Brain amyloid-β oligomers in ageing and Alzheimer’s disease

Lesné, Sylvain; Sherman, Mathew A.; Grant, Marianne; Kuskowski, Michael A.; Schneider, Julie A.; Bennett, David A.; Ashe, Karen H.

doi:10.1093/brain/awt062

Cited by 377 publications

(402 citation statements)

References 57 publications

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“…Brain specimens and subject characteristics were described previously (65). The Religious Orders Study was approved by the Institutional Review Board of Rush University Medical Center and all participants gave informed consent, signed an Anatomical Gift Act for organ donation, and signed a repository consent to allow data and biospecimen sharing.…”

Section: Methodsmentioning

confidence: 99%

Selective lowering of synapsins induced by oligomeric α-synuclein exacerbates memory deficits

Larson

Greimel

Amar

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Mounting evidence indicates that soluble oligomeric forms of amyloid proteins linked to neurodegenerative disorders, such as amyloid-β (Aβ), tau, or α-synuclein (αSyn) might be the major deleterious species for neuronal function in these diseases. Here, we found an abnormal accumulation of oligomeric αSyn species in AD brains by custom ELISA, size-exclusion chromatography, and nondenaturing/denaturing immunoblotting techniques. Importantly, the abundance of αSyn oligomers in human brain tissue correlated with cognitive impairment and reductions in synapsin expression. By overexpressing WT human αSyn in an AD mouse model, we artificially enhanced αSyn oligomerization. These bigenic mice displayed exacerbated Aβ-induced cognitive deficits and a selective decrease in synapsins. Following isolation of various soluble αSyn assemblies from transgenic mice, we found that in vitro delivery of exogenous oligomeric αSyn but not monomeric αSyn was causing a lowering in synapsin-I/II protein abundance. For a particular αSyn oligomer, these changes were either dependent or independent on endogenous αSyn expression. Finally, at a molecular level, the expression of synapsin genes SYN1 and SYN2 was down-regulated in vivo and in vitro by αSyn oligomers, which decreased two transcription factors, cAMP response element binding and Nurr1, controlling synapsin gene promoter activity. Overall, our results demonstrate that endogenous αSyn oligomers can impair memory by selectively lowering synapsin expression.α-synuclein | oligomer | memory | Alzheimer's disease | synapsins

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Section: Methodsmentioning

confidence: 99%

Selective lowering of synapsins induced by oligomeric α-synuclein exacerbates memory deficits

Larson

Greimel

Amar

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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“…A␤ is the major protein component of senile plaques observed in the brain of Alzheimer's disease (AD) subjects, and soluble A␤ oligomer(s) are thought to impair synaptic functions prior to A␤ deposition in the brain (17)(18)(19). Therefore, to understand AD pathogenesis and develop effective AD ther-…”

Section: Edited By F Anne Stephensonmentioning

confidence: 99%

“…1B). To this end, we transiently expressed mAPP-(695) and hAPP-(695) in mouse N2a and human SHSY5Y neuroblastoma cells, and then analyzed the secreted A␤ forms by MALDI-TOF/MS following immunoprecipitation with pan-A␤ antibody 4G8, which recognizes an epitope within the A␤ (17)(18)(19)(20)(21)(22)(23)(24) region. We identified several A␤ species in which the amino-terminal amino acid was Asp (A␤(1-XX), a product of ␤-site cleavage) or Glu (A␤(11-XX), a product of ␤Ј-site cleavage).…”

Section: Alternative Cleavage Of App By Bace1 Depends On the Amino Acmentioning

confidence: 99%

“…into the medium (1 ml) and mixed mouse CSF (C57BL/6, 100 l) were recovered by immunoprecipitation with anti-pan A␤ antibody 4G8, which was raised to A␤ [17][18][19][20][21][22][23][24] epitope (BioLegend, San Diego, CA) plus Protein G-Sepharose 4B (GE Healthcare Bio-Sciences) following pre-clearing with the same beads without antibody. The beads were sequentially washed, and the bound proteins were eluted with trifluoroacetic acid/acetonitrile/water (1:20: 20) saturated with sinapinic acid as described (51).…”

Section: Immunoprecipitation Maldi-tof/ms (Ip-ms) and -Ms/ms Analysismentioning

confidence: 99%

“…Cleavage of CTF␤Ј/C89 by ␥-secretase yields A␤(11-XX), which lacks the first 10 amino acids of the A␤ domain. This ␤Ј-site cleavage of APP is also thought to be amyloidolytic, because the structural analysis suggests that A␤(11-40) and A␤(11-42) are less toxic than A␤(1-40) and A␤(1-42) (14), and the A␤(11-42) showed reduced neurotoxicity compared with A␤(1-42) and A␤(3-42) in a study with transgenic fly (15), although the neurotoxicity of A␤(11-XX) in human brain is controversial (16).A␤ is the major protein component of senile plaques observed in the brain of Alzheimer's disease (AD) subjects, and soluble A␤ oligomer(s) are thought to impair synaptic functions prior to A␤ deposition in the brain (17)(18)(19). Therefore, to understand AD pathogenesis and develop effective AD ther-…”

mentioning

confidence: 99%

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Alternative Selection of β-Site APP-Cleaving Enzyme 1 (BACE1) Cleavage Sites in Amyloid β-Protein Precursor (APP) Harboring Protective and Pathogenic Mutations within the Aβ Sequence

