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Literature DB >> 18436960

Correlation between 13Calpha chemical shifts and helix content of peptide ensembles.

Daniel S Weinstock¹, Chitra Narayanan, Jean Baum, Ronald M Levy.

Abstract

Replica exchange molecular dynamics simulations are used to generate three ensembles of an S-peptide analog (AETAAAKFLREHMDS). Percent helicity of the peptide ensembles calculated using STRIDE is compared to percent helicity calculated from (13)C(alpha) chemical shift deviations (CSD) from random coil in order to test the assumption that CSD can be correlated to percent helicity. The two estimates of helicity, one based on structure and the other on CSD, are in close to quantitative agreement, except at the edges of helical stretches where disagreements of as much as 50% can be found. These disagreements can occur by CSDs both as an under- and an overestimate of peptide helicity. We show that underestimation arises due to ensemble averaging of positive CSDs from conformers with torsion angles in the helical region of Ramachandran space with negative CSDs corresponding to conformers of the peptide in the extended region. In contrast, overestimation comes about due to the fact that a large number of conformations with torsion angles in the helical region are not counted as helical by STRIDE due to a lack of correlated helical torsion angles in neighboring residues.

Mesh：

Substances：
Carbon Isotopes
Peptides

Year: 2008 PMID： 18436960 PMCID： PMC2327285 DOI： 10.1110/ps.073365408

Source DB: PubMed Journal: Protein Sci ISSN： 0961-8368 Impact factor: 6.725

17 in total

1. Sequence-dependent correction of random coil NMR chemical shifts.

Authors: S Schwarzinger; G J Kroon; T R Foss; J Chung; P E Wright; H J Dyson
Journal: J Am Chem Soc Date: 2001-04-04 Impact factor: 15.419

2. Probability-based protein secondary structure identification using combined NMR chemical-shift data.

Authors: Yunjun Wang; Oleg Jardetzky
Journal: Protein Sci Date: 2002-04 Impact factor: 6.725

3. AGBNP: an analytic implicit solvent model suitable for molecular dynamics simulations and high-resolution modeling.

Authors: Emilio Gallicchio; Ronald M Levy
Journal: J Comput Chem Date: 2004-03 Impact factor: 3.376

4. Molecular dynamics simulations of the unfolding of an alpha-helical analogue of ribonuclease A S-peptide in water.

Authors: J Tirado-Rives; W L Jorgensen
Journal: Biochemistry Date: 1991-04-23 Impact factor: 3.162

5. Studies on the conformation of ribonuclease S-peptide.

Authors: W A Klee
Journal: Biochemistry Date: 1968-08 Impact factor: 3.162

6. Sensitivity of secondary structure propensities to sequence differences between alpha- and gamma-synuclein: implications for fibrillation.

Authors: Joseph A Marsh; Vinay K Singh; Zongchao Jia; Julie D Forman-Kay
Journal: Protein Sci Date: 2006-11-06 Impact factor: 6.725

7. Rapid and accurate calculation of protein 1H, 13C and 15N chemical shifts.

Authors: Stephen Neal; Alex M Nip; Haiyan Zhang; David S Wishart
Journal: J Biomol NMR Date: 2003-07 Impact factor: 2.835

8. The design and production of semisynthetic ribonucleases with increased thermostability by incorporation of S-peptide analogues with enhanced helical stability.

Authors: C Mitchinson; R L Baldwin
Journal: Proteins Date: 1986-09

9. The 13C chemical-shift index: a simple method for the identification of protein secondary structure using 13C chemical-shift data.

Authors: D S Wishart; B D Sykes
Journal: J Biomol NMR Date: 1994-03 Impact factor: 2.835

Correlation between 13Calpha chemical shifts and helix content of peptide ensembles.

1. Sequence-dependent correction of random coil NMR chemical shifts.

2. Probability-based protein secondary structure identification using combined NMR chemical-shift data.

3. AGBNP: an analytic implicit solvent model suitable for molecular dynamics simulations and high-resolution modeling.

4. Molecular dynamics simulations of the unfolding of an alpha-helical analogue of ribonuclease A S-peptide in water.

5. Studies on the conformation of ribonuclease S-peptide.

6. Sensitivity of secondary structure propensities to sequence differences between alpha- and gamma-synuclein: implications for fibrillation.

7. Rapid and accurate calculation of protein 1H, 13C and 15N chemical shifts.

8. The design and production of semisynthetic ribonucleases with increased thermostability by incorporation of S-peptide analogues with enhanced helical stability.

9. The 13C chemical-shift index: a simple method for the identification of protein secondary structure using 13C chemical-shift data.

10. Secondary and tertiary structural effects on protein NMR chemical shifts: an ab initio approach.

1. Cooperative formation of native-like tertiary contacts in the ensemble of unfolded states of a four-helix protein.

2. The AGBNP2 Implicit Solvation Model.

Review 3. Biophysical characterization of intrinsically disordered proteins.

4. L17A/F19A Substitutions Augment the α-Helicity of β-Amyloid Peptide Discordant Segment.

5. Conformational Characterization of Native and L17A/F19A-Substituted Dutch-Type β-Amyloid Peptides.