Difference between revisions of "2017 AMBER tutorial with 4qmz"
Stonybrook (talk | contribs) (→IV. Simulation Production) |
Stonybrook (talk | contribs) (→III. Structural Equilibration) |
||
Line 63: | Line 63: | ||
imin = 1: flag to do minimization only | imin = 1: flag to do minimization only | ||
+ | |||
ntx = 1: read coordinates only from rst file | ntx = 1: read coordinates only from rst file | ||
+ | |||
ntc = 1: flag for shake to perform bond length constraints. ntc =1 is the default, meaning SHAKE is not performed. In other words, minimization is performed on every bond. | ntc = 1: flag for shake to perform bond length constraints. ntc =1 is the default, meaning SHAKE is not performed. In other words, minimization is performed on every bond. | ||
+ | |||
ntb = 1: flag for constant volume | ntb = 1: flag for constant volume | ||
+ | |||
ntp = 0: NO constant pressure | ntp = 0: NO constant pressure | ||
+ | |||
ntwx = 1000: saving snapshot to a trajectory file every 1000 steps. | ntwx = 1000: saving snapshot to a trajectory file every 1000 steps. | ||
+ | |||
ntwe = 0: human readable energy file is appended every 0 steps. | ntwe = 0: human readable energy file is appended every 0 steps. | ||
+ | |||
ntpr = 1000: newest calculated energy is stored in .info file every 1000 steps. | ntpr = 1000: newest calculated energy is stored in .info file every 1000 steps. | ||
+ | |||
cut: cutoff for energy evaluation (Angstroms) | cut: cutoff for energy evaluation (Angstroms) | ||
+ | |||
ntr = 1: flag for restraining specified atoms | ntr = 1: flag for restraining specified atoms | ||
+ | |||
restraintmask = ':1-224 & !@H='; String that specifies restrained atoms (all atoms except hydrogens are restrained) | restraintmask = ':1-224 & !@H='; String that specifies restrained atoms (all atoms except hydrogens are restrained) | ||
+ | |||
restraint_wt = 5.0; restraint strength (kcal/molA^2) | restraint_wt = 5.0; restraint strength (kcal/molA^2) | ||
Revision as of 16:09, 3 April 2017
In this tutorial, we will learn how to run a molecular dynamics simulation of a protein-ligand complex. We will then post-process that simulation by calculating structural fluctuations (with RMSD) and free energies of binding (MM-GBSA).
Contents
Introduction
Amber -Assisted Model Building with Energy Refinement - is a multi-program suite for macromolecular simulations.Amber is distributed in two parts: AmberTools15 and Amber14.Amber14 is the most recent version of the software and it includes new force fields such as ff14SB. In addition, in this release, more features from sander have been added to pmemd for both CPU and GPU platforms, including performance improvements, and support for extra points, multi-dimension replica exchange, a Monte Carlo barostat, ScaledMD, Jarzynski sampling, explicit solvent constant pH, GBSA, and hydrogen mass repartitioning. Support is also included for the latest Kepler, Titan and GTX7xx GPUs expanded options for Poisson-Boltzmann solvation calculations, accelerated molecular dynamics, additional features in sander pmemd code, and expanded methods for free energy calculations. Our lab is set up with Ambe r14 and the latest update of AmberTools15 which contains the programs such as antechamber and tleap to set up your simulation. The Amber 14 Manualis available to get started with using Amber14. You can search the document for keywords such as "tleap" if you use Adobe Acrobat to view the file. Additionally, AmberTools Reference Manualis another reference for the programs available under Amber tools.
Here below are some of the programs available in both Amber and AmberTools:
1.LEaP: LEaP is an X-windows-based program that provides for basic model building and Amber coordinate parameter/topology input file creation. It includes a molecular editor which allows for building residues and manipulating molecules.
2.ANTECHAMBER: This program suite automates the process of developing force field descriptors for most organic molecules. It starts with structures (usually in PDB format), and generates files that can be read into LEaP for use in molecular modeling. The force field description that is generated is designed to be compatible with the usual Amber force fields for proteins and nucleic acids.
3.SANDER: Sander is short for Simulated annealing with NMR-derived energy restraints. This allows for NMR refinement based on NOE-derived distance restraints, torsion angle restraints, and penalty functions based on chemical shifts and NOESY volumes. Sander is also the "main" program used for molecular dynamics simulations, and is also used for replica-exchange, thermodynamic integration, and potential of mean force (PMF) calculations. Sander also includes QM/MM capability.
4.PMEMD: This is an extensively-modified version (originally by Bob Duke) of the sander program, optimized for periodic, PME simulations, and for GB simulations. It is faster than sander and scales better on parallel machines.
5.PTRAJandCPPTRAJ: These are used to analyze MD trajectories, computing a variety of things, like RMS deviation from a reference structure, hydrogen bonding analysis, time-correlation functions, diffusional behavior, and so on.
6.MM_PBSA andMM_PBSA.py: These are scripts that automate post-processing of MD trajectories, to analyze energetics using continuum solvent ideas. It can be used to break energies energies into "pieces" arising from different residues, and to estimate free energy differences between conformational basins.
