Scholars@Duke publication: Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states.

Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states.

Publication , Journal Article

Yang, X; Wang, M; Fitzgerald, MC

Published in: Journal of molecular biology

October 2006

Here we investigate the role of backbone-backbone hydrogen bonding interactions in stabilizing the protein folding transition states of two model protein systems, the B1 domain of protein L (ProtL) and the P22 Arc repressor. A backbone modified analogue of ProtL containing an amide-to-ester bond substitution between residues 105 and 106 was prepared by total chemical synthesis, and the thermodynamic and kinetic parameters associated with its folding reaction were evaluated. Ultimately, these parameters were used in a Phi-value analysis to determine if the native backbone-backbone hydrogen bonding interaction perturbed in this analogue (i.e. a hydrogen bond in the first beta-turn of ProtL's beta-beta-alpha-beta-beta fold) was formed in the transition state of ProtL's folding reaction. Also determined were the kinetic parameters associated with the folding reactions of two Arc repressor analogues, each containing an amide-to-ester bond substitution in the backbone of their polypeptide chains. These parameters were used together with previously established thermodynamic parameters for the folding of these analogues in Phi-value analyses to determine if the native backbone-backbone hydrogen bonding interactions perturbed in these analogues (i.e. a hydrogen bond at the end of the intersubunit beta-sheet interface and hydrogen bonds at the beginning of the second alpha-helix in Arc repressor's beta-alpha-alpha structure) were formed in the transition state of Arc repressor's folding reaction. Our results reveal that backbone-backbone hydrogen bonding interactions are formed in the beta-turn and alpha-helical transition state structures of ProtL and Arc repressor, respectively; and they were not formed in the intersubunit beta-sheet interface of Arc repressor, a region of Arc repressor's polypeptide chain previously shown to have other non-native-like conformations in Arc's protein folding transition state.

Duke Scholars

Author Michael C. Fitzgerald Chemistry

Published In

Journal of molecular biology

DOI

10.1016/j.jmb.2006.07.058

EISSN

1089-8638

ISSN

0022-2836

Publication Date

October 2006

Volume

363

Issue

Start / End Page

506 / 519

Related Subject Headings

Viral Proteins
Thermodynamics
Repressor Proteins
Protein Folding
Protein Denaturation
Protein Conformation
Peptide Fragments
Molecular Sequence Data
Models, Molecular
Hydrogen Bonding

Citation

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Chicago

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MLA

NLM

Yang, X., Wang, M., & Fitzgerald, M. C. (2006). Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states. Journal of Molecular Biology, 363(2), 506–519. https://doi.org/10.1016/j.jmb.2006.07.058

Yang, Xiaoye, Min Wang, and Michael C. Fitzgerald. “Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states.” Journal of Molecular Biology 363, no. 2 (October 2006): 506–19. https://doi.org/10.1016/j.jmb.2006.07.058.

Yang X, Wang M, Fitzgerald MC. Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states. Journal of molecular biology. 2006 Oct;363(2):506–19.

Yang, Xiaoye, et al. “Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states.” Journal of Molecular Biology, vol. 363, no. 2, Oct. 2006, pp. 506–19. Epmc, doi:10.1016/j.jmb.2006.07.058.

Yang X, Wang M, Fitzgerald MC. Direct analysis of backbone-backbone hydrogen bond formation in protein folding transition states. Journal of molecular biology. 2006 Oct;363(2):506–519.