Mechanism for the α‐helix to β‐hairpin transition

Ding, Feng; Borreguero, Jose M.; Buldyrey, Sergey V.; Stanley, H. Eugene; Dokholyan, Nikolay V.

doi:10.1002/prot.10468

Cited by 255 publications

(301 citation statements)

References 53 publications

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“…Our results show that both a repulsive db and a physically realistic range of cm attraction of ∼5.0Å between methyl or methylene groups tend to favor β over α structures, at least for the polyalanine, polyvaline, and polyleucine chains we have studied. This finding may help to assess prior studies that used effective ranges of cm attraction as large as 6.5Å [31,32]. db's arise from empty spaces created by water exclusion between hydrophobic groups [37][38][39][40]42] and are the hallmark of interactions between nonpolar groups [33,34,[36][37][38][39][40][41][42][43] that are partially exposed to water.…”

Section: Discussionmentioning

confidence: 99%

“…An early simulation of a 12mer polyalanine indicated that its ground state was an α helix in vacuum and a β hairpin in aqueous solution [30]. However, subsequent simulations of aqueous short hydrophobic-polar [31] and polyalanine [32] peptides using different potential functions predicted an α-helical ground state except for very high hydrophobic interaction strengths [32].…”

Section: Introductionmentioning

confidence: 99%

“…We also considered desolvation barrier (db) effects as they are critical in protein energetics [33][34][35][36][37][38][39][40][41][42][43]. db effects were neglected in many implicit-water potential functions [31,32] despite studies showing its importance for protein structure prediction [44]. For polyalanine, we found that sidechains subjected to hydrophobic interactions in α helices are constrained to the db region and thus are disfavored [45,46].…”

Section: Introductionmentioning

confidence: 99%

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Hydrophobic interactions in the formation of secondary structures in small peptides

2011

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Effects of the attractive and repulsive parts of hydrophobic interactions on α helices and β sheets in small peptides are investigated using a simple atomic potential. Typically, a physical spatial range of attraction tends to favor β sheets, but α helices would be favored if the attractive range were more extended. We also found that desolvation barriers favor β sheets in collapsed conformations of polyalanine, polyvaline, polyleucine, and three fragments of amyloid peptides tested in this study. Our results provide insight into the multifaceted role of hydrophobicity in secondary structure formation, including the α to β transitions in certain amyloid peptides.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Hydrophobic interactions in the formation of secondary structures in small peptides

2011

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“…The detailed implementation of the covalent bonds and constraints that maintain the correct geometry of each residue and the peptide connectivity is described by Ding et al 34 Clustering Methods. Clustering is the procedure that categorizes or groups similar entities together on the basis of quantitative distance (similarity) measures.…”

Section: Dmd Simulation and Four-bead Protein Modelmentioning

confidence: 99%

Fidelity of the Protein Structure Reconstruction from Inter-Residue Proximity Constraints

2007

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Inter-residue proximity constraints obtained in such experiments as cross-linking/mass spectrometry are important sources of information for protein structure determination. A central question in structure determination using these constraints is, What is the minimal number of inter-residue constraints needed to determine the fold of a protein? It is also unknown how the different structural aspects of constraints differentiate their ability in determining the native fold and whether there is a rational strategy for selecting constraints that feature higher fidelity in structure determination. To shed light on these questions, we study the fidelity of protein fold determination using theoretical inter-residue proximity constraints derived from protein native structures and the effect of various subsets of such constraints on fold determination. We show that approximately 70% randomly selected constraints are sufficient for determining the fold of a domain (with an average root-mean-square deviation of e3.4 Å from their native structures). We find that random constraint selection often outperforms the rational strategy that predominantly favors the constraints representing global structural features. To uncover a strategy for constraint selection for the optimal structure determination, we study the role of the topological properties of these constraints. Interestingly, we do not observe any correlation between various simple topological properties of the selected constraints, emphasizing different global and local structural features, and the performance of these constraints, suggesting that accurate protein structure determination relies on a composite of global and local structural information.

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“…We describe the use of simplified protein models in conjunction with the rapid simulations methodology, discrete molecular dynamics (DMD). Despite the use of DMD in simulating polymer fluids [6,7], single homopolymers [7,8], proteins [9][10][11][12][13][14][15][16][17][18][19][20][21][22][23][24][25], protein aggregates [13,17,23,24,26], and gases and liquids [27,28], we believe it is significantly underutilized in the molecular-modeling field.…”

Section: Introductionmentioning

confidence: 99%