Solvent and mutation effects on the nucleation of amyloid β-protein folding

Cruz, Luis; Urbanc, Brigita; Borreguero, Jose M.; Lazo, Noel D.; Teplow, David B.; Stanley, H. Eugene

doi:10.1073/pnas.0509276102

Cited by 115 publications

(180 citation statements)

References 49 publications

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“…Additionally, as Wu and coworkers have demonstrated, the use of scattering-based techniques [73], including X-ray / neutron scattering and light scattering, combined with theory and simulation should be very useful in the study of aggregation-prone IDPs. Several groups in the amyloid field are already pursuing these types of multi-faceted approaches [5,84,[94][95][96][97][98][99][100][101][102][103][104][105][106][107]. However, we remain blind to interactions and conformational fluctuations that occur at low concentrations.…”

Section: Tests Of the Predictions Made By Raos And Allegramentioning

confidence: 99%

A polymer physics perspective on driving forces and mechanisms for protein aggregation

Pappu

Wang

Vitalis

et al. 2008

Archives of Biochemistry and Biophysics

156

172

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Protein aggregation is a commonly occurring problem in biology. Cells have evolved stress-response mechanisms to cope with problems posed by protein aggregation. Yet, these quality control mechanisms are overwhelmed by chronic aggregation-related stress and the resultant consequences of aggregation become toxic to cells. As a result, a variety of systemic and neurodegenerative diseases are associated with various aspects of protein aggregation and rational approaches to either inhibit aggregation or manipulate the pathways to aggregation might lead to an alleviation of disease phenotypes. To develop such approaches, one needs a rigorous and quantitative understanding of protein aggregation. Much work has been done in this area. However, several unanswered questions linger, and these pertain primarily to the actual mechanism of aggregation as well as to the types of intermolecular associations and intramolecular fluctuations realized at low protein concentrations. It has been suggested that the concepts underlying protein aggregation are similar to those used to describe the aggregation of synthetic polymers. Following this suggestion, the relevant concepts of polymer aggregation are introduced. The focus is on explaining the driving forces for polymer aggregation and how these driving forces vary with chain length and solution conditions. It is widely accepted that protein aggregation is a nucleation-dependent process. This view is based mainly on the presence of long times for the accumulation of aggregates and the elimination of these lag times with "seeds". In this sense, protein aggregation is viewed as being analogous to the aggregation of colloidal particles. The theories for polymer aggregation reviewed in this work suggest an alternative mechanism for the origin of long lag times in protein aggregation. The proposed mechanism derives from the recognition that polymers have unique dynamics that distinguish them from other aggregation-prone systems such as colloidal particles.

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Section: Tests Of the Predictions Made By Raos And Allegramentioning

confidence: 99%

A polymer physics perspective on driving forces and mechanisms for protein aggregation

Pappu

Wang

Vitalis

et al. 2008

Archives of Biochemistry and Biophysics

156

172

View full text Add to dashboard Cite

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“…Kirschner and coworkers12 used theoretical predictors of β-turn propensity13 to show that the region of sequence centered about residue 26 (as well as residue 8) as having high β-turn potential. Limited proteolysis studies14 identified β-turn in the SNKG (26)(27)(28)(29) region of the full length peptide. NMR and CD spectroscopy15 for the full length Aβ-protein and fragments in a trifluoroethanol and water solution to show that the VGSN (24)(25)(26)(27)) region forms stable turn structures.…”

Section: Introductionmentioning

confidence: 99%

“…Limited proteolysis studies14 identified β-turn in the SNKG (26)(27)(28)(29) region of the full length peptide. NMR and CD spectroscopy15 for the full length Aβ-protein and fragments in a trifluoroethanol and water solution to show that the VGSN (24)(25)(26)(27)) region forms stable turn structures. Several other studies16-19 also identified a helix-turn-helix structure for the Aβ-peptide in non-polar or membrane mimicking environments.…”

Section: Introductionmentioning

confidence: 99%

“…The aqueous solution phase NMR structure of the Aβ congener peptide20, 21 shows that, in addition to the LVFFA(17-21) "central hydrophobic cluster" region, a turn centered at the VGSN (24)(25)(26)(27) region of the peptide is a key structural motif. Subsequent studies of the Aβ -peptide demonstrated that the C α proton chemical shift in the VGSNKG(24-29) region does not change over a range of temperature, which suggests that the peptide structure surrounding the VGSN (24)(25)(26)(27) region is stable in the temperature range from 5°-35°.…”

Section: Introductionmentioning

confidence: 99%

“…Subsequent studies of the Aβ -peptide demonstrated that the C α proton chemical shift in the VGSNKG(24-29) region does not change over a range of temperature, which suggests that the peptide structure surrounding the VGSN (24)(25)(26)(27) region is stable in the temperature range from 5°-35°. 21,22 Simulation studies21,23,24 lent support for the stability of the proposed structure of the LVFFA(17-21) central hydrophobic cluster and VGSN (24)(25)(26)(27) turn regions on the nanosecond time scale. 21 The conservation of the VGSN (24)(25)(26)(27) turn region in the putative β-fibril25 and the "collapsed coil" structures leads to the conjecture that the VGSN (24)(25)(26)(27) may nucleate the formation of Aβ aggregates.…”

Section: Introductionmentioning

confidence: 99%

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Structures and Free-Energy Landscapes of the Wild Type and Mutants of the Aβ21–30 Peptide Are Determined by an Interplay between Intrapeptide Electrostatic and Hydrophobic Interactions

Tarus

Straub

Thirumalai

2008

Journal of Molecular Biology

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The initial events in protein aggregation involve fluctuations that populate monomer conformations which lead to oligomerization and fibril assembly. The highly populated structures, driven by a balance between hydrophobic and electrostatic interactions in the protease-resistant wild type Aβ 21-30 -peptide and mutants E22Q (Dutch), D23N (Iowa), and K28N, are analyzed using molecular dynamics simulations. Intra-peptide electrostatic interactions were connected to calculated pK a values that compare well with the experimental estimates. The pK a values of the titratable residues show that E22 and D23 side-chains form salt-bridges only infrequently with the K28 side-chain. Contacts between E22-K28 are more probable in "dried" salt-bridges whereas D23-K28 contacts are more probable in solvated salt-bridges. The strength of the intra-peptide hydrophobic interactions increase as D23N

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