Cross-Seeding Interaction between β-Amyloid and Human Islet Amyloid Polypeptide

Hu, Rundong; Zhang, Mingzhen; Chen, Hong; Jiang, Binbo; Zheng, Jie

doi:10.1021/acschemneuro.5b00192

Cited by 81 publications

(87 citation statements)

References 62 publications

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“…As a control, for the pure Aβ 1-42 peptides incubated at 25 µΜ, ThT profile showed a typical nucleation-polymerization aggregation profiles, consisting of a very short lag phase of 1 h, a rapid growth phase between 2-7 h, and a final equilibrium phase after 7 h, where the final ThT fluorescence intensity reflects the amount of fibrillar material formed. Since pure Aβ at 25 µM experienced rapid aggregation at the early stage, lag phase only existed for a very short time period (~1 h), consistent with our previous works 12, 36,45 . In Fig.…”

Section: Hp-β-cd Inhibits Aβ42 Fibrillizationsupporting

confidence: 90%

“…To prevent reinventing the wheel, we proposed to search the existing drug database for other diseases to identify potential Aβ inhibitors. Since pure Aβ at 25 µM experienced rapid aggregation at the early stage, lag phase only existed for a very short time period (~1 h), consistent with our previous works 12, 36,45 . Experimental data showed that HP-β-CD were not only nontoxic to cells, but also greatly inhibited Aβ fibrillation and reduced Aβ-induced toxicity in a concentration-dependent manner.…”

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confidence: 90%

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HP-β-cyclodextrin as an inhibitor of amyloid-β aggregation and toxicity

Ren

Jiang

et al. 2016

Phys. Chem. Chem. Phys.

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Amyloid deposits of misfolded amyloid-β protein (Aβ) on neuronal cells are a pathological hallmark of Alzheimer's disease (AD). Prevention of the abnormal Aβ aggregation has been considered as a promising therapeutic strategy for AD treatment. To prevent reinventing the wheel, we proposed to search the existing drug database for other diseases to identify potential Aβ inhibitors. Herein, we reported the inhibitory activity of HP-β-cyclodextrin (HP-β-CD), a well-known sugar used in drug delivery, genetic vector, environmental protection and treatment of Niemann-Pick disease type C1 (NPC1), against Aβ1-42 aggregation and Aβ-induced toxicity, with the aim of adding a new function as a sugar-based Aβ inhibitor. Experimental data showed that HP-β-CD molecules were not only nontoxic to cells, but also greatly inhibited Aβ fibrillization and reduced Aβ-induced toxicity in a concentration-dependent manner. At an optimal molar ratio of Aβ : HP-β-CD = 1 : 2, HP-β-CD enabled the reduction of 60% of Aβ fibrils and increased the cell viability to 92%. Such concentration-dependent inhibitor capacity of HP-β-CD was likely attributed to several combined effects, including the enhancement of Aβ-HP-β-CD interactions, prevention of structural transition of Aβ peptides towards β-sheet structures, and reduction of self-aggregation of HP-β-CD. In parallel, molecular simulations further revealed the atomic details of HP-β-CD interacting with the Aβ oligomer, showing that HP-β-CD had a high tendency to interact with hydrophobic residues of Aβ in two β-strands and the N-terminal tail. More importantly, we identified that the inner hydrophobic cavity of HP-β-CD was a key active site for Aβ inhibition. Once the inner cavity of HP-β-CD was blocked by a small hydrophobic molecule of ferulic acid, HP-β-CD completely lost its inhibition capacity against Aβ. Given the already established pharmaceutical functions of HP-β-CD in drug delivery, our findings suggest that HP-β-CD has great potential to be designed as a sugar-based Aβ inhibitor.

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Section: Hp-β-cd Inhibits Aβ42 Fibrillizationsupporting

confidence: 90%

supporting

confidence: 90%

HP-β-cyclodextrin as an inhibitor of amyloid-β aggregation and toxicity

Ren

Jiang

et al. 2016

Phys. Chem. Chem. Phys.

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“…Centrifuge the Aβ-hIAPP mixture solution at 13,148 × g for 30 min at 4 °C to remove any potential oligomers, followed by extracting 90% of the top Aβ-hIAPP solution (1.8 mL) in the monomeric state of both peptides for cross-seeding tests [23] (Fig 2). …”

Section: Methodsmentioning

confidence: 99%

Experimental and Computational Protocols for Studies of Cross-Seeding Amyloid Assemblies

Ren

Zhang

et al. 2018

Methods in Molecular Biology

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Alzheimer's disease (AD) and type 2 diabetes (T2D) are two common protein aggregation diseases. Compelling evidence has shown a link between AD and T2D, which may derive from interspecies cross-sequence interactions between amyloid-β peptide (Aβ), associated with AD, and human islet amyloid polypeptide (hIAPP), associated with T2D. Herein, we present experimental and computational protocols and tools to study the aggregate structures and kinetics, conformational conversion, and molecular interactions of Aβ-hIAPP mixtures. These protocols could be generally applied to other cross-seeding behaviors of amyloid peptides.

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“…In vitro, l'hété-ronucléation d'Ab par d'autres protéines amyloïdes telles que la caséine, l'a-synucléine (impliquée dans la maladie de Parkinson) ou des dépôts amyloïdes des îlots de Langerhans pancréatiques (« Islet Amyloid Protein » (IAPP, s'accumulant dans le diabète de type II)) a été montrée (O'Nuallain et al 2004;Ono et al 2014;Hu et al 2015). Les données in vivo sont plus contradictoires.…”

Section: Risques D'ensemencement Par Des Hétéronucléantsunclassified

Transmission des lésions amyloïdes de la maladie d’Alzheimer : apports des modèles animaux

Gary¹,

Comoy²,

Dhénain³

2017

bavf

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Depuis la découverte du caractère transmissible des maladies à prions, d'autres protéinopathies cérébrales ont été soupçonnées d'être similairement transmissibles. La maladie d'Alzheimer (MA) est caractérisée par des dépôts cérébraux de peptides b-amyloïdes (Ab) et de protéines Tau hyperphosphorylées, respectivement en plaques amyloïdes et dégénérescences neurofibrillaires. Bien qu'aucune étude épidémiologique ne montre que la MA se transmette entre individus, plusieurs études ont récemment soulevé des soupçons de transmission iatrogène des dépôts b-amyloïdes chez l'Homme. Elles suggèrent que le changement de conformation (ou mépliement) de l'Ab et son agrégation se produit par des mécanismes de nucléation-élongation et de propagation, similaires à ceux décrits pour les maladies à prions. Ici, nous présentons une revue de la littérature démontrant à partir d'études in vivo la pertinence des mécanismes de mépliement et agrégation de type prion pour la pathologie b-amyloïde.

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Cross-Seeding Interaction between β-Amyloid and Human Islet Amyloid Polypeptide

Cited by 81 publications

References 62 publications

HP-β-cyclodextrin as an inhibitor of amyloid-β aggregation and toxicity

HP-β-cyclodextrin as an inhibitor of amyloid-β aggregation and toxicity

Experimental and Computational Protocols for Studies of Cross-Seeding Amyloid Assemblies

Transmission des lésions amyloïdes de la maladie d’Alzheimer : apports des modèles animaux

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