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Amyloid
The Journal of Protein Folding Disorders
Volume 14, 2007 - Issue 2
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Original

Aggregation drives “misfolding” in protein amyloid fiber formation

Pages 119-131 | Published online: 06 Jul 2009
 

Abstract

Protein amyloid fibers are often found to have a β-pleated sheet structure regardless of their sequence, leading some to believe that it is the molecule's misfolding that leads to aggregation. In this article, an alternative model is introduced for the amyloid community to consider, that fiber formation is a surface-energy minimization process, starting with the generation of colloidal particles and their linear assembly, and ending with structural evolution of the aggregates into mature fibers. We propose that aggregation drives conformational change and that a conformational change is not essential to initiate the aggregation process.

Abbreviations
AFM=

atomic force microscopy

AD=

Alzheimer's disease

NMR=

nuclear magnetic resonance

MW=

molecular weight

PrPC=

cellular prion protein

PrPSc=

scrapie prion protein

CPrPSc=

concentration of PrPSc

CNucU=

nucleation unit concentration

[PrPSc]Nuc=

nucleation concentration for PrPSc

[PrPSc]Sat=

saturation concentration for PrPSc

polyQ=

polyglutamine

α-syn=

α-synuclein

TEM=

transmission electron microscopy

2° and 3°=

secondary and tertiary structure of protein

Abbreviations
AFM=

atomic force microscopy

AD=

Alzheimer's disease

NMR=

nuclear magnetic resonance

MW=

molecular weight

PrPC=

cellular prion protein

PrPSc=

scrapie prion protein

CPrPSc=

concentration of PrPSc

CNucU=

nucleation unit concentration

[PrPSc]Nuc=

nucleation concentration for PrPSc

[PrPSc]Sat=

saturation concentration for PrPSc

polyQ=

polyglutamine

α-syn=

α-synuclein

TEM=

transmission electron microscopy

2° and 3°=

secondary and tertiary structure of protein

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