheimer’s Disease Neuroimaging; Worley, Paul F.

doi:10.1016/j.trci.2019.11.002

Cited by 94 publications

(142 citation statements)

References 48 publications

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“…Synaptotagmin-1 ↑ = In CSF 159,161,158 Alpha-synuclein ↓ R In CSF [163][164][165][166][167][168][169][171][172][173][174][175][176][177][178]180,207,281 , in blood 189,190,278 Oligomeric = ↑ = ↑ S, P,R In CSF 169,174,197,198,207 , in blood 193,[199][200][201][202][203][204] Phosporylated = ↑ ↑ ↑ S In CSF 165,169,174,179,181,207 , in blood 185,203 Postsynaptic Neurogranin ↓ E In CSF 1,3,18,121,150,…”

Section: Conclusion and Future Perspectivementioning

confidence: 99%

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Fluid Biomarkers for Synaptic Dysfunction and Loss

et al. 2020

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Synapses are the site for brain communication where information is transmitted between neurons and stored for memory formation. Synaptic degeneration is a global and early pathogenic event in neurodegenerative disorders with reduced levels of pre- and postsynaptic proteins being recognized as a core feature of Alzheimer’s disease (AD) pathophysiology. Together with AD, other neurodegenerative and neurodevelopmental disorders show altered synaptic homeostasis as an important pathogenic event, and due to that, they are commonly referred to as synaptopathies. The exact mechanisms of synapse dysfunction in the different diseases are not well understood and their study would help understanding the pathogenic role of synaptic degeneration, as well as differences and commonalities among them and highlight candidate synaptic biomarkers for specific disorders. The assessment of synaptic proteins in cerebrospinal fluid (CSF), which can reflect synaptic dysfunction in patients with cognitive disorders, is a keen area of interest. Substantial research efforts are now directed toward the investigation of CSF synaptic pathology to improve the diagnosis of neurodegenerative disorders at an early stage as well as to monitor clinical progression. In this review, we will first summarize the pathological events that lead to synapse loss and then discuss the available data on established (eg, neurogranin, SNAP-25, synaptotagmin-1, GAP-43, and α-syn) and emerging (eg, synaptic vesicle glycoprotein 2A and neuronal pentraxins) CSF biomarkers for synapse dysfunction, while highlighting possible utilities, disease specificity, and technical challenges for their detection.

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Section: Conclusion and Future Perspectivementioning

confidence: 99%

“…In CSF 171,[282][283][284][285][286] , in blood 132,134,135,287,288 Heavy chain ↑ In CSF 286 Emerging Synaptophysin In CSF 44,150,235,236,242 , in blood 277…”

Section: Conclusion and Future Perspectivementioning

confidence: 99%

Fluid Biomarkers for Synaptic Dysfunction and Loss

et al. 2020

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“…Of the 227 DE genes, 17 were dysregulated in all 5 clusters, and an additional 46 were dysregulated in 4 of the 5 clusters (MAST test; adjusted p-value < 0.05; log fold change > 0.1; detection in ≥ 20% of cells) ( Figures 6C and S7). Notably, among the commonly upregulated genes were genes encoding proteins that are biomarkers for neurodegeneration and cognitive decline in AD: NEFL, encoding neurofilament light chain; SNAP25, encoding synaptosomal-associated protein 25, a SNARE complex protein with a role in synaptic vesicle exocytosis; and SYT1, encoding synaptotagmin-1, an integral membrane protein of synaptic vesicles implicated in calcium-dependent vesicular trafficking and exocytosis (Brinkmalm et al, 2014;Davidsson et al, 1996;Galasko et al, 2019;Mattsson et al, 2017;Mattsson et al, 2019;Preische et al, 2019) (Figures 6B and S7; Table S8). Other upregulated genes related to the synaptic vesicle cycle were the synaptotagmin genes STY4 and STY11; SV2B, encoding synaptic vesicle glycoprotein 2B; and BSN, encoding the 9 presynaptic cytomatrix protein bassoon.…”

Section: Dysregulation Of Synaptic Transmission Pathways In Neurons Wmentioning

confidence: 99%

Single-soma transcriptomics of tangle-bearing neurons in Alzheimer’s disease reveals the signatures of tau-associated synaptic dysfunction

