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The human peripheral subunit‐binding domain folds rapidly while overcoming repulsive Coulomb forces
Author(s) -
Arbely Eyal,
Neuweiler Hannes,
Sharpe Timothy D.,
Johnson Christopher M.,
Fersht Alan R.
Publication year - 2010
Publication title -
protein science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.353
H-Index - 175
eISSN - 1469-896X
pISSN - 0961-8368
DOI - 10.1002/pro.453
Subject(s) - chemistry , ionic strength , protein subunit , biophysics , kinetics , protein folding , circular dichroism , folding (dsp implementation) , static electricity , chemical physics , crystallography , biochemistry , biology , physics , quantum mechanics , aqueous solution , electrical engineering , gene , engineering
Peripheral subunit binding domains (PSBDs) are integral parts of large multienzyme complexes involved in carbohydrate metabolism. PSBDs facilitate shuttling of prosthetic groups between different catalytic subunits. Their protein surface is characterized by a high density of positive charges required for binding to subunits within the complex. Here, we investigated folding thermodynamics and kinetics of the human PSBD (HSBD) using circular dichroism and tryptophan fluorescence experiments. HSBD was only marginally stable under physiological solvent conditions but folded within microseconds via a barrier‐limited apparent two‐state transition, analogous to its bacterial homologues. The high positive surface‐charge density of HSBD leads to repulsive Coulomb forces that modulate protein stability and folding kinetics, and appear to even induce native‐state movement. The electrostatic strain was alleviated at high solution‐ionic‐strength by Debye‐Hückel screening. Differences in ionic‐strength dependent characteristics among PSBD homologues could be explained by differences in their surface charge distributions. The findings highlight the trade‐off between protein function and stability during protein evolution.