7.NAB: Originally named as "nucleic acid builder", NAB is a specialized language for writing programs that manipulate molecules and carry out molecular mechanics or distance-geometry based modeling. NAB provides and interface to Poisson-Boltzmann and RISM integral-equation solvent models. The "amberlite" package uses NAB to study protein-ligand interaction energetics. There is also a mailing list available as an additional resource. What you can do with it is: you document your questions and sent to this mail address, some specialists of Amber will be assigned to reply your email and help you.
4qmz:
Organizing Directories It makes things easier to organize your files in a clean and logical way. The following directory structure and naming scheme is a convenient way to organize your files. We could make these directories first before doing anything further
~username/AMS536-Spring2016/Amber_Tutorial/000.parameters/ 001.tleap_build/ 002.equilibration/ 003.production/ 004.analysis/
II. Structural Preparation
Zach
III. Structural Equilibration
Steve
We first start by performing a series of minimization and short MD simulation steps for the receptor and ligand. The purpose of these steps is to remove steric clashes (minimization) and allow the receptor:ligand to equilibrate into a low energy state (MD simulation). After minimization, we can perform MD simulations in which we could record the trajectories to predict the folded state of protein.
1) In the first minimization step, we use a large restraint_wt on all heavy atoms (5.0 kcal/molA^2). Thus, only hydrogens are allowed to relax and only steric clashes involving hydrogens are removed. Create the input file 01.min.in:
Minmize all the hydrogens &cntrl imin=1, ! Minimize the initial structure maxcyc=5000, ! Maximum number of cycles for minimization ntb=1, ! Constant volume ntp=0, ! No pressure scaling ntf=1, ! Complete force evaluation ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=5.0, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format
imin = 1: flag to do minimization only
ntx = 1: read coordinates only from rst file
ntc = 1: flag for shake to perform bond length constraints. ntc =1 is the default, meaning SHAKE is not performed. In other words, minimization is performed on every bond.
ntb = 1: flag for constant volume
ntp = 0: NO constant pressure
ntwx = 1000: saving snapshot to a trajectory file every 1000 steps.
ntwe = 0: human readable energy file is appended every 0 steps.
ntpr = 1000: newest calculated energy is stored in .info file every 1000 steps.
cut: cutoff for energy evaluation (Angstroms)
ntr = 1: flag for restraining specified atoms
restraintmask = ':1-224 & !@H='; String that specifies restrained atoms (all atoms except hydrogens are restrained)
restraint_wt = 5.0; restraint strength (kcal/molA^2)
2) The second step is a short MD simulation to bring the receptor:ligand system into a more equilibrated state. Create an input file 02.equil.mdin by copying and editing 01.min.mdin. cp 01.min.mdin 02.equil.mdin
MD simualation &cntrl imin=0, ! Perform MD nstlim=50000 ! Number of MD steps ntb=2, ! Constant Pressure ntc=1, ! No SHAKE on bonds between hydrogens dt=0.001, ! Timestep (ps) ntp=1, ! Isotropic pressure scaling barostat=1 ! Berendsen taup=0.5 ! Pressure relaxtion time (ps) ntf=1, ! Complete force evaluation ntt=3, ! Langevin thermostat gamma_ln=2.0 ! Collision Frequency for thermostat ig=-1, ! Random seed for thermostat temp0=298.15 ! Simulation temperature (K) ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=5.0, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format iwrap=1, ! iwrap is turned on
imin = 0: flag to do MD simulation
ntc = 2: flag for SHAKE to perform bond length constraints involving hydrogen
ntb = 2: flag for constant pressure
ntp = 1: constant pressure
ntr = 1: flag for restraining specified atoms
restraintmask = ':1-224 & !@H='; String that specifies restrained atoms (all atoms except hydrogens are restrained)
restraint_wt = 5.0; restraint strength (kcal/molA^2)
3) Create more minimization input files with decreasing restraint_wt (03.min.mdin, 04.min.mdin, 05.min.mdin). Create more MD simulation input files with different restraints (06.equil.mdin, 07.equil.mdin, 08.equil.mdin, 09.equil.mdin:
03.min.mdin:
Minmize all the hydrogens &cntrl imin=1, ! Minimize the initial structure maxcyc=1000, ! Maximum number of cycles for minimization ntb=1, ! Constant volume ntp=0, ! No pressure scaling ntf=1, ! Complete force evaluation ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=2.0, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format
04.min.mdin:
Minmize all the hydrogens &cntrl imin=1, ! Minimize the initial structure maxcyc=1000, ! Maximum number of cycles for minimization ntb=1, ! Constant volume ntp=0, ! No pressure scaling ntf=1, ! Complete force evaluation ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=0.1, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format
