Easy to use, easy to expand, high-performance Amber simulation package
v0.0.5 Added support for multiple ligands.
This software only supports Linux because some Linux system functions are called.Mac OS X and Windows are not supported.
Ambertools, python3, and python3-dev are required. Amber acceleration package is optional, but we strongly recommend installing high-performance pmemd module. Amber
You can refer to the Amber installation tutorial to install Amber.
Then, you can choose several installation methods.
- Anaconda(recommend)
conda install ambermdrun -c zjack- PYPI PYPI installation requires a c++compiler that supports the c++17 standard. GCC-8 does not fully support the file system in the c++17 standard, so GCC-9 or higher is required. Therefore, different systems have different processing methods, and we recommend using conda for installation.
Ubuntu >= 20
apt install g++ libpython3-dev
pip install AmberMDruncentos7 We recommend Red Hat Developer Toolset for higher version of gcc.
yum update
yum install epel-release
yum install centos-release-scl-rh
yum install devtoolset-9
source /opt/rh/devtoolset-9/enable # enable gcc-9
yum install python3-devel
pip install AmberMDrun- You can also choose to build from source code.
git clone https://github.com/9527567/AmberMD --recursive
python setup.py install --userIf you want to use AmberMDrun to calculate MMPB (GB) SA, then additional programs are necessary.
usage: amberMDrun [-h] --parm7 PARM7 --rst7 RST7 [--temp TEMP] [--ns NS] [--addmask ADDMASK] [--gamd GAMD] [--MIN MIN] [--MD MD]
Tools for automated operation of AMBER MD
options:
-h, --help show this help message and exit
--parm7 PARM7, -p PARM7
amber top file
--rst7 RST7, -c RST7 amber rst file
--temp TEMP, -t TEMP Temperature
--ns NS, -n NS time for MD(ns)
--addmask ADDMASK add restarint mask
--gamd GAMD if run gamd
--MIN MIN Engine for MIN
--MD MD Engine for MDusage: mmpbsa [-h] --protein PROTEIN [--mol2 MOL2 [MOL2 ...]] [--temp TEMP] [--ns NS] [-g] [-uc] [-c CHARGE [CHARGE ...]] [--multiplicity MULTIPLICITY [MULTIPLICITY ...]]
[--MIN MIN] [--MD MD]
Tools for automating the operation of MMPBSA
options:
-h, --help show this help message and exit
--protein PROTEIN, -p PROTEIN
pdb file for protein
--mol2 MOL2 [MOL2 ...], -m MOL2 [MOL2 ...]
mol2 file for mol
--temp TEMP, -t TEMP Temperature
--ns NS, -n NS time for MD(ns)
-g, --guess_charge guess charge
-uc, --user_charge user charge
-c CHARGE [CHARGE ...], --charge CHARGE [CHARGE ...]
charge of mol
--multiplicity MULTIPLICITY [MULTIPLICITY ...]
multiplicity of mol
--MIN MIN Engine for MIN
--MD MD Engine for MDTypically, the complex structure after molecular docking is used to perform MMPBSA calculations.Therefore, we have provided a short code to handle the pdb format of the complex. Therefore, when your complex structure is docked and the ligand is in the desired initial position, you can directly provide the pdb format file of the complex.The following is an example.It should be noted that we will not actively assist you in handling the hydrogen atom of the ligand. We need you to ensure that the hydrogen of the ligand is correct.
mmpbsa -p complex.pdbJust follow the files of multiple ligands after -m, and add an option -g to guess the static charge of small molecules, or manually specify the static charge, for example:
mmpbsa -p pro.pdb -m lig1.mol2 lig2.mol2 -g -n 100Will be described in the near future
bibtex:
@Article{biom13040635,
AUTHOR = {Zhang, Zhi-Wei and Lu, Wen-Cai},
TITLE = {AmberMDrun: A Scripting Tool for Running Amber MD in an Easy Way},
JOURNAL = {Biomolecules},
VOLUME = {13},
YEAR = {2023},
NUMBER = {4},
ARTICLE-NUMBER = {635},
URL = {https://www.mdpi.com/2218-273X/13/4/635},
ISSN = {2218-273X},
DOI = {10.3390/biom13040635}
}@article{CUI2023134812,
title = {A TastePeptides-Meta system including an umami/bitter classification model Umami_YYDS, a TastePeptidesDB database and an open-source package Auto_Taste_ML},
journal = {Food Chemistry},
volume = {405},
pages = {134812},
year = {2023},
issn = {0308-8146},
doi = {https://doi.org/10.1016/j.foodchem.2022.134812},
url = {https://www.sciencedirect.com/science/article/pii/S0308814622027741},
author = {Zhiyong Cui and Zhiwei Zhang and Tianxing Zhou and Xueke Zhou and Yin Zhang and Hengli Meng and Wenli Wang and Yuan Liu},
keywords = {Peptides, Umami prediction, TastePeptidesDB, Machine learning},
abstract = {Taste peptides with umami/bitterness play a role in food attributes. However, the taste mechanisms of peptides are not fully understood, and the identification of these peptides is time-consuming. Here, we created a taste peptide database by collecting the reported taste peptide information. Eight key molecular descriptors from di/tri-peptides were selected and obtained by modeling screening. A gradient boosting decision tree model named Umami_YYDS (89.6\% accuracy) was established by data enhancement, comparison algorithm and model optimization. Our model showed a great prediction performance compared to other models, and its outstanding ability was verified by sensory experiments. To provide a convenient approach, we deployed a prediction website based on Umami_YYDS and uploaded the Auto_Taste_ML machine learning package. In summary, we established the system TastePeptides-Meta, containing a taste peptide database TastePeptidesDB an umami/bitter taste prediction model Umami_YYDS and an open-source machine learning package Auto_Taste_ML, which were helpful for rapid screening of umami peptides.}
}