Heparan Sulfate Proteoglycans (HSPGs) Serve as the Mediator Between Monomeric Tau and Its Subsequent Intracellular ERK1/2 Pathway Activation

Song, Liqing; Oseid, Daniel E.; Wells, Evan A.; Coaston, Troy; Robinson, Anne S.

doi:10.1007/s12031-021-01943-2

Cited by 14 publications

(28 citation statements)

References 91 publications

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“…The presence of negatively charge sialic acids on apoE repels the negatively charge heparin, thus reducing its binding. HSPGs not only promote Aβ aggregation, but also promote glia cell in ammation response and the propagation of toxic tau species [40]. They further veri ed that apoE3ch produced the lowest levels of Aβ 42 toxic oligomers, then further veri ed apoE3ch had the lowest binding a nity to heparin among the other three isoforms (E2 < E3 < E4) [42].…”

Section: Discussionmentioning

confidence: 92%

“…Heparan sulfate proteoglycans (HSPGs) recognize apoE's LDLR binding region and affect Aβ cellular uptake [40]. Interestingly, a new apoE isoform stemming from a unique mutation in the APOE3 gene and resulting in the replacement of Arg 136 with Ser 136 , dubbed Christchurch ApoE3 (APOE3ch), was shown to have a 98% reduced a nity for HSPGs and 60% reduced a nity for LDLR, indicating that ApoE3ch has a LDLR binding a nity between apoE2 and apoE3 [41].…”

Section: Discussionmentioning

confidence: 99%

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An Association of CSF Apolipoprotein E glycosylation and amyloid-beta 42 in individuals who carry the APOE4 allele

Meuret

Hu²,

Smadi

et al. 2022

Preprint

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Carrying the Apolipoprotein E (apoE) ε4 allele is associated with an increased risk of cerebral amyloidosis, but the degree to which apoE glycosylation affects its development is not clear. In a previous pilot study, we identified distinct total and secondary isoform-specific cerebral spinal fluid (CSF) apoE glycosylation profiles, with the apoE4 isoform having the lowest glycosylation percentage (E2 > E3 > E4). In this work, we extend the analysis to a larger cohort of individuals (n = 106), utilizing matched plasma and CSF samples with clinical measures of AD biomarkers. The results confirm the isoform-specific glycosylation of apoE in CSF, resulting from secondary CSF apoE glycosylation patterns. CSF apoE glycosylation percentages positively correlated with CSF Aβ42 levels (r = 0.53, p < 0.0001). These correlations were not observed for plasma apoE glycosylation. CSF total and secondary apoE glycosylation percentages also correlated with the concentration of CSF small high-density lipoprotein (HDL) particles which we have previously shown to be correlated with CSF Aβ42 levels and measures of cognitive function. Desialylation of apoE3 purified from CSF showed increased binding affinity to heparin. These results indicate that apoE glycosylation has a new and important role in influencing brain Aβ metabolism and can be a potential target of treatment.

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Section: Discussionmentioning

confidence: 92%

Section: Discussionmentioning

confidence: 99%

An Association of CSF Apolipoprotein E glycosylation and amyloid-beta 42 in individuals who carry the APOE4 allele

Meuret

Hu²,

Smadi

et al. 2022

Preprint

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“…Compromising heparan sulfate biosynthesis in mature neurons or ectopic expression of an enzyme that degrades heparan sulfate suppress the accumulation of amyloid in mouse models of AD ( Jendresen et al, 2015 ; Liu et al, 2016 ). Later, it was discovered that HSPGs internalize Tau, affect Tau aggregation and release of misfolded Tau to neighboring cells, providing a mechanism of intercellular spread mediated by this protein ( Holmes et al, 2013 ; Mah et al, 2021 ; Huynh et al, 2022 ; Song et al, 2022 ). HSPG-mediated uptake of monomeric Tau also activates Erk signaling, promoting pro-inflammatory processes ( Song et al, 2022 ), another potential aspect of this heparan sulfate-mediated process.…”

Section: Heparan Sulfate Proteoglycans In the Context Of Alzheimer’s ...mentioning

confidence: 99%

“…Later, it was discovered that HSPGs internalize Tau, affect Tau aggregation and release of misfolded Tau to neighboring cells, providing a mechanism of intercellular spread mediated by this protein ( Holmes et al, 2013 ; Mah et al, 2021 ; Huynh et al, 2022 ; Song et al, 2022 ). HSPG-mediated uptake of monomeric Tau also activates Erk signaling, promoting pro-inflammatory processes ( Song et al, 2022 ), another potential aspect of this heparan sulfate-mediated process. More recently HSPGs were found to regulate autophagy ( Ning et al, 2015 ; Reynolds-Peterson et al, 2017 ; Reynolds-Peterson et al, 2020 ), and affect lipid accumulation ( Yamashita et al, 2018 ), two processes that are also disrupted in AD.…”

Section: Heparan Sulfate Proteoglycans In the Context Of Alzheimer’s ...mentioning

confidence: 99%

Regulation of autophagy, lipid metabolism, and neurodegenerative pathology by heparan sulfate proteoglycans

Schultheis

Becker²,

Berhanu³

et al. 2023

Front. Genet.

