Electrostatic Contributions to the Stability of Hyperthermophilic Proteins

Overview

Journal J Mol Biol

Publisher Elsevier

Specialties Microbiology
Molecular Biology

Date 1999 Jun 22

PMID 10373377

Citations 70

Authors

L Xiao

B Honig

Affiliations

Soon will be listed here.

Abstract

Electrostatic contributions to the folding free energy of several hyperthermophilic proteins and their mesophilic homologs are calculated. In all the cases studied, electrostatic interactions are more favorable in the hyperthermophilic proteins. The electrostatic free energy is found not to be correlated with the number of ionizable amino acid residues, ion pairs or ion pair networks in a protein, but rather depends on the location of these groups within the protein structure. Moreover, due to the large free energy cost associated with burying charged groups, buried ion pairs are found to be destabilizing unless they undergo favorable interactions with additional polar groups, including other ion pairs. The latter case involves the formation of stabilizing ion pair networks as is observed in a number of proteins. Ion pairs located on the protein surface also provide stabilizing interactions in a number of cases. Taken together, our results suggest that many hyperthermophilic proteins enhance electrostatic interactions through the optimum placement of charged amino acid residues within the protein structure, although different design strategies are used in different cases. Other physical mechanisms are also likely to contribute, however optimizing electrostatic interactions offers a simple means of enhancing stability without disrupting the core residues characteristic of different protein families.

Citing Articles

The role of Gln269Leu mutation on the thermostability and structure of uricase from Aspergillus flavus.

Akhlaghi M, Seyedalipour B, Pazhang M, Imani M Sci Rep. 2025; 15(1):8285.

PMID: 40064946 PMC: 11894227. DOI: 10.1038/s41598-025-89605-w.

Characterization of LL37 Binding to Collagen through Peptide Modification with a Collagen-Binding Domain.

Wei Z, Rolle M, Camesano T ACS Omega. 2023; 8(38):35370-35381.

PMID: 37779975 PMC: 10536065. DOI: 10.1021/acsomega.3c05328.

Engineering enhanced thermostability into the nitrile hydratase.

Van Wyk J, Sewell B, Danson M, Tsekoa T, Sayed M, Cowan D Curr Res Struct Biol. 2022; 4:256-270.

PMID: 36106339 PMC: 9465369. DOI: 10.1016/j.crstbi.2022.07.002.

Structural Analysis and Construction of a Thermostable Antifungal Chitinase.

Kozome D, Uechi K, Taira T, Fukada H, Kubota T, Ishikawa K Appl Environ Microbiol. 2022; 88(12):e0065222.

PMID: 35652665 PMC: 9238372. DOI: 10.1128/aem.00652-22.

Glycosyl hydrolase 11 (xynA) gene with xylanase activity from thermophilic bacteria isolated from thermal springs.

Joshi J, Priyadharshini R, Uthandi S Microb Cell Fact. 2022; 21(1):62.

PMID: 35428308 PMC: 9013152. DOI: 10.1186/s12934-022-01788-3.