05.min.mdin:
Minmize all the hydrogens &cntrl imin=1, ! Minimize the initial structure maxcyc=1000, ! Maximum number of cycles for minimization ntb=1, ! Constant volume ntp=0, ! No pressure scaling ntf=1, ! Complete force evaluation ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=0.05, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format
06.equil.mdin:
MD simualation &cntrl imin=0, ! Perform MD nstlim=50000 ! Number of MD steps ntb=2, ! Constant Pressure ntc=1, ! No SHAKE on bonds between hydrogens dt=0.001, ! Timestep (ps) ntp=1, ! Isotropic pressure scaling barostat=1 ! Berendsen taup=0.5 ! Pressure relaxtion time (ps) ntf=1, ! Complete force evaluation ntt=3, ! Langevin thermostat gamma_ln=2.0 ! Collision Frequency for thermostat ig=-1, ! Random seed for thermostat temp0=298.15 ! Simulation temperature (K) ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=1.0, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format iwrap=1, ! iwrap is turned on
07.equil.mdin:
MD simulation &cntrl imin=0, ! Perform MD nstlim=50000 ! Number of MD steps ntx=5, ! Positions and velocities read formatted irest=1, ! Restart calculation ntc=1, ! No SHAKE on for bonds with hydrogen dt=0.001, ! Timestep (ps) ntb=2, ! Constant Pressure ntp=1, ! Isotropic pressure scaling barostat=1 ! Berendsen taup=0.5 ! Pressure relaxtion time (ps) ntf=1, ! Complete force evaluation ntt=3, ! Langevin thermostat gamma_ln=2.0 ! Collision Frequency for thermostat ig=-1, ! Random seed for thermostat temp0=298.15 ! Simulation temperature (K) ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-288 & !@H=", ! atoms to be restrained restraint_wt=0.5, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format iwrap=1, ! iwrap is turned on
08.equil.mdin:
MD simulations &cntrl imin=0, ! Perform MD nstlim=50000 ! Number of MD steps ntx=5, ! Positions and velocities read formatted irest=1, ! Restart calculation ntc=1, ! No SHAKE on for bonds with hydrogen dt=0.001, ! Timestep (ps) ntb=2, ! Constant Pressure ntp=1, ! Isotropic pressure scaling barostat=1 ! Berendsen taup=0.5 ! Pressure relaxtion time (ps) ntf=1, ! Complete force evaluation ntt=3, ! Langevin thermostat gamma_ln=2.0 ! Collision Frequency for thermostat ig=-1, ! Random seed for thermostat temp0=298.15 ! Simulation temperature (K) ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-287@CA,C,N", ! atoms to be restrained restraint_wt=0.1, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format iwrap=1, ! iwrap is turned on
09.equil.mdin:
MD simulations &cntrl imin=0, ! Perform MD nstlim=50000 ! Number of MD steps ntx=5, ! Positions and velocities read formatted irest=1, ! Restart calculation ntc=1, ! No SHAKE on for bonds with hydrogen dt=0.001, ! Timestep (ps) ntb=2, ! Constant Pressure ntp=1, ! Isotropic pressure scaling barostat=1 ! Berendsen taup=0.5 ! Pressure relaxtion time (ps) ntf=1, ! Complete force evaluation ntt=3, ! Langevin thermostat gamma_ln=2.0 ! Collision Frequency for thermostat ig=-1, ! Random seed for thermostat temp0=298.15 ! Simulation temperature (K) ntwx= 1000, ! Write to trajectory file every ntwx steps ntpr= 1000, ! Print to mdout every ntpr steps ntwr= 1000, ! Write a restart file every ntwr steps cut= 8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-287@CA,C,N", ! atoms to be restrained restraint_wt=0.1, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format iwrap=1, ! iwrap is turned on
IV. Simulation Production
Change your directory to 003.production. Once here, create two new directories, 001.restrained and 002.unrestrained. The simulation will be run twice, once with a restraint on the backbone and once with no restraint.
Move to the 001.restrained directory and create an input file called 10.prod.mdin using the command
vi 10.prod.mdin
write the following in the file
MD simulations &cntrl imin=0, ! Perform MD nstlim=5000000, ! Number of MD steps ntx=5, ! Positions and velocities read formatted irest=1, ! Restart calculation ntc=2, ! SHAKE on for bonds with hydrogen dt=0.002, ! Timestep (ps) ntb=2, ! Constant Pressure ntp=1, ! Isotropic pressure scaling barostat=1 ! Berendsen taup=0.5 ! Pressure relaxtion time (ps) ntf=2, ! No force evaluation for bonds with hydrogen ntt=3, ! Langevin thermostat gamma_ln=2.0 ! Collision Frequency for thermostat ig=-1, ! Random seed for thermostat temp0=298.15 ! Simulation temperature (K) ntwx= 2500, ! Write to trajectory file every ntwx steps ntpr= 2500, ! Print to mdout every ntpr steps ntwr= 5000000, ! Write a restart file every ntwr steps cut=8.0, ! Nonbonded cutoff in Angstroms ntr=1, ! Turn on restraints restraintmask=":1-287@CA,C,N", ! atoms to be restrained restraint_wt=0.1, ! force constant for restraint ntxo=1, ! Write coordinate file in ASCII format ioutfm=0, ! Write trajectory file in ASCII format iwrap=1, ! iwrap is turned on
IV. Simulation Analysis
Roy