SOBA: Development and testing of a soluble oligomer binding assay for detection of amyloidogenic toxic oligomers

Shea, Dylan; Colasurdo, Elizabeth; Smith, Alec S.T.; Paschall, Courtnie; Jayadev, Suman; Keene, C. Dirk; Galasko, Douglas; Li, Ge; Peskind, Elaine R.; Daggett, Valerie

doi:10.1073/pnas.2213157119

Cited by 35 publications

(38 citation statements)

References 38 publications

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“…The application of a new blood test, a not complicated binding assay, has recently been published for very early detection of soluble toxic Aβ peptides (SOBA) [ 115 ]. Further studies should demonstrate the suitability of the SOBA method for identifying patients at risk of cognitive decline.…”

Section: Alzheimer’s Diseasementioning

confidence: 99%

New Pathways Identify Novel Drug Targets for the Prevention and Treatment of Alzheimer’s Disease

Penke

Szücs

Bogár³

2023

IJMS

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Alzheimer’s disease (AD) is an incurable, progressive neurodegenerative disorder. AD is a complex and multifactorial disease that is responsible for 60–80% of dementia cases. Aging, genetic factors, and epigenetic changes are the main risk factors for AD. Two aggregation-prone proteins play a decisive role in AD pathogenesis: β-amyloid (Aβ) and hyperphosphorylated tau (pTau). Both of them form deposits and diffusible toxic aggregates in the brain. These proteins are the biomarkers of AD. Different hypotheses have tried to explain AD pathogenesis and served as platforms for AD drug research. Experiments demonstrated that both Aβ and pTau might start neurodegenerative processes and are necessary for cognitive decline. The two pathologies act in synergy. Inhibition of the formation of toxic Aβ and pTau aggregates has been an old drug target. Recently, successful Aβ clearance by monoclonal antibodies has raised new hopes for AD treatments if the disease is detected at early stages. More recently, novel targets, e.g., improvements in amyloid clearance from the brain, application of small heat shock proteins (Hsps), modulation of chronic neuroinflammation by different receptor ligands, modulation of microglial phagocytosis, and increase in myelination have been revealed in AD research.

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Section: Alzheimer’s Diseasementioning

confidence: 99%

New Pathways Identify Novel Drug Targets for the Prevention and Treatment of Alzheimer’s Disease

Penke

Szücs

Bogár³

2023

IJMS

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“…Based on this discrimination between different Aβ conformers (figure 9 b,c ), we explored the detection of toxic oligomers in biological fluids, including cerebrospinal fluid (CSF) and blood. SOBA was able to distinguish between individuals with mild cognitive impairment and moderate to severe AD from non-cognitively impaired controls in both CSF and plasma [84]. The generality of the approach was tested by modifying SOBA to detect α-sheet containing α-synuclein oligomers in samples from patients with PD with excellent discrimination between control and PD cases [84].…”

Section: α-Sheet In Amyloid Systemsmentioning

confidence: 99%

“…SOBA was able to distinguish between individuals with mild cognitive impairment and moderate to severe AD from non-cognitively impaired controls in both CSF and plasma [84]. The generality of the approach was tested by modifying SOBA to detect α-sheet containing α-synuclein oligomers in samples from patients with PD with excellent discrimination between control and PD cases [84].…”

Section: α-Sheet In Amyloid Systemsmentioning

confidence: 99%

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The role of α-sheet structure in amyloidogenesis: characterization and implications

Prosswimmer

Daggett

2022

Open Biol.

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Amyloid diseases are linked to protein misfolding whereby the amyloidogenic protein undergoes a conformational change, aggregates and eventually forms amyloid fibrils. While the amyloid fibrils and plaques are hallmarks of these diseases, they typically form late in the disease process and do not correlate with disease. Instead, there is growing evidence that smaller, soluble toxic oligomers form prior and appear to be early triggers of the molecular pathology underlying these diseases. Nearly 20 years ago, we proposed the α-sheet hypothesis after discovering that the early conformational changes observed during atomistic molecular dynamics simulations involve the formation of a non-standard protein structure, α-sheet. Furthermore, we proposed that toxic oligomers contain α-sheet structure and that preferentially targeting this structure could neutralize the toxicity, prevent further aggregation and serve as the basis for early detection of disease. Here, we present the origin of the α-sheet hypothesis and describe α-sheet structure and the corresponding mechanisms of conversion. We discuss experimental studies demonstrating that both mammalian and bacterial amyloid systems form α-sheet oligomers before converting to conventional β-sheet fibrils. Furthermore, we show that the process can be inhibited with de novo designed α-sheet peptides complementary to the structure in the toxic oligomers.

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“…Aβ*56 is but one of many variants of brain-derived Aβ oligomers. Other brain-derived, oligomeric variants include dimers and trimers 3 , prefibrillar oligomers that bind A11 antibodies 4 , amylospheroids 5 , globulomers 6 , fibrillar oligomers that bind OC antibodies 7 , protofibrillar oligomers that bind mAb158/lecanumab antibodies 8 , intraneuronal oligomers that bind NU-1 anti-ADDL antibodies 9 , annular protofibrils 10 , amyloid pores 11 , oligomers that bind crenezumab 12 , oligomers that bind aducanumab 13 , oligomers that bind ACU3B3/ACU193 anti-ADDL antibodies 14 , oligomers that bind α-sheets 15 , and oligomers that bind JD1 antibodies 16 , whose structure, spatial distribution, temporal expression, biogenesis, and effects on brain function are topics of active study with important therapeutic implications.…”

Section: Introductionmentioning

confidence: 99%

Aβ*56 is a stable oligomer that correlates with age-related memory loss in Tg2576 mice

Ashe

Liu

Lapcinski

et al. 2023

Preprint

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Amyloid-beta (Abeta) oligomers consist of fibrillar and non-fibrillar soluble assemblies of the Abeta peptide. Tg2576 human amyloid precursor protein (APP)-expressing transgenic mice modeling Alzheimer disease produce Abeta*56, a non-fibrillar Abeta assembly that has been shown by several groups to relate more closely to memory deficits than plaques. Previous studies did not decipher specific forms of Abeta present in Abeta*56. Here, we confirm and extend the biochemical characterization of Abeta*56. We used anti-Abeta(1-x), anti-Abeta(x-40), and A11 anti-oligomer antibodies in conjunction with western blotting, immunoaffinity purification, and size-exclusion chromatography to probe aqueous brain extracts from Tg2576 mice of different ages. We found that Abeta*56 is a ~56-kDa, SDS-stable, A11-reactive, non-plaque-related, water-soluble, brain-derived oligomer containing canonical Abeta(1-40) that correlates with age-related memory loss. The unusual stability of this high molecular-weight oligomer renders it an attractive candidate for studying relationships between molecular structure and effects on brain function.

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SOBA: Development and testing of a soluble oligomer binding assay for detection of amyloidogenic toxic oligomers

Cited by 35 publications

References 38 publications

New Pathways Identify Novel Drug Targets for the Prevention and Treatment of Alzheimer’s Disease

New Pathways Identify Novel Drug Targets for the Prevention and Treatment of Alzheimer’s Disease

The role of α-sheet structure in amyloidogenesis: characterization and implications

Aβ*56 is a stable oligomer that correlates with age-related memory loss in Tg2576 mice

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