2021
DOI: 10.1021/acsami.1c04163
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Polyoxometalates as Effective Nano-inhibitors of Amyloid Aggregation of Pro-inflammatory S100A9 Protein Involved in Neurodegenerative Diseases

Abstract: Pro-inflammatory and amyloidogenic S100A9 protein is central to the amyloid-neuroinflammatory cascade in neurodegenerative diseases. Polyoxometalates (POMs) constitute a diverse group of nanomaterials, which showed potency in amyloid inhibition. Here, we have demonstrated that two selected nanosized niobium POMs, Nb 10 and TiNb 9 , can act as potent inhibitors of S100A9 amyloid assembly. Kinetics analysis based on ThT fluorescence experiments showed that addition o… Show more

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Cited by 19 publications
(15 citation statements)
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“…( Narasimhan et al, 2011 ; Prudent et al, 2010 ; Prudent et al, 2008 ; Hu et al, 2007 ; Tiago et al, 2007 ; Pezza et al, 2002 ; Judd et al, 2001 ; Sarafianos et al, 1996 ). Owing to the intrinsic limitations of docking methods, atomistic molecular dynamics (MD) simulations have been more recently performed to reveal the driving forces that are responsible for the specific interactions ( Figure 1A )[ ( Solé-Daura et al, 2016 ; Paul et al, 2018 ; Solé-Daura et al, 2020a ; Sciortino et al, 2021 ; Chaudhary et al, 2021 )] Pioneer MD simulations analysed the interaction between model protein hen egg-white lysoszyme (HEWL) and three different POMs, the Ce-substituted Keggin-type anion [PW 11 O 39 Ce(OH 2 ) 4 ] 3− the corresponding 1:2 dimer [Ce(PW 11 O 39 ) 2 ] 10− and the Zr-substituted Lindqvist-type anion [W 5 O 18 Zr(OH 2 ) (OH)] 3− , which differ in the overall charge, the size, the shape and the type of substituted metal. ( Solé-Daura et al, 2016 ).…”
Section: Interaction Between Polyoxometalates and Biomoleculesmentioning
confidence: 99%
“…( Narasimhan et al, 2011 ; Prudent et al, 2010 ; Prudent et al, 2008 ; Hu et al, 2007 ; Tiago et al, 2007 ; Pezza et al, 2002 ; Judd et al, 2001 ; Sarafianos et al, 1996 ). Owing to the intrinsic limitations of docking methods, atomistic molecular dynamics (MD) simulations have been more recently performed to reveal the driving forces that are responsible for the specific interactions ( Figure 1A )[ ( Solé-Daura et al, 2016 ; Paul et al, 2018 ; Solé-Daura et al, 2020a ; Sciortino et al, 2021 ; Chaudhary et al, 2021 )] Pioneer MD simulations analysed the interaction between model protein hen egg-white lysoszyme (HEWL) and three different POMs, the Ce-substituted Keggin-type anion [PW 11 O 39 Ce(OH 2 ) 4 ] 3− the corresponding 1:2 dimer [Ce(PW 11 O 39 ) 2 ] 10− and the Zr-substituted Lindqvist-type anion [W 5 O 18 Zr(OH 2 ) (OH)] 3− , which differ in the overall charge, the size, the shape and the type of substituted metal. ( Solé-Daura et al, 2016 ).…”
Section: Interaction Between Polyoxometalates and Biomoleculesmentioning
confidence: 99%
“…It is important to note that DOPA and cyclen-based ligands did not interact with the region on the S100A9 surface, including Lys 50 to Lys 54, which has been shown previously to be critical for S100A9 amyloid self-assembly and by blocking this specific amino acid sequence by polyoxoniobates, we were able effectively hinder S100A9 amyloid growth [53]. However, as the S100A9 amyloid surface is important for its quaternary complex formation and amyloid co-aggregation with Aβ peptide [18] and potentially with other proteins and disease-related and functional amyloids, the amyloid morphology-modifying effect of DOPA and cyclen-based compounds co-aggregated together with S100A9 into fibrils should be taken into account in future studies of protein hetero-aggregation.…”
Section: Discussionmentioning
confidence: 74%
“…The amyloid formation of S100A9 in the absence and presence of DOPA and cyclenbased compounds was monitored by ThT fluorescence and is presented in Figure 2. The amyloid formation correlates with the increase of the ThT fluorescence, and the initial parts of the fibrillation kinetic curves were fitted by using an isodesmic polymerization model [50,51] to derive the kinetic rates; this model has previously been used in kinetic analysis of S100A9 amyloid self-assembly [52,53]. The rates of fibrillation in the presence of the compounds do not deviate significantly from the rate of self-assembly of S100A9 alone (Table 1).…”
Section: Kinetic Analysis Of S100a9 Amyloid Formation In the Absence And Presence Of Dopa And Cyclen-based Compounds Monitored By Tht Flumentioning
confidence: 99%
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“…POMs are effective in the degradation and prevention of toxic effects of Aβ displaying both protease-like activity for Aβ disaggregation and SOD-like activity to scavenge ROS produced by Aβ reactivity [344]. POM nanostructures associated with Niobium act as potent inhibitors of S100A9 assembly [345], which is a protein present in neuron cells and involved in the aggregation of Aβ and α-syn [366,367] and related to cognitive deficits in an AD animal model [368]. A bimetallic nanosystem composed of a nanozyme core of platinum-copper (PtCu) and coated with polyvinyl pyrrolidone significantly inhibits α-syn aggregation and spread in the brain of mice after intrastriatal injection of α-syn fibrils.…”
Section: Nanozymes: Nanomaterials With Enzymatic Activitymentioning
confidence: 99%