Your search keyword '"Nikolaos Louros"' showing total 4 results

1. Heterotypic amyloid interactions: Clues to polymorphic bias and selective cellular vulnerability?

Author

Nikolaos Louros, Joost Schymkowitz, and Frederic Rousseau

Subjects

Amyloid, Structural Biology, Humans, Amyloidogenic Proteins, Molecular Biology

Abstract

The number of atomic-resolution structures of disease-associated amyloids has greatly increased in recent years. These structures have confirmed not only the polymorphic nature of amyloids but also the association of specific polymorphs to particular proteinopathies. These observations are strengthening the view that amyloid polymorphism is a marker for specific pathological subtypes (e.g. in tauopathies or synucleinopathies). The nature of this association and how it relates to the selective cellular vulnerability of amyloid nucleation, propagation and toxicity are still unclear. Here, we provide an overview of the mechanistic insights provided by recent patient-derived amyloid structures. We discuss the framework organisation of amyloid polymorphism and how heterotypic amyloid interactions with the physiological environment could modify the solubility and assembly of amyloidogenic proteins. We conclude by hypothesising how such interactions could contribute to selective cellular vulnerability.

Published

2022

2. StAmP-DB: a platform for structures of polymorphic amyloid fibril cores

Author

Nikolaos Louros, Rob van der Kant, Joost Schymkowitz, and Frederic Rousseau

Subjects

Statistics and Probability, Amyloid, Computational Mathematics, Computational Theory and Mathematics, Humans, Neurodegenerative Diseases, Molecular Biology, Biochemistry, Computer Science Applications

Abstract

Summary Amyloid polymorphism is emerging as a key property that is differentially linked to various conformational diseases, including major neurodegenerative disorders, but also as a feature that potentially relates to complex structural mechanisms mediating transmissibility barriers and selective vulnerability of amyloids. In response to the rapidly expanding number of amyloid fibril structures formed by full-length proteins, we here have developed StAmP-DB, a public database that supports the curation and cross-comparison of experimentally determined three-dimensional amyloid polymorph structures. Availability and implementation StAmP-DB is freely accessible for queries and downloads at https://stamp.switchlab.org.

Published

2022

3. Investigating the Sequence Determinants of the Curling of Amyloid Fibrils Using Ovalbumin as a Case Study

Author

Joëlle A.J. Housmans, Bert Houben, Margarita Monge-Morera, Diego Asvestas, Hung Huy Nguyen, Grigoria Tsaka, Nikolaos Louros, Sebastien Carpentier, Jan A. Delcour, Frederic Rousseau, and Joost Schymkowitz

Subjects

Biomaterials, Amyloid, Polymers and Plastics, Ovalbumin, Materials Chemistry, Humans, Bioengineering, Amyloidosis, Peptides, Hydrophobic and Hydrophilic Interactions

Abstract

Highly ordered, straight amyloid fibrils readily lend themselves to structure determination techniques and have therefore been extensively characterized. However, the less ordered curly fibrils remain relatively understudied, and the structural organization underlying their specific characteristics remains poorly understood. We found that the exemplary curly fibril-forming protein ovalbumin contains multiple aggregation prone regions (APRs) that form straight fibrils when isolated as peptides or when excised from the full-length protein through hydrolysis. In the context of the intact full-length protein, however, the regions separating the APRs facilitate curly fibril formation. In fact, a meta-analysis of previously reported curly fibril-forming proteins shows that their inter-APRs are significantly longer and more hydrophobic when compared to straight fibril-forming proteins, suggesting that they may cause strain in the amyloid state. Hence, inter-APRs driving curly fibril formation may not only apply to our model protein but rather constitute a more general mechanism.

Published

2022

4. Thermodynamic analysis of amyloid fibril structures reveals a common framework for stability in amyloid polymorphs

Author

Rob van der Kant, Nikolaos Louros, Joost Schymkowitz, and Frederic Rousseau

Subjects

Amyloid, Amyloid beta-Peptides, amyloid polymorphism, Protein Conformation, aggregation-prone regions, aggregation, amyloid-fibril structures, FoldX, Structural Biology, Thermodynamics, cryo-EM, solid-state NMR, thermodynamic stability, fibril stability, Molecular Biology, amyloid strains

Abstract

The increasing number of amyloid structures offers an opportunity to investigate the general principles determining amyloid stability and polymorphism. We find that amyloid stability is dominated by ∼30% of residues localized in segments that favor the cross-β conformation. These correspond to known aggregation-nucleating regions and constitute a stabilizing cross-β structural framework that is shared among polymorphs. Alternative packing of these segments with structurally frustrated regions within the protofilament results in conformationally different, but energetically similar, polymorphs. Differential analysis of distributions of interatomic distances in amyloid and globular structures revealed that unconventional residue contacts, such as identical charges in close proximity, are located in energetically frustrated segments of amyloids. These observations suggest that polymorphism results from a framework mechanism consisting of conserved stabilizing regions of high cross-β propensity. These are interspersed by structurally suboptimal regions that are potential sites of conformational plasticity and interaction with stabilizing cofactors such as (poly)ions. ispartof: STRUCTURE vol:30 issue:8 pages:1178-+ ispartof: location:United States status: published

Published

2022