Kimura¹,

Hata²,

Suzuki

2016

Journal of Biological Chemistry

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Edited by F. Anne Stephenson␤␤-Site APP-cleaving enzyme 1 (BACE1), 3 a type I transmembrane aspartic protease, was identified as the ␤-secretase that cleaves amyloid ␤-protein precursor (APP) to generate neurotoxic amyloid ␤ (A␤) (1-4). BACE1 cleaves APP at the peptide bond between Met 671 and Asp 672 (␤-site; sequence numbering refers to the APP770 isoform) (5, 6). This primary cleavage of APP generates the secreted form of the amino-terminal large fragment (sAPP␤) and the membrane-associated carboxyl-terminal fragment (CTF␤/C99) (reviewed in Ref. 7). Because CTF␤/C99 includes the complete amino acid sequence of the A␤ region, and subsequent cleavage of CTF␤/C99 by ␥-secretase generates the A␤(1-XX) peptides (A␤1 indicates the position of Asp 672 ), the ␤-site cleavage is referred to as amyloidogenic processing of APP (reviewed in Ref. 8). Alternatively, APP can also be cleaved by ␣-secretase (mainly ADAM10/17), at the peptide bond between Lys 687 and Leu 688 , generating sAPP␣ and CTF␣/C83 including the A␤(17-XX) region; accordingly, this cleavage is referred to as amyloidolytic processing of APP (9 -11). BACE1 also cleaves APP at another peptide bond between Tyr 681 and Gln 682 (␤Ј-site), resulting in generation of sAPP␤Ј and CTF␤Ј/C89 (12, 13). Cleavage of CTF␤Ј/C89 by ␥-secretase yields A␤(11-XX), which lacks the first 10 amino acids of the A␤ domain. This ␤Ј-site cleavage of APP is also thought to be amyloidolytic, because the structural analysis suggests that A␤(11-40) and A␤(11-42) are less toxic than A␤(1-40) and A␤(1-42) (14), and the A␤(11-42) showed reduced neurotoxicity compared with A␤(1-42) and A␤(3-42) in a study with transgenic fly (15), although the neurotoxicity of A␤(11-XX) in human brain is controversial (16).A␤ is the major protein component of senile plaques observed in the brain of Alzheimer's disease (AD) subjects, and soluble A␤ oligomer(s) are thought to impair synaptic functions prior to A␤ deposition in the brain (17)(18)(19). Therefore, to understand AD pathogenesis and develop effective AD ther-

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Association of Cortical β-Amyloid Protein in the Absence of Insoluble Deposits With Alzheimer Disease

Petyuk

Tasaki

et al. 2019

JAMA Neurol

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IMPORTANCE β-Amyloid deposits are a pathologic hallmark of Alzheimer disease (AD). However, the extent to which cortical β-amyloid protein in the absence of insoluble deposits is associated with classic features of AD appear to be unknown. OBJECTIVE To examine the associations of cortical β-amyloid protein in the absence of insoluble deposits with cognitive decline, neurofibrillary tangles, other age-associated neuropathologic conditions, and APOE. DESIGN, SETTING, AND PARTICIPANTS This analysis combines data from 2 community-based clinicopathologic cohort studies of aging. The Religious Orders Study started in 1994, and the Rush Memory and Aging Project started in 1997. Both studies are ongoing. Participants without known dementia were enrolled and agreed to annual clinical evaluations and brain donation after death. Primary analyses focused on individuals without β-amyloid deposits. Data analyses occurred in mid-September 2018. MAIN OUTCOMES AND MEASURES β-Amyloid protein abundance was measured by targeted proteomics using selected reaction monitoring. β-Amyloid deposits were detected using immunohistochemistry. Other neuropathologic indices were quantified via uniform structured evaluation. Linear mixed models were used to examine the association of β-amyloid protein with cognitive decline. Regression models examined the protein associations with neuropathologic outcomes and the APOE genotype. RESULTS By mid-September 2018, 3575 older persons were enrolled, and 1559 had died and undergone brain autopsy. Proteomic data were collected in 1208 individuals, and 5 with missing cognitive scores were excluded. Of the remaining 1203, primary analyses focused on 148 individuals (12.3%) without β-amyloid deposits. In this group, the mean (SD) age at death was 87.0 (7.0) years, and 84 individuals (56.8%) were women. In the absence of β-amyloid deposits, we did not observe an association of β-amyloid protein with decline in episodic memory, but the protein was associated with faster rates of decline in processing speed (mean [SE] change, −0.014 [0.005]; P = .008) and visuospatial abilities (mean [SE] change, −0.013 [0.005]; P = .006). We did not observe protein association with paired helical filament tau tangle density. The protein was associated with amyloid angiopathy (odds ratio, 1.38 [95% CI, 1.15-1.67]; P < .001) but no other brain pathology. The associations with cognitive decline were unchanged after controlling for amyloid angiopathy. Neither APOE ε4 nor a polygenic Alzheimer risk score was associated with β-amyloid protein. CONCLUSIONS AND RELEVANCE Cortical β-amyloid protein was associated with faster cognitive decline in the absence of β-amyloid deposits, which supports the role of cortical soluble β-amyloid as a neurotoxic agent in aging. The lack of protein association with paired helical filament tau tangles, episodic memory decline, or strong genetic drivers of deposited β-amyloid suggests an underlying neuropathologic change that may differ from that of AD.

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Brain amyloid-β oligomers in ageing and Alzheimer’s disease

Cited by 377 publications

References 57 publications

Selective lowering of synapsins induced by oligomeric α-synuclein exacerbates memory deficits

Selective lowering of synapsins induced by oligomeric α-synuclein exacerbates memory deficits

Alternative Selection of β-Site APP-Cleaving Enzyme 1 (BACE1) Cleavage Sites in Amyloid β-Protein Precursor (APP) Harboring Protective and Pathogenic Mutations within the Aβ Sequence

Association of Cortical β-Amyloid Protein in the Absence of Insoluble Deposits With Alzheimer Disease

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