Literature DB >> 20483312

Alzheimer's abeta(1-40) amyloid fibrils feature size-dependent mechanical properties.

Zhiping Xu1, Raffaella Paparcone, Markus J Buehler.   

Abstract

Amyloid fibrils are highly ordered protein aggregates that are associated with several pathological processes, including prion propagation and Alzheimer's disease. A key issue in amyloid science is the need to understand the mechanical properties of amyloid fibrils and fibers to quantify biomechanical interactions with surrounding tissues, and to identify mechanobiological mechanisms associated with changes of material properties as amyloid fibrils grow from nanoscale to microscale structures. Here we report a series of computational studies in which atomistic simulation, elastic network modeling, and finite element simulation are utilized to elucidate the mechanical properties of Alzheimer's Abeta(1-40) amyloid fibrils as a function of the length of the protein filament for both twofold and threefold symmetric amyloid fibrils. We calculate the elastic constants associated with torsional, bending, and tensile deformation as a function of the size of the amyloid fibril, covering fibril lengths ranging from nanometers to micrometers. The resulting Young's moduli are found to be consistent with available experimental measurements obtained from long amyloid fibrils, and predicted to be in the range of 20-31 GPa. Our results show that Abeta(1-40) amyloid fibrils feature a remarkable structural stability and mechanical rigidity for fibrils longer than approximately 100 nm. However, local instabilities that emerge at the ends of short fibrils (on the order of tens of nanometers) reduce their stability and contribute to their disassociation under extreme mechanical or chemical conditions, suggesting that longer amyloid fibrils are more stable. Moreover, we find that amyloids with lengths shorter than the periodicity of their helical pitch, typically between 90 and 130 nm, feature significant size effects of their bending stiffness due the anisotropy in the fibril's cross section. At even smaller lengths (50 nm), shear effects dominate lateral deformation of amyloid fibrils, suggesting that simple Euler-Bernoulli beam models fail to describe the mechanics of amyloid fibrils appropriately. Our studies reveal the importance of size effects in elucidating the mechanical properties of amyloid fibrils. This issue is of great importance for comparing experimental and simulation results, and gaining a general understanding of the biological mechanisms underlying the growth of ectopic amyloid materials. Copyright 2010 Biophysical Society. Published by Elsevier Inc. All rights reserved.

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Year:  2010        PMID: 20483312      PMCID: PMC2872369          DOI: 10.1016/j.bpj.2009.12.4317

Source DB:  PubMed          Journal:  Biophys J        ISSN: 0006-3495            Impact factor:   4.033


  39 in total

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Review 4.  Fabrication of novel biomaterials through molecular self-assembly.

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Review 5.  Probing the pressure-temperature stability of amyloid fibrils provides new insights into their molecular properties.

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6.  Amyloid-like fibrils in elastin-related polypeptides: structural characterization and elastic properties.

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10.  Role of intermolecular forces in defining material properties of protein nanofibrils.

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  27 in total

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Review 2.  Mechanical Properties and Failure of Biopolymers: Atomistic Reactions to Macroscale Response.

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3.  Mapping the Broad Structural and Mechanical Properties of Amyloid Fibrils.

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4.  Normal modes of prion proteins: from native to infectious particle.

Authors:  Abraham O Samson; Michael Levitt
Journal:  Biochemistry       Date:  2011-03-04       Impact factor: 3.162

5.  Structural and Mechanical Properties of Amyloid Beta Fibrils: A Combined Experimental and Theoretical Approach.

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Review 6.  Nanomechanics of functional and pathological amyloid materials.

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7.  Assessing the Stability of Biological Fibrils by Molecular-Scale Simulations.

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8.  Viscoelastic Properties of Human Autopsy Brain Tissues as Biomarkers for Alzheimer's Diseases.

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9.  Membrane Incorporation, Channel Formation, and Disruption of Calcium Homeostasis by Alzheimer's β-Amyloid Protein.

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10.  Nanomaterials: amyloids reflect their brighter side.

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