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Heparan sulfate modified proteins or proteoglycans (HSPGs) are an abundant class of cell surface and extracellular matrix molecules. They serve important co-receptor functions in the regulation of signaling as well as membrane trafficking. Many of these activities directly affect processes associated with neurodegeneration including uptake and export of Tau protein, disposition of Amyloid Precursor Protein-derived peptides, and regulation of autophagy. In this review we focus on the impact of HSPGs on autophagy, membrane trafficking, mitochondrial quality control and biogenesis, and lipid metabolism. Disruption of these processes are a hallmark of Alzheimer’s disease (AD) and there is evidence that altering heparan sulfate structure and function could counter AD-associated pathological processes. Compromising presenilin function in several systems has provided instructive models for understanding the molecular and cellular underpinnings of AD. Disrupting presenilin function produces a constellation of cellular deficits including accumulation of lipid, disruption of autophagosome to lysosome traffic and reduction in mitochondrial size and number. Inhibition of heparan sulfate biosynthesis has opposing effects on all these cellular phenotypes, increasing mitochondrial size, stimulating autophagy flux to lysosomes, and reducing the level of intracellular lipid. These findings suggest a potential mechanism for countering pathology found in AD and related disorders by altering heparan sulfate structure and influencing cellular processes disrupted broadly in neurodegenerative disease. Vertebrate and invertebrate model systems, where the cellular machinery of autophagy and lipid metabolism are conserved, continue to provide important translational guideposts for designing interventions that address the root cause of neurodegenerative pathology.

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“…Similarly to CSPGs, HSPGs not only appear in the close neighborhood of β-amyloid plaques, but also co-localize with hyperphosphorilated tau. Actually, HSPGs regulate cellular immune responses to tau protein monomers, which creates a neuroinflammatory environment for tangle formation [ 179 ]. The early accumulation of HSPGs, as well as the related molecular mechanisms in disease development, made HSPGs primary and key players in the unifying hypothesis of Alzheimer’s disease [ 180 , 181 ].…”

Section: Extracellular Matrix Components and Neurodegenerative Diseasesmentioning

confidence: 99%

The Role of Extracellular Matrix in Human Neurodegenerative Diseases

Pintér

Alpár

2022

IJMS

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The dense neuropil of the central nervous system leaves only limited space for extracellular substances free. The advent of immunohistochemistry, soon followed by advanced diagnostic tools, enabled us to explore the biochemical heterogeneity and compartmentalization of the brain extracellular matrix in exploratory and clinical research alike. The composition of the extracellular matrix is critical to shape neuronal function; changes in its assembly trigger or reflect brain/spinal cord malfunction. In this study, we focus on extracellular matrix changes in neurodegenerative disorders. We summarize its phenotypic appearance and biochemical characteristics, as well as the major enzymes which regulate and remodel matrix establishment in disease. The specifically built basement membrane of the central nervous system, perineuronal nets and perisynaptic axonal coats can protect neurons from toxic agents, and biochemical analysis revealed how the individual glycosaminoglycan and proteoglycan components interact with these molecules. Depending on the site, type and progress of the disease, select matrix components can either proactively trigger the formation of disease-specific harmful products, or reactively accumulate, likely to reduce tissue breakdown and neuronal loss. We review the diagnostic use and the increasing importance of medical screening of extracellular matrix components, especially enzymes, which informs us about disease status and, better yet, allows us to forecast illness.

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Heparan Sulfate Proteoglycans (HSPGs) Serve as the Mediator Between Monomeric Tau and Its Subsequent Intracellular ERK1/2 Pathway Activation

Cited by 14 publications

References 91 publications

An Association of CSF Apolipoprotein E glycosylation and amyloid-beta 42 in individuals who carry the APOE4 allele

An Association of CSF Apolipoprotein E glycosylation and amyloid-beta 42 in individuals who carry the APOE4 allele

Regulation of autophagy, lipid metabolism, and neurodegenerative pathology by heparan sulfate proteoglycans

The Role of Extracellular Matrix in Human Neurodegenerative Diseases

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