Otero-García

Xue

Shakouri

et al. 2020

Preprint

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Aggregation of hyperphosphorylated tau in neurofibrillary tangles (NFTs) is closely associated with neuronal death and cognitive decline in Alzheimer's disease (AD). To define the signatures that distinguish between aggregation-prone and resistant cell states in AD, we developed a FACS-based method for the high-throughput isolation and transcriptome profiling of individual cells with cytoplasmic aggregates and profiled 63,110 somas from human AD brains. By comparing NFTbearing and NFT-free somas within and across neuronal subtypes, we identified the cell-type-specific and shared states. NFT-bearing neurons shared a marked upregulation of genes associated with synaptic transmission, including a core set of 63 genes enriched for synaptic vesicle cycle and transsynaptic signaling, whereas glucose metabolism and oxidative phosphorylation changes were highly neuronal-subtype-specific. Apoptosis was modestly enriched in NFT-bearing neurons despite the strong link between tau and cell death. Our datasets provide a resource for investigating taumediated neurodegeneration and a platform for biomarker and drug target discovery.

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“…Before we figure out the pathway that includes pathological molecular changes and related association, we cannot make a clear definition of the timing. CSF Ng was increased in AD compared to CN or Parkinson's disease frontotemporal dementia and amyotrophic lateral sclerosis [15][16][17].…”

Section: Introductionmentioning

confidence: 89%

“…Ng/BACE1 levels were elevated in both subjective cognitive decline and mild cognitive impairment compared to healthy controls [18], and can distinguish between depression and AD among patients with similar cognitive deficits, along with the classic AD biomarkers [19]. SNAP25 increased in AD or MCI versus CN [12,15]. However Beeri [20] and Shimohama [21] indicated dementia to be associated with reductions in SNAP-25.…”

Section: Introductionmentioning

confidence: 99%

Clinical Utility of the Pathogenesis-related Proteins in Alzheimer’s Disease

Zhou

Fukushima²

2020

Preprint

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The Aβ cascade and alternations of biomarkers in neuro-inflammation, synaptic dysfunction and neuronal injury followed by Aβ have progressed. But the question is how to use the biomarkers. Here, we examine the evidence and pathogenic implications of protein interactions and the time order of alternation. After the deposition of Aβ, the change of tau, NfL and NG is the main alternation and connection to others. The neuro-inflammation, synaptic dysfunction and neuronal injury function is exhibited prior the structural and metabolic changes in the brain following Aβ deposition. The time order of such biomarkers compared to the tau protein is not clear. Despite the close relationship between biomarkers and plaque Aβ deposition, several factors favor one or the other. There is an interaction between the proteins that CSF SNAP-25, VILIP-1 and YKL-40 can predict the brain amyloid burden. The Aβ cascade hypothesis could be the pathway, but not all subjects are converted to AD, even with very high elevated Aβ. The interaction of biomarkers and the time order of change require further research to identify the right subjects and right molecular target for precision medicine therapies.

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Synaptic biomarkers in CSF aid in diagnosis, correlate with cognition and predict progression in MCI and Alzheimer's disease

Cited by 94 publications

References 48 publications

Fluid Biomarkers for Synaptic Dysfunction and Loss

Fluid Biomarkers for Synaptic Dysfunction and Loss

Single-soma transcriptomics of tangle-bearing neurons in Alzheimer’s disease reveals the signatures of tau-associated synaptic dysfunction

Clinical Utility of the Pathogenesis-related Proteins in Alzheimer’s Disease

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Synaptic biomarkers in CSF aid in diagnosis, correlate with cognition and predict progression in MCI and Alzheimer's disease

Cited by 94 publications

References 48 publications

Fluid Biomarkers for Synaptic Dysfunction and Loss

Fluid Biomarkers for Synaptic Dysfunction and Loss

Single-soma transcriptomics of tangle-bearing neurons in Alzheimer’s disease reveals the signatures of tau-associated synaptic dysfunction

Clinical Utility of the Pathogenesis-related Proteins in Alzheimer&rsquo;s Disease

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Clinical Utility of the Pathogenesis-related Proteins in Alzheimer’s Disease