Electrostatic contributions to the kinetics and thermodynamics of protein assembly

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Electrostatic contributions to the kinetics and thermodynamics of protein assembly. / Dell'Orco, D; Xue, Wei-Feng; Thulin, Eva; Linse, Sara.

I: Biophysical Journal, Vol. 88, Nr. 3, 2005, s. 1991-2002.

Forskningsoutput: TidskriftsbidragArtikel i vetenskaplig tidskrift

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Dell'Orco, D ; Xue, Wei-Feng ; Thulin, Eva ; Linse, Sara. / Electrostatic contributions to the kinetics and thermodynamics of protein assembly. I: Biophysical Journal. 2005 ; Vol. 88, Nr. 3. s. 1991-2002.

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TY - JOUR

T1 - Electrostatic contributions to the kinetics and thermodynamics of protein assembly

AU - Dell'Orco, D

AU - Xue, Wei-Feng

AU - Thulin, Eva

AU - Linse, Sara

PY - 2005

Y1 - 2005

N2 - The role of electrostatic interactions in the assembly of a native protein structure was studied using fragment complementation. Contributions of salt, pH, or surface charges to the kinetics and equilibrium of calbindin D-9k reconstitution was measured in the presence of Ca2+ using surface plasmon resonance and isothermal titration calorimetry. Whereas surface charge substitutions primarily affect the dissociation rate constant, the association rates are correlated with subdomain net charge in a way expected for Coulomb interactions. The affinity is reduced in all mutants, with the largest effect (260-fold) observed for the double mutant K25E+K29E. At low net charge, detailed charge distribution is important, and charges remote from the partner EF-hand have less influence than close ones. The effects of salt and pH on the reconstitution are smaller than mutational effects. The interaction between the wild-type EF-hands occurs with high affinity (K-A = 1.3 x 10(10) M-1; K-D = 80 pM). The enthalpy of association is overall favorable and there appears to be a very large favorable entropic contribution from the desolvation of hydrophobic surfaces that become buried in the complex. Electrostatic interactions contribute significantly to the affinity between the subdomains, but other factors, such as hydrophobic interactions, dominate.

AB - The role of electrostatic interactions in the assembly of a native protein structure was studied using fragment complementation. Contributions of salt, pH, or surface charges to the kinetics and equilibrium of calbindin D-9k reconstitution was measured in the presence of Ca2+ using surface plasmon resonance and isothermal titration calorimetry. Whereas surface charge substitutions primarily affect the dissociation rate constant, the association rates are correlated with subdomain net charge in a way expected for Coulomb interactions. The affinity is reduced in all mutants, with the largest effect (260-fold) observed for the double mutant K25E+K29E. At low net charge, detailed charge distribution is important, and charges remote from the partner EF-hand have less influence than close ones. The effects of salt and pH on the reconstitution are smaller than mutational effects. The interaction between the wild-type EF-hands occurs with high affinity (K-A = 1.3 x 10(10) M-1; K-D = 80 pM). The enthalpy of association is overall favorable and there appears to be a very large favorable entropic contribution from the desolvation of hydrophobic surfaces that become buried in the complex. Electrostatic interactions contribute significantly to the affinity between the subdomains, but other factors, such as hydrophobic interactions, dominate.

U2 - 10.1529/biophysj.104.049189

DO - 10.1529/biophysj.104.049189

M3 - Article

VL - 88

SP - 1991

EP - 2002

JO - Biophysical Journal

JF - Biophysical Journal

SN - 1542-0086

IS - 3

ER -