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RNAglib: Tools for learning on the structure of RNA using 2.5D geometric representations
rnaglib
)RNAglib
is a Python package for studying RNA 2.5D and 3D structures. Functionality includes automated data loading,
analysis,
visualization, ML model building and benchmarking.
We host RNAs annotated with molecule, base pair, and nucleotide level attributes. These include, but are not limited to:
The package can be cloned and the source code used directly. We also deploy it as a pip package and recommend using this install in conda environments.
If one wants to use GPU support, one should install Pytorch and DGL with the appropriate options. Otherwise, you can just skip this step and the pip installs of Pytorch and DGL will be used.
Then, one just needs to run :
pip install rnaglib
Then one can start using the packages functionalities by importing them in one's python script.
Optional Dependencies
We use fr3d-python
to build 2.5D annotations from PDBs and mmCIFs. This has to be installed manually with:
pip install git+https://github.com/cgoliver/fr3d-python.git
To load graphs and train with dgl:
pip install dgl
To load graphs and train with pytorch geometric:
pip install torch_geometric
Advanced data splitting of datasets (i.e. by sequence or structure-based similarity) depends on executables cd-hit and RNAalign. You may install these yourself or use the convenience script provided in this repo as follows, though we do not guarantee it will work on any system and has only bee tested on linux:
chmod u+x install_dependencies.sh
./install_dependencids /my/path/to/executables
Run the rnaglib_download
script to fetch the database of annotated structures. By default it will download to ~/.rnaglib
.
Use the --help
flag for more options.
$ rnaglib_download
In addition to analysing RNA data, RNAglib also distributes available parsed RNA structures.
Databases of annotated structures can be downloaded directly from Zenodo, either the non-redundant subset
link
or all rna structures link.
They can also be obtained through the provided command line utility $ rnaglib_download -r all|nr
.
Version | Date | Total RNAs | Total Non-Redundant | Non-redundant version | rnaglib commit |
---|---|---|---|---|---|
1.0.0 | 15-02-23 | 5759 | 1176 | 3.269 | 5446ae2c |
0.0.0 | 20-07-21 | 3739 | 899 | 3.186 | eb25dabd |
To speed up some functions we also build an efficient index of the data. This is needed for the rnaglib.tasks
functionality.
$ rnaglib_index
rnaglib
?Datasets of RNA 3D structures ready-to-use for machine learning model benchmarking in various biologically relevant tasks.
All tasks take as input an RNA 3D structure and have as output either residue or whole RNA-level properties.
We currently support the following 6 prediction tasks and the ability to create new tasks:
See docs for more info on usage.
Each link for the tasks above takes you to a demo.py
file with example usage for each task.
Here is a snippet for a full data loading and model training of the RNA Binding Site Detection task. All tasks follow a similar pattern.
from torch.nn import BCELoss
from rnaglib.tasks import BindingSiteDetection
from rnaglib.transforms import GraphRepresentation
# Load the task data and annotations
ta = BindingSiteDetection("my_root")
# Select a data representation and framework (see docs for support of other data modalities and deep learning frameworks)
ta.dataset.add_representation(GraphRepresentation(framework="pyg"))
train_loader, val_loader, test_loader = ta.get_split_loaders()
# most tasks ship with a dummy model for debugging, gives random outputs of the right shape
model = ta.dummy_model
# Access the predefined splits
for batch in train_loader:
pred = ta.dummy_model(batch["graph"])
y = batch["graph"].y
loss = BCELoss()(y, pred)
Have a look at a full implemenation in one of the demos for a full example.
The rnaglib.tasks
subpackage defines an abstract class to quickly implement machine learning tasks.
You can create a task from the databases available through rnaglib as well as custom annotations to open up your
challenge to the rest of the community.
If you implement a task we encourage you to submit a pull request.
To implement a task you must subclass rnaglib.tasks.Task
and define the following methods:
default_splitter()
: a method that takes as input a dataset and returns train, validation, and test indices.build_dataset()
: a method that returns a rnaglib.RNADataset
object containing the RNAs needed for the task.See here for an example of a full custom task implementation.
Current release contains annotations generated by x3dna-dssr as well as some additional ones that we added for all available PDBs at the time of release.
Each RNA is stored as a networkx graph where nodes are residues and edges are backbone and base pairing edges. The networkx graph object has graph-level, node-level and edge-level attributes. Here is a reference for all the annotations currently available.
from rnaglib.utils import available_pdbids
from rnaglib.utils import graph_from_pdbid
# load a graph containing annotations from a PDBID
rna = graph_from_pdbid('4v9i')
# you can get list of pdbids currently available in RNAglib
pdbids = available_pdbids()
# print(rna.graph)
{'dbn': {'all_chains': {'num_nts': 143, 'num_chars': 144,
'bseq': 'GCCCGGAUAGCUCAGUCGGUAGAGCAGGGGAUUGAAAAUCCCCGUGUCCUUGGUUCGAUUCCGAGUCUGGGCAC&CGGAUAGCUCAGUCGGUAGAGCAGGGGAUUGAAAAUCCCCGUGUCCUUGGUUCGAUUCCGAGUCCGGGC',
'sstr': '(((((((..((((.....[..)))).(((((.......))))).....(((((..]....))))))))))))..&((((..((((.....[..)))).(((((.......))))).....(.(((..]....))).)))))...',
'form': 'AAAAAA...AA...A.......AAA.AAAA.......A.AAA......AAAAA..A....AAAAAAAAAAAA.-&.AA...AA...A.......AAA.AAAA.......A.AAA......AAAAA..A....A...AAAA.A.-'}...,
You can extract Leontis-Westhof interactions and convert 3D structures to 2.5D graphs. We wrap a fork of fr3d-python to support this functionality.
from rnaglib.prepare_data import fr3d_to_graph
G = fr3d_to_graph("../data/structures/1fmn.cif")
Warning: this method currently does not support non-standard residues. Support coming soon. Up to version 1.0.0 of the RNA database were created using x3dna-dssr which do contain non-standard residues.
We customize networkx graph drawing functionalities to give some convenient visualization of 2.5D base pairing networks. This is not a dedicated visualization tool, it is only intended for quick debugging. We point you to VARNAhttps://varna.lisn.upsaclay.fr/ or RNAscape for a full-featured visualizer.
from rnaglib.drawing import rna_draw
rna_draw(G, show=True, layout="spring")
When dealing with 3D structures as 2.5D graphs we support graph-level comparison through the graph edit distance.
from rnaglib.ged import graph_edit_distance
from rnaglib.utils import graph_from_pdbid
G = graph_from_pdbid("4nlf")
print(graph_edit_distance(G, G)) # 0.0
Go to root of the rnaglib directory from a git clone and run pytest.
pip install pytest
pytest tests/
@article{mallet2022rnaglib,
title={RNAglib: a python package for RNA 2.5 D graphs},
author={Mallet, Vincent and Oliver, Carlos and Broadbent, Jonathan and Hamilton, William L and Waldisp{\"u}hl, J{\'e}r{\^o}me},
journal={Bioinformatics},
volume={38},
number={5},
pages={1458--1459},
year={2022},
publisher={Oxford University Press}
}
rnaglib
If you use rnaglib in one of your projects, please cite and feel free to make a pull request so we can list your project here.
rnaglib@cs.mcgill.ca
FAQs
RNAglib: Tools for learning on the structure of RNA using 2.5D geometric representations
We found that rnaglib demonstrated a healthy version release cadence and project activity because the last version was released less than a year ago. It has 2 open source maintainers collaborating on the project.
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