Abstract

Retinoic acid (t-RA) is an important regulator of cell growth and differentiation in both the adult and developing embryo. The effects of t-RA are mediated through the retinoic acid receptor (RAR) that binds all-trans-RA (t-RA) but the underlying mechanism is still not known [106]. Using Steered Molecular Dynamics (SMD) [100] we studied the transition between the bound and unbound form of the retinoic acid receptor, known from experiment to be accompanied by a conformational change that enables the hormone-receptor complex to bind to specific sequences of DNA and other transcriptional coactivators or repressors*. The crystal structure of the ligand binding domain (the receptor domain responsible for recognizing and binding the hormone) of the human retinoic acid receptor hRAR-( bound to all-trans retinoic acid [107] was used for simulating different unbinding pathways. Examination of the crystal structure of the hRAR-( bound to t-RA suggests three entry/exit points for the hormone that were explored using SMD. In all simulations, the protein-ligand system was surrounded by a water bath, the total number of atoms being (15,000. One atom of the hormone was harmonically restrained (K=10 kcal mol-1/E2) to a point moving with a constant velocity v=0.032 E/ps in a chosen direction. The molecular dynamics program NAMD [19], was used to compute three different trajectories of 750 ps each. The results of our simulations show that, if strong enough forces are applied, it is possible to extract the hormone out of the binding pocket, with little or almost no effect on the protein structure. Along one of the pathways the hormone has to overcome the strong electrostatic forces between its carboxylate group and the charged Lys and Arg residues lining the opening. In the other two cases, before the hormone is completely out of the protein, the carboxylate group of the hormone interacts strongly with some of the neighboring residues. It may indicate that those residu es are the ones to attract and guide the hormone toward the binding pocket. Further studies of the unbinding mechanism will be conducted using the Targeted Molecular Dynamics (TMD) method [105]. TMD imposes time-dependent holonomic constraints that drive the system from the bound to the unbound state. The resulting pathways may be used for choosing the direction of the applied force in SMD simulations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Biotechnology Resource Grants (P41)
Project #
5P41RR005969-11
Application #
6348230
Study Section
Project Start
2000-08-01
Project End
2001-07-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
11
Fiscal Year
2000
Total Cost
$34,752
Indirect Cost

  Institution

Name
University of Illinois Urbana-Champaign
Department
Type
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820

  Publications

Shim, Jiwook; Banerjee, Shouvik; Qiu, Hu et al. (2017) Detection of methylation on dsDNA using nanopores in a MoS2 membrane. Nanoscale 9:14836-14845
Wolfe, Aaron J; Si, Wei; Zhang, Zhengqi et al. (2017) Quantification of Membrane Protein-Detergent Complex Interactions. J Phys Chem B 121:10228-10241
Decker, Karl; Page, Martin; Aksimentiev, Aleksei (2017) Nanoscale Ion Pump Derived from a Biological Water Channel. J Phys Chem B 121:7899-7906
Radak, Brian K; Chipot, Christophe; Suh, Donghyuk et al. (2017) Constant-pH Molecular Dynamics Simulations for Large Biomolecular Systems. J Chem Theory Comput 13:5933-5944
Sun, Chang; Taguchi, Alexander T; Vermaas, Josh V et al. (2016) Q-Band Electron-Nuclear Double Resonance Reveals Out-of-Plane Hydrogen Bonds Stabilize an Anionic Ubisemiquinone in Cytochrome bo3 from Escherichia coli. Biochemistry 55:5714-5725
Belkin, Maxim; Aksimentiev, Aleksei (2016) Molecular Dynamics Simulation of DNA Capture and Transport in Heated Nanopores. ACS Appl Mater Interfaces 8:12599-608
Poudel, Kumud R; Dong, Yongming; Yu, Hang et al. (2016) A time course of orchestrated endophilin action in sensing, bending, and stabilizing curved membranes. Mol Biol Cell 27:2119-32
Vermaas, Josh V; Taguchi, Alexander T; Dikanov, Sergei A et al. (2015) Redox potential tuning through differential quinone binding in the photosynthetic reaction center of Rhodobacter sphaeroides. Biochemistry 54:2104-16
Belkin, Maxim; Chao, Shu-Han; Jonsson, Magnus P et al. (2015) Plasmonic Nanopores for Trapping, Controlling Displacement, and Sequencing of DNA. ACS Nano 9:10598-611
Shen, Rong; Han, Wei; Fiorin, Giacomo et al. (2015) Structural Refinement of Proteins by Restrained Molecular Dynamics Simulations with Non-interacting Molecular Fragments. PLoS Comput Biol 11:e